Your search keyword '"Sjoerd H. van der Burg"' showing total 236 results

1. Interferon‐γ and <scp>IL</scp> ‐5 associated cell‐mediated immune responses to <scp>HPV16 E2</scp> and <scp>E6</scp> distinguish between persistent oral <scp>HPV16</scp> infections and noninfected mucosa

Author

Sjoerd H. van der Burg, Katja Kero, K Syrjänen, Marij J. P. Welters, Stina Syrjänen, Hanna-Mari Koskimaa, Jaana Rautava, and Anna Paaso

Subjects

0303 health sciences, business.industry, viruses, medicine.medical_treatment, virus diseases, Lymphocyte proliferation, female genital diseases and pregnancy complications, 3. Good health, Serology, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine.anatomical_structure, Cytokine, Antigen, Immunity, 030220 oncology & carcinogenesis, Immunology, Medicine, Oral mucosa, business, General Dentistry, 030304 developmental biology, Blood sampling

Abstract

Objectives Natural history of human papillomavirus (HPV) infection in the head and neck region is poorly understood, and their impact on collective HPV-specific immunity is not known. Materials and methods In this study, we have performed a systematic analysis of HPV16-specific cell-mediated immunity (CMI) in 21 women with known oral and genital HPV DNA status and HPV serology (Ab) based on 6-year follow-up data. These women being a subgroup from the Finnish Family HPV Study were recalled for blood sampling to be tested for their CMI-responses to HPV16 E2, E6, and E7 peptides. Results The results showed that HPV16 E2-specific lymphocyte proliferation was more prevalent in women who tested HPV16 DNA negative in oral mucosa and were either HPV16 seropositive or negative than in HPV16 DNA+/Ab+ women (p = 0.046 and p = 0.035). In addition, the HPV16 DNA-/Ab- women most often displayed E6-specific proliferation (p = 0.020). Proportional cytokine profiles indicated that oral HPV16-negative women were characterized by prominent IFN-γ and IL-5 secretion not found in women with persisting oral HPV16 (p = 0.014 and p = 0.040, respectively). Conclusions Our results indicate that the naturally arising immune response induced by oral HPV infections displays a mixed Th1/Th2/Th17 cytokine profile while women with persisting oral HPV16 might have an impaired HPV16-specific CMI, shifted partly toward a Th2 profile, similarly as seen earlier among patients with high-grade genital HPV lesions. Thus, the lack of HPV 16 E2 and E6 specific T memory cells and Th2 cytokines might also predispose women for persistent oral HPV16 infection which might be related to the risk of cancer.

Published

2021

2. CD39 Identifies the CD4+ Tumor-Specific T-cell Population in Human Cancer

Author

Sjoerd H. van der Burg, Gregor Sturm, Saskia J. A. M. Santegoets, Francesca Finotello, Kim E. Kortekaas, Zlatko Trajanoski, Ilina Ehsan, Marij J. P. Welters, Mariette I.E. van Poelgeest, and Sylvia L. van Egmond

Subjects

0301 basic medicine, Cancer Research, education.field_of_study, Chemistry, Effector, medicine.medical_treatment, T cell, Immunology, Population, hemic and immune systems, chemical and pharmacologic phenomena, Immunotherapy, In vitro, 3. Good health, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Antigen, 030220 oncology & carcinogenesis, Cancer research, medicine, education, CD8, Ex vivo

Abstract

The accumulation of tumor-specific CD4+ and CD8+ effector T cells is key to an effective antitumor response. Locally, CD4+ T cells promote the recruitment and effector function of tumor-specific CD8+ T cells and activate innate killer cells in the tumor. Here, we show that tumor-specific CD4+ T cells were predominantly present in the CD39+ subset of tumor-infiltrating lymphocytes (TIL). The CD39+ CD4+ and CD8+ TILs were detected in three different tumor types, and displayed an activated (PD-1+, HLA-DR+) effector memory phenotype. CD4+CD39+ single-cell RNA-sequenced TILs shared similar well-known activation, tissue residency, and effector cell–associated genes with CD8+CD39+CD103+ TILs. Finally, analysis of directly ex vivo cell-sorted and in vitro expanded pure populations of CD39-positive and negative CD4+ and CD8+ TILs revealed that tumor-specific antigen reactivity was almost exclusively detected among CD39+ cells. Immunotherapy of cancer is based on the activation of tumor-reactive CD4+ and CD8+ T cells. We show that the expression of CD39 can be used to identify, isolate, and expand tumor-reactive T-cell populations in cancers.

Published

2020

3. Interleukin‐6‐mediated resistance to immunotherapy is linked to impaired myeloid cell function

Author

Camilla Labrie, Elham Beyranvand Nejad, Kees L. M. C. Franken, Sjoerd H. van der Burg, Tetje C. van der Sluis, Rueshandra Roosenhoff, Suzanne van Duikeren, Thorbald van Hall, and Ramon Arens

Subjects

Cancer Research, Myeloid, medicine.medical_treatment, Tumor Immunology and Microenvironment, chemotherapy, Major histocompatibility complex, Cancer Vaccines, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Neoplasms, medicine, Animals, Humans, tumor microenvironment, Myeloid Cells, Cisplatin, Human papillomavirus 16, MHC class II, Chemotherapy, Tumor microenvironment, biology, business.industry, interleukin-6, Papillomavirus Infections, Histocompatibility Antigens Class II, Cancer, Immunotherapy, medicine.disease, Disease Models, Animal, medicine.anatomical_structure, Oncology, Drug Resistance, Neoplasm, interleukin‐6, 030220 oncology & carcinogenesis, Vaccines, Subunit, biology.protein, Cancer research, Female, immunotherapy, business, medicine.drug

Abstract

High serum levels of interleukin‐6 (IL‐6) correlate with poor prognosis and chemotherapy resistance in several cancers. The underlying mechanisms and its effects on immunotherapy are largely unknown. To address this, we developed a human papillomavirus type 16 (HPV16)‐associated tumor model expressing IL‐6 to investigate the impact of tumor‐expressed IL‐6 during cisplatin chemotherapy and HPV16 synthetic long peptide vaccination as immunotherapy. The effects of tumor‐produced IL‐6 on tumor growth, survival and the tumor microenvironment were analyzed. Our data demonstrated that tumor‐produced IL‐6 conferred resistance to cisplatin and therapeutic vaccination. This was not caused by a changed in vitro or in vivo growth rate of tumor cells, or a changed sensitivity of tumor cells to chemotherapy or T‐cell‐mediated killing. Furthermore, no overt differences in the frequencies of tumor‐infiltrating subsets of T cells or CD11b+ myeloid cells were observed. IL‐6, however, affected the systemic and local function of myeloid cells, reflected by a strong reduction of major histocompatibility complex (MHC) class II expression on all major myeloid cell subtypes. Resistance to both therapies was associated with a changed intratumoral influx of MHC class II+ myeloid cells toward myeloid cells with no or lower MHC class II expression. Importantly, while these IL‐6‐mediated effects provided resistance to the immunotherapy and chemotherapy as single therapies, their combination still successfully mediated tumor control. In conclusion, IL‐6‐mediated therapy resistance is caused by an extrinsic mechanism involving an impaired function of intratumoral myeloid cells. The fact that resistance can be overcome by combination therapies provides direction to more effective therapies for cancer., What's new? Interleukin‐6 (IL‐6) cytokine has multiple effects on hematopoiesis and immune function and typically circulates at low levels. In cancer, however, IL‐6 serum levels are significantly elevated, with suspected impacts on tumor behavior. In this study, using a mouse model of human papillomavirus‐induced cancer with IL‐6 expression, the authors show that tumor‐produced IL‐6 confers resistance to both chemotherapy and immunotherapy. Resistance was associated with impaired myeloid cell maturation, with no evidence of involvement of mechanisms intrinsic to tumor cells. Resistance was overcome by combining chemotherapy and immunotherapy, providing insight into a potentially effective therapeutic approach for cancers with IL‐6‐mediated resistance.

Published

2020

4. A pre‐existing coordinated inflammatory microenvironment is associated with complete response of vulvar high‐grade squamous intraepithelial lesions to different forms of immunotherapy

Author

Mariette I.E. van Poelgeest, Ziena Abdulrahman, Bart W. J. Hellebrekers, Sjoerd H. van der Burg, Peggy J. de Vos van Steenwijk, Edith M.G. van Esch, Noel F C C de Miranda, RS: GROW - R2 - Basic and Translational Cancer Biology, Obstetrie & Gynaecologie, and MUMC+: MA Medische Staf Obstetrie Gynaecologie (9)

Subjects

Adult, CD4-Positive T-Lymphocytes, Cancer Research, Myeloid, cell carcinoma, Squamous Intraepithelial Lesions, medicine.medical_treatment, immune microenvironment, NEOPLASIA, Cell Count, Imiquimod, CD8-Positive T-Lymphocytes, 03 medical and health sciences, 0302 clinical medicine, Immune system, Adjuvants, Immunologic, Tumor Microenvironment, medicine, Humans, Myeloid Cells, Aged, TLR7, Vulvar Neoplasms, business.industry, IMMUNOLOGICAL CONSTANT, Tumor Immunology And Microenvironment, FOXP3, Immunotherapy, Middle Aged, vaccination, medicine.disease, phase-ii trial, vulvar HSIL, Squamous intraepithelial lesion, Treatment Outcome, medicine.anatomical_structure, Oncology, Case-Control Studies, 030220 oncology & carcinogenesis, Cancer research, Female, therapeutic vaccine, Neoplasm Grading, business, CD8, medicine.drug

Abstract

Immunotherapy of vulvar high‐grade squamous intraepithelial lesion (vHSIL) is investigated as an alternative for surgery, because of high comorbidity and risk of recurrence. Limited evidence exists on the role and composition of the immune microenvironment in current immunotherapeutic approaches for vHSIL. The vHSIL of 29 patients biopsied before treatment with imiquimod were analyzed by two multiplex seven‐color immunofluorescence panels to investigate the pre‐existing T‐cell and myeloid cell composition in relation to treatment response. The samples were scanned with the Vectra multispectral imaging system. Cells were automatically phenotyped and counted with inForm advanced image analysis software. Cell counts and composition were compared to that of vHSIL patients before therapeutic vaccination (n = 29) and to healthy vulva (n = 27). Our data show that the immune microenvironment of complete responders (CR) to imiquimod resembled the coordinated infiltration with type 1 CD4+ and CD8+ T cells and CD14+ inflammatory myeloid cells also found in healthy vulva. However, more CD8+ T cells and FoxP3+ regulatory T cells were present in CR. The lesions of partial responders (PR) lacked such a coordinated response and displayed an impaired influx of CD14+ inflammatory myeloid cells. Importantly, complete responses after imiquimod or therapeutic vaccination showed the same dependency on a pre‐existing coordinated type 1 T‐cell and CD14+ myeloid cell infiltration. In conclusion, a good clinical outcome after two different forms of immunotherapy for vHSIL is associated with the presence of a primary inflammatory process resulting in the coordinated influx of several types of immune cells which is then amplified., What's new? Premalignant vulvar high‐grade squamous intraepithelial lesions (vHSIL) are predominantly induced by human papilloma virus infection. The immune microenvironment in vHSIL and its role in immunotherapeutic approaches remain largely unknown. This study is the first to show that a complete clinical response in patients is associated with a pre‐existent coordinated influx of type 1 T cells and CD14+ myeloid cells, irrespective of the type of successful immunotherapy given (topical imiquimod therapy or therapeutic vaccination). This coordinated immune microenvironment closely resembles that of healthy vulvar tissue, suggesting that an impaired primary inflammatory process acts as an immune resistance mechanism in non‐complete responders.

Published

2020

5. 35 Chemokine-driven spatial organization of immune cell microaggregates marks oropharyngeal squamous cell carcinomas containing tumor-specific T cells

Author

Marij J. P. Welters, Marieke E. Ijsselsteijn, Zlatko Trajanoski, Saskia J. A. M. Santegoets, Noel F C C de Miranda, Sylvia I. Van Egmond, Pornpimol Charoentong, Thomas Höllt, Gregor Sturm, Ziena Abdulrahman, Dana A M Mustafa, Antonios Somarakis, Francesca Finotello, and Sjoerd H. van der Burg

Subjects

Pharmacology, Cancer Research, Chemokine, biology, Immunology, Cell, Tumor specific, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Immune system, medicine.anatomical_structure, Oncology, Cancer research, biology.protein, medicine, Molecular Medicine, Immunology and Allergy, Spatial organization, RC254-282

Abstract

BackgroundOropharyngeal squamous cell carcinoma (OPSCC) is the most prevalent type of head and neck cancer. The survival of patients with OPSCC is tightly linked to the intratumoral presence of tumor-specific CD4+ and CD8+ T cells. Yet, immunotherapy is currently far from effective in OPSCC partly due to our limited understanding of its immune microenvironment.MethodsHere a multi-modal, high-dimensional approach was used to dissect the immune landscape in a unique cohort of pre-therapy OPSCC patient samples (n=20) in which intratumoral tumor-specific T cells were either detected (immune response positive, IR+) or not (IR-). This included imaging mass cytometry (Hyperion) for high-dimensional phenotyping, spatial localization and interaction analyses of the cells in the tumor mircoenvironment with our newly developed imaging processing pipeline employing machine learning, Nanostring PanCancer IO360 panel analysis of immune signaling pathways, and combined single-cell gene expression profiling and T cell receptor sequencing (scRNAseq) to characterize the transcriptional states of clonally expanded tumor-infiltrating T cells.ResultsImmune cell infiltration in IR+ tumors is stronger and highly coordinated, with a distinct spatial phenotypic signature characterized by microaggregates of tumor-resident (CD103+) CD8+ and CD4+ T cells and dendritic cells within the tumor cell beds, which retained after permutation based correction for differences in cell frequencies. Furthermore, the increased expression of CXCL12 and LTB produced by CD4+ T cells, both involved in the spatial organization of immune cell infiltration, and the clonal expansion of CD8+ T cells producing the DC-attracting chemokines CCL4 or XCL1 in IR+ OPSCC, indicate that tumor-reactive T cells act as a positive feedback loop in the formation of these aggregates. The impact of these chemokines on local immunity and clinical outcome was confirmed in an independent TCGA OPSCC cohort. In contrast, the IR- OPSCC signature comprised spatial interactions between lymphocytes and different subpopulations of immunosuppressive myeloid cells.ConclusionsOur study reveals that the chemokine-driven spatial immune signature of OPSCC has strong potential as a prognostic and predictive biomarker. While the immune signature of IR+ OPSCC suggests potential benefit from neoadjuvant immunotherapeutic approaches to limit the side effects of current radio(chemo)therapy, that of IR- OPSCC calls for strategies focused on stimulating T cells and counteracting immune suppressive mechanisms.

Published

2021

6. PROTECT: prospective phase-II-trial evaluating adaptive proton therapy for cervical cancer to reduce the impact on morbidity and the immune system

Author

Helena C. van Doorn, Carien L. Creutzberg, Judith R. Kroep, Uulke A. van der Heide, Jeremy Godart, Stephanie M. de Boer, Nanda Horeweg, Sjoerd H. van der Burg, Marij J. P. Welters, Mariette I.E. van Poelgeest, Jan Willem M. Mens, Mischa S. Hoogeman, Sander C. Kuipers, Hein Putter, Remi A. Nout, Ingrid A. Boere, Ellen M. Kerkhof, and Anouk Corbeau

Subjects

Cancer Research, medicine.medical_specialty, bone marrow, cervical cancer, medicine.medical_treatment, Brachytherapy, chemoradiotherapy, bowel, Study Protocol, Quality of life, medicine, Clinical endpoint, proton therapy, Proton therapy, RC254-282, Cervical cancer, business.industry, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, toxicity, medicine.disease, Radiation therapy, Oncology, Tolerability, dose reduction, quality of life, Radiology, business, Chemoradiotherapy

Abstract

Simple Summary Chemoradiation with photon radiotherapy is very effective as a locally advanced cervical cancer (LACC) treatment. However, the majority of women with LACC experience treatment-related toxicity involving the gastrointestinal and urogenital tracts and the immune system. Compared to that of photon therapy, proton therapy substantially reduces undesired dose to the organs around the tumor, leading to a decrease in radiotherapy-related side-effects. At present, few studies on proton therapy in patients with LACC will be conducted. The PROTECT trial aims to evaluate the differences in side effects between photon therapy and proton therapy, both combined with chemotherapy, for LACC. Fifteen patients will be enrolled per treatment group. Information will be collected on the differences in dose to the organs around the tumor, treatment-related side effects, and the impact on the immune system. This information will be used to assess the potential of proton therapy as an innovative treatment for LACC. Abstract External beam radiation therapy (EBRT) with concurrent chemotherapy followed by brachytherapy is a very effective treatment for locally advanced cervical cancer (LACC). However, treatment-related toxicity is common and reduces the patient’s quality of life (QoL) and ability to complete treatment or undergo adjuvant therapies. Intensity modulated proton therapy (IMPT) enables a significant dose reduction in organs at risk (OAR), when compared to that of standard intensity-modulated radiation therapy (IMRT) or volumetric-modulated arc therapy (VMAT). However, clinical studies evaluating whether IMPT consequently reduces side effects for LACC are lacking. The PROTECT trial is a nonrandomized prospective multicenter phase-II-trial comparing clinical outcomes after IMPT or IMRT/VMAT in LACC. Thirty women aged >18 years with a histological diagnosis of LACC will be included in either the IMPT or IMRT/VMAT group. Treatment includes EBRT (45 Gy in 25 fractions of 1.8 Gy), concurrent five weekly cisplatin (40 mg/m2), and 3D image (MRI)-guided adaptive brachytherapy. The primary endpoint is pelvic bones Dmean and mean bowel V15Gy. Secondary endpoints include dosimetric parameters, oncological outcomes, health-related QoL, immune response, safety, and tolerability. This study provides the first data on the potential of IMPT to reduce OAR dose in clinical practice and improve toxicity and QoL for patients with LACC.

