Your search keyword '"IMMUNOTHERAPY"' showing total 35,057 results

1. Immune Cell Dynamics in EGFR-Mutated NSCLC Treated With Afatinib and Pembrolizumab: Results From a Phase IB Study.

Author

Riess, Jonathan, Lara, Matthew, Lopez de Rodas, Miguel, Luxardi, Guillaume, Herbert, Samantha, Shimoda, Michiko, Kelly, Karen, Meerlev, Alexander, Moore, Elizabeth, Beckett, Laurel, Monjazeb, Arta, Schalper, Kurt, Maverakis, Emanual, and Gandara, David

Subjects

Epidermal growth factor, Immunotherapy, Lung cancer, Targeted therapy

Abstract

INTRODUCTION: EGFR-mutated NSCLC is minimally responsive to programmed cell death protein 1 or programmed death-ligand 1 blockade. We evaluated the safety, tolerability, and immunomodulatory effects of the EGFR tyrosine kinase inhibitor (TKI) afatinib in combination with the programmed cell death protein 1 antibody pembrolizumab in patients with EGFR-mutant NSCLC. METHODS: Patients with advanced EGFR-mutant NSCLC with progression (PD) on previous EGFR TKI(s), aged above or equal to 18 years, Eastern Cooperative Oncology Group performance status less than or equal to 1, acceptable organ function, no significant autoimmune disease, measurable disease, and controlled brain metastases were eligible. Primary end point was determination of the maximum tolerated dose and recommended phase 2 dose. Serial specimens were collected to assess for alterations in cytokines and immune cell subsets by quantitative immunofluorescence in tissue and Luminex and flow cytometry in the blood. RESULTS: A total of 11 patients were enrolled, six in dose finding and five in dose expansion. No dose-limiting toxicities were observed. The maximum tolerated dose was determined to be afatinib 40 mg orally daily and pembrolizumab 200 mg intravenously every 21 days. Four (36%) patients had immune-related adverse events (irAEs). Ten patients were assessable for response: two partial response, seven stable disease, and one PD. Peripheral natural killer and natural killer T-cells (p = 0.027, p = 0.01) increased and exhausted CD8+ T-cells decreased on treatment (p = 0.0035). Peripheral CD4/CD8 T-cells (area under the curve = 0.96, p = 0.042) and central memory T-cells (CD4/CD8) (area under the curve = 1.0, p = 0.0006) increased in patients who had disease control more than 6 months or partial response to afatinib/pembrolizumab as did CD3+ T-cells in a patient with progression-free survival more than 6 months after afatinib/pembrolizumab treatment. CONCLUSIONS: Afatinib and pembrolizumab were found to have modest activity associated with irAEs after PD on previous EGFR TKI setting. Proinflammatory changes in immune cell subsets in tissue and blood were detected and associated with antitumor activity and irAEs.

Published

2024

2. Advanced endometrial cancer-The next generation of treatment: A society of gynecologic oncology journal club clinical commentary.

Author

Tillmanns, Todd, Masri, Amal, Stewart, Chelsea, Chase, Dana, Karnezis, Anthony, Chen, Lee-May, and Urban, Renata

Subjects

Clinical trials, Endometrial cancer, Immunotherapy, Individualized therapy, PARP inhibitor

Abstract

In February of 2024, the Society of Gynecologic Oncology (SGO) hosted a journal club focused on new treatment options for the management of advanced and metastatic endometrial cancer. This clinical commentary is intended to provide a summary report of that presentation. The session described the importance of molecular characterization shown in the work of The Cancer Genome Atlas (TCGA). The updated 2023 FIGO staging of endometrial cancer was reviewed. The panel then described the role of upfront immunotherapy for the treatment of advanced or recurrent endometrial cancer as demonstrated in four recent trials (RUBY, NRG-GY018, AtTEnd, and DUO-E studies). The DUO-E study uniquely examined the combination immunotherapy with a PARP inhibitor. The trials had unique differences in inclusion criteria, primary outcomes, and length of maintenance therapy, but all boasted similarly promising results particularly in mismatch repair deficient (dMMR) endometrial cancer. This era of rapid innovation in advanced and recurrent endometrial cancer will hopefully enhance individualized treatment approaches and improved outcomes for patients with endometrial cancer.

Published

2024

3. Immune checkpoint inhibitor-induced gastrointestinal injury: prevalence of cytomegalovirus, adenovirus and Epstein-Barr virus

Author

Chornenkyy, Yevgen, LaBoy, Carissa, De Hoyos, Sergei Xavier, Hu, Jingjing, and Pezhouh, Maryam

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Immunology, Autoimmune Disease, Cancer, Infectious Diseases, Clinical Research, Colo-Rectal Cancer, Immunotherapy, Digestive Diseases, 2.1 Biological and endogenous factors, 2.2 Factors relating to the physical environment, Infection, COLITIS, Cytomegalovirus, Gastrointestinal Diseases, Viruses, Epstein-Barr Virus Infections, Medical Microbiology, Pathology, Clinical sciences, Oncology and carcinogenesis

Abstract

AimsWidespread use of immune checkpoint inhibitors (ICIs) for treatment of advanced malignancies led to an increase in number of immune-related adverse events such as ICI gastrointestinal (GI) injury (ICIGI). The resulting immune dysregulation of the GI mucosa is believed to predispose patients to viral infections. We characterised the histopathological features of ICIGI and the frequency of viral infections such as cytomegalovirus (CMV), adenovirus, and Epstein-Barr virus (EBV).MethodsSingle-centre retrospective study (2011-2020).Results81 GI biopsies from 31 patients with ICIGI (65% male (20/31), 35% female (11/31)) with advanced malignancies were reviewed. Most patients received ipilimumab and nivolumab (14/31, 45%), followed by pembrolizumab (9/31, 29%), ipilimumab (4/31, 13%), nivolumab (2/31, 6%) and combination of all three medications (2/31, 6%). Average regimen prior to incidence of diarrhea was three cycles. Evidence of colitis or erythema by endoscopy was present in 77% of cases, while 23% showed normal endoscopy. Histologically, the predominant ICIGI findings were active inflammation (84%), including cryptitis (77%), crypt abscesses (65%), lymphocytic colitis-like (LCL) pattern (61%), increase in epithelial apoptosis (74%) and/or surface injury (81%). Only one case showed diffuse CMV positivity (3%) with characteristic CMV viral cytopathic effects present on H&E stain and four cases were positive for rare EBV (13%). Adenovirus infection was not identified.ConclusionWhile our cohort is small, ICIGI generally demonstrates active inflammation including cryptitis and crypt abscesses in the colon, LCL pattern, and an increase in epithelial apoptosis. Upfront immunohistochemistry for viral infection without high-degree of clinical and histologic suspicion is not recommended.

Published

2024

4. Total-Body Dynamic Imaging and Kinetic Modeling of [18F]F-AraG in Healthy Individuals and a Non-Small Cell Lung Cancer Patient Undergoing Anti-PD-1 Immunotherapy.