Published

2021

7. Primary vulvar squamous cell carcinomas with high T cell infiltration and active immune signaling are potential candidates for neoadjuvant PD-1/PD-L1 immunotherapy

Author

Saskia J. A. M. Santegoets, Kim E. Kortekaas, Pornpimol Charoentong, Sjoerd H. van der Burg, Helena C. van Doorn, Liselotte Tas, Mariette I.E. van Poelgeest, Dana A M Mustafa, Ilina Ehsan, Gynecological Oncology, and Pathology

Subjects

Adult, Cancer Research, endocrine system, Myeloid, Lymphocyte, T cell, medicine.medical_treatment, T-Lymphocytes, Immunology, Biology, B7-H1 Antigen, Immune system, SDG 3 - Good Health and Well-being, PD-L1, medicine, gene expression profiling, Immunology and Allergy, Cytotoxic T cell, tumor microenvironment, Humans, RC254-282, Aged, Pharmacology, Aged, 80 and over, Tumor microenvironment, Vulvar Neoplasms, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Basic Tumor Immunology, Immunotherapy, Middle Aged, medicine.anatomical_structure, Oncology, Cancer research, biology.protein, Carcinoma, Squamous Cell, Molecular Medicine, Female

Abstract

BackgroundA profound insight into the immune landscape of vulvar squamous cell carcinoma (VSCC) is lacking. Here, an in-depth interrogation of T cell infiltration, local immune contexture, signaling pathways and checkpoint molecule expression was performed in early-stage and late-stage VSCC.MethodsThe type, location, and infiltration pattern of T cells were studied in 109 patients with primary VSCC FIGO stage I–III. RNA expression of genes involved in immune oncology and oncogenic signaling pathways was analyzed in 40 VSCC, matched for prognostic clinicopathological variables, analyzed for HPV and p53 status, and selected based on T cell infiltration.ResultsHigh intraepithelial infiltration with CD4 or CD8 T cells was associated with longer overall and recurrence-free survival and formed an independent prognostic factor, outperforming molecular subtype and stage of the disease. Strong T cell infiltrated VSCC displayed a coordinated immune response reflected by a positive association between T cells and different lymphocyte and myeloid cell subsets. The expression of genes involved in the migration of T cells and myeloid cells, T cell activation and costimulation, interferon (IFN)-γ signaling, cytotoxicity and apoptosis was higher than in low infiltrated tumors. An active immune signaling profile was observed in all inflamed, part of the altered-excluded and not in altered-immunosuppressed or deserted VSCC. While several checkpoint molecules were overexpressed, only PD-L1 expression displayed discriminatory ability and clinical usefulness. High PD-L1 expression was detected in all inflamed and ~60% of the altered-excluded VSCC.ConclusionAn active immune signaling profile is present in 35% of primary FIGO I–III VSCCs, suggesting potential responsiveness to neoadjuvant PD-1/PD-L1 immunotherapy.

Published

2021

8. Neoantigen-specific immunity in low mutation burden colorectal cancers of the consensus molecular subtype 4

Author

Marieke E. Ijsselsteijn, Els M. E. Verdegaal, Noel F C C de Miranda, Arantza Farina-Sarasqueta, Ruud van der Breggen, Dina Ruano, Andrew D. Weinberg, Natasja L. de Vries, Jitske van den Bulk, Sjoerd H. van der Burg, Jan Oosting, Koen C. M. J. Peeters, Marten Visser, Thomas Duhen, and Manon van der Ploeg

Subjects

Colorectal cancer, Adoptive T cell transfer (ACT), medicine.medical_treatment, lcsh:Medicine, Cancer immunotherapy, CD8-Positive T-Lymphocytes, DNA Mismatch Repair, Tumor-infiltrating lymphocytes, Epitopes, T-Lymphocyte Subsets, Transforming Growth Factor beta, Genetics (clinical), biology, integumentary system, CMS, Mismatch repair-proficient (MMR-p), Microfilament Proteins, Cell sorting, DNA-Binding Proteins, Transforming growth factor-beta, medicine.anatomical_structure, Molecular Medicine, Immunotherapy, Colorectal Neoplasms, lcsh:QH426-470, T cell, Low mutation burden, Interferon-gamma, Lymphocytes, Tumor-Infiltrating, Antigens, Neoplasm, Genetics, medicine, Humans, Molecular Biology, business.industry, Research, lcsh:R, Cancer, Transforming growth factor beta, medicine.disease, lcsh:Genetics, Mutation, Cancer research, biology.protein, business, Neoantigen, Peptides, Transcription Factors

Abstract

Background The efficacy of checkpoint blockade immunotherapies in colorectal cancer is currently restricted to a minority of patients diagnosed with mismatch repair-deficient tumors having high mutation burden. However, this observation does not exclude the existence of neoantigen-specific T cells in colorectal cancers with low mutation burden and the exploitation of their anti-cancer potential for immunotherapy. Therefore, we investigated whether autologous neoantigen-specific T cell responses could also be observed in patients diagnosed with mismatch repair-proficient colorectal cancers. Methods Whole-exome and transcriptome sequencing were performed on cancer and normal tissues from seven colorectal cancer patients diagnosed with mismatch repair-proficient tumors to detect putative neoantigens. Corresponding neo-epitopes were synthesized and tested for recognition by in vitro expanded T cells that were isolated from tumor tissues (tumor-infiltrating lymphocytes) and from peripheral mononuclear blood cells stimulated with tumor material. Results Neoantigen-specific T cell reactivity was detected to several neo-epitopes in the tumor-infiltrating lymphocytes of three patients while their respective cancers expressed 15, 21, and 30 non-synonymous variants. Cell sorting of tumor-infiltrating lymphocytes based on the co-expression of CD39 and CD103 pinpointed the presence of neoantigen-specific T cells in the CD39+CD103+ T cell subset. Strikingly, the tumors containing neoantigen-reactive TIL were classified as consensus molecular subtype 4 (CMS4), which is associated with TGF-β pathway activation and worse clinical outcome. Conclusions We have detected neoantigen-targeted reactivity by autologous T cells in mismatch repair-proficient colorectal cancers of the CMS4 subtype. These findings warrant the development of specific immunotherapeutic strategies that selectively boost the activity of neoantigen-specific T cells and target the TGF-β pathway to reinforce T cell reactivity in this patient group.

Published

2019

9. Identification of Tumor Antigens Among the HLA Peptidomes of Glioblastoma Tumors and Plasma

Author

Harpreet Singh, Christian H. Ottensmeier, Judith R. Kroep, Michael Platten, Andreas von Deimling, Juan Sahuquillo, Eilon Barnea, Cedrik M. Britten, Francisco Martínez-Ricarte, Sebastian Kreiter, Itzhak Rosner, Ghazaleh Tabatabai, Wolfgang Wick, Gleb Slobodin, Hans Skovgaard Poulsen, Sabrina Kuttruff, Sjoerd H. van der Burg, Per thor Straten, Marcos Tatagiba, Dganit Melamed Kadosh, Norbert Hilf, Colette Song, Hans-Georg Rammensee, Frank Winkler, Valérie Dutoit, Ulrik Lassen, Arie Admon, Katrin Frenzel, Pierre-Yves Dietrich, Yael Haimovich, Hideho Okada, Ugur Sahin, Berta Ponsati, Jordi Rodon, John C. Castle, Carlos López-Larrea, and Bracha Shraibman

Subjects

0301 basic medicine, Proteome, medicine.medical_treatment, MHC - major histocompatibility complex, HLA - human leukocytes antigen, Immunoaffinity, Biochemistry, Analytical Chemistry, Cancer Biomarker(s), 0302 clinical medicine, HLA Antigens, Medicine, Withdrawals/Retractions, Peptidomics, Cancer, ddc:616, 0303 health sciences, Tumor, medicine.diagnostic_test, Brain Neoplasms, CTA - cancer/testis antigens, 3. Good health, HLA, 030220 oncology & carcinogenesis, CTA (Cancer/Testis Antigens), Immunotherapy, HLA (Human Leukocytes Antigen), Biochemistry & Molecular Biology, Immunology, Brain tumor, Plasma or Serum Analysis, Human leukocyte antigen, Cancer Therapeutics, 03 medical and health sciences, Rare Diseases, Antigen, Antigens, Neoplasm, Clinical Research, Biomarkers, Tumor, Humans, Blood test, Amino Acid Sequence, Antigens, Gene, Molecular Biology, Alleles, 030304 developmental biology, MHC (Major Histocompatibility Complex), CTA, business.industry, Research, Cell Membrane, Histocompatibility Antigens Class I, Neurosciences, medicine.disease, Brain Disorders, Brain Cancer, Good Health and Well Being, 030104 developmental biology, Solubility, Cancer research, Neoplasm, MHC, Glioblastoma, Peptides, business, Biomarkers

Abstract

Glioblastoma multiforme (GBM) is the most aggressive brain tumor with poor prognosis to most patients. Immunotherapy of GBM is a potentially beneficial treatment option, whose optimal implementation may depend on familiarity with tumor specific antigens, presented as HLA peptides by the GBM cells. Furthermore, early detection of GBM, such as by a routine blood test, may improve survival, even with the current treatment modalities. This study includes large-scale analyses of the HLA peptidome (immunopeptidome) of the plasma-soluble HLA molecules (sHLA) of 142 plasma samples, and the membranal HLA of GBM tumors of 10 of these patients' tumor samples. Tumor samples were fresh-frozen immediately after surgery and the plasma samples were collected before, and at multiple visits after surgery. In total, this HLA peptidome analysis involved 52 different HLA allotypes and resulted in the identification of more than 35,000 different HLA peptides. Strong correlations were observed in the signal intensities and in the repertoires of identified peptides between the tumors and plasma-soluble HLA peptidomes of the individual patients, whereas low correlations were observed between these HLA peptidomes and the tumors' proteomes. HLA peptides derived from Cancer/Testis Antigens (CTAs) were selected based on their presence among the HLA peptidomes of the patients and absence of expression of their source genes from any healthy and essential human tissues, except from immune-privileged sites. Additionally, peptides were selected as potential biomarkers if their levels in the plasma-sHLA peptidome were significantly reduced after the removal of tumor mass. The CTAs identified among the analyzed HLA peptidomes provide new opportunities for personalized immunotherapy and for early diagnosis of GBM.

Published

2019

10. Epitope Selection for HLA-DQ2 Presentation: Implications for Celiac Disease and Viral Defense

Author

Nan Wang, William W. Kwok, Ludvig M. Sollid, Shuo-Wang Qiao, Sjoerd H. van der Burg, I-Ting Chow, Shu-Chen Hung, Elizabeth D. Mellins, David M. Koelle, Tieying Hou, Xiaodan Liu, and Wei Jiang

Subjects

CD4-Positive T-Lymphocytes, T cell, Immunology, Antigen presentation, Mutant, Antigen-Presenting Cells, Epitopes, T-Lymphocyte, Hemagglutinin (influenza), Biology, Article, Gliadin, Epitope, Cell Line, Viral Proteins, HLA-DQ Antigens, medicine, Humans, Immunology and Allergy, Antigen Presentation, MHC class II, nutritional and metabolic diseases, Molecular biology, Celiac Disease, medicine.anatomical_structure, Virus Diseases, Cell culture, biology.protein

Abstract

We have reported that the major histocompatibility molecule HLA-DQ2 (DQA1*05:01/DQB1*02:01) (DQ2) is relatively resistant to HLA-DM (DM), a peptide exchange catalyst for MHC class II. In this study, we analyzed the role of DQ2/DM interaction in the generation of DQ2-restricted gliadin epitopes, relevant to celiac disease, or DQ2-restricted viral epitopes, relevant to host defense. We used paired human APC, differing in DM expression (DMnull versus DMhigh) or differing by expression of wild-type DQ2, versus a DM-susceptible, DQ2 point mutant DQ2α+53G. The APC pairs were compared for their ability to stimulate human CD4+ T cell clones. Despite higher DQ2 levels, DMhigh APC attenuated T cell responses compared with DMnull APC after intracellular generation of four tested gliadin epitopes. DMhigh APC expressing the DQ2α+53G mutant further suppressed these gliadin-mediated responses. The gliadin epitopes were found to have moderate affinity for DQ2, and even lower affinity for the DQ2 mutant, consistent with DM suppression of their presentation. In contrast, DMhigh APC significantly promoted the presentation of DQ2-restricted epitopes derived intracellularly from inactivated HSV type 2, influenza hemagglutinin, and human papillomavirus E7 protein. When extracellular peptide epitopes were used as Ag, the DQ2 surface levels and peptide affinity were the major regulators of T cell responses. The differential effect of DM on stimulation of the two groups of T cell clones implies differences in DQ2 presentation pathways associated with nonpathogen- and pathogen-derived Ags in vivo.

Published

2019

11. Cross-presentation of a TAP-independent signal peptide induces CD8 T immunity to escaped cancers but necessitates anchor replacement

Author

Lisa Griffioen, Sjoerd H. van der Burg, Laura Blijleven, Thorbald van Hall, and Koen A. Marijt

Subjects

Signal peptide, Cancer Research, Lung Neoplasms, T cell, medicine.medical_treatment, Immunology, Epitopes, T-Lymphocyte, Adenocarcinoma of Lung, Biology, CD8-Positive T-Lymphocytes, Protein Sorting Signals, Dendritic cells, Synthetic long peptide (SLP) vaccine, 03 medical and health sciences, 0302 clinical medicine, Cross-Priming, Antigen, Antigens, Neoplasm, HLA-A2 Antigen, medicine, Tumor Cells, Cultured, Transporter associated with antigen processing (TAP), Immunology and Allergy, Cytotoxic T cell, Humans, ATP Binding Cassette Transporter, Subfamily B, Member 2, LDL-Receptor Related Protein-Associated Protein, 030304 developmental biology, 0303 health sciences, Antigen Presentation, Cross-presentation, Immune escape, Immunotherapy, Peptide Fragments, Cell biology, medicine.anatomical_structure, Oncology, Cancer cell, Original Article, Tumor Escape, CD8, 030215 immunology, T-Lymphocytes, Cytotoxic

Abstract

Cancer cells frequently display defects in their antigen-processing pathway and thereby evade CD8 T cell immunity. We described a novel category of cancer antigens, named TEIPP, that emerge on cancers with functional loss of the peptide pump TAP. TEIPPs are non-mutated neoantigens despite their ‘self’ origin by virtue of their absence on normal tissues. Here, we describe the development of a synthetic long peptide (SLP) vaccine for the most immunogenic TEIPP antigen identified thus far, derived from the TAP-independent LRPAP1 signal sequence. LRPAP121–30-specific CD8 T cells were present in blood of all tested healthy donors as well as patients with non-small cell lung adenocarcinoma. SLPs with natural flanking, however, failed to be cross-presented by monocyte-derived dendritic cells. Since the C-terminus of LRPAP121–30 is an unconventional and weakly binding serine (S), we investigated if replacement of this anchor would result in efficient cross-presentation. Exchange into a valine (V) resulted in higher HLA-A2 binding affinity and enhanced T cell stimulation. Importantly, CD8 T cells isolated using the V-variant were able to bind tetramers with the natural S-variant and respond to TAP-deficient cancer cells. A functional screen with an array of N-terminal and C-terminal extended SLPs pointed at the 24-mer V-SLP, elongated at the N-terminus, as most optimal vaccine candidate. This SLP was efficiently cross-presented and consistently induced a strong polyclonal LRPAP121–30-specific CD8 T cells from the endogenous T cell repertoire. Thus, we designed a TEIPP SLP vaccine from the LRPAP1 signal sequence ready for validation in clinical trials. Supplementary Information The online version contains supplementary material available at 10.1007/s00262-021-02984-7.

Published

2021

12. Photochemical Internalization Enhanced Vaccination Is Safe, and Gives Promising Cellular Immune Responses to an HPV Peptide-Based Vaccine in a Phase I Clinical Study in Healthy Volunteers

Author

Tone Otterhaug, Sylvia Janetzki, Marij J. P. Welters, Monika Håkerud, Anne Grete Nedberg, Victoria Tudor Edwards, Sanne Boekestijn, Nikki M. Loof, Pål Kristian Selbo, Hans Olivecrona, Sjoerd H. van der Burg, and Anders Høgset

Subjects

Adult, Male, lcsh:Immunologic diseases. Allergy, phase I study photochemical enhancement of T-cell responses, Papillomavirus E7 Proteins, T-Lymphocytes, medicine.medical_treatment, Immunology, immunologic adjuvant, multifunctional T-cells, Young Adult, Immune system, Antigen, Humans, Immunology and Allergy, Medicine, Papillomavirus Vaccines, Cells, Cultured, Lighting, Human papillomavirus 16, Immunity, Cellular, Photosensitizing Agents, peptide vaccines, business.industry, photochemical internalization, ELISPOT, Papillomavirus Infections, Vaccination, Middle Aged, Photochemical Processes, vaccine delivery, Clinical Trial, Healthy Volunteers, Immunologic adjuvant, Vaccines, Subunit, Conventional PCI, Peptide vaccine, Female, Peptides, lcsh:RC581-607, business, Adjuvant, multifunctional T-cells, phase I study photochemical enhancement of T-cell responses

Abstract

Background and AimsPhotochemical internalization (PCI) is a technology for inducing release of endocytosed antigens into the cell cytosol via a light-induced process. Preclinical experiments have shown that PCI improves MHC class I antigen presentation, resulting in strongly enhanced CD8+ T-cell responses to polypeptide antigens. In PCI vaccination a mixture of the photosensitizing compound fimaporfin, vaccine antigens, and an adjuvant is administered intradermally followed by illumination of the vaccination site. This work describes an open label, phase I study in healthy volunteers, to assess the safety, tolerability, and immune response to PCI vaccination in combination with the adjuvant poly-ICLC (Hiltonol) (ClinicalTrials.gov Identifier: NCT02947854).MethodsThe primary objective of the study was to assess the safety and local tolerance of PCI mediated vaccination, and to identify a safe fimaporfin dose for later clinical studies. A secondary objective was to analyze the immunological responses to the vaccination. Each subject received 3 doses of HPV16 E7 peptide antigens and two doses of Keyhole Limpet Hemocyanin (KLH) protein. A control group received Hiltonol and vaccine antigens only, whereas the PCI groups in addition received fimaporfin + light. Local and systemic adverse effects were assessed by standard criteria, and cellular and humoral immune responses were analyzed by ELISpot, flow cytometry, and ELISA assays.Results96 healthy volunteers were vaccinated with fimaporfin doses of 0.75–50 µg. Doses below 17.5 µg were safe and tolerable, higher doses exhibited local tolerability issues in some study subjects, mainly erythema, and pain during illumination. There were few, and only mild and expected systemic adverse events. The employment of PCI increased the number of subjects exhibiting a T-cell response to the HPV peptide vaccine about 10-fold over what was achieved with the antigen/Hiltonol combination without PCI. Moreover, the use of PCI seemed to result in a more consistent and multifunctional CD8+ T-cell response. An enhancement of the humoral immune response to KLH vaccination was also observed.ConclusionsUsing PCI in combination with Hiltonol for intradermal vaccination is safe at fimaporfin doses below 17.5 µg, and gives encouraging immune responses to peptide and protein based vaccination.

Published

2021

13. Simplified monopalmitoyl toll-like receptor 2 ligand mini-U pam for self-adjuvanting neoantigen-based synthetic cancer vaccines

Author

Els M. E. Verdegaal, Nataschja I Ho, Geoffroy P.P. Gential, Ferry Ossendorp, Marten Visser, Wim Jiskoot, Thomas C. van den Ende, Dmitri V. Filippov, Gijsbert A. van der Marel, Sjoerd H. van der Burg, Nico J. Meeuwenoord, Herman S. Overkleeft, Jeroen D. C. Codée, A. Rob P. M. Valentijn, Jeroen Heuts, and Michel J. van de Graaff

Subjects

Synthetic vaccine, solid-phase synthesis, medicine.medical_treatment, Lipoylation, Peptide, 010402 general chemistry, Ligands, Lymphocyte Activation, 01 natural sciences, Biochemistry, Epitope, Cell Line, Solid-phase synthesis, TLR2 ligand, Antigens, Neoplasm, medicine, Humans, dendritic cells, Molecular Biology, chemistry.chemical_classification, Vaccines, Synthetic, neoepitopes, Full Paper, 010405 organic chemistry, Chemistry, Immunogenicity, Organic Chemistry, Interleukin-8, Full Papers, Ligand (biochemistry), lipopeptides, Toll-Like Receptor 2, 0104 chemical sciences, Drug Design, Molecular Medicine, Adjuvant, cancer vaccines, Conjugate

Abstract

Synthetic vaccines, based on antigenic peptides that comprise MHC−I and MHC‐II T‐cell epitopes expressed by tumors, show great promise for the immunotherapy of cancer. For optimal immunogenicity, the synthetic peptides (SPs) should be adjuvanted with suitable immunostimulatory additives. Previously, we have shown that improved immunogenicity in vivo is obtained with vaccine modalities in which an SP is covalently connected to an adjuvanting moiety, typically a ligand to Toll‐like receptor 2 (TLR2). SPs were covalently attached to UPam, which is a derivative of the classic TLR2 ligand Pam3CysSK4. A disadvantage of the triply palmitoylated UPam is its high lipophilicity, which precludes universal adoption of this adjuvant for covalent modification of various antigenic peptides as it renders the synthetic vaccine insoluble in several cases. Here, we report a novel conjugatable TLR2 ligand, mini‐UPam, which contains only one palmitoyl chain, rather than three, and therefore has less impact on the solubility and other physicochemical properties of a synthetic peptide. In this study, we used SPs that contain the clinically relevant neoepitopes identified in a melanoma patient who completely recovered after T‐cell therapy. Homogeneous mini‐UPam‐SP conjugates have been prepared in good yields by stepwise solid‐phase synthesis that employed a mini‐UPam building block pre‐prepared in solution and the standard set of Fmoc‐amino acids. The immunogenicity of the novel mini‐UPam‐SP conjugates was demonstrated by using the cancer patient's T‐cells., Less lipophilic ligands: A novel TLR2 ligand has been designed and synthesized to be subsequently conjugated with synthetic peptides containing clinically relevant neoepitopes. By treating HEK‐TLR2 cells, human moDCs and antigen specific human T‐cells with these new constructs, the immunogenic potential of the new TLR2 ligand and the conjugation of TLR ligands with neoepitopes was assessed.

Published

2020

14. Blood-based kinase activity profiling

Author

Joachim G.J.V. Aerts, Els M. E. Verdegaal, Reno Debets, Ellen Kapiteijn, Ron H.J. Mathijssen, Mandy van Brakel, Reinhard Dummer, Rik de Wijn, John P. Groten, Harmen J.G. van de Werken, Mitchell P. Levesque, Dianne M.A. van den Heuvel, Edwin A. Basak, Cor H. J. Lamers, Marij J. P. Welters, Sjoerd H. van der Burg, Daan P. Hurkmans, Rob Ruijtenbeek, Lies Hovestad, Herbert M Pinedo, Sabrina A. Hogan, Pulmonary Medicine, Medical Oncology, and Urology

Subjects

0301 basic medicine, Adult, Male, Cancer Research, medicine.medical_treatment, Immunology, lung neoplasms, Peripheral blood mononuclear cell, 03 medical and health sciences, 0302 clinical medicine, SDG 3 - Good Health and Well-being, Neoplasms, melanoma, medicine, Immunology and Allergy, Humans, Kinase activity, Neoplasm Metastasis, Lung cancer, Immune Checkpoint Inhibitors, RC254-282, Aged, Clinical/Translational Cancer Immunotherapy, Pharmacology, business.industry, Kinase, Melanoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Immunotherapy, Middle Aged, medicine.disease, immunity, Immune checkpoint, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, Molecular Medicine, Female, business, cellular, Tyrosine kinase

Abstract

BackgroundMany cancer patients do not obtain clinical benefit from immune checkpoint inhibition. Checkpoint blockade targets T cells, suggesting that tyrosine kinase activity profiling of baseline peripheral blood mononuclear cells may predict clinical outcome.MethodsHere a total of 160 patients with advanced melanoma or non-small-cell lung cancer (NSCLC), treated with anti-cytotoxic T-lymphocyte-associated protein 4 (anti-CTLA-4) or anti-programmed cell death 1 (anti-PD-1), were divided into five discovery and cross-validation cohorts. The kinase activity profile was generated by analyzing phosphorylation of peripheral blood mononuclear cell lysates in a microarray comprising of 144 peptides derived from sites that are substrates for protein tyrosine kinases. Binary grouping into patients with or without clinical benefit was based on Response Evaluation Criteria in Solid Tumors V.1.1. Predictive models were trained using partial least square discriminant analysis (PLS-DA), performance of the models was evaluated by estimating the correct classification rate (CCR) using cross-validation.ResultsThe kinase phosphorylation signatures segregated responders from non-responders by differences in canonical pathways governing T-cell migration, infiltration and co-stimulation. PLS-DA resulted in a CCR of 100% and 93% in the anti-CTLA-4 and anti-PD1 melanoma discovery cohorts, respectively. Cross-validation cohorts to estimate the accuracy of the predictive models showed CCRs of 83% for anti-CTLA-4 and 78% or 68% for anti-PD-1 in melanoma or NSCLC, respectively.ConclusionBlood-based kinase activity profiling for response prediction to immune checkpoint inhibitors in melanoma and NSCLC revealed increased kinase activity in pathways associated with T-cell function and led to a classification model with a highly accurate classification rate in cross-validation groups. The predictive value of kinase activity profiling is prospectively verified in an ongoing trial.

Published

2020

15. The tumor microenvironment and immunotherapy of oropharyngeal squamous cell carcinoma

Author

Sjoerd H. van der Burg, Saskia J. A. M. Santegoets, and Marij J. P. Welters

Subjects

0301 basic medicine, Cancer Research, oropharyngeal cancer, medicine.medical_treatment, T cells, clinical outcome, Context (language use), Review, lcsh:RC254-282, survival, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, tumor microenvironment, Oropharyngeal squamous cell carcinoma, Tumor microenvironment, business.industry, Immunotherapy, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Clinical trial, 030104 developmental biology, Oncology, Preclinical phase, 030220 oncology & carcinogenesis, Potential biomarkers, myeloid cells, Cancer research, immunotherapy, business

Abstract

Oropharyngeal squamous cell carcinoma (OPSCC) develops as a consequence of several mutations in the tumor suppressor pathways or after a progressive infection with high risk human papillomavirus (HPV). The dismal side effects of the current standard of care and the clear involvement of the immune system has led to a surge in clinical trials that aim to reinforce the tumor-specific immune response as a new treatment option. In this review, we have focused on the most recent literature to discuss the new findings and insights on the role of different immune cells in the context of OPSCC and its etiology. We then applied this knowledge to describe potential biomarkers and analyzed the rationale and outcomes of earlier and ongoing immunotherapy trials. Finally, we describe new developments that are still at the preclinical phase and provide an outlook on what the near future may bring, now that several new and exciting techniques to study the immune system at the single cell level are being exploited.

Published

2020

16. Vulvar cancer subclassification by HPV and p53 status results in three clinically distinct subtypes

Author

Tjalling Bosse, Mariette I.E. van Poelgeest, Esther Bastiaannet, Patricia C. Ewing-Graham, Helena C. van Doorn, Peggy J. de Vos van Steenwijk, Carien L. Creutzberg, Kadir Akdeniz, Linda S. Nooij, Kim E. Kortekaas, Sjoerd H. van der Burg, Obstetrie & Gynaecologie, MUMC+: MA Medische Staf Obstetrie Gynaecologie (9), RS: GROW - R2 - Basic and Translational Cancer Biology, Gynecological Oncology, and Pathology

Subjects

0301 basic medicine, Oncology, p53, PROGNOSIS, Vulvar Squamous Cell Carcinoma, RELATIVE SURVIVAL, p16, DISEASE, 0302 clinical medicine, SEPARATE, Risk Factors, TP53, Papillomaviridae, Aged, 80 and over, RISK, Univariate analysis, Vulvar Neoplasms, Relative survival, Absolute risk reduction, Obstetrics and Gynecology, Middle Aged, 030220 oncology & carcinogenesis, Molecular classification, Carcinoma, Squamous Cell, Vulvectomy, Immunohistochemistry, Female, SQUAMOUS-CELL CARCINOMA, Adult, HUMAN-PAPILLOMAVIRUS HPV, endocrine system, medicine.medical_specialty, Human papillomavirus, Clinical Decision-Making, Risk Assessment, Vulva, Young Adult, 03 medical and health sciences, SDG 3 - Good Health and Well-being, Internal medicine, medicine, MANAGEMENT, Humans, Survival analysis, Aged, Retrospective Studies, LESIONS, business.industry, Papillomavirus Infections, Retrospective cohort study, Vulvar cancer, medicine.disease, TRENDS, Vulvar squamous cell carcinoma, 030104 developmental biology, Mutation, Neoplasm Recurrence, Local, Tumor Suppressor Protein p53, business

Abstract

Objective. There is great need for better risk stratification in vulvar squamous cell carcinoma (VSCC). Our aim was to define the prognostic significance of stratifying VSCC based on p16 and p53 immunohistochemistry (IHC) as surrogate markers for HPV and TP53 mutations.Methods. A large retrospective cohort of surgically treated women with primary VSCC was used. VSCC were classified into three subtypes: HPV-positive (HPVpos), HPV-negative/p53 mutant (HPVneg/p53mut), and HPVnegative/p53 wildtype (HPVneg/p53wt). Overall survival (OS), relative survival (RS), and recurrence-free period (RFP) were depicted using the Kaplan-Meier method and survival curves for relative survival; associations were studied using univariable and multivariable Cox proportional hazard models.Results. Of the 413 VSCCs, 75 (18%) were HPVpos, 63 (15%) HPVneg/p53wt, and 275 (66%) HPVneg/p53mut VSCC. Patients with HPVneg/p53mut VSCC had worse OS and RS (HR 3.43, 95%CI 1.80-6.53, and relative excess risk (RER) of 4.02; 95%CI 1.48-10.90, respectively, and worse RFP (HR 3.76, 95%CI 2.02-7.00). HPVpos VSCC patients showed most favorable outcomes. In univariate analysis, the molecular subtype of VSCC was a prognostic marker for OS, RS and RFP (p = 0.003, p = 0.009, p Conclusions. Stratification of VSCC by p16and p53-IHC has potential to be used routinely in diagnostic pathology. It results in the identification of three clinically distinct subtypes and may be used to guide treatment and follow-up, and in stratifying patients in future clinical trials. (C) 2020 Elsevier Inc. All rights reserved.

Published

2020

17. IL-6 signaling in macrophages is required for immunotherapy-driven regression of tumors

Author

Jan Willem Kleinovink, Thorbald van Hall, Marit J van Elsas, Kees L. M. C. Franken, Sjoerd H. van der Burg, Hans-Willi Mittrücker, Elham Beyranvand Nejad, Ramon Arens, Thomas Korn, Sylvia Heink, and Camilla Labrie

Subjects

Cytotoxicity, Immunologic, Cancer Research, medicine.medical_treatment, Injections, Subcutaneous, Papillomavirus E7 Proteins, Immunology, active, CD8-Positive T-Lymphocytes, Cancer Vaccines, Lymphocytes, Tumor-Infiltrating, Cell Line, Tumor, Neoplasms, Tumor-Associated Macrophages, medicine, Immunology and Allergy, Macrophage, Animals, SOCS3, RC254-282, Pharmacology, Mice, Knockout, Tumor microenvironment, business.industry, Interleukin-6, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Interleukin, Basic Tumor Immunology, Immunotherapy, adaptive immunity, Acquired immune system, Receptors, Interleukin-6, Blockade, Tumor Burden, macrophages, ddc, Mice, Inbred C57BL, Cytokine, Phenotype, Oncology, Oligodeoxyribonucleotides, Cancer research, Molecular Medicine, Female, immunotherapy, business, Signal Transduction, immune evation

Abstract

BackgroundHigh serum interleukin (IL-6) levels may cause resistance to immunotherapy by modulation of myeloid cells in the tumor microenvironment. IL-6 signaling blockade is tested in cancer, but as this inflammatory cytokine has pleiotropic effects, this treatment is not always effective.MethodsIL-6 and IL-6R blockade was applied in an IL-6-mediated immunotherapy-resistant TC-1 tumor model (TC-1.IL-6) and immunotherapy-sensitive TC-1.control. Effects on therapeutic vaccination-induced tumor regression, recurrence and survival as well on T cells and myeloid cells in the tumor microenvironment were studied. The effects of IL-6 signaling in macrophages under therapy conditions were studied in Il6rafl/fl×LysMcre+ mice.ResultsOur therapeutic vaccination protocol elicits a strong tumor-specific CD8+ T-cell response, leading to enhanced intratumoral T-cell infiltration and recruitment of tumoricidal macrophages. Blockade of IL-6 signaling exacerbated tumor outgrowth, reflected by fewer complete regressions and more recurrences after therapeutic vaccination, especially in TC-1.IL-6 tumor-bearing mice. Early IL-6 signaling blockade partly inhibited the development of the vaccine-induced CD8+ T-cell response. However, the main mechanism was the malfunction of macrophages during therapy-induced tumor regression. Therapy efficacy was impaired in Il6rafl/fl×LysMcre+ but not cre-negative control mice, while no differences in the vaccine-induced CD8+ T-cell response were found between these mice. IL-6 signaling blockade resulted in decreased expression of suppressor of cytokine signaling 3, essential for effective M1-type function in macrophages, and increased expression of the phagocytic checkpoint molecule signal-regulatory protein alpha by macrophages.ConclusionIL-6 signaling is critical for macrophage function under circumstances of immunotherapy-induced tumor tissue destruction, in line with the acute inflammatory functions of IL-6 signaling described in infections.

Published

2020

18. 721 AT1412, a patient-derived CD9 antibody in preclinical development promoting tumor immune infiltration and inducing tumor rejection

Author

Susan van Hal, Pauline M. van Helden, Els M. E. Verdegaal, Daniel Go, Martijn Kedde, Madalina Cercel, Hans van Eenennaam, Esmay Frankin, Etsuko Yasuda, Hergen Spits, Christien Fatmawati, Julien Villaudy, Sjoerd H. van der Burg, Wouter Pos, Gemma Moiset, and Remko Schotte

Subjects

Antibody-dependent cell-mediated cytotoxicity, Adoptive cell transfer, biology, business.industry, medicine.medical_treatment, Melanoma, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Acquired immune system, medicine.disease, lcsh:RC254-282, Immune system, Cancer immunotherapy, Cancer cell, Cancer research, biology.protein, Medicine, Antibody, business

Abstract

Background Adaptive immunity to cancer cells forms a crucial part of cancer immunotherapy. Recently, the importance of tumor B-cell signatures were shown to correlate with melanoma survival. We investigated whether tumor-targeting antibodies could be isolated from a patient that cured (now 13 years tumor-free) metastatic melanoma following adoptive transfer of ex vivo expanded autologous T cells. Methods Patient‘s peripheral blood B cells were isolated and tested for the presence of tumor-reactive B cells using AIMM’s immmortalisation technology. Antibody AT1412 was identified by virtue of its differential binding to melanoma cells as compared to healthy melanocytes. AT1412 binds the tetraspanin CD9, a broadly expressed protein involved in multiple cellular activities in cancer and induces ADCC and ADCP by effector cells. Results Spontaneous immune rejection of tumors was observed in human immune system (HIS) mouse models implanted with CD9 genetically-disrupted A375 melanoma (A375-CD9KO) tumor cells, while A375wt cells were not cleared. Most notably, no tumor rejection of A375-CD9KO tumors was observed in NSG mice, indicating that blockade of CD9 makes tumor cells susceptible to immune rejection.CD9 has been described to regulate integrin signaling, e.g. LFA-1, VLA-4, VCAM-1 and ICAM-1. AT1412 was shown to modulate CD9 function by enhancing adhesion and transmigration of T cells to endothelial (HUVEC) cells. AT1412 was most potently enhancing transendothelial T-cell migration, in contrast to a high affinity version of AT1412 or other high affinity anti-CD9 reference antibodies (e.g. ALB6). Enhanced immune cell infiltration is also observed in immunodeficient mice harbouring a human immune system (HIS). AT1412 strongly enhanced CD8 T-cell and macrophage infiltration resulting in tumor rejection (A375 melanoma). PD-1 checkpoint blockade is further sustaining this effect. In a second melanoma model carrying a PD-1 resistant and highly aggressive tumor (SK-MEL5) AT1412 together with nivolumab was inducing full tumor rejection, while either one of the antibodies alone did not. Conclusions The safety of AT1412 has been assessed in preclinical development and is well tolerated up to 10 mg/kg (highest dose tested) by non human primates. AT1412 demonstrated a half-life of 8.5 days, supporting 2–3 weekly administration in humans. Besides transient thrombocytopenia no other pathological deviations were observed. No effect on coagulation parameters, bruising or bleeding were observed macro- or microscopically. The thrombocytopenia is reversible, and its recovery accelerated in those animals developing anti-drug antibodies. First in Human clinical study is planned to start early 2021. Ethics Approval Study protocols were approved by the Medical Ethical Committee of the Leiden University Medical Center (Leiden, Netherlands). Consent Blood was obtained after written informed consent by the patient.