Author

Omidvari, Negar, Levi, Jelena, Abdelhafez, Yasser, Wang, Yiran, Nardo, Lorenzo, Daly, Megan, Wang, Guobao, and Cherry, Simon

Subjects

NSCLC, T cells, immunotherapy, kinetic modeling, total-body PET, Humans, Carcinoma, Non-Small-Cell Lung, Lung Neoplasms, Immunotherapy, Kinetics, Male, Programmed Cell Death 1 Receptor, Whole Body Imaging, Female, Models, Biological, Middle Aged, Adult, Aged, Immune Checkpoint Inhibitors

Abstract

Immunotherapies, especially checkpoint inhibitors such as anti-programmed cell death protein 1 (anti-PD-1) antibodies, have transformed cancer treatment by enhancing the immune systems capability to target and kill cancer cells. However, predicting immunotherapy response remains challenging. 18F-arabinosyl guanine ([18F]F-AraG) is a molecular imaging tracer targeting activated T cells, which may facilitate therapy response assessment by noninvasive quantification of immune cell activity within the tumor microenvironment and elsewhere in the body. The aim of this study was to obtain preliminary data on total-body pharmacokinetics of [18F]F-AraG as a potential quantitative biomarker for immune response evaluation. Methods: The study consisted of 90-min total-body dynamic scans of 4 healthy subjects and 1 non-small cell lung cancer patient who was scanned before and after anti-PD-1 immunotherapy. Compartmental modeling with Akaike information criterion model selection was used to analyze tracer kinetics in various organs. Additionally, 7 subregions of the primary lung tumor and 4 mediastinal lymph nodes were analyzed. Practical identifiability analysis was performed to assess the reliability of kinetic parameter estimation. Correlations of the SUVmean, the tissue-to-blood SUV ratio (SUVR), and the Logan plot slope (K Logan) with the total volume of distribution (V T) were calculated to identify potential surrogates for kinetic modeling. Results: Strong correlations were observed between K Logan and SUVR with V T, suggesting that they can be used as promising surrogates for V T, especially in organs with a low blood-volume fraction. Moreover, practical identifiability analysis suggested that dynamic [18F]F-AraG PET scans could potentially be shortened to 60 min, while maintaining quantification accuracy for all organs of interest. The study suggests that although [18F]F-AraG SUV images can provide insights on immune cell distribution, kinetic modeling or graphical analysis methods may be required for accurate quantification of immune response after therapy. Although SUVmean showed variable changes in different subregions of the tumor after therapy, the SUVR, K Logan, and V T showed consistent increasing trends in all analyzed subregions of the tumor with high practical identifiability. Conclusion: Our findings highlight the promise of [18F]F-AraG dynamic imaging as a noninvasive biomarker for quantifying the immune response to immunotherapy in cancer patients. Promising total-body kinetic modeling results also suggest potentially wider applications of the tracer in investigating the role of T cells in the immunopathogenesis of diseases.

Published

2024

5. Cemiplimab monotherapy in Japanese patients with recurrent or metastatic cervical cancer.

Author

Hasegawa, Kosei, Takahashi, Shunji, Ushijima, Kimio, Okadome, Masao, Yonemori, Kan, Yokota, Harushige, Vergote, Ignace, Monk, Bradley, Tewari, Krishnansu, Fujiwara, Keiichi, Li, Jingjin, Jamil, Shaheda, Paccaly, Anne, Takehara, Kazuhiro, Usami, Tomoka, Aoki, Yoichi, Suzuki, Nao, Kobayashi, Yoichi, Yoshida, Yoshio, Watari, Hidemichi, Seebach, Frank, Lowy, Israel, Mathias, Melissa, Fury, Matthew, and Oaknin, Ana

Subjects

cemiplimab, cervical cancer, chemotherapy, immunotherapy, programmed cell death‐1, Humans, Female, Uterine Cervical Neoplasms, Middle Aged, Antibodies, Monoclonal, Humanized, Adult, Aged, Japan, Neoplasm Recurrence, Local, Progression-Free Survival, Antineoplastic Agents, Immunological, East Asian People

Abstract

BACKGROUND: In the phase 3 EMPOWER-Cervical 1/GOG-3016/ENGOT-cx9 study, cemiplimab significantly improved overall survival (OS) versus chemotherapy for patients with recurrent or metastatic cervical cancer who progressed after first-line platinum-based chemotherapy. We present a post hoc subgroup analysis of patients enrolled in Japan. METHODS: Patients were enrolled regardless of programmed cell death-ligand 1 status and randomized 1:1 to cemiplimab 350 mg intravenously every 3 weeks or investigators choice  single-agent chemotherapy for up to 96 weeks. Primary endpoint was OS. Key secondary endpoints were progression-free survival (PFS) and objective response rate (ORR). RESULTS: Overall, 608 patients were randomized, of whom 56 (9.2%) were in Japan (cemiplimab, n = 29; chemotherapy, n = 27). The median (range) duration of follow-up was 13.6 (6.0-25.3) versus 18.2 (6.0-38.2) months for patients in Japan and for the overall population, respectively. Median OS (95% confidence interval [CI]) was 8.4 (7.0-not evaluable) and 9.4 (5.4-14.9) months for cemiplimab versus chemotherapy (hazard ratio [HR]: 0.86; 95% CI: 0.43-1.68). Median PFS (95% CI) was 4.0 (1.4-8.2) versus 3.7 (1.8-4.2) months with cemiplimab and chemotherapy (HR: 0.90; 95% CI: 0.50-1.61), respectively. ORR was 17.2% for cemiplimab and 7.4% for chemotherapy (odds ratio, 2.47; 95% CI, 0.44-13.99). Incidence of treatment-emergent adverse events at any grade was 79.3% for cemiplimab and 100% for chemotherapy. Grade ≥3 adverse events were 37.9% versus 66.7% with cemiplimab and chemotherapy, respectively. DISCUSSION: While acknowledging limitations inherent to a small subgroup analysis, the HR of 0.86 observed in Japanese patients suggests an emerging survival benefit despite a 4.6-month shorter median duration of follow-up versus the overall study population.

Published

2024

6. Somatic CpG hypermutation is associated with mismatch repair deficiency in cancer.

Author

Flynn, Aidan, Waszak, Sebastian, and Weischenfeldt, Joachim

Subjects

CpG Hypermutator, Immunotherapy, MMR, Pan-Cancer, TMB, Humans, DNA Mismatch Repair, Neoplasms, CpG Islands, Mutation, MutS Homolog 2 Protein, DNA-Binding Proteins, Immune Checkpoint Inhibitors, Tumor Suppressor Protein p53

Abstract

Somatic hypermutation in cancer has gained momentum with the increased use of tumour mutation burden as a biomarker for immune checkpoint inhibitors. Spontaneous deamination of 5-methylcytosine to thymine at CpG dinucleotides is one of the most ubiquitous endogenous mutational processes in normal and cancer cells. Here, we performed a systematic investigation of somatic CpG hypermutation at a pan-cancer level. We studied 30,191 cancer patients and 103 cancer types and developed an algorithm to identify somatic CpG hypermutation. Across cancer types, we observed the highest prevalence in paediatric leukaemia (3.5%), paediatric high-grade glioma (1.7%), and colorectal cancer (1%). We discovered germline variants and somatic mutations in the mismatch repair complex MutSα (MSH2-MSH6) as genetic drivers of somatic CpG hypermutation in cancer, which frequently converged on CpG sites and TP53 driver mutations. We further observe an association between somatic CpG hypermutation and response to immune checkpoint inhibitors. Overall, our study identified novel cancer types that display somatic CpG hypermutation, strong association with MutSα-deficiency, and potential utility in cancer immunotherapy.