Published

2020

19. Phase I/II study protocol to assess safety and efficacy of adoptive cell therapy with anti-PD-1 plus low-dose pegylated-interferon-alpha in patients with metastatic melanoma refractory to standard of care treatments: the ACTME trial

Author

Els M. E. Verdegaal, Mare A. Jonker, Caroline E. van der Minne, Pauline Meij, Linda de Bruin, Shelley van den Bosch, Sjoerd H. van der Burg, Frank M. Speetjens, Marten Visser, Gerrit-Jan Liefers, Ellen Kapiteijn, Inge Roozen, and Monique K van der Kooij

Subjects

Oncology, medicine.medical_specialty, Standard of care, medicine.medical_treatment, Cell- and Tissue-Based Therapy, Alpha (ethology), dermatological tumours, Polyethylene Glycols, Cell therapy, immunology, 03 medical and health sciences, 0302 clinical medicine, Refractory, Pegylated interferon, Internal medicine, medicine, Humans, 030212 general & internal medicine, Melanoma, Netherlands, Protocol (science), Clinical Trials, Phase I as Topic, business.industry, Interferon-alpha, Standard of Care, General Medicine, Immunotherapy, Clinical Trials, Phase III as Topic, Cohort, Medicine, business, 030217 neurology & neurosurgery, medicine.drug

Abstract

IntroductionTreatment with anti-PD-1 immunotherapy does not lead to long-lasting clinical responses in approximately 60% of patients with metastatic melanoma. These refractory patients, however, can still respond to treatment with tumour infiltrating lymphocytes (TIL) and interferon-alpha (IFNa). A combination of TIL, pegylated-interferon-alpha (PEG-IFNa) and anti-PD-1 is expected to provide a safe, feasible and effective therapy for patients with metastatic melanoma, who are refractory to standard of care treatment options.Methods and analysisPatients are treated in two phases. In phase I, the safety of the combination TIL and anti-PD-1 is assessed (cohort 1) according to CTCAE 4.03 criteria. Subsequently, the safety of cotreatment with PEG-IFNa is tested in cohort 2. The efficacy will be evaluated in the second phase of the trial. Efficacy is evaluated according to RECIST 1.1 and immune-related response criteria. Clinical and immunological parameters will be evaluated for their relation with clinical responsiveness.Ethics and disseminationEthical approval of the trial was obtained from the Central Committee on Research Involving Human Subjects in the Netherlands. The trial results will be shared with the scientific community at (inter)national conferences and by publication in a peer-reviewed journal.Trial registration numberNCT03638375.

Published

2020

20. Host genetics and tumor environment determine the functional impact of neutrophils in mouse tumor models

Author

Marit J van Elsas, G. Feiss, Jan Willem Kleinovink, Hailiang Mei, Sjoerd H. van der Burg, Matthijs Moerland, Peter H. Nibbering, Guillaume Beyrend, Ramon Arens, Thorbald van Hall, and Silvana M.G. Jirka

Subjects

Cancer Research, Neutrophils, medicine.medical_treatment, Immunology, Antimicrobial peptides, Biology, Mice, Immune system, Immunity, Cell Line, Tumor, medicine, Tumor Microenvironment, innate, gene expression profiling, Immunology and Allergy, Animals, Humans, Pharmacology, Tumor microenvironment, Cancer, Basic Tumor Immunology, Immunotherapy, medicine.disease, immunity, Gene expression profiling, Disease Models, Animal, Oncology, Tumor progression, Cancer research, Molecular Medicine, Female, immunotherapy, immune evation

Abstract

BackgroundNeutrophils have been reported to have protumor, antitumor or neutral effects in cancer progression. The underlying causes for this functional variability are not clear.MethodsWe studied the role of neutrophils in six different mouse tumor models by intratumoral injection of antimicrobial peptides or vaccination. Changes in systemic and intratumoral immune cells were analyzed by flow-cytometry and mass-cytometry. The role of neutrophils was studied by antibody-mediated neutrophil depletion. Neutrophils from different mouse strains were compared by RNA sequencing.ResultsThe antimicrobial peptide Omiganan reduced the growth of TC-1 tumors in BL/6 mice and CT26 tumors in BALB/c mice. No significant effects were observed in B16F10, MC38 and 4T1 tumors. Growth delay was associated with increased abundance of neutrophils in TC-1 but not CT26 tumors. Systemic neutrophil depletion abrogated Omiganan efficacy in TC-1 but further reduced growth of CT26, indicating that neutrophils were required for the antitumor effect in TC-1 but suppressed tumor control in CT26. Neutrophils were also required for a therapeutic vaccine-induced T-cell mediated control of RMA tumors in BL/6 mice. Clearly, the circulating and intratumoral neutrophils differed in the expression of Ly6G and CD62L, between TC-1 and CT26 and between blood neutrophils of tumor-naïve BL/6 and BALB/c mice. RNA-sequencing revealed that neutrophils from BL/6 mice but not BALB/c mice displayed a robust profile of immune activation, matching their opposing roles in TC-1 and RMA versus CT26.ConclusionsNeutrophil functionality differs strongly between mouse strains and tumor types, with consequences for tumor progression and therapy.

Published

2020

21. CD163+ cytokine-producing cDC2 stimulate intratumoral type 1 T cell responses in HPV16-induced oropharyngeal cancer

Author

Chantal L. Duurland, Nikki M. Loof, Ekaterina J Jordanova, Sjoerd H. van der Burg, Saskia J. A. M. Santegoets, Florent Ginhoux, Vipin Narang, Charles A Dutertre, Vanessa J. van Ham, Ilina Ehsan, Sylvia L. van Egmond, Marij J. P. Welters, Obstetrics and gynaecology, CCA - Cancer biology and immunology, and Amsterdam Reproduction & Development (AR&D)

Subjects

lymphocytes, Cancer Research, Immunology, Mutant, immunity, cellular, Virulence, lymphocytes, tumor-infiltrating, Antigens, Differentiation, Myelomonocytic, Receptors, Cell Surface, medicine.disease_cause, T-Lymphocytes, Regulatory, Virulence factor, Microbiology, head and neck neoplasms, Antigens, CD, medicine, Tumor Microenvironment, Immunology and Allergy, Humans, dendritic cells, Escherichia coli, Pharmacology, Clinical/Translational Cancer Immunotherapy, Human papillomavirus 16, biology, Chemistry, Biofilm, tumor-infiltrating, biology.organism_classification, Prognosis, immunity, Acinetobacter baumannii, Complementation, Oropharyngeal Neoplasms, Oncology, Molecular Medicine, Female, Heterologous expression, cellular

Abstract

BackgroundHuman papillomavirus (HPV)-associated oropharyngeal squamous cell carcinoma (OPSCC) is a distinct clinical entity with a much better prognosis after (chemo)radiotherapy than HPV-negative OPSCC, especially in patients with a concomitant intratumoral HPV-specific and type-1 cytokine-oriented T cell response. However, knowledge on the type of myeloid cells and their coordination with intratumoral T cells and influence on patient outcome in OPSCC is lacking.MethodsWe analyzed the presence of intratumoral myeloid cells and their relationship to tumor-infiltrating T cells and patient outcome in a well-described cohort of HPV16+ patients with OPSCC using multispectral immunofluorescence, flow cytometry and functional analyses.ResultsWe show that the tumor microenvironment of HPV16+ OPSCC tumors with such an ongoing HPV16-specific T cell response is highly infiltrated with a newly defined CD163+ cytokine-producing subset of conventional dendritic cell type 2 (cDC2), called DC3. These CD163+ cDC2 predominantly stimulated type 1 T cell polarization and produced high levels of interleukin-12 (IL-12) and IL-18, required for IFNγ and IL-22 production by T cells after cognate antigen stimulation. Tumor-infiltration with these CD163+ cDC2 positively correlated with the infiltration by Tbet+ and tumor-specific T cells, and with prolonged survival.ConclusionsThese data suggest an important role for intratumoral CD163+ cDC2 in stimulating tumor-infiltrating T cells to exert their antitumor effects.

Published

2020

22. Low-dose interferon-alpha preconditioning and adoptive cell therapy in patients with metastatic melanoma refractory to standard (immune) therapies: a phase I/II study

Author

Saskia J. A. M. Santegoets, Els M. E. Verdegaal, Ellen Kapiteijn, Caroline E. van der Minne, Noel F C C de Miranda, Monique K van der Kooij, Marij J. P. Welters, Linda de Bruin, Anton G. T. Terwisscha van Scheltinga, Pauline Meij, Gerrit-Jan Liefers, Marten Visser, Inge Roozen, and Sjoerd H. van der Burg

Subjects

Adult, Male, Oncology, Cancer Research, medicine.medical_specialty, medicine.medical_treatment, Lymphocyte, T cell, Cell- and Tissue-Based Therapy, Alpha interferon, tumours, Cell therapy, immunology, Internal medicine, medicine, Humans, Immunology and Allergy, Cytotoxic T cell, RC254-282, Aged, Pharmacology, Leukopenia, Immune Cell Therapies and Immune Cell Engineering, business.industry, Interferon-alpha, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Immunotherapy, interferon, Middle Aged, medicine.anatomical_structure, Molecular Medicine, Female, medicine.symptom, business, CD8

Abstract

BackgroundAdoptive cell therapy (ACT) with tumor-reactive T cells has shown consistent clinical efficacy. We evaluated the response to ACT in combination with interferon alpha (IFNa) preconditioning in patients with stage IV metastatic melanoma, most of which were progressive on cytotoxic T-lymphocyte-associated protein 4 and/or programmed cell death protein 1 checkpoint blockade therapy.MethodsThirty-four patients were treated with ex vivo expanded tumor reactive T cells, derived from mixed lymphocyte autologous tumor cultures, or with autologous tumor-infiltrating lymphocytes and evaluated for clinical response. Clinical and immunological parameters associated with response were also evaluated.ResultsBest overall response defined as clinical benefit, comprising either complete response, partial response or stable disease >6 months, was observed in 29% of the patients. Forty-three per cent of the 14 immunotherapy-naïve patients and 20% of the 20 patients progressive on prior immunotherapy benefited from ACT. The overall survival (OS) was 90% versus 28.6% at 1 year and 46.7% versus 0% at 3 years follow-up, of responder and non-responder patients, respectively. Median OS was 36 versus 7 months, respectively. IFNa pretreatment resulted in leukopenia, neutropenia and lymphopenia, which was sustained during the treatment in clinical responders and associated with response. Differences in antigen specificity, but not in phenotype, cytokine profile or CD8+ T cell number of the ACT products correlated with clinical response. Cross-reactivity of the ACT products to one or more allogeneic human leukocyte antigen-matched melanoma cell lines was associated with short OS after treatment while the ACT products of very long-term survivors showed no cross-reactivity but recognized patient-specific neoantigens.ConclusionThis study demonstrates that ACT in combination with a mild IFNa preconditioning regimen can induce clinical benefit even in immunotherapy pretreated patients, although with lower success than in immunotherapy-naïve patients. ACT products comprising neoantigen reactivity may be more effective.

Published

2020

23. Tumor mutational load, CD8+ T cells, expression of PD-L1 and HLA class I to guide immunotherapy decisions in NSCLC patients

Author

Jasper Smit, Ronald van Marion, Piet E. Postmus, Ron H.J. Mathijssen, Daan P. Hurkmans, Merian E. Kuipers, Joachim G.J.V. Aerts, Sjoerd H. van der Burg, Jan H. von der Thüsen, Pieter S. Hiemstra, Pulmonary Medicine, Medical Oncology, Rotterdam School of Management, and Pathology

Subjects

Oncology, Cancer Research, medicine.medical_specialty, medicine.medical_treatment, T cell, Immunology, Human leukocyte antigen, NSCLC, 03 medical and health sciences, 0302 clinical medicine, SDG 3 - Good Health and Well-being, PD-L1, Internal medicine, medicine, Immunology and Allergy, Cytotoxic T cell, 030304 developmental biology, 0303 health sciences, biology, business.industry, TMB, Immunotherapy, Biomarker, medicine.disease, medicine.anatomical_structure, Nivolumab, Tumor microenvironment, 030220 oncology & carcinogenesis, biology.protein, Adenocarcinoma, business, CD8, Progressive disease

Abstract

Objectives A minority of NSCLC patients benefit from anti-PD1 immune checkpoint inhibitors. A rational combination of biomarkers is needed. The objective was to determine the predictive value of tumor mutational load (TML), CD8+ T cell infiltration, HLA class-I and PD-L1 expression in the tumor. Materials and methods Metastatic NSCLC patients were prospectively included in an immune-monitoring trial (NTR7015) between April 2016-August 2017, retrospectively analyzed in FFPE tissue for TML (NGS: 409 cancer-related-genes) and by IHC staining to score PD-L1, CD8+ T cell infiltration, HLA class-I. PFS (RECISTv1.1) and OS were analyzed by Kaplan–Meier methodology. Results 30 patients with adenocarcinoma (67%) or squamous cell carcinoma (33%) were included. High TML was associated with better PFS (p = 0.004) and OS (p = 0.025). Interaction analyses revealed that patients with both high TML and high total CD8+ T cell infiltrate (p = 0.023) or no loss of HLA class-I (p = 0.026), patients with high total CD8+ T cell infiltrate and no loss of HLA class-I (p = 0.041) or patients with both high PD-L1 and high TML (p = 0.003) or no loss of HLA class-I (p = 0.032) were significantly associated with better PFS. Unsupervised cluster analysis based on these markers revealed three sub-clusters, of which cluster-1A was overrepresented by patients with progressive disease (15 out of 16), with significant effect on PFS (p = 0.007). Conclusion This proof-of-concept study suggests that a combination of PD-L1 expression, TML, CD8+ T cell infiltration and HLA class-I functions as a better predictive biomarker for response to anti-PD-1 immunotherapy. Consequently, refinement of this set of biomarkers and validation in a larger set of patients is warranted.

Published

2020

24. Immunotherapeutic Potential of TGF-beta Inhibition and Oncolytic Viruses

Author

Peter ten Dijke, Nadine van Montfoort, Christianne Groeneveldt, Sjoerd H. van der Burg, and Thorbald van Hall

Subjects

0301 basic medicine, medicine.medical_treatment, animal diseases, Immunology, chemical and pharmacologic phenomena, 03 medical and health sciences, 0302 clinical medicine, Immune system, Cancer immunotherapy, Transforming Growth Factor beta, Neoplasms, medicine, Immunology and Allergy, Humans, Oncolytic Virotherapy, business.industry, Immunogenicity, Cancer, Immunotherapy, biochemical phenomena, metabolism, and nutrition, medicine.disease, Immune checkpoint, Blockade, Oncolytic virus, Oncolytic Viruses, 030104 developmental biology, bacteria, business, 030215 immunology

Abstract

In cancer immunotherapy, a patient's own immune system is harnessed against cancer. Immune checkpoint inhibitors release the brakes on tumor-reactive T cells and, therefore, are particularly effective in treating certain immune-infiltrated solid tumors. By contrast, solid tumors with immune-silent profiles show limited efficacy of checkpoint blockers due to several barriers. Recent discoveries highlight transforming growth factor-beta (TGF-beta)-induced immune exclusion and a lack of immunogenicity as examples of these barriers. In this review, we summarize preclinical and clinical evidence that illustrates how the inhibition of TGF-beta signaling and the use of oncolytic viruses (OVs) can increase the efficacy of immunotherapy, and discuss the promise and challenges of combining these approaches with immune checkpoint blockade.

Published

2020

25. Future Challenges in Cancer Resistance to Immunotherapy

Author

Thorbald van Hall, Marit J van Elsas, and Sjoerd H. van der Burg

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Cancer resistance, T cell, Immune checkpoint inhibitors, medicine.medical_treatment, Review, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Acquired resistance, Immune system, Internal medicine, medicine, primary resistance, business.industry, Cancer, Immunotherapy, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, secondary resistance, Clinical trial, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, immunotherapy, business

Abstract

Cancer immunotherapies, including checkpoint inhibitors, adoptive T cell transfer and therapeutic cancer vaccines, have shown promising response rates in clinical trials. Unfortunately, there is an increasing number of patients in which initially regressing tumors start to regrow due to an immunotherapy-driven acquired resistance. Studies on the underlying mechanisms reveal that these can be similar to well-known tumor intrinsic and extrinsic primary resistance factors that precluded the majority of patients from responding to immunotherapy in the first place. Here, we discuss primary and secondary immune resistance and point at strategies to identify potential new mechanisms of immune evasion. Ultimately, this may lead to improved immunotherapy strategies with improved clinical outcomes.

Published

2020

26. Strong vaccine responses during chemotherapy are associated with prolonged cancer survival

Author

Petronella B. Ottevanger, Willem Jan Krebber, Sanne Boekestijn, Judith R. Kroep, Gemma G. Kenter, Nikki M. Loof, Roy I. Lalisang, Hannelore Denys, Sjoerd H. van der Burg, Richard B. Stead, Cornelis J. M. Melief, Thierry Velu, Winald R. Gerritsen, Marij J. P. Welters, Anna K.L. Reyners, Brent A. Blumenstein, Frédéric Goffin, Hans W. Nijman, Sonja Visscher, Leon Hooftman, Ignace Vergote, Mariette I.E. van Poelgeest, Wiebren A.A. Tjalma, RS: GROW - R3 - Innovative Cancer Diagnostics & Therapy, MUMC+: MA Medische Oncologie (9), Translational Immunology Groningen (TRIGR), Targeted Gynaecologic Oncology (TARGON), and Guided Treatment in Optimal Selected Cancer Patients (GUTS)

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, CERVICAL-CANCER, Myeloid, Papillomavirus E7 Proteins, medicine.medical_treatment, Uterine Cervical Neoplasms, Cancer Vaccines, LEUKOCYTOSIS, 03 medical and health sciences, chemistry.chemical_compound, CISPLATIN, All institutes and research themes of the Radboud University Medical Center, 0302 clinical medicine, Immune system, Chemoimmunotherapy, Internal medicine, CLASS-I, medicine, Humans, Papillomavirus Vaccines, REGULATORY T-CELLS, RECURRENT, Biology, E6, Human papillomavirus 16, Chemotherapy, CARBOPLATIN, business.industry, INDUCTION, Papillomavirus Infections, Cancer, NIVOLUMAB, General Medicine, medicine.disease, Carboplatin, Women's cancers Radboud Institute for Health Sciences [Radboudumc 17], Vaccination, 030104 developmental biology, medicine.anatomical_structure, chemistry, Urological cancers Radboud Institute for Health Sciences [Radboudumc 15], 030220 oncology & carcinogenesis, Female, Human medicine, Nivolumab, business

Abstract

Therapeutic cancer vaccines have effectively induced durable regressions of premalignant oncogenic human papilloma virus type 16 (HPV16)-induced anogenital lesions. However, the treatment of HPV16-induced cancers requires appropriate countermeasures to overcome cancer-induced immune suppression. We previously showed that standard-of-care carboplatin/paclitaxel chemotherapy can reduce abnormally high numbers of immunosuppressive myeloid cells in patients, allowing the development of much stronger therapeutic HPV16 vaccine (ISA101)-induced tumor immunity. We now show the clinical effects of ISA101 vaccination during chemotherapy in 77 patients with advanced, recurrent, or metastatic cervical cancer in a dose assessment study of ISA101. Tumor regressions were observed in 43% of 72 evaluable patients. The depletion of myeloid suppressive cells by carboplatin/paclitaxel was associated with detection of low frequency of spontaneous HPV16-specific immunity in 21 of 62 tested patients. Patients mounted type 1 T cell responses to the vaccine across all doses. The group of patients with higher than median vaccine-induced immune responses lived longer, with a flat tail on the survival curve. This demonstrates that chemoimmunotherapy can be exploited to the benefit of patients with advanced cancer based on a defined mode of action.