Published

2024

7. Unleashing the potential of CD39-targeted cancer therapy: Breaking new ground and future prospects

Author

Zhou, Qiongyan, Shao, Shengwen, Minev, Theia, and Ma, Wenxue

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Cancer, Precision Medicine, 5.1 Pharmaceuticals, Good Health and Well Being, CD39, Tumor Microenvironment, Immunotherapy, Angiogenesis, Metabolic Reprogramming, Animals, Humans, Neoplasms, Apyrase, Molecular Targeted Therapy, Pharmacology and Pharmaceutical Sciences, Oncology & Carcinogenesis, Pharmacology and pharmaceutical sciences

Abstract

The review article titled CD39 Transforming Cancer Therapy by Modulating Tumor Microenvironment published in June 2024 in Cancer Letters provides a comprehensive overview of CD39's multifaceted roles in cancer, particularly its influence on immunoregulation, angiogenesis, and metabolic reprogramming within the tumor microenvironment (TME). This commentary builds on that foundation by incorporating recent advancements in CD39 research, highlighting unresolved issues, and proposing future research directions. We delve into the therapeutic potential of targeting CD39, addressing clinical translation challenges, and exploring the integration of CD39-based strategies into precision oncology.

Published

2024

8. The CCL2-CCR4 axis promotes Regulatory T cell trafficking to canine glioma tissues

Author

Panek, WK, Toedebusch, RG, Mclaughlin, BE, Dickinson, PJ, Van Dyke, JE, Woolard, KD, Berens, ME, Lesniak, MS, Sturges, BK, Vernau, KM, Li, C, Miska, J, and Toedebusch, Christine M

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Immunotherapy, Brain Cancer, Cancer, Brain Disorders, Rare Diseases, Neurosciences, 2.1 Biological and endogenous factors, Dogs, Animals, Receptors, CCR4, T-Lymphocytes, Regulatory, Glioma, Chemokine CCL2, Brain Neoplasms, Cell Line, Tumor, Cell Movement, Humans, Dog, Glioblastoma, Tumor-infiltrating lymphocyte, CCL2, CCR4, Oncology & Carcinogenesis, Oncology and carcinogenesis

Abstract

PurposeSpontaneously occurring glioma in pet dogs is increasingly recognized as a valuable translational model for human glioblastoma. Canine high-grade glioma and human glioblastomas share many molecular similarities, including the accumulation of immunosuppressive regulatory T cells (Tregs) that inhibit anti-tumor immune responses. Identifying in dog mechanisms responsible for Treg recruitment may afford to target the cellular population driving immunosuppression, the results providing a rationale for translational clinical studies in human patients. Our group has previously identified C-C motif chemokine 2 (CCL2) as a glioma-derived T-reg chemoattractant acting on chemokine receptor 4 (CCR4) in a murine orthotopic glioma model. Recently, we demonstrated a robust increase of CCL2 in the brain tissue of canine patients bearing high-grade glioma.MethodsWe performed a series of in vitro experiments using canine Tregs and patient-derived canine glioma cell lines (GSC 1110, GSC 0514, J3T-Bg, G06A) to interrogate the CCL2-CCR4 signaling axis in the canine.ResultsWe established a flow cytometry gating strategy for identifying and isolating FOXP3+ Tregs in dogs. The canine CD4 + CD25high T-cell population was highly enriched in FOXP3 and CCR4 expression, indicating they are bona fide Tregs. Canine Treg migration was enhanced by CCL2 or by glioma cell line-derived supernatant. Blockade of the CCL2-CCR4 axis significantly reduced migration of canine Tregs. CCL2 mRNA was expressed in all glioma cell lines, and expression increased when exposed to Tregs but not CD4 + helper T-cells.ConclusionOur study validates CCL2-CCR4 as a bi-directional Treg-glioma immunosuppressive and tumor-promoting axis in canine high-grade glioma.

Published

2024

9. Adverse jaw outcomes from immune checkpoint inhibitors for head and neck cancer? Case reports.

Author

Subramanian, Gayathri, Yeung, Vincent, Baredes, Soly, Sung Kim, Bergsbaken, Tessa, and Quek, Samuel Y. P.

Subjects

THERAPEUTIC use of vitamin E, THERAPEUTIC use of antineoplastic agents, THERAPEUTIC use of monoclonal antibodies, JAW diseases, OSTEORADIONECROSIS, CANCER relapse, HEAD & neck cancer, IMMUNOTHERAPY, CHEMORADIOTHERAPY, AMOXICILLIN, POSITRON emission tomography, IMMUNE checkpoint inhibitors, PENTOXIFYLLINE, STRUCTURED treatment interruption, JAWS, METRONIDAZOLE, DENTAL extraction

Abstract

Radiation treatment plays a mainstream role in the management of head and necksquamous cell carcinomas (HNSCCs). Adverse effects from radiation therapy include osteoradionecrosis of the jaw, and rarely, pathologic fracture. Immune checkpoint inhibitors (ICI) such as pembrolizumab are of growing relevance to the management of metastatic and recurrent HNSCCs. Adverse impacts on bone secondary to medications such as pembrolizumab and nivolumab have been sporadically documented in the literature. The objective of this manuscript is to raise awareness of possible increase in risk for adverse jaw outcomes in patients with HNSCCs exposed to both radiation treatment to the jaws and ICI therapy. This manuscript documents adverse jaw outcomes including osteonecrosis and pathologic fracture of the mandible in two patients receiving pembrolizumab for management of HNSCC who had received prior radiation treatment. A potential link between immunotherapy and adverse jaw outcomes is consistent with the growing understanding of osteoimmunology, investigating the closely interrelated processes in bone remodeling and immune system function, in health and disease. It is important to ascertain if pembrolizumab poses an incremental risk for such outcomes, beyond the risk from prior radiation, for patients managed with radiation treatment and ICI therapy for HNSCC. The general dental practitioner may encoun-tersuch patients either in the context of facilitating dental clearance prior to initiation of chemotherapy, or rarely, with poorly explained jaw symptoms and must be alert to the possibility of occurrence of such adverse jaw events to facilitate timely diagnosis and optimal patient management. [ABSTRACT FROM AUTHOR]

Published

2024

10. Immune Checkpoint Inhibitor-Induced Primary Adrenal Insufficiency: A Case Report

Author

Gupta, Rahul and Lubkin, Cary

Subjects

Immunotherapy, shock, adrenal insufficiency, immune checkpoint inhibitor, case report

Abstract

Introduction: One of the less common and more life-threatening etiologies of adrenal insufficiency is immune checkpoint inhibitor (ICI)-induced primary adrenal insufficiency (PAI). Patients typically present with fatigue, malaise, and nausea and are treated empirically with hydrocortisone.  Case Report: We present the case of a 59-year-old female who presented with hypotension, which initially was thought to be due to hypovolemia or medication-related, but was ultimately found to have PAI. Conclusion: This case highlights the importance of early detection of ICI-induced primary adrenal insufficiency, given its associated morbidity and mortality and its incidence in patients with a history of immunotherapy.