Published

2020

27. Identification of non-mutated neoantigens presented by TAP-deficient tumors

Author

Els M. E. Verdegaal, Thorbald van Hall, Sjoerd H. van der Burg, Mirjam H.M. Heemskerk, Koen A. Marijt, Stefan Stevanovic, Daniel J. Kowalewski, Hans-Georg Rammensee, Laura Blijleven, and Michel G.D. Kester

Subjects

Male, 0301 basic medicine, T cell, Immunology, Antigen presentation, Human leukocyte antigen, CD8-Positive T-Lymphocytes, News, Biology, Insights, Article, 03 medical and health sciences, Antigen, Antigens, Neoplasm, Neoplasms, HLA-A2 Antigen, Tumor Cells, Cultured, medicine, Humans, Immunology and Allergy, LDL-Receptor Related Protein-Associated Protein, Research Articles, Antigen Presentation, integumentary system, Melanoma, Cancer, medicine.disease, Neoplasm Proteins, 030104 developmental biology, medicine.anatomical_structure, Tumor Escape, Cancer research, ATP-Binding Cassette Transporters, Female, CD8

Abstract

A hybrid forward-reversed immunological screen is performed to identify 16 novel HLA-A2 presented cancer antigens. These peptides are selectively presented by immune-escaped cancer cells with defects in the peptide transporter TAP. In contrast to mutated neoantigens, these “self” neoantigens are universally presented across different cancer types., Most T cell–based immunotherapies of cancer depend on intact antigen presentation by HLA class I molecules (HLA-I). However, defects in the antigen-processing machinery can cause downregulation of HLA-I, rendering tumor cells resistant to CD8+ T cells. Previously, we demonstrated that a unique category of cancer antigens is selectively presented by tumor cells deficient for the peptide transporter TAP, enabling a specific attack of such tumors without causing immunopathology in mouse models. With a novel combinatorial screening approach, we now identify 16 antigens of this category in humans. These HLA-A*02:01 presented peptides do not derive from the mutanome of cancers, but are of “self” origin and therefore constitute universal neoantigens. Indeed, CD8+ T cells specific for the leader peptide of the ubiquitously expressed LRPAP1 protein recognized TAP-deficient, HLA-Ilow lymphomas, melanomas, and renal and colon carcinomas, but not healthy counterparts. In contrast to personalized mutanome-targeted therapies, these conserved neoantigens and their cognate receptors can be exploited for immune-escaped cancers across diverse histological origins., Graphical Abstract

Published

2018

28. 356 Personalized immunotherapy by adoptive T cell transfer during chemotherapy with or without interferon-alpha in patients with recurrent platinum-sensitive epithelial ovarian cancer

Author

Pauline Meij, Els M. E. Verdegaal, Marten Visser, Linda de Bruin, Inge Roozen, Sjoerd H. van der Burg, Lien van der Minne, and Judith R. Kroep

Subjects

Pharmacology, Cancer Research, Chemotherapy, business.industry, medicine.medical_treatment, T cell, Immunology, Alpha interferon, Immunotherapy, medicine.anatomical_structure, Oncology, Cancer research, Molecular Medicine, Immunology and Allergy, Medicine, Platinum sensitive, Epithelial ovarian cancer, In patient, business

Abstract

BackgroundEpithelial ovarian cancer (EOC) is considered an immunogenic tumor, as illustrated by the clear correlation between T-cell infiltration and overall survival. This suggests that patients with EOC may be eligible for immunotherapy including adoptive cell therapy with autologous Tumor Infiltrating Lymphocytes (TIL). However, immunosuppressive cells including myeloid derived suppressor cells an regulatory T cells are also abundant in EOC and may need to be targeted simultaneously to achieve the full potential of the infused TIL. Carboplatin-paclitaxel chemotherapy (CPC) reduces the number of immunosuppressive cells in cervical cancer patients,1 creating a window-of-opportunity for TIL to exert their full effector function. Interferon-alpha further supports infused TIL. A phase I/II trial (NCT04072263) was initiated to study the feasibility and safety of TIL during CPC with or without additional interferon-alpha in patients with recurrent platinum-sensitive EOC.MethodsFifteen patients with recurrent platinum-sensitive EOC received 6 cycles of CPC intravenously every 3 weeks and TIL intravenously 2 weeks after the 2nd,3rd and 4th CPC cycle. Pegylated-interferon-alpha was added in the second cohort for 12 weeks, starting one week before the first TIL infusion. Patients who received 3 TIL infusions were evaluable. The primary endpoint was feasibility and safety of TIL administration during CPC with or without interferon-alpha. As secondary endpoints signs of activity, underlying mechanisms, immunomodulation, and T-cell reactivity were studied.ResultsThirteen patients were available for analysis. Median age 63 years (range, 29–77). TIL could be successfully expanded for all patients. Treatment with TIL during CPC was safe and did not add toxicity. Addition of IFNα resulted in grade 3 leucopenia and grade 3 trombocytopenia in the first 2 patients and was therefore omitted in subsequent patients. CPC alleviated the immunosuppressive status, reflected by reduced plasma IL-6 levels and circulating myeloid-cell numbers, while lymphocytes numbers are not affected. This was most prominently at 1–2 weeks after the 2nd CPC and is suggested to reflect improved conditions promoting intra-tumoral T-cell reactivity. Objective responses were observed in 10/13 (77%) patients and 3 patients had stable disease. Interestingly, in at least one patient the ongoing platinum-free interval of 25 months far exceeds the first platinum-free interval of 8 months after similar CPC. In depth studies on immune modulation by chemotherapy and by TIL/Interferon-alpha, and correlations between TIL phenotype and clinical outcome are ongoing and will be presented.ConclusionsCombined treatment with CP chemotherapy and properly timed TIL may result in clinical benefit for patients with EOC.AcknowledgementsThe unrestricted funding of the trial by Ovacure is greatly acknowledged.Trial RegistrationThe trial is registered at www.clinicaltrials.gov under number NCT04072263.ReferenceWelters MJ, van der Sluis TC, van Meir H, Loof NM, van Ham VJ, van Duikeren S, Santegoets SJ, Arens R, de Kam ML, Cohen AF, van Poelgeest MI, Kenter GG, Kroep JR, Burggraaf J, Melief CJ, van der Burg SH. Vaccination during myeloid cell depletion by cancer chemotherapy fosters robust T cell responses. Sci Transl Med 2016;8(334):334ra52. doi: 10.1126/scitranslmed.aad8307Ethics ApprovalThis study was approved by Leiden University Medical Center‘s Ethics Board; approval number L18-012 and the Central Committee on Research Involving Human Subjects; approval number NL63434.000.17.

Published

2021

29. IDO and galectin-3 hamper the ex vivo generation of clinical grade tumor-specific T cells for adoptive cell therapy in metastatic melanoma

Author

Els M. E. Verdegaal, Sjoerd H. van der Burg, Sara M. Melief, and Marten Visser

Subjects

0301 basic medicine, Interleukin 2, CD4-Positive T-Lymphocytes, Cancer Research, Adoptive cell transfer, Skin Neoplasms, Lymphocyte, T cell, medicine.medical_treatment, Galectin 3, Immunology, Metastatic melanoma, CD8-Positive T-Lymphocytes, IDO, Immunophenotyping, Cell therapy, 03 medical and health sciences, Interleukin 21, Interferon-gamma, Lymphocytes, Tumor-Infiltrating, Tumor Cells, Cultured, Tumor Microenvironment, Immunology and Allergy, Medicine, Galectin-3, Humans, Indoleamine-Pyrrole 2,3,-Dioxygenase, Melanoma, Tumor microenvironment, business.industry, GMP, Interleukin-2 Receptor alpha Subunit, Immunotherapy, Flow Cytometry, Adoptive Transfer, Coculture Techniques, 030104 developmental biology, medicine.anatomical_structure, Oncology, Interleukin-2, Original Article, business, medicine.drug

Abstract

Adoptive T cell transfer (ACT) with ex vivo-expanded tumor-reactive T cells proved to be successful for the treatment of metastatic melanoma patients. Mixed lymphocyte tumor cell cultures (MLTC) can be used to generate tumor-specific T cells for ACT; however, in a number of cases tumor-reactive T cell, expansion is far from optimal. We hypothesized that this is due to tumor intrinsic and extrinsic factors and aimed to identify and manipulate these factors so to optimize our clinical, GMP-compliant MLTC protocol. We found that the tumor cell produced IDO and/or galectin-3, and the accumulation of CD4+CD25hiFoxP3+ T cells suppressed the expansion of tumor-specific T cells in the MLTC. Strategies to eliminate CD4+CD25hiFoxP3+ T cells during culture required the depletion of the whole CD4+ T cell population and were found to be undesirable. Blocking of IDO and galectin-3 was feasible and resulted in improved efficiency of the MLTC. Implementation of these findings in clinical protocols for ex vivo expansion of tumor-reactive T cells holds promise for an increased therapeutic potential of adoptive cell transfer treatments with tumor-specific T cells. Electronic supplementary material The online version of this article (doi:10.1007/s00262-017-1995-x) contains supplementary material, which is available to authorized users.

Published

2017

30. The NKG2A-HLA-E Axis as a Novel Checkpoint in the Tumor Microenvironment

Author

Linda Borst, Sjoerd H. van der Burg, and Thorbald van Hall

Subjects

0301 basic medicine, Cancer Research, Programmed Cell Death 1 Receptor, Human leukocyte antigen, Cancer Vaccines, B7-H1 Antigen, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, HLA-E, Neoplasms, Tumor Microenvironment, Medicine, Cytotoxic T cell, Humans, Immune Checkpoint Inhibitors, Tumor microenvironment, business.industry, Histocompatibility Antigens Class I, Blockade, Killer Cells, Natural, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, Monalizumab, business, NK Cell Lectin-Like Receptor Subfamily C

Abstract

The success of checkpoint blockade therapy revolutionized cancer treatment. However, we need to increase the fraction of responding patients and overcome acquired resistance to these therapies. Recently, the inhibitory receptor NKG2A received attention as a new kid on the block of immune checkpoints. This receptor is selectively expressed on cytotoxic lymphocytes, including natural killer cells and CD8 T cells, and NKG2A+ T cells are preferentially residing in tissues, like the tumor microenvironment. Its ligand, histocompatibility leucocyte antigen E (HLA-E), is a conserved nonclassical HLA class I molecule that binds a limited peptide repertoire and its expression is commonly detected in human cancer. NKG2A blockade as a standalone therapy appears poorly effective in mouse tumor models, however, in the presence of activated T cells, for example, induced by PD-1/PD-L1 blockade or cancer vaccines, exerts strongly enhanced efficacy. Clinical trials demonstrated safety of the humanized NKG2A-blocking antibody, monalizumab, and first results of phase II trials demonstrate encouraging durable response rates. Further development of this axis is clearly warranted.

Published

2020

31. Pre-existing inflammatory immune microenvironment predicts the clinical response of vulvar high-grade squamous intraepithelial lesions to therapeutic HPV16 vaccination

Author

Hans W. Nijman, Edith M.G. van Esch, Mariette I.E. van Poelgeest, Ziena Abdulrahman, Sjoerd H. van der Burg, Noel F C C de Miranda, Marij J. P. Welters, and Peggy J. de Vos van Steenwijk

Subjects

0301 basic medicine, Cancer Research, Myeloid, CARCINOMA, medicine.medical_treatment, T cell, Immunology, NEOPLASIA, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immunotherapy Biomarkers, medicine, Immunology and Allergy, Cytotoxic T cell, tumor microenvironment, CERVICAL-CANCER PATIENTS, RC254-282, E7, E6, Pharmacology, Tumor microenvironment, business.industry, therapeutic vaccination, FOXP3, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Immunotherapy, vulvar HSIL, 030104 developmental biology, medicine.anatomical_structure, Oncology, INFILTRATION, 030220 oncology & carcinogenesis, HUMAN-PAPILLOMAVIRUS-16, T-CELLS, Molecular Medicine, IMIQUIMOD, immunotherapy, business, CD8

Abstract

BackgroundVulvar high-grade squamous intraepithelial lesion (vHSIL) is predominantly induced by high-risk human papilloma virus type 16 (HPV16). In two independent trials, therapeutic vaccination against the HPV16 E6 and E7 oncoproteins resulted in objective partial and complete responses (PRs/CRs) in half of the patients with HPV16+vHSIL at 12-month follow-up. Here, the prevaccination and postvaccination vHSIL immune microenvironment in relation to the vaccine-induced clinical response was investigated.MethodsTwo novel seven-color multiplex immunofluorescence panels to identify T cells (CD3, CD8, Foxp3, Tim3, Tbet, PD-1, DAPI) and myeloid cells (CD14, CD33, CD68, CD163, CD11c, PD-L1, DAPI) were designed and fully optimized for formalin-fixed paraffin-embedded tissue. 29 prevaccination and 24 postvaccination biopsies of patients with vHSIL, and 27 healthy vulva excisions, were stained, scanned with the Vectra multispectral imaging system, and automatically phenotyped and counted using inForm advanced image analysis software.ResultsHealthy vulvar tissue is strongly infiltrated by CD4 and CD8 T cells expressing Tbet and/or PD-1 and CD14+HLA-DR+inflammatory myeloid cells. The presence of such a coordinated pre-existing proinflammatory microenvironment in HPV16+vHSIL is associated with CR after vaccination. In partial responders, a disconnection between T cell and CD14+myeloid cell infiltration was observed, whereas clinical non-responders displayed overall lower immune cell infiltration. Vaccination improved the coordination of local immunity, reflected by increased numbers of CD4+Tbet+T cells and HLA-DR+CD14+expressing myeloid cells in patients with a PR or CR, but not in patients with no response. CD8+T cell infiltration was not increased after vaccination.ConclusionA prevaccination inflamed type 1 immune contexture is required for stronger vaccine-induced immune infiltration and is associated with better clinical response. Therapeutic vaccination did not overtly increase immune infiltration of cold lesions.

Published

2020

32. Adoptive cell therapy in combination with checkpoint inhibitors in ovarian cancer

Author

Lars Rønn Olsen, Brad H. Nelson, Sjoerd H. van der Burg, Morten Nielsen, Özcan Met, Saskia J. A. M. Santegoets, Magnus Pedersen, Troels Holz Borch, Inge Marie Svane, Marco Donia, Anders Handrup Kverneland, Katy Milne, Gitte Aasbjerg, and Marie Christine Wulff Westergaard

Subjects

0301 basic medicine, T cell, Ipilimumab, chemical and pharmacologic phenomena, Tumor-infiltrating lymphocytes, Cell therapy, 03 medical and health sciences, 0302 clinical medicine, SDG 3 - Good Health and Well-being, Ovarian cancer, medicine, Cytotoxic T cell, Checkpoint inihibors, business.industry, adoptive cell therapy, hemic and immune systems, combinational immune therapy, Combinational immune therapy, medicine.disease, Adoptive cell therapy, ovarian cancer, 030104 developmental biology, medicine.anatomical_structure, Oncology, tumor-infiltrating lymphocytes, 030220 oncology & carcinogenesis, Cancer research, Nivolumab, business, checkpoint inihibors, Ex vivo, Checkpoint inhibitors, Research Paper, medicine.drug

Abstract

Immune therapy is a promising field within oncology but has been unsuccessful in ovarian cancer (OC). Still, there is rationale and evidence supporting immune therapy in OC. We investigated the potential for adoptive cell therapy (ACT) from in vitro expanded tumor-infiltrating lymphocytes (TILs) in combination with checkpoint inhibitors (ICI) and conducted immunological testing of ex vivo expanded TILs (REP-TILs). Six patients with late-stage metastatic high-grade serous OC were treated with immune therapy consisting of ipilimumab followed by surgery to obtain TILs and infusion of REP-TILs, low-dose IL-2 and nivolumab. One patient achieved a partial response and 5 others experienced disease stabilization for up to 12 months. Analysis of the REP-TILs with flow- and mass-cytometry show primarily activated and differentiated effector memory T cells. REP-TILs showed in vitro reactivity and expression of inhibitory receptors, such as LAG-3 and PD-1. Furthermore, our data indicate that addition of ipilimumab therapy improves the T cell fold expansion during production, increase the level of CD8 T cell tumor reactivity, and favorably affect the T cell phenotype. We show that the combination of ICI and ACT is feasible and safe. With one partial response and one long-lasting SD, we demonstrated the potential of ACT in OC.