Published

2024

11. The next frontier in immunotherapy: potential and challenges of CAR-macrophages.

Author

Li, Jing, Chen, Ping, and Ma, Wenxue

Subjects

CAR macrophage (CAR-MΦ), Clinical trials, Combination therapies, Immunotherapy, Tumor Microenvironment (TME)

Abstract

Chimeric antigen receptor macrophage (CAR-MΦ) represents a significant advancement in immunotherapy, especially for treating solid tumors where traditional CAR-T therapies face limitations. CAR-MΦ offers a promising approach to target and eradicate tumor cells by utilizing macrophages phagocytic and antigen-presenting abilities. However, challenges such as the complex tumor microenvironment (TME), variability in antigen expression, and immune suppression limit their efficacy. This review addresses these issues, exploring mechanisms of CAR-MΦ action, optimal construct designs, and interactions within the TME. It also delves into the ex vivo manufacturing challenges of CAR-MΦ, discussing autologous and allogeneic sources and the importance of stringent quality control. The potential synergies of integrating CAR-MΦ with existing cancer therapies like checkpoint inhibitors and conventional chemotherapeutics are examined to highlight possible enhanced treatment outcomes. Furthermore, regulatory pathways for CAR-MΦ therapies are scrutinized alongside established protocols for CAR-T cells, identifying unique considerations essential for clinical trials and market approval. Proposed safety monitoring frameworks aim to manage potential adverse events, such as cytokine release syndrome, crucial for patient safety. Consolidating current research and clinical insights, this review seeks to refine CAR-MΦ therapeutic applications, overcome barriers, and suggest future research directions to transition CAR-MΦ therapies from experimental platforms to standard cancer care options.

Published

2024

12. CD94+ Natural Killer cells potentiate pulmonary ischemia-reperfusion injury.

Author

Tsao, Tasha, Qiu, Longhui, Bharti, Reena, Shemesh, Avishai, Hernandez, Alberto M, Cleary, Simon J, Greenland, Nancy Y, Santos, Jesse, Shi, Ruoshi, Bai, Lu, Richardson, Jennifer, Dilley, Kimberley, Will, Matthias, Tomasevic, Nenad, Sputova, Tereza, Salles, Adam, Kang, Jeffrey, Zhang, Dongliang, Hays, Steve R, Kukreja, Jasleen, Singer, Jonathan P, Lanier, Lewis L, Looney, Mark R, Greenland, John R, and Calabrese, Daniel R

Subjects

Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Immunology, Transplantation, Lung, Clinical Research, Organ Transplantation, Immunotherapy, 2.1 Biological and endogenous factors, 5.1 Pharmaceuticals, 5.2 Cellular and gene therapies, 1.1 Normal biological development and functioning, Respiratory, Killer Cells, Natural, Bronchoalveolar Lavage Fluid, Animals, Mice, Inbred C57BL, Humans, Mice, Reperfusion Injury, Disease Models, Animal, Antibodies, Monoclonal, Lung Transplantation, Female, Male, NK Cell Lectin-Like Receptor Subfamily D, Medical and Health Sciences, Respiratory System, Cardiovascular medicine and haematology

Abstract

BackgroundPulmonary ischaemia-reperfusion injury (IRI) is a major contributor to poor lung transplant outcomes. We recently demonstrated a central role of airway-centred natural killer (NK) cells in mediating IRI; however, there are no existing effective therapies for directly targeting NK cells in humans.MethodsWe hypothesised that a depleting anti-CD94 monoclonal antibody (mAb) would provide therapeutic benefit in mouse and human models of IRI based on high levels of KLRD1 (CD94) transcripts in bronchoalveolar lavage samples from lung transplant patients.ResultsWe found that CD94 is highly expressed on mouse and human NK cells, with increased expression during IRI. Anti-mouse and anti-human mAbs against CD94 showed effective NK cell depletion in mouse and human models and blunted lung damage and airway epithelial killing, respectively. In two different allogeneic orthotopic lung transplant mouse models, anti-CD94 treatment during induction reduced early lung injury and chronic inflammation relative to control therapies. Anti-CD94 did not increase donor antigen-presenting cells that could alter long-term graft acceptance.ConclusionsLung transplant induction regimens incorporating anti-CD94 treatment may safely improve early clinical outcomes.

Published

2024

13. Venous Thromboembolism Risk in Hematological Malignancies Post-Chimeric Antigen Receptor T-Cell (CAR-T) Therapy: A Meta-Analysis of Phase 2 and Phase 3 Clinical Trials.

Author

Chitkara, Akshit, Sreenivasan, Sushanth, Yin, Yue, Rai, Maitreyee, and Sadashiv, Santhosh

Subjects

B-cell lymphoma, Chimeric Antigen Receptor T-cell (CAR-T), hematological malignancies, mantle cell lymphoma, meta-analysis, multiple myeloma, venous thromboembolism, Humans, Venous Thromboembolism, Hematologic Neoplasms, Clinical Trials, Phase III as Topic, Clinical Trials, Phase II as Topic, Immunotherapy, Adoptive, Receptors, Chimeric Antigen

Abstract

Chimeric Antigen Receptor T-cell (CAR-T) therapy uses genetically engineered T-cells with specific binding sites. This therapy allows for tumor specificity and durable treatment responses for patients with hematological malignancies. In this review, we study the risk of venous thromboembolism (VTE) associated with CAR-T therapy. We searched the National Institutes of Health library, Cochrane Library Databases, ClinicalTrials.gov database, and medical literature search engines PubMed and Google Scholar for Phase 2 and Phase 3 drug-efficacy and safety trials to determine the aggregate incidence and risk of VTE treated with CAR-T. Of 1127 search results, nine studies were identified and included in our meta-analysis. Of the 1017 patients who received therapy, 805 patients (79.15%) experienced some degree of CRS, and 122 patients (11.9%) experienced severe CRS (higher than grade 3). Only three out of one thousand and seventeen patients were reported to have experienced venous thromboembolism. Our study did not find a statistically significant association between increased VTE incidence (OR = 0.0005, 95% CI [0.0001, 0.0017]) and CRS/ICANS (p < 0.0001). There was a 0.0050 (95% confidence interval [0.0019, 0.0132]) relative risk for VTE. In our study, we did not find a statistically significantly increased risk of developing VTE despite CRS and underlying malignancy, which have been associated with increased risk of VTE.