Published

2020

33. Dendritic cell vaccination and CD40-agonist combination therapy licenses T cell-dependent antitumor immunity in a pancreatic carcinoma murine model

Author

Ralph Stadhouders, Menno van Nimwegen, Thorbald van Hall, Koen A. Marijt, Sanne L A Lievense, Sai Ping Lau, Andrew P. Stubbs, Sjoerd H. van der Burg, Jasper Dumas, Larissa Klaase, Heleen Vroman, Yunlei Li, Christianne Groeneveldt, Priscilla Kinderman, Floris Dammeijer, Nadine van Montfoort, Joachim G.J.V. Aerts, Casper H.J. van Eijck, Melanie Lukkes, Dana A M Mustafa, Mandy van Gulijk, Pulmonary Medicine, Surgery, Pathology, and Cell biology

Subjects

Cancer Research, medicine.medical_treatment, T cell, Immunology, Adenocarcinoma, Cancer Vaccines, Mice, Immune system, SDG 3 - Good Health and Well-being, Pancreatic cancer, medicine, Animals, Humans, Immunology and Allergy, dendritic cells, T-lymphocytes, Clinical/Translational Cancer Immunotherapy, Pharmacology, Tumor microenvironment, business.industry, Immunotherapy, Dendritic cell, medicine.disease, vaccination, Disease Models, Animal, medicine.anatomical_structure, Oncology, Tumor progression, Cancer research, Molecular Medicine, Female, immunotherapy, business, CD8, Carcinoma, Pancreatic Ductal

Abstract

BackgroundPancreatic ductal adenocarcinoma (PDAC) is notoriously resistant to treatment including checkpoint-blockade immunotherapy. We hypothesized that a bimodal treatment approach consisting of dendritic cell (DC) vaccination to prime tumor-specific T cells, and a strategy to reprogram the desmoplastic tumor microenvironment (TME) would be needed to break tolerance to these pancreatic cancers. As a proof-of-concept, we investigated the efficacy of combined DC vaccination with CD40-agonistic antibodies in a poorly immunogenic murine model of PDAC. Based on the rationale that mesothelioma and pancreatic cancer share a number of tumor associated antigens, the DCs were loaded with either pancreatic or mesothelioma tumor lysates.MethodsImmune-competent mice with subcutaneously or orthotopically growing KrasG12D/+;Trp53R172H/+;Pdx-1-Cre (KPC) PDAC tumors were vaccinated with syngeneic bone marrow-derived DCs loaded with either pancreatic cancer (KPC) or mesothelioma (AE17) lysate and consequently treated with FGK45 (CD40 agonist). Tumor progression was monitored and immune responses in TME and lymphoid organs were analyzed using multicolor flow cytometry and NanoString analyzes.ResultsMesothelioma-lysate loaded DCs generated cross-reactive tumor-antigen-specific T-cell responses to pancreatic cancer and induced delayed tumor outgrowth when provided as prophylactic vaccine. In established disease, combination with stimulating CD40 antibody was necessary to improve survival, while anti-CD40 alone was ineffective. Extensive analysis of the TME showed that anti-CD40 monotherapy did improve CD8 +T cell infiltration, but these essential effector cells displayed hallmarks of exhaustion, including PD-1, TIM-3 and NKG2A. Combination therapy induced a strong change in tumor transcriptome and mitigated the expression of inhibitory markers on CD8 +T cells.ConclusionThese results demonstrate the potency of DC therapy in combination with CD40-stimulation for the treatment of pancreatic cancer and provide directions for near future clinical trials.

Published

2020

34. Preconditioning of the tumor microenvironment with oncolytic reovirus converts CD3-bispecific antibody treatment into effective immunotherapy

Author

Diana J. M. van den Wollenberg, Nadine van Montfoort, Thorbald van Hall, Priscilla Kinderman, Dana A M Mustafa, Ruben L van den Oever, Jim Middelburg, Christianne Groeneveldt, Sjoerd H. van der Burg, Rob C. Hoeben, Pathology, and Gastroenterology & Hepatology

Subjects

0301 basic medicine, Male, lymphocytes, Cancer Research, medicine.medical_treatment, Immunology, 03 medical and health sciences, Mice, 0302 clinical medicine, Cancer immunotherapy, interferon inducers, Interferon, Pancreatic cancer, Antibodies, Bispecific, medicine, Immunology and Allergy, Animals, Humans, tumor microenvironment, RC254-282, Pharmacology, Oncolytic Virotherapy, Tumor microenvironment, Interferon inducer, business.industry, FOXP3, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Immunotherapy, tumor-infiltrating, medicine.disease, Oncolytic virus, Oncolytic and Local Immunotherapy, 030104 developmental biology, Oncology, oncolytic viruses, 030220 oncology & carcinogenesis, Cancer research, Molecular Medicine, Female, immunotherapy, business, medicine.drug

Abstract

BackgroundT-cell-engaging CD3-bispecific antibodies (CD3-bsAbs) are promising modalities for cancer immunotherapy. Although this therapy has reached clinical practice for hematological malignancies, the absence of sufficient infiltrating T cells is a major barrier for efficacy in solid tumors. In this study, we exploited oncolytic reovirus as a strategy to enhance the efficacy of CD3-bsAbs in immune-silent solid tumors.MethodsThe mutant p53 and K-ras induced murine pancreatic cancer model KPC3 resembles human pancreatic ductal adenocarcinomas with a desmoplastic tumor microenvironment, low T-cell density and resistance to immunotherapy. Immune-competent KPC3 tumor-bearing mice were intratumorally injected with reovirus type 3 Dearing strain and the reovirus-induced changes in the tumor microenvironment and spleen were analyzed over time by NanoString analysis, quantitative RT-PCR and multicolor flow cytometry. The efficacy of reovirus in combination with systemically injected CD3-bsAbs was evaluated in immune-competent mice with established KPC3 or B16.F10 tumors, and in the close-to-patient human epidermal growth factor receptor 2 (HER2)+ breast cancer model BT474 engrafted in immunocompromised mice with human T cells as effector cells.ResultsReplication-competent reovirus induced an early interferon signature, followed by a strong influx of natural killer cells and CD8+ T cells, at the cost of FoxP3+ Tregs. Viral replication declined after 7 days and was associated with a systemic activation of lymphocytes and the emergence of intratumoral reovirus-specific CD8+ T cells. Although tumor-infiltrating T cells were mostly reovirus-specific and not tumor-specific, they served as non-exhausted effector cells for the subsequently systemically administered CD3-bsAbs. Combination treatment of reovirus and CD3-bsAbs led to the regression of large, established KPC3, B16.F10 and BT474 tumors. Reovirus as a preconditioning regimen performed significantly better than simultaneous or early administration of CD3-bsAbs. This combination treatment induced regressions of distant lesions that were not injected with reovirus, and systemic administration of both reovirus and CD3-bsAbs also led to tumor control. This suggests that this therapy might also be effective for metastatic disease.ConclusionsOncolytic reovirus administration represents an effective strategy to induce a local interferon response and strong T-cell influx, thereby sensitizing the tumor microenvironment for subsequent CD3-bsAb therapy. This combination therapy warrants further investigation in patients with non-inflamed solid tumors.

Published

2020

35. Lack of myeloid cell infiltration as an acquired resistance strategy to immunotherapy

Author

Jan Willem Kleinovink, Jan Oosting, Elham Beyranvand Nejad, Suzanne van Duikeren, Aart G. Jochemsen, Thorbald van Hall, Camilla Labrie, Eva Rademaker, Tetje C. van der Sluis, Ziena Abdulrahman, Sjoerd H. van der Burg, Ramon Arens, Marit J van Elsas, Amina F A S Teunisse, and Noel F C C de Miranda

Subjects

0301 basic medicine, Cancer Research, Myeloid, medicine.medical_treatment, Immunology, active, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, Immunology and Allergy, Medicine, Animals, Humans, tumor microenvironment, Myeloid Cells, RC254-282, Pharmacology, Tumor microenvironment, business.industry, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Basic Tumor Immunology, tumor escape, Immunotherapy, vaccination, Immune checkpoint, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Oncology, Tumor Escape, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, Molecular Medicine, Tumor necrosis factor alpha, immunotherapy, business, CD8

Abstract

BackgroundImmunotherapy of cancer is successful but tumor regression often is incomplete and followed by escape. Understanding the mechanisms underlying this acquired resistance will aid the development of more effective treatments.MethodsWe exploited a mouse model where tumor-specific therapeutic vaccination results in tumor regression, followed by local recurrence and resistance. In depth studies on systemic, local and tumor intrinsic changes were performed with flow and mass cytometry, immunohistochemistry, transcriptomics and several perturbation studies with inhibitors or agonistic antibodies in mice. Main findings were recapitulated in vaccinated patients.ResultsFull tumor regression and cure of tumor-bearing mice is dependent on the magnitude of the vaccine-induced T-cell response. Recurrence of tumors did not involve classical immune escape mechanisms, such as antigen-presentation alterations, immune checkpoint expression, resistance to killing or local immune suppression. However, the recurrent tumors displayed a changed transcriptome with alterations in p53, tumor necrosis factor-α and transforming growth factor-β signaling pathways and they became immunologically cold. Remarkably, ex vivo cell-sorted recurrent tumors, directly reinjected in naïve hosts retained their resistance to vaccination despite a strong infiltration with tumor-specific CD8+ T cells, similar to that of vaccine-responsive tumors. The influx of inflammatory mature myeloid effector cells in the resistant tumors, however, was impaired and this turned out to be the underlying mechanisms as restoration of inflammatory myeloid cell infiltration reinstated the sensitivity of these refractory tumors to vaccination. Notably, impaired myeloid cell infiltration after vaccination was also associated with vaccine resistance in patients.ConclusionAn immunotherapy-induced disability of tumor cells to attract innate myeloid effector cells formed a major mechanism underlying immune escape and acquired resistance. These data not only stresses the importance of myeloid effector cells during immunotherapy but also demands for new studies to harness their tumoricidal activities.

Published

2020

36. Targeting of the Cancer-Associated Fibroblast-T-Cell Axis in Solid Malignancies

Author

Els M. E. Verdegaal, James C. H. Hardwick, Tom J. Harryvan, Lukas J. A. C. Hawinkels, and Sjoerd H. van der Burg

Subjects

0301 basic medicine, T cell, cancer-associated fibroblast, lcsh:Medicine, Review, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, Stroma, medicine, Cytotoxic T cell, tumor immunology, Tumor microenvironment, business.industry, lcsh:R, Cancer, General Medicine, medicine.disease, T-cell based immunotherapy, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, business

Abstract

The introduction of a wide range of immunotherapies in clinical practice has revolutionized the treatment of cancer in the last decade. The majority of these therapeutic modalities are centered on reinvigorating a tumor-reactive cytotoxic T-cell response. While impressive clinical successes are obtained, the majority of cancer patients still fail to show a clinical response, despite the fact that their tumors express antigens that can be recognized by the immune system. This is due to a series of other cellular actors, present in or attracted towards the tumor microenvironment, including regulatory T-cells, myeloid-derived suppressor cells and cancer-associated fibroblasts (CAFs). As the main cellular constituent of the tumor-associated stroma, CAFs form a heterogeneous group of cells which can drive cancer cell invasion but can also impair the migration and activation of T-cells through direct and indirect mechanisms. This singles CAFs out as an important next target for further optimization of T-cell based immunotherapies. Here, we review the recent literature on the role of CAFs in orchestrating T-cell activation and migration within the tumor microenvironment and discuss potential avenues for targeting the interactions between fibroblasts and T-cells.

Published

2019

37. Long-term HPV-specific immune response after one versus two and three doses of bivalent HPV vaccination in Dutch girls

Author

Fiona R. M. van der Klis, Hester E. de Melker, Anne-Marie Buisman, Marjan J.M. Bogaard, Marij J. P. Welters, Hella Pasmans, Tessa M Schurink-van 't Klooster, Sjoerd H. van der Burg, and Debbie M. van Rooijen

Subjects

medicine.medical_treatment, T-Lymphocytes, Antibody Affinity, Antibodies, Viral, 0302 clinical medicine, Medicine, 030212 general & internal medicine, Netherlands, B-Lymphocytes, Human papillomavirus 16, Vaccines, biology, Human papillomavirus 18, Vaccination, Hpv vaccination, Acquired immune system, Infectious Diseases, Cytokine, Molecular Medicine, Cytokines, Female, Antibody, HPV, Adolescent, 030231 tropical medicine, Immunology, B-cells, Bivalent (genetics), Antibodies, 03 medical and health sciences, Young Adult, Immune system, Humans, Avidity, Papillomavirus Vaccines, Immunization Schedule, General Veterinary, General Immunology and Microbiology, business.industry, T-cells, Papillomavirus Infections, Public Health, Environmental and Occupational Health, Antibodies, Neutralizing, Immunoglobulin A, Immunoglobulin G, biology.protein, business, Immunologic Memory

Abstract

Background In view of further reduction of HPV vaccination schedules, gaining more insight into humoral and cellular immune responses after a single HPV vaccine is of great interest. Therefore, these responses were evaluated after different doses of the bivalent (2v) HPV-vaccine in girls. Methods Blood was collected yearly up to seven years post-vaccination with one-, two- or three-doses of the 2vHPV vaccine (N = 890). HPV-type-specific IgG and IgA-antibody levels, IgG-isotypes and avidity indexes were measured by a virus-like-particle-based multiplex-immuno-assay for two vaccine and five non-vaccine HPV types. HPV-type-specific memory B-cell numbers- and T-cell cytokine responses were determined in a subpopulation. Results HPV-type-specific antibody concentrations were significantly lower in one- than in two- and three-dose vaccinated girls but remained stable over seven years. The lower antibody response coincided with reduced HPV-type-specific B- and T-cell responses. There were no differences in both the IgG subtypes and the avidity of the HPV16-specific antibodies between the groups. Conclusions One-dose of the 2vHPV vaccine is immunogenic, but results in less B- and T-cell memory and considerable lower antibody responses when compared with more doses. Therefore, at least of some of girls receiving the one-dose of the vaccination might be at higher risk for waning immunity to HPV in the long-term.

Published

2019

38. Monalizumab: inhibiting the novel immune checkpoint NKG2A

Author

Thorbald van Hall, Dan Fu Ruan, Robert Zerbib, Pascale Andre, Amir Horowitz, Eric Vivier, Sjoerd H. van der Burg, Emilie Narni-Mancinelli, Linda Borst, Innate Pharma, Departments of Chemistry and of Structural Biology, Stanford University, Centre d'Immunologie de Marseille - Luminy (CIML), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), and ANR-17-RHUS-0007,PIONEER,Precision Immuno-Oncology for advanced Non small cell lung cancer patients with PD-1 ICI Resistance(2017)

Subjects

0301 basic medicine, Cancer Research, HLA-E, medicine.medical_treatment, Cancer immunotherapy, Review, NK cells, NKG2A, Mice, 0302 clinical medicine, Antineoplastic Agents, Immunological, Neoplasms, Immunology and Allergy, Cytotoxic T cell, biology, HLA-E/Qa-1, Qa-1, Inhibitory immune receptor, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 3. Good health, Killer Cells, Natural, Oncology, 030220 oncology & carcinogenesis, Molecular Medicine, [SDV.IMM]Life Sciences [q-bio]/Immunology, Antibody, NK Cell Lectin-Like Receptor Subfamily C, Immunology, CD8 T cells, Antibodies, Monoclonal, Humanized, lcsh:RC254-282, 03 medical and health sciences, Immune system, Blocking antibody, medicine, Animals, Humans, Pharmacology, business.industry, Histocompatibility Antigens Class I, Cancer, medicine.disease, Immune checkpoint, Disease Models, Animal, 030104 developmental biology, Cancer research, biology.protein, Monalizumab, business, T-Lymphocytes, Cytotoxic

Abstract

The implementation of immune checkpoint inhibitors to the oncology clinic signified a new era in cancer treatment. After the first indication of melanoma, an increasing list of additional cancer types are now treated with immune system targeting antibodies to PD-1, PD-L1 and CTLA-4, alleviating inhibition signals on T cells. Recently, we published proof-of-concept results on a novel checkpoint inhibitor, NKG2A. This receptor is expressed on cytotoxic lymphocytes, including NK cells and subsets of activated CD8+ T cells. Blocking antibodies to NKG2A unleashed the reactivity of these effector cells resulting in tumor control in multiple mouse models and an early clinical trial. Monalizumab is inhibiting this checkpoint in human beings and future clinical trials will have to reveal its potency in combination with other cancer treatment options.

Published

2019

39. High numbers of activated helper T cells are associated with better clinical outcome in early stage vulvar cancer, irrespective of HPV or p53 status

Author

Saskia J. A. M. Santegoets, Ilina Ehsan, Marij van der Tol, Helena C. van Doorn, Sjoerd H. van der Burg, Tjalling Bosse, Vanessa J. van Ham, Kim E. Kortekaas, Ziena Abdulrahman, Mariëtte I.E. van Poelgeest, and Obstetrics & Gynecology

Subjects

0301 basic medicine, Cancer Research, Vulvar Squamous Cell Carcinoma, medicine.medical_treatment, CD38, 0302 clinical medicine, PD-1, Immunology and Allergy, Papillomaviridae, Aged, 80 and over, Vulvar Neoplasms, Vulvar cancer, medicine.diagnostic_test, FOXP3, T-Lymphocytes, Helper-Inducer, Middle Aged, Prognosis, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Survival Rate, Tumor microenvironment, Oncology, 030220 oncology & carcinogenesis, Carcinoma, Squamous Cell, Molecular Medicine, Female, Immunotherapy, Research Article, Adult, Immunology, T cells, lcsh:RC254-282, Flow cytometry, 03 medical and health sciences, SDG 3 - Good Health and Well-being, Biomarkers, Tumor, medicine, Humans, Neoplasm Invasiveness, Aged, Pharmacology, business.industry, Papillomavirus Infections, medicine.disease, 030104 developmental biology, Case-Control Studies, Mutation, Cancer research, Tumor Suppressor Protein p53, business, Immunologic Memory, CD8, Follow-Up Studies

Abstract

Background Vulvar squamous cell carcinoma (VSCC) has been suggested to consist of three subtypes; HPV-positive, HPV-negative mutated TP53 or HPV-negative TP53 wildtype, with different clinical courses. To analyze the immune infiltrate in these molecular subtypes and its impact on clinical outcome, an in-depth study of the tumor immune microenvironment was performed. Methods Sixty-five patients with invasive VSCC matched for age, FIGO stage and treatment modality, were grouped according to the presence of HPV and p53 protein expression status. Archived tissues were analyzed for intraepithelial and stromal expression of CD3, CD8, Foxp3, PD-1, and pan-keratin in randomly selected areas using immunofluorescence. Additional phenotyping of T cells was performed ex-vivo on VSCC (n = 14) and blood samples by flow cytometry. Healthy vulvar samples and blood served as controls. Results Based on T-cell infiltration patterns about half of the VSCC were classified as inflamed or altered-excluded while one-third was immune-deserted. High intraepithelial helper T cell infiltration was observed in 78% of the HPV-induced VSCC, 60% of the HPVnegVSCC/p53wildtype and 40% of the HPVnegVSCC with abnormal p53 expression. A high intraepithelial infiltration with activated (CD3+PD-1+), specifically helper T cells (CD3+CD8−Foxp3−), was associated with a longer recurrence-free period and overall survival, irrespective of HPV and p53 status. Flow cytometry confirmed the tumor-specific presence of activated (CD4+PD-1++CD161−CD38+HLA-DR+ and CD8+CD103+CD161−NKG2A+/−PD1++CD38++HLA-DR+) effector memory T cells. Conclusion This is the first study demonstrating an association between intraepithelial T cells and clinical outcome in VSCC. Our data suggest that abnormal p53 expressing VSCCs mostly are cold tumors whereas HPV-driven VSCCs are strongly T-cell infiltrated. Electronic supplementary material The online version of this article (10.1186/s40425-019-0712-z) contains supplementary material, which is available to authorized users.