Published

2024

14. Phase II basket trial of Dual Anti-CTLA-4 and Anti-PD-1 blockade in Rare Tumors (DART) SWOG S1609: adrenocortical carcinoma cohort.

Author

Patel, Sandip, Othus, Megan, Chae, Young, Huynh, Tridu, Tan, Benjamin, Kuzel, Timothy, McLeod, Christine, Lopez, Gabby, Chen, Helen, Sharon, Elad, Streicher, Howard, Ryan, Christopher, Blanke, Charles, and Kurzrock, Razelle

Subjects

Combination therapy, Immune Checkpoint Inhibitor, Immune modulatory, Immunotherapy, Neuroendocrine and Adrenal Tumor, Humans, Female, Middle Aged, Male, Adult, Adrenocortical Carcinoma, Aged, CTLA-4 Antigen, Immune Checkpoint Inhibitors, Ipilimumab, Prospective Studies, Programmed Cell Death 1 Receptor, Adrenal Cortex Neoplasms, Nivolumab, Antineoplastic Combined Chemotherapy Protocols

Abstract

OBJECTIVES: Multiple common cancers benefit from immunotherapy; however, less is known about efficacy in rare tumors. We report the results of the adrenocortical carcinoma cohort of NCI/SWOG S1609 Dual Anti-CTLA-4 and Anti-PD-1 blockade in Rare Tumors. DESIGN/SETTING: A prospective, phase 2 clinical trial of ipilimumab plus nivolumab was conducted by the SWOG Early Therapeutics and Rare Cancers Committee for multiple rare tumor cohorts across >1,000 National Clinical Trial Network sites. PARTICIPANTS: 21 eligible patients were registered. Median age was 53 years (range 26-69); 16 (76%) were women. INTERVENTIONS: Ipilimumab 1 mg/kg intravenously every 6 weeks with nivolumab 240 mg intravenously every 2 weeks was administered until disease progression, symptomatic deterioration, treatment delay for any reason >56 days, unacceptable or immune-related toxicity with inability to decrease prednisone to 6 months), progression-free survival (PFS), overall survival (OS), and toxicity. Immune-related outcomes included immune ORR (iORR), immune CBR (iCBR), and immune PFS (iPFS). A two-stage design was used assuming: null=5% alternative=30%, n=6 in the first stage, 16 max, one-sided alpha=13%. RESULTS: The median number of prior therapy lines was 2 (range: 1-9). 3 of 21 patients attained confirmed partial response (PR) (ORR=14%). In addition, one patient had an unconfirmed PR; one, stable disease (SD)>6 months; one, immune-related RECIST (iRECIST) PR (iPR); and one patient attained iSD>6 months: clinical benefit rate (response or SD>6 months)=5/21 (24%), iORR=4/21 (19%), iCBR=7/21 (33%). The 6-month PFS was 24%; 6-month iPFS, 33%. The PFS for patients (N=7) with iRECIST clinical benefit were 57, 52, 18, 15, 13, 7, and 7 months. The 6-month OS was 76%; the median OS, was 15.8 months. The most common toxicities were fatigue (62%) and rash (38%), and the most common grade 3/4 immune-related adverse events were hepatic dysfunction (9.5%) and adrenal insufficiency (9.5%). Treatment-related adverse events leading to discontinuation of therapy in four patients (21%). There were no grade 5 adverse events. CONCLUSIONS: Ipilimumab plus nivolumab is active in refractory metastatic adrenocortical cancer meeting the primary endpoint of the study, with a 19% iORR and 33% iCBR (includes SD/iSD>6 months) and with the longest PFS/iPFS of 52 and 57 months. TRIAL REGISTRATION NUMBER: NCT02834013 (registered 15 July, 2016; https://clinicaltrials.gov/ct2/show/NCT02834013).

Published

2024

15. γδ T cells as critical anti-tumor immune effectors

Author

Arias-Badia, Marcel, Chang, Ryan, and Fong, Lawrence

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Immunotherapy, Cancer, 1.1 Normal biological development and functioning, 2.1 Biological and endogenous factors, Infection, Inflammatory and immune system, Oncology and carcinogenesis

Abstract

While the effector cells that mediate anti-tumor immunity have historically been attributed to αβ T cells and natural killer cells, γδ T cells are now being recognized as a complementary mechanism mediating tumor rejection. γδ T cells possess a host of functions ranging from antigen presentation to regulatory function and, importantly, have critical roles in eliciting anti-tumor responses where other immune effectors may be rendered ineffective. Recent discoveries have elucidated how these differing functions are mediated by γδ T cells with specific T cell receptors and spatial distribution. Their relative resistance to mechanisms of dysfunction like T cell exhaustion has spurred the development of therapeutic approaches exploiting γδ T cells, and an improved understanding of these cells should enable more effective immunotherapies.

Published

2024

16. Incidence and outcomes of cytomegalovirus reactivation after chimeric antigen receptor T-cell therapy.

Author

Lin, Rick, Anderson, Anthony, Natori, Yoichiro, Raja, Mohammed, Morris, Michele, Jimenez, Antonio, Beitinjaneh, Amer, Wang, Trent, Goodman, Mark, Lekakis, Lazaros, Spiegel, Jay, Holtzman, Noa, Pereira, Denise, Benjamin, Cara, Natori, Akina, Komanduri, Krishna, and Camargo, Jose

Subjects

Humans, Cytomegalovirus Infections, Male, Virus Activation, Middle Aged, Female, Cytomegalovirus, Incidence, Immunotherapy, Adoptive, Adult, Receptors, Chimeric Antigen, Aged

Abstract

Cytomegalovirus (CMV) reactivation is a major complication among seropositive allogeneic hematopoietic cell transplantation recipients; however, data on CMV reactivation after chimeric antigen receptor (CAR) T-cell therapy are limited. We report the incidence and outcomes of 95 adult CMV-seropositive patients who received CAR T-cell therapy between February 2018 and February 2023. CMV outcomes were CMV reactivation (any viremia) and clinically significant CMV infection (cs-CMV). Thirty-one patients (33%) had evidence of CMV reactivation (any viremia), and 10 patients (11%) had cs-CMV. The median time from CAR T-cell infusion to CMV reactivation was 19 days (interquartile range [IQR], 9-31). The cumulative incidence of CMV (any viremia) was significantly higher among patients with grade 3 to 4 cytokine release syndrome (67 vs 28%; P = .01), and those who received corticosteroids (39 vs 21%; P = .03), anakinra (56 vs 28%; P = .02), or ≥2 immunosuppressants (41 vs 21%; P = .02). Receipt of corticosteroids (18 vs 0%; P = .004), tocilizumab (14 vs 0%; P = .04), anakinra (33 vs 7%; P = .008), and ≥2 immunosuppressants (20 vs 0%; P = .001) were all associated with cs-CMV. Receiving ≥2 immunosuppressants was associated with a twofold increase in CMV reactivation in multivariate analyses (adjusted odds ratio [aOR], 2.27; 95% confidence interval, 1.1-4.8; P = .03). Overall, the 1-year mortality was significantly higher in those with CMV reactivation (57% vs 23%; P = .001). Immunosuppression, particularly with corticosteroids, for the management of CAR T-cell toxicities, is a major risk factor for CMV reactivation.

Published

2024

17. Safety and clinical activity of durvalumab combined with tremelimumab in recurrent/metastatic head and neck squamous cell carcinoma: a multicenter phase I study.

Author

Algazi, Alain, Papadopoulos, K, Tsai, F, Hansen, A, Angra, N, Das, M, Sheth, S, and Siu, L

Subjects

CTLA-4 inhibitor, PD-L1 inhibitor, head and neck squamous cell carcinoma, immunotherapy

Abstract

BACKGROUND: Programmed cell death protein 1 (PD-1) inhibitors prolong survival versus chemotherapy in recurrent/metastatic head and neck squamous cell carcinoma (R/M HNSCC), which often expresses cytotoxic T-lymphocyte-associated protein 4 (CTLA-4) and programmed cell death-ligand 1 (PD-L1), providing a rationale for combined PD-(L)1 and CTLA-4 blockade. We report a phase I, open-label study of the PD-L1 inhibitor durvalumab plus the CTLA-4 inhibitor tremelimumab (NCT02262741). METHODS: In dose exploration, two cohorts of previously treated patients received durvalumab 10 mg/kg plus tremelimumab 3 mg/kg, or durvalumab 20 mg/kg plus tremelimumab 1 mg/kg, for up to 12 months. Dose expansion comprised two cohorts of previously untreated patients with R/M HNSCC having baseline PD-L1 tumor cell (TC) expression ≥25% and

Published

2024

18. CD4+ CAR T-cell exhaustion associated with early relapse of multiple myeloma after BCMA CAR T-cell therapy.

Author

Ledergor, Guy, Fan, Zenghua, Wu, Kai, McCarthy, Elizabeth, Hyrenius-Wittsten, Axel, Starzinski, Alec, Chang, Hewitt, Bridge, Mark, Kwek, Serena, Cheung, Alexander, Bylsma, Sophia, Hansen, Erik, Wolf, Jeffrey, Wong, Sandy, Shah, Nina, Roybal, Kole, Martin, Thomas, Ye, Chun, and Fong, Lawrence

Subjects

Multiple Myeloma, Humans, B-Cell Maturation Antigen, Immunotherapy, Adoptive, Receptors, Chimeric Antigen, CD4-Positive T-Lymphocytes, Recurrence, Male, Female, T-Cell Exhaustion

Abstract

Multiple myeloma is characterized by frequent clinical relapses after conventional therapy. Recently, chimeric antigen receptor (CAR) T cells targeting B-cell maturation antigen (BCMA) has been established as a treatment option for patients with relapsed or refractory disease. However, although >70% of patients initially respond to this treatment, clinical relapse and disease progression occur in most cases. Recent studies showed persistent expression of BCMA at the time of relapse, indicating that immune-intrinsic mechanisms may contribute to this resistance. Although there were no preexisting T-cell features associated with clinical outcomes, we found that patients with a durable response to CAR T-cell treatment had greater persistence of their CAR T cells than patients with transient clinical responses. They also possessed a significantly higher proportion of CD8+ T-effector memory cells. In contrast, patients with short-lived responses to treatment have increased frequencies of cytotoxic CD4+ CAR T cells. These cells expand in vivo early after infusion but express exhaustion markers (hepatitis A virus cellular receptor 2 [HAVCR2] and T-cell immunoglobulin and mucin domain-containing-3 [TIGIT]) and remain polyclonal. Finally, we demonstrate that nonclassical monocytes are enriched in the myeloma niche and may induce CAR T-cell dysfunction through mechanisms that include transforming growth factor β. These findings shed new light on the role of cytotoxic CD4+ T cells in disease progression after CAR T-cell therapy.

Published

2024

19. Circadian control of tumor immunosuppression affects efficacy of immune checkpoint blockade

Author

Fortin, Bridget M, Pfeiffer, Shannon M, Insua-Rodríguez, Jacob, Alshetaiwi, Hamad, Moshensky, Alexander, Song, Wei A, Mahieu, Alisa L, Chun, Sung Kook, Lewis, Amber N, Hsu, Alex, Adam, Isam, Eng, Oliver S, Pannunzio, Nicholas R, Seldin, Marcus M, Marazzi, Ivan, Marangoni, Francesco, Lawson, Devon A, Kessenbrock, Kai, and Masri, Selma

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Genetics, Cancer, Immunotherapy, Colo-Rectal Cancer, Sleep Research, Digestive Diseases, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Animals, Mice, Immune Checkpoint Inhibitors, Myeloid-Derived Suppressor Cells, Circadian Clocks, B7-H1 Antigen, Mice, Inbred C57BL, Circadian Rhythm, CD8-Positive T-Lymphocytes, Colorectal Neoplasms, Tumor Microenvironment, Immune Tolerance, Humans, Female, Cell Line, Tumor, Single-Cell Analysis, Immunosuppression Therapy, Cytokines, Male, Biochemistry and cell biology

Abstract

The circadian clock is a critical regulator of immunity, and this circadian control of immune modulation has an essential function in host defense and tumor immunosurveillance. Here we use a single-cell RNA sequencing approach and a genetic model of colorectal cancer to identify clock-dependent changes to the immune landscape that control the abundance of immunosuppressive cells and consequent suppression of cytotoxic CD8+ T cells. Of these immunosuppressive cell types, PD-L1-expressing myeloid-derived suppressor cells (MDSCs) peak in abundance in a rhythmic manner. Disruption of the epithelial cell clock regulates the secretion of cytokines that promote heightened inflammation, recruitment of neutrophils and the subsequent development of MDSCs. We also show that time-of-day anti-PD-L1 delivery is most effective when synchronized with the abundance of immunosuppressive MDSCs. Collectively, these data indicate that circadian gating of tumor immunosuppression informs the timing and efficacy of immune checkpoint inhibitors.