Published

2019

40. Tissue-Specific Gene Expression during Productive Human Papillomavirus 16 Infection of Cervical, Foreskin, and Tonsil Epithelium

Author

Sreejata Chatterjee, Anna C. Salzberg, Janice Milici, Willard M. Freeman, Samina Alam, Sjoerd H. van der Burg, Sa Do Kang, and Craig Meyers

Subjects

Keratinocytes, Male, HPV16, Foreskin, Palatine Tonsil, Immunology, Cellular Response to Infection, Cervix Uteri, Biology, Virus Replication, medicine.disease_cause, Microbiology, tissue specific, immune response, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Cell Line, Tumor, Virology, medicine, Humans, Gene Regulatory Networks, human papillomavirus, 030304 developmental biology, Human papillomavirus 16, 0303 health sciences, Innate immune system, Gene Expression Profiling, Papillomavirus Infections, Tissue-Specific Gene Expression, Cell Differentiation, Microarray Analysis, Epithelium, epithelial differentiation, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Organ Specificity, 030220 oncology & carcinogenesis, Insect Science, Tonsil, Cancer research, gene expression, Female, Carcinogenesis, Signal Transduction, Extracellular matrix organization

Abstract

Epidemiological data confirm a much higher incidence of high-risk human papillomavirus 16 (HPV16)-mediated carcinogenesis of the cervical epithelium than for other target sites. In order to elucidate tissue-specific responses to virus infection, we compared gene expression changes induced by productive HPV16 infection of cervical, foreskin, and tonsil organotypic rafts. These rafts closely mimic persistent HPV16 infection, long before carcinogenesis sets in. The total number of gene expression changes varied considerably across the tissue types, with only 32 genes being regulated in common. Among them, we confirmed the Kelch-like family protein KLHL35 and the laminin-5 complex to be upregulated and downregulated, respectively, in all the three tissues. HPV16 infection induces upregulation of genes involved in cell cycle control, cell division, mitosis, DNA replication, and DNA damage repair in all the three tissues, indicative of a hyperproliferative environment. In the cervical and tonsil epithelium, we observe significant downregulation of genes involved in epidermis development, keratinocyte differentiation, and extracellular matrix organization. On the other hand, in HPV16-positive foreskin (HPV16 foreskin) tissue, several genes involved in interferon-mediated innate immunity, cytokine signaling, and cellular defenses were downregulated. Furthermore, pathway analysis and experimental validations identified important cellular pathways like STAT1 and transforming growth factor beta (TGF-beta) to be differentially regulated among the three tissue types. The differential modulation of important cellular pathways like TGF-beta 1 and STAT1 can explain the sensitivity of tissues to HPV cancer progression.IMPORTANCE Although the high-risk human papillomavirus 16 infects anogenital and oropharyngeal sites, the cervical epithelium has a unique vulnerability to progression of cancer. Host responses during persistent infection and preneoplastic stages can shape the outcome of cancer progression in a tissue-dependent manner. Our study for the first time reports differential regulation of critical cellular functions and signaling pathways during productive HPV16 infection of cervical, foreskin, and tonsil tissues. While the virus induces hyperproliferation in infected cells, it downregulates epithelial differentiation, epidermal development, and innate immune responses, according to the tissue type. Modulation of these biological functions can determine virus fitness and pathogenesis and illuminate key cellular mechanisms that the virus employs to establish persistence and finally initiate disease progression.

Published

2019

41. Loss of BAP1 Is Associated with Upregulation of the NFkB Pathway and Increased HLA Class I Expression in Uveal Melanoma

Author

Martine J. Jager, Wilma G. M. Kroes, Christiaan van Weeghel, Pieter A. van der Velden, Zahra Souri, Sjoerd H. van der Burg, Gregorius P M Luyten, Aart G. Jochemsen, and Annemijn P A Wierenga

Subjects

0301 basic medicine, HLA Class I, Cancer Research, Inflammation, Human leukocyte antigen, Biology, lcsh:RC254-282, Article, NFkB pathway, 03 medical and health sciences, 0302 clinical medicine, Immune system, Downregulation and upregulation, medicine, BAP1, RELB, Melanoma, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, NFKB1, Phenotype, 030104 developmental biology, inflammation, 030220 oncology & carcinogenesis, oncology, Cancer research, medicine.symptom, uveal melanoma

Abstract

One of the characteristics of prognostically infaust uveal melanoma (UM) is an inflammatory phenotype, which is characterized by high numbers of infiltrating T cells and macrophages, and a high HLA Class I expression. We wondered how this inflammation is regulated, and considered that one of the most important regulators of inflammation, the NFkB pathway, might play a role. We analyzed 64 UM samples for expression of HLA Class I, its regulators, and of members of the NFkB transcription family, using an Illumina HT12V4 array. HLA Class I expression and infiltrating immune cells were also determined by immunohistochemical staining. Information was obtained regarding chromosome status by Affymetrix Nsp array. Our analysis shows that expression of NFkB1, NFkB2 and RELB positively correlates with the level of HLA Class I expression and the number of infiltrating T cells and macrophages, while SPP1 and PPAR&gamma, are negatively correlated. Increased levels of NFkB1 and NFkB2 and decreased levels of SPP1 and PPAR&gamma, are seen in Monosomy 3/BAP1-negative tumors. This is also the case in non-inflammatory UM, indicating that our observation not only involves infiltrating leukocytes but the tumor cells themselves. We report that the NFkB pathway is associated with inflammation and HLA Class I expression in UM, and is upregulated when BAP1 expression is lost.

Published

2019

42. TEIPP peptides: exploration of unTAPped cancer antigens

Author

Koen A. Marijt, Sjoerd H. van der Burg, and Thorbald van Hall

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, medicine.medical_treatment, cancer antigens, Immunology, Peptide, Human leukocyte antigen, Biology, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, medicine, Immunology and Allergy, hla class i, Antigenic peptide, Author’s View, t cells, chemistry.chemical_classification, Cancer, Immunotherapy, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 030104 developmental biology, Oncology, chemistry, Biochemistry, 030220 oncology & carcinogenesis, immunotherapy, lcsh:RC581-607, Intracellular

Abstract

The intracellular peptide pump TAP feeds antigenic peptides for loading onto HLA class I molecules, and its down-modulation is a frequent immune evasion mechanism in human cancers. Two recent papers describe which ‘hidden‘ antigens we might exploit to target these escaped cancer variants by CD8 T cells. These unTAPped peptides are now ready for clinical testing.

Published

2019

43. Tumor-derived GDF-15 to suppress t-lymphocyte recruitment to the tumor microenvironment resulting in resistance to ANTI-PD-1 treatment

Author

J Wischhusen, Mitchell P. Levesque, Falk Nimmerjahn, Sjoerd H. van der Burg, Kilian Wistuba-Hamprecht, Benjamin Weide, Reinhard Dummer, Marij J. P. Welters, Christine Schuberth-Wagner, Manfred Ruediger, Patrick N. Harter, Michel Mittelbronn, Sabrina Genßler, Alexander Martens, Neha Vashist, Markus Haake, and Eugen Leo

Subjects

Cancer Research, Tumor microenvironment, business.industry, Anti pd 1, Healthy tissue, SUPERFAMILY, T lymphocyte, Tumor-Derived, Oncology, embryonic structures, Cancer research, Medicine, business, Transforming growth factor

Abstract

e14532 Background: Growth and differentiation factor 15 (GDF-15) is a divergent member of the TGF-β superfamily with low to absent expression in healthy tissue. GDF-15 has been linked to feto-maternal immune tolerance, to prevention of excessive immune cell infiltration during tissue damage, and to anorexia. Various major tumor types secrete high levels of GDF-15. In cancer patients, elevated GDF-15 serum levels correlate with poor prognosis and reduced overall survival (OS). Methods: Impact of a proprietary GDF-15 neutralizing antibody (CTL-002) regarding T cell trafficking was analyzed by whole blood adhesion assays, a HV18-MK melanoma-bearing humanized mouse model and a GDF-15-transgenic MC38 model. Additionally, patient GDF-15 serum levels were correlated with clinical response and overall survival in oropharyngeal squamous cell carcinoma (OPSCC) and melanoma brain metastases. Results: In whole blood cell adhesion assays GDF-15 impairs adhesion of T and NK cells to activated endothelial cells. Neutralization of GDF-15 by CTL-002 rescued T cell adhesion. In HV18-MK-bearing humanized mice CTL-002 induced a strong increase in TIL numbers. Subset analysis revealed an overproportional enrichment of T cells, in particular CD8+ T cells. As immune cell exclusion is detrimental for checkpoint inhibitor (CPI) therapy, a GDF-15-transgenic MC38 model was tested for anti-PD-1 therapy efficacy. In GDF-15 overexpressing MC38 tumors response to anti PD-1 therapy was reduced by 90% compared to wtMC38 tumors. Combining aPD-1 with CTL-002 resulted in 50% of the mice rejecting their GDF-15 overexpressing tumors. Clinically, inverse correlations of GDF-15 levels with CD8+ T cell infiltration were shown for HPV+ OPSCC and for melanoma brain metastases. GDF-15 serum levels were significantly higher in HPV- than in HPV+ OPSCC patient (p < 0.0001). Low GDF-15 levels corresponded to longer OS in both HPV- and HPV+ OPSCC. In two independent melanoma patient cohorts treated with nivolumab or pembrolizumab low baseline serum GDF-15 levels were predictive for clinical response to anti-PD1 treatment and superior OS. Bivariate analysis including LDH indicates that GDF-15 independently predicts poor survival in aPD-1 treated melanoma patients. Conclusions: Taken together our in vitro and in vivo data show that elevated GDF-15 levels block T-cell infiltration into tumor tissues. Neutralizing GDF-15 with CTL-002 restores the ability of T cells to extravasate blood vessels and enter tumor tissue both in vitro and in vivo. In melanoma, patients with higher GDF-15 levels have significantly shorter survival and are less likely to respond to anti-PD1 therapy. GDF-15 may thus serve as a new predictive biomarker for anti-PD1 response, but most importantly also represents a novel target for cancer immunotherapy to improve tumor immune cell infiltration and response to anti-PD1 therapy.

Published

2021

44. Phase I trial to determine safety and immunogenicity of amplivant, a synthetic toll-like receptor 2 ligand, conjugated to two HPV16 E6 synthetic long peptides

Author

Hans Gelderblom, Gijs G. Zom, Sjoerd H. van der Burg, Peggy J. de Vos van Steenwijk, Willem-Jan Krebber, Ferry Ossendorp, Nikki M. Loof, Inge Roozen, Sanne Boekestijn, Cornelis J M Melief, Dmitri V. Filippov, Frank M. Speetjens, Marij J. P. Welters, Marije Slingerland, and Rob Valentijn

Subjects

Cancer Research, Toll-like receptor, business.industry, Immunogenicity, medicine.medical_treatment, Cancer, Immunotherapy, Human leukocyte antigen, Conjugated system, Ligand (biochemistry), medicine.disease, Hpv16 e6, Oncology, Cancer research, Medicine, business

Abstract

Background: Therapeutic vaccines based on synthetic long peptides (SLPs) have a great potential for immunotherapy of cancer patients as these SLPs include both human leukocyte antigen (HLA) class I and II epitopes and no patient selection for HLA types is required. The antigen-induced immune response can be strengthened with immune stimulating additives. Amplivant (AV) is a synthetic Toll-like receptor 2 ligand which can be directly conjugated to tumor peptide antigens. In preclinical studies, AV-conjugation to antigens led to both enhanced antigen presentation by dendritic cells and T-cell priming and caused superior induction of effective anti-tumor responses. Moreover, AV-conjugated SLPs showed a 100 times higher immune response compared to unconjugated SLP. The current study is a first-in-human trial to investigate safety and immunogenicity of AV-conjugated human papillomavirus (HPV)16-SLPs. Methods: A dose escalation phase I trial was performed in 24 patients with HPV16 positive (pre-) malignant lesions. AV was conjugated to two SLPs derived from the most immunodominant regions of the HPV16 E6 oncoprotein. Four dose groups (1, 5, 20 or 50 μg of each peptide) in 6 patients each were studied. The vaccine was injected three times intradermally in DMSO / water with a three-week interval. Adverse events (AE) were collected according to CTCAE v4.0 up to 26 weeks. Peptide-specific T-cell immune responses were determined in blood samples taken before and after vaccination using complementary immunological assays (proliferation assay, IFNγ-ELISPOT and cytokine bead array). Results: Toxicity after three AV-conjugated HPV16-SLP vaccinations was limited to CTCAE grade 1 or 2, with predominantly inflammation at the vaccination site and sometimes flu-like symptoms, which generally resolved within one day. Dose increase resulted from no AE in the lowest dose group to mild/moderate AE in all vaccinated persons in the highest dose group. In the lowest dose group, minor vaccine-induced T-cell responses were observed in three of six vaccinated persons. In the highest dose group, all patients displayed a strong HPV16-specific T-cell response after vaccination. The induced T-cell response against HPV16 lasted until the end of the trial. Conclusions: This first-in-human study showed that AV conjugated to SLPs can safely be used as an intradermal therapeutic vaccine. AV-conjugated HPV16-SLP was able to induce robust HPV16-specific T-cell immunity in patients treated for HPV16 positive (pre-) malignancies without any other vaccine adjuvant or formulation. Increase in dose resulted in both a higher number of mild adverse events as well as stronger T-cell immunity. Clinical trial information: NCT02821494.

Published

2021

45. Potential use of lymph node-derived HPV-specific T cells for adoptive cell therapy of cervical cancer

Author

Els M. E. Verdegaal, Moniek Heusinkveld, A. Rob P. M. Valentijn, Caroline E. van der Minne, Vanessa J. van Ham, Maarten L. Zandvliet, Zohara Aghai, Mariette I.E. van Poelgeest, J. Baptist Trimbos, Marij J. P. Welters, Valeria Visconti, Sjoerd H. van der Burg, and Renske Goedemans

Subjects

Adult, Human papillomavirus, Cancer Research, Adoptive cell transfer, T-Lymphocytes, medicine.medical_treatment, T cell, Immunology, Uterine Cervical Neoplasms, Immunotherapy, Adoptive, HPV-specific T cells, Cell therapy, 03 medical and health sciences, 0302 clinical medicine, Tumor-draining lymph node, medicine, Humans, Immunology and Allergy, IL-2 receptor, Lymph node, Aged, business.industry, Cancer, Middle Aged, medicine.disease, Cytokine, medicine.anatomical_structure, Oncology, Good manufacturing practice, 030220 oncology & carcinogenesis, Cervical cancer, Original Article, Female, Lymph Nodes, business, CD8, 030215 immunology

Abstract

Adoptive transfer of tumor-specific T cells, expanded from tumor-infiltrating lymphocytes or from peripheral blood, is a promising immunotherapeutic approach for the treatment of cancer. Here, we studied whether the tumor-draining lymph nodes (TDLN) of patients with human papillomavirus (HPV)-induced cervical cancer can be used as a source for ACT. The objectives were to isolate lymph node mononuclear cells (LNMC) from TDLN and optimally expand HPV-specific CD4+ and CD8+ T cells under clinical grade conditions. TDLN were isolated from 11 patients with early-stage cervical cancer during radical surgery. Isolated lymphocytes were expanded in the presence of HPV16 E6 and E7 clinical grade synthetic long peptides and IL-2 for 22 days and then analyzed for HPV16 specificity by proliferation assay, multiparameter flow cytometry and cytokine analysis as well as for CD25 and FoxP3 expression. Stimulation of LNMC resulted in expansion of polyclonal HPV-specific T cells in all patients. On average a 36-fold expansion of a CD4+ and/or CD8+ HPV16-specific T cell population was observed, which maintained its capacity for secondary expansion. The T helper type 1 cytokine IFNγ was produced in all cell cultures and in some cases also the Th2 cytokines IL-10 and IL-5. The procedure was highly reproducible, as evidenced by complete repeats of the stimulation procedures under research and under full good manufacturing practice conditions. In conclusion, TDLN represent a rich source of polyclonal HPV16 E6- and E7-specific T cells, which can be expanded under clinical grade conditions for adoptive immunotherapy in patients with cervical cancer. Electronic supplementary material The online version of this article (doi:10.1007/s00262-016-1892-8) contains supplementary material, which is available to authorized users.

Published

2016

46. Vaccination against Oncoproteins of HPV16 for Noninvasive Vulvar/Vaginal Lesions: Lesion Clearance Is Related to the Strength of the T-Cell Response

Author

J Hanneke N G Oude Elberink, Marij J. P. Welters, Marjolein J. Kagie, Nikki M. Loof, Theo Stijnen, Linda F. M. Stynenbosch, Bart W. J. Hellebrekers, Marc van Beurden, Margriet J. G. Löwik, A. Rob P. M. Valentijn, Ineke E. Hamming, Sjoerd H. van der Burg, Tjalling Bosse, Henk W.R. Schreuder, Dorien M A Berends-van der Meer, Hans W. Nijman, Mariëtte I.E. van Poelgeest, Edith M G van Esch, Renee Vermeij, Gert Jan Fleuren, Toos Daemen, J. Baptist Trimbos, Cornelis J. M. Melief, Harry Hollema, Lorraine M. Fathers, Gemma G. Kenter, Jaap Oostendorp, CCA -Cancer Center Amsterdam, Obstetrics and Gynaecology, Microbes in Health and Disease (MHD), Targeted Gynaecologic Oncology (TARGON), Groningen Research Institute for Asthma and COPD (GRIAC), Translational Immunology Groningen (TRIGR), Obstetrics and gynaecology, CCA - Cancer immunology, and AII - Cancer immunology

Subjects

0301 basic medicine, Cancer Research, Papillomavirus E7 Proteins, medicine.medical_treatment, viruses, Uterine Cervical Neoplasms, Imiquimod, CD8-Positive T-Lymphocytes, Gastroenterology, law.invention, 0302 clinical medicine, Randomized controlled trial, law, IMMUNE-RESPONSE, FAILURE, CERVICAL-CANCER PATIENTS, VULVAR INTRAEPITHELIAL NEOPLASIA, E6, Human papillomavirus 16, Vulvar Neoplasms, integumentary system, Vaccination, virus diseases, Middle Aged, PHASE-1 TRIAL, female genital diseases and pregnancy complications, Oncology, 030220 oncology & carcinogenesis, Aminoquinolines, SURVIVAL, Female, medicine.symptom, Carcinoma in Situ, medicine.drug, Adult, medicine.medical_specialty, Vaginal Neoplasms, Cancer Vaccines, Lesion, Interferon-gamma, Young Adult, 03 medical and health sciences, Internal medicine, medicine, Journal Article, Humans, Papillomavirus Vaccines, IMMUNOTHERAPY, neoplasms, Aged, Vaginal intraepithelial neoplasia, business.industry, Papillomavirus Infections, Cancer, Oncogene Proteins, Viral, Immunotherapy, medicine.disease, Vulvar intraepithelial neoplasia, 030104 developmental biology, Immunology, IMIQUIMOD, business, PEPTIDE VACCINATION

Abstract

Purpose: Therapeutic vaccination with human papillomavirus type 16 (HPV16) E6 and E7 synthetic long peptides (SLP) is effective against HPV16-induced high-grade vulvar and vaginal intraepithelial neoplasia (VIN/VaIN). However, clinical nonresponders displayed weak CD8+ T-cell reactivity. Here, we studied if imiquimod applied at the vaccine site could improve CD8+ T-cell reactivity, clinical efficacy, and safety of HPV16-SLP (ISA101). Experimental Design: A multicenter open-label, randomized controlled trial was conducted in patients with HPV16+ high-grade VIN/VaIN. Patients received ISA101 vaccination with or without application of 5% imiquimod at the vaccine site. The primary objective was the induction of a directly ex vivo detectable HPV16-specific CD8+ T-cell response. The secondary objectives were clinical responses (lesion size, histology, and virology) and their relation with the strength of vaccination-induced immune responses. Results: Forty-three patients were assigned to either ISA101 with imiquimod (n = 21) or ISA101 only (n = 22). Imiquimod did not improve the outcomes of vaccination. However, vaccine-induced clinical responses were observed in 18 of 34 (53%; 95% CI, 35.1–70.2) patients at 3 months and in 15 of 29 (52%; 95% CI, 32.5–70.6) patients, 8 of whom displayed a complete histologic response, at 12 months after the last vaccination. All patients displayed vaccine-induced T-cell responses, which were significantly stronger in patients with complete responses. Importantly, viral clearance occurred in all but one of the patients with complete histologic clearance. Conclusions: This new study confirms that clinical efficacy of ISA101 vaccination is related to the strength of vaccine-induced HPV16-specific T-cell immunity and is an effective therapy for HPV16-induced high-grade VIN/VaIN. Clin Cancer Res; 22(10); 2342–50. ©2016 AACR. See related commentary by Karaki et al., p. 2317

Published

2016

47. Abstract 1582: A pre-existing inflammatory immune microenvironment predicts the clinical and immunological response of vulvar high-grade squamous intraepithelial lesions to therapeutic HPV16 peptide vaccination

Author

Sjoerd H. van der Burg, Mariette I.E. van Poelgeest, Noel F C C de Miranda, and Ziena Abdulrahman

Subjects

Vaccination, chemistry.chemical_classification, Cancer Research, Oncology, chemistry, business.industry, Immune microenvironment, Immunology, Medicine, Peptide, business, High-Grade Squamous Intraepithelial Lesions

Abstract

Background: Vulvar High-grade Squamous Intraepithelial Lesion (vHSIL) is predominantly induced by high-risk Human Papilloma Virus type 16 (HPV16). In two independent trials, therapeutic vaccination against the oncoproteins of HPV16 with synthetic long peptides (SLP) resulted in vHSIL regression in about half of the patients after 12 months. Several studies have shown that the immune microenvironment influences therapy outcome. Therefore, a thorough investigation of the vHSIL immune microenvironment before and after SLP vaccination was performed, and its impact on clinical response was studied. Methods: Two novel multiplex immunofluorescence panels were designed and fully optimized for formalin-fixed paraffin-embedded tissue, one for T cells (CD3, CD8, Foxp3, Tim3, Tbet, PD-1, DAPI) and one for myeloid cells (CD14, CD33, CD68, CD163, CD11c, PD-L1, DAPI). Pre- and post-vaccination biopsies of 29 vHSIL patients, as well as 27 healthy vulva excisions, were stained, scanned with the Vectra multispectral imaging system, and automatically phenotyped and counted with inForm advanced image analysis software. Results: A pre-existing pro-inflammatory tumor microenvironment, marked by high numbers of CD4+ and CD8+ T cells expressing Tbet and/or PD-1 as well as CD14+ inflammatory macrophages, is a strong predictor for good clinical response to therapeutic HPV16 SLP vaccination. A clear stepwise increase in pre-vaccination infiltrating Tbet+, CD4+, CD8+ T cells and CD14+ macrophages, and decrease in Foxp3+ regulatory T cells was observed as response increased from non to partial to complete response. Moreover, the pre-vaccination immune microenvironment of complete responders resembled healthy vulva. Vaccination further increased infiltrating CD4+ and Tbet+ T cells and CD14+ macrophages, and decreased Foxp3+ regulatory T cells and CD68+CD163+ M2 macrophages in the complete and partial responders, but not in the non responders. Conclusion: Clinical responsiveness to therapeutic HPV16 SLP vaccination requires a pre-existing inflamed type 1 immune contexture in vHSIL. Hence, only patients with an inflamed microenvironment should be selected for monotherapy by therapeutic peptide vaccination, since this strategy is incapable of overcoming an immunologically cold tumor microenvironment. Citation Format: Ziena Abdulrahman, Noel F. de Miranda, Mariette I. van Poelgeest, Sjoerd H. van der Burg. A pre-existing inflammatory immune microenvironment predicts the clinical and immunological response of vulvar high-grade squamous intraepithelial lesions to therapeutic HPV16 peptide vaccination [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 1582.

Published

2020

48. Abstract 532: A patient-derived anti-CD9 antibody induces tumor rejection and synergistically enhances anti-PD1 activity

Author

Els M. E. Verdegaal, Piet Gros, Susan van Hal, Hans van Eenennaam, Hergen Spits, Julien Villaudy, Yvonne Claasen, Christien Fatmawati, Pauline M. van Helden, Viviana Neviani, Koen Wagner, Etsuko Yasuda, Martijn Kedde, Wouter Pos, Sjoerd H. van der Burg, Remko Schotte, and Daniel Go

Subjects

Cancer Research, Oncology, biology, business.industry, Tumor rejection, Cancer research, biology.protein, Medicine, Antibody, business, Anti pd1

Abstract

Background Adaptive immunity to cancer cells has been shown to form a crucial part of cancer immunotherapy. Recently, the importance of tumor B-cell signatures were shown to correlate with melanoma survival. We investigated whether anti-tumor antibodies could be isolated from a patient with metastatic melanoma that was tumor-free for 6 years following adoptive transfer of ex vivo expanded autologous T cells (Verdegaal 2011). Methods Peripheral blood memory B cells were immortalized using AIMM's immmortalisation technology (ectopic Bcl-6 and Bcl-xL; Kwakkenbos 2010) expression and analyzed for the presence of tumor-reactive B cells. Results AT1412 antibody was identified by virtue of its differential binding to melanoma cells as compared to healthy melanocytes. AT1412 was found to bind the tetraspanin CD9, a broadly expressed protein involved in multiple cellular activities and disease progression. The crystal structure of the CD9 large extracellular loop in complex with an AT1412 Fab fragment revealed that AT1412 binds the CD9 epitope in an extended and unfolded conformation. In addition to melanoma, AT1412 binds other tumor types including gastric, colon- and pancreatic cancer. AT1412 was shown to induce antibody dependent cellular cytotoxicity (ADCC) and antibody dependent cellular phagocytosis (ADCP) of cancer cells. In addition, AT1412 demonstrated activation of monocytes, most likely via activation of CD9 on platelets-bound monocytes. In mice carrying a human immune system (HIS-mice; van Lent 2010) AT1412 strongly enhanced tumor rejection of A375 and SKMEL-5 tumor cells. AT1412 treatment was shown to enhance tumor infiltration of CD8 T cells and macrophages. AT1412 efficacy was further synergistically enhanced when combined with an anti-PD1 antibody (nivolumab). Other groups have shown that anti-CD9 antibodies can induce tumor rejection in mice. However, these antibodies could not be advanced due to induction of platelet aggregation. We show that AT1412 does not induce aggregation of both human and cynomolgus platelets. Also affinity matured versions of AT1412 do not induce platelet aggregation, supporting that AT1412 binds a unique epitope on CD9. In addition, we studied the safety of AT1412 during a one month exposure in a weekly administration in cynomolgus monkeys. Besides a transient thrombocytopenia AT1412 was well tolerated up to 10 mg/kg antibody (highest dose tested) and did not lead to other adverse events nor were any coagulation factors affected Conclusions Taken together, applying AIMM's proprietary B-cell immortalization technology we isolated antibody AT1412 that targets a unique epitope on CD9. AT1412 was shown to induce tumor rejection as a single agent and enhances the activity of anti-PD-1 antibodies, while not inducing platelet aggregation. One month exposure of AT1412 in monkeys indicated that AT1412 can be safely administered. Preclinical development of AT1412 is ongoing to initiate clinical evaluation in 2020. Funding Dutch Cancer Society, grant UVA 2010-4822 Citation Format: Remko Schotte, Julien Villaudy, Martijn Kedde, Wouter Pos, Koen Wagner, Viviana Neviani, Daniel Go, Etsuko Yasuda, Christien Fatmawati, Els Verdegaal, Susan van Hal, Yvonne Claasen, Hans van Eenennaam, Pauline van Helden, Piet Gros, Sjoerd van der Burg, Hergen Spits. A patient-derived anti-CD9 antibody induces tumor rejection and synergistically enhances anti-PD1 activity [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 532.

Published

2020

49. Abstract 531: AT1412, a patient-derived antibody in development for the treatment of CD9-positive precursor B-acute lymphoblastic leukemia

Author

Mette D. Hazenberg, Hergen Spits, Anikó Szabó, Greta de Jong, Remko Schotte, Madalina Cercel, Hans van Eenennaam, Martijn Kedde, Etsuko Yasuda, Pauline M. van Helden, Els M. E. Verdegaal, Sjoerd H. van der Burg, Wouter Pos, Sophie E. Levie, Esmay Frankin, Julien Villaudy, Daniel Go, Susan van Hal, and Anita van Rijneveld

Subjects

Cancer Research, Oncology, biology, business.industry, Cancer research, biology.protein, Medicine, B Acute Lymphoblastic Leukemia, Antibody, business

Abstract

Introduction Despite rapid advances in immunotherapeutic options for precursor B-acute lymphoblastic leukemia (BCP-ALL), outcomes remain poor especially for adult ALL and relapsed pediatric ALL. With conventional chemotherapy remission percentages in adult ALL range from 75 to 90%, but relapse rates are high and long-term leukemia-free survival ranges between 35-70% depending on age and risk group. The introduction of CD19-targeting immunotherapy has significantly improved patient outcomes in (relapsed) BCP-ALL. However, tumor escape via downregulation of CD19 occurs in a significant number of patients. An ongoing medical need remains for the identification of alternative immunotherapeutic targets for treatment of ALL. Methods CD9 is expressed in 60-80% of BCP-ALL, is correlated with adverse prognosis and has been proposed as therapeutic target for BCP-ALL. AT1412 is a fully human CD9-targeting antibody, that was identified from a patient cured of metastatic melanoma after adoptive T-cell therapy, using our B-cell immortalization technology (AIMSelect) [Kwakkenbos et al. Nat. Med. 2010]. The antibody was selected based on differential binding to melanoma cells as compared to healthy melanocytes and was shown to be successful in killing melanoma cells in vitro and in vivo. Results Binding of AT1412 to BCP-ALL cell lines SUP-B15, MHH-CALL-2 and CCRF-SB varied as expected based on CD9 levels that we detected using a commercial CD9 antibody. AT1412-induced antibody dependent cellular cytotoxicity (ADCC) and antibody dependent cellular phagocytosis (ADCP) correlated with the level of AT1412 binding. No binding was seen to the T-ALL cell line Jurkat. These findings were confirmed in primary ALL samples, obtained prospectively at diagnosis from a cohort of patients with T- or B-ALL (n=38). AT1412 showed binding to the majority of B-ALL samples but not to T-ALL samples. AT1412 induced ADCC of nearly all B-ALL samples it bound to (10/11) and of none of the non-binding B-ALL or T-ALL samples. Cytotoxicity significantly correlated with the level of AT1412 binding. These findings were corroborated by the observation that AT1412 induced specific B-ALL cell death when a bone marrow sample from a newly diagnosed BCP-ALL patient was incubated with AT1412. Remarkably, AT1412 induced cell death in the absence of added effector cells or other (chemo)therapeutic agents, while the sample contained over 80% blasts and as little as 3% lymphocytes. We are currently investigating the in vivo efficacy of the antibody in a humanized immune system mouse model with human BCP-ALL. Conclusion Taken together, the majority of BCP-ALL express CD9 and this is associated with poor prognosis. Our data demonstrate that CD9 can be successfully targeted by the human CD9 antibody AT1412, suggesting that AT1412 has the potential to be developed as a therapeutic antibody for B-ALL. AT1412 is currently being advanced through preclinical development. Citation Format: Greta de Jong, Sophie E. Levie, Remko Schotte, Wouter Pos, Daniel Go, Etsuko Yasuda, Madalina Cercel, Susan E. van Hal, Esmay Frankin, Aniko Szabo, Martijn Kedde, Els Verdegaal, Julien Villaudy, Sjoerd van der Burg, Pauline M. van Helden, Hans van Eenennaam, Hergen Spits, Anita van Rijneveld, Mette D. Hazenberg. AT1412, a patient-derived antibody in development for the treatment of CD9-positive precursor B-acute lymphoblastic leukemia [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 531.

Published

2020

50. Abstract CT194: Low-dose Interferon-alpha pre-conditioning and adoptive cell therapy in metastatic melanoma patients refractory to standard (immune) therapies - a phase 1/2 study

Author

Linda de Bruin, Anton G. T. Terwisscha van Scheltinga, Sjoerd H. van der Burg, Els M. E. Verdegaal, Noel F C C de Miranda, Carolien E. van der Minne, Monique K van der Kooij, Marten Visser, Saskia J. A. M. Santegoets, Gerrit-Jan Liefers, Ellen Kapiteijn, Inge Roozen, Pauline Meij, and Marij J. P. Welters

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Disease Response, business.industry, medicine.medical_treatment, T cell, Cancer, Alpha interferon, Immunotherapy, medicine.disease, Cell therapy, medicine.anatomical_structure, Internal medicine, Medicine, Prior Immunotherapy, business, CD8

Abstract

Background: Adoptive cell therapy (ACT) with tumor-reactive T cells has shown consistent clinical efficacy. We evaluated the response to ACT in combination with interferon alpha (IFNa) preconditioning in stage IV metastatic melanoma patients, most of which were progressive on CTLA-4 and/or PD-1 checkpoint blockade therapy. Methods: Thirty-four patients were treated with ex vivo expanded tumor reactive T cells, derived from mixed-lymphocyte-autologous tumor cultures, or with autologous tumor-infiltrating lymphocytes and evaluated for clinical response. Clinical and immunological parameters associated with response were also evaluated. Results: Best overall response defined as clinical benefit, comprising either complete response, partial response or stable disease for more than 6 months, was observed in 29% of the patients. Six of the 14 (43%) immunotherapy naïve patients and 4 of the 20 (20%) patients progressive on prior immunotherapy benefited from ACT. The overall survival (OS) was 90% versus 28.6% at 1 year and 46.7% versus 0% at 3 years follow-up, of clinical responder and non-responder patients, respectively. Median OS was 36 versus 7 months, respectively. IFNa pre-treatment resulted in leuko-, neutro- and lymphopenia, which was sustained during the treatment in clinical responders and associated with response. Differences in antigen-specificity, but not in phenotype, cytokine profile, or CD8+ T cell number of the ACT products correlated with clinical response. Cross-reactivity of the ACT products to one or more allogeneic HLA-matched melanoma cell lines was associated with short OS after treatment while the ACT products of very long-term survivors showed solely recognition of patient-specific neo-antigens. Conclusion: This study demonstrates that ACT in combination with a mild IFNa preconditioning regimen can induce clinical benefit even in immunotherapy pre-treated patients, albeit with lower success than in immunotherapy naïve patients. ACT products comprising neo-antigen reactivity may be more effective. Future Perspectives: As a substantial percentage of the infused T cells expressed one or more inhibitory checkpoint molecules (CTLA-4, PD-1, or TIM-3), we started a new trial combining ACT and anti-PD-1 (ACTME trial; NCT03638375). The phase Ia of this trial was just completed with nine immunotherapy pre-treated patients showing that the combined treatment is feasible and safe. Updated and accumulated disease response data will be presented. Citation Format: Monique K. van der Kooij, Els M. Verdegaal, Marten Visser, Carolien E. van der Minne, Linda de Bruin, Pauline Meij, Anton G. Terwisscha van Scheltinga, Marij J. Welters, Saskia J. Santegoets, Noel F. de Miranda, Inge C. Roozen, Gerrit-Jan Liefers, Ellen Kapiteijn, Sjoerd H. van der Burg. Low-dose Interferon-alpha pre-conditioning and adoptive cell therapy in metastatic melanoma patients refractory to standard (immune) therapies - a phase 1/2 study [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr CT194.

Published

2020