Published

2024

20. Anti-acetylated-tau immunotherapy is neuroprotective in tauopathy and brain injury.

Author

Parra Bravo, Celeste, Krukowski, Karen, Barker, Sarah, Wang, Chao, Li, Yaqiao, Fan, Li, Vázquez-Rosa, Edwin, Shin, Min-Kyoo, Wong, Man, McCullough, Louise, Kitagawa, Ryan, Choi, H, Cacace, Angela, Sinha, Subhash, Pieper, Andrew, Rosi, Susanna, Chen, Xu, and Gan, Li

Subjects

Acetylated tau, Human plasma, Immunotherapy, TBI, Tauopathy, Animals, Tauopathies, tau Proteins, Mice, Acetylation, Humans, Immunotherapy, Disease Models, Animal, Mice, Transgenic, Brain Injuries, Traumatic, Brain Injuries, Brain, Neuroprotective Agents

Abstract

BACKGROUND: Tau is aberrantly acetylated in various neurodegenerative conditions, including Alzheimers disease, frontotemporal lobar degeneration (FTLD), and traumatic brain injury (TBI). Previously, we reported that reducing acetylated tau by pharmacologically inhibiting p300-mediated tau acetylation at lysine 174 reduces tau pathology and improves cognitive function in animal models. METHODS: We investigated the therapeutic efficacy of two different antibodies that specifically target acetylated lysine 174 on tau (ac-tauK174). We treated PS19 mice, which harbor the P301S tauopathy mutation that causes FTLD, with anti-ac-tauK174 and measured effects on tau pathology, neurodegeneration, and neurobehavioral outcomes. Furthermore, PS19 mice received treatment post-TBI to evaluate the ability of the immunotherapy to prevent TBI-induced exacerbation of tauopathy phenotypes. Ac-tauK174 measurements in human plasma following TBI were also collected to establish a link between trauma and acetylated tau levels, and single nuclei RNA-sequencing of post-TBI brain tissues from treated mice provided insights into the molecular mechanisms underlying the observed treatment effects. RESULTS: Anti-ac-tauK174 treatment mitigates neurobehavioral impairment and reduces tau pathology in PS19 mice. Ac-tauK174 increases significantly in human plasma 24 h after TBI, and anti-ac-tauK174 treatment of PS19 mice blocked TBI-induced neurodegeneration and preserved memory functions. Anti-ac-tauK174 treatment rescues alterations of microglial and oligodendrocyte transcriptomic states following TBI in PS19 mice. CONCLUSIONS: The ability of anti-ac-tauK174 treatment to rescue neurobehavioral impairment, reduce tau pathology, and rescue glial responses demonstrates that targeting tau acetylation at K174 is a promising neuroprotective therapeutic approach to human tauopathies resulting from TBI or genetic disease.

Published

2024

21. Safety and Efficacy of Laser Interstitial Thermal Therapy as Upfront Therapy in Primary Glioblastoma and IDH-Mutant Astrocytoma: A Meta-Analysis.

Author

Pandey, Aryan, Chandla, Anubhav, Mekonnen, Mahlet, Hovis, Gabrielle, Teton, Zoe, Patel, Kunal, Everson, Richard, Wadehra, Madhuri, and Yang, Isaac

Subjects

5-ALA, LITT, glioblastoma, immunotherapy, malignant gliomas, meningioma, molecular targeted therapy, primary brain tumors, skull-based tumors, vaccine therapy

Abstract

Although primary studies have reported the safety and efficacy of LITT as a primary treatment in glioma, they are limited by sample sizes and institutional variation in stereotactic parameters such as temperature and laser power. The current literature has yet to provide pooled statistics on outcomes solely for primary brain tumors according to the 2021 WHO Classification of Tumors of the Central Nervous System (WHO CNS5). In the present study, we identify recent articles on primary CNS neoplasms treated with LITT without prior intervention, focusing on relationships with molecular profile, PFS, and OS. This meta-analysis includes the extraction of data from primary sources across four databases using the Covidence systematic review manager. The pooled data suggest LITT may be a safe primary management option with tumor ablation rates of 94.8% and 84.6% in IDH-wildtype glioblastoma multiforme (GBM) and IDH-mutant astrocytoma, respectively. For IDH-wildtype GBM, the pooled PFS and OS were 5.0 and 9.0 months, respectively. Similar to rates reported in the prior literature, the neurologic and non-neurologic complication rates for IDH-wildtype GBM were 10.3% and 4.8%, respectively. The neurologic and non-neurologic complication rates were somewhat higher in the IDH-mutant astrocytoma cohort at 33% and 8.3%, likely due to a smaller cohort size.

Published

2024

22. Opposing tumor-cell-intrinsic and -extrinsic roles of the IRF1 transcription factor in antitumor immunity

Author

Purbey, Prabhat K, Seo, Joowon, Paul, Manash K, Iwamoto, Keisuke S, Daly, Allison E, Feng, An-Chieh, Champhekar, Ameya S, Langerman, Justin, Campbell, Katie M, Schaue, Dörthe, McBride, William H, Dubinett, Steven M, Ribas, Antoni, Smale, Stephen T, and Scumpia, Philip O

Subjects

Biological Sciences, Immunotherapy, Genetics, Cancer, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Inflammatory and immune system, Animals, Humans, Mice, B7-H1 Antigen, Cell Line, Tumor, Immunity, Interferon Regulatory Factor-1, Mice, Inbred C57BL, Neoplasms, STAT1 Transcription Factor, Male, Female, CP: Cancer, CP: Immunology, IRF1, PD-L1 regulation, TLR signaling, antitumor immunity, cytotoxic T lymphocytes, immune checkpoint blockade, immune evasion, interferon signaling, scRNA-seq, transcription, Biochemistry and Cell Biology, Medical Physiology, Biological sciences

Abstract

Type I interferon (IFN-I) and IFN-γ foster antitumor immunity by facilitating T cell responses. Paradoxically, IFNs may promote T cell exhaustion by activating immune checkpoints. The downstream regulators of these disparate responses are incompletely understood. Here, we describe how interferon regulatory factor 1 (IRF1) orchestrates these opposing effects of IFNs. IRF1 expression in tumor cells blocks Toll-like receptor- and IFN-I-dependent host antitumor immunity by preventing interferon-stimulated gene (ISG) and effector programs in immune cells. In contrast, expression of IRF1 in the host is required for antitumor immunity. Mechanistically, IRF1 binds distinctly or together with STAT1 at promoters of immunosuppressive but not immunostimulatory ISGs in tumor cells. Overexpression of programmed cell death ligand 1 (PD-L1) in Irf1-/- tumors only partially restores tumor growth, suggesting multifactorial effects of IRF1 on antitumor immunity. Thus, we identify that IRF1 expression in tumor cells opposes host IFN-I- and IRF1-dependent antitumor immunity to facilitate immune escape and tumor growth.

Published

2024

23. A Pipeline for Evaluation of Machine Learning/Artificial Intelligence Models to Quantify Programmed Death Ligand 1 Immunohistochemistry

Author

Knudsen, Beatrice S, Jadhav, Alok, Perry, Lindsey J, Thagaard, Jeppe, Deftereos, Georgios, Ying, Jian, Brintz, Ben J, and Zhang, Wei

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Cancer, Machine Learning and Artificial Intelligence, Lung Cancer, Bioengineering, Immunotherapy, Lung, Networking and Information Technology R&D (NITRD), Humans, Lung Neoplasms, Immunohistochemistry, Artificial Intelligence, Machine Learning, Biomarkers, Tumor, B7-H1 Antigen, cancer segmentation, digital pathology, programmed death ligand 1, tumor proportion scores, Clinical Sciences, Pathology, Clinical sciences

Abstract

Immunohistochemistry (IHC) is used to guide treatment decisions in multiple cancer types. For treatment with checkpoint inhibitors, programmed death ligand 1 (PD-L1) IHC is used as a companion diagnostic. However, the scoring of PD-L1 is complicated by its expression in cancer and immune cells. Separation of cancer and noncancer regions is needed to calculate tumor proportion scores (TPS) of PD-L1, which is based on the percentage of PD-L1-positive cancer cells. Evaluation of PD-L1 expression requires highly experienced pathologists and is often challenging and time-consuming. Here, we used a multi-institutional cohort of 77 lung cancer cases stained centrally with the PD-L1 22C3 clone. We developed a 4-step pipeline for measuring TPS that includes the coregistration of hematoxylin and eosin, PD-L1, and negative control (NC) digital slides for exclusion of necrosis, segmentation of cancer regions, and quantification of PD-L1+ cells. As cancer segmentation is a challenging step for TPS generation, we trained DeepLab V3 in the Visiopharm software package to outline cancer regions in PD-L1 and NC images and evaluated the model performance by mean intersection over union (mIoU) against manual outlines. Only 14 cases were required to accomplish a mIoU of 0.82 for cancer segmentation in hematoxylin-stained NC cases. For PD-L1-stained slides, a model trained on PD-L1 tiles augmented by registered NC tiles achieved a mIoU of 0.79. In segmented cancer regions from whole slide images, the digital TPS achieved an accuracy of 75% against the manual TPS scores from the pathology report. Major reasons for algorithmic inaccuracies include the inclusion of immune cells in cancer outlines and poor nuclear segmentation of cancer cells. Our transparent and stepwise approach and performance metrics can be applied to any IHC assay to provide pathologists with important insights on when to apply and how to evaluate commercial automated IHC scoring systems.

Published

2024

24. The Burden of Invasive Fungal Disease Following Chimeric Antigen Receptor T-Cell Therapy and Strategies for Prevention.

Author

Little, Jessica, Kampouri, Eleftheria, Friedman, Daniel, McCarty, Todd, Thompson, George, Kontoyiannis, Dimitrios, Vazquez, Jose, Baddley, John, and Hammond, Sarah

Subjects

CAR T-cell therapy, antifungal prophylaxis, antifungal stewardship, immunotherapy, invasive fungal disease

Abstract

Chimeric antigen receptor (CAR) T-cell therapy is a novel immunotherapy approved for the treatment of hematologic malignancies. This therapy leads to a variety of immunologic deficits that could place patients at risk for invasive fungal disease (IFD). Studies assessing IFD in this setting are limited by inconsistent definitions and heterogeneity in prophylaxis use, although the incidence of IFD after CAR T-cell therapy, particularly for lymphoma and myeloma, appears to be low. This review evaluates the incidence of IFD after CAR T-cell therapy, and discusses optimal approaches to prevention, highlighting areas that require further study as well as future applications of cellular therapy that may impact IFD risk. As the use of CAR T-cell therapy continues to expand for hematologic malignancies, solid tumors, and most recently to include non-oncologic diseases, understanding the risk for IFD in this uniquely immunosuppressed population is imperative to prevent morbidity and mortality.

Published

2024

25. “De novo replication repair deficient glioblastoma, IDH-wildtype” is a distinct glioblastoma subtype in adults that may benefit from immune checkpoint blockade

Author

Hadad, Sara, Gupta, Rohit, Oberheim Bush, Nancy Ann, Taylor, Jennie W, Villanueva-Meyer, Javier E, Young, Jacob S, Wu, Jasper, Ravindranathan, Ajay, Zhang, Yalan, Warrier, Gayathri, McCoy, Lucie, Shai, Anny, Pekmezci, Melike, Perry, Arie, Bollen, Andrew W, Phillips, Joanna J, Braunstein, Steve E, Raleigh, David R, Theodosopoulos, Philip, Aghi, Manish K, Chang, Edward F, Hervey-Jumper, Shawn L, Costello, Joseph F, de Groot, John, Butowski, Nicholas A, Clarke, Jennifer L, Chang, Susan M, Berger, Mitchel S, Molinaro, Annette M, and Solomon, David A

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Brain Cancer, Cancer, Precision Medicine, Brain Disorders, Genetics, Human Genome, Clinical Research, Cancer Genomics, Neurosciences, Immunotherapy, Orphan Drug, Rare Diseases, 2.1 Biological and endogenous factors, Good Health and Well Being, Adult, Humans, Child, Middle Aged, Aged, Glioblastoma, Immune Checkpoint Inhibitors, Homozygote, Prospective Studies, Brain Neoplasms, Sequence Deletion, Mutation, Isocitrate Dehydrogenase, Giant cell glioblastoma, Hypermutation, Ultrahypermutation, Mismatch repair deficiency, POLE, Lynch syndrome, Immune checkpoint blockade, Molecular neuropathology, Molecular neuro-oncology, Neurology & Neurosurgery

Abstract

Glioblastoma is a clinically and molecularly heterogeneous disease, and new predictive biomarkers are needed to identify those patients most likely to respond to specific treatments. Through prospective genomic profiling of 459 consecutive primary treatment-naïve IDH-wildtype glioblastomas in adults, we identified a unique subgroup (2%, 9/459) defined by somatic hypermutation and DNA replication repair deficiency due to biallelic inactivation of a canonical mismatch repair gene. The deleterious mutations in mismatch repair genes were often present in the germline in the heterozygous state with somatic inactivation of the remaining allele, consistent with glioblastomas arising due to underlying Lynch syndrome. A subset of tumors had accompanying proofreading domain mutations in the DNA polymerase POLE and resultant "ultrahypermutation". The median age at diagnosis was 50 years (range 27-78), compared with 63 years for the other 450 patients with conventional glioblastoma (p

Published

2024

26. Human cytomegalovirus (HCMV) genetic diversity, drug resistance testing and prevalence of the resistance mutations: A literature review

Author

Grgic, Ivana and Gorenec, Lana

Published

2024

27. Landscape and Treatment Options of Shapeshifting Small Cell Lung Cancer.

Author

Gu, Yijun and Benavente, Claudia

Subjects

immunotherapy, small cell lung cancer, targeted therapy, tumor plasticity

Abstract

Small cell lung cancer (SCLC) is a deadly neuroendocrine malignancy, notorious for its rapid tumor growth, early metastasis, and relatively cold immune environment. Only standard chemotherapies and a few immune checkpoint inhibitors have been approved for SCLC treatment, revealing an urgent need for novel therapeutic approaches. Moreover, SCLC has been recently recognized as a malignancy with high intratumoral and intertumoral heterogeneity, which explains the modest response rate in some patients and the early relapse. Molecular subtypes defined by the expression of lineage-specific transcription factors (ASCL1, NEUROD1, POU2F3, and, in some studies, YAP1) or immune-related genes display different degrees of neuroendocrine differentiation, immune cell infiltration, and response to treatment. Despite the complexity of this malignancy, a few biomarkers and targets have been identified and many promising drugs are currently undergoing clinical trials. In this review, we integrate the current progress on the genomic landscape of this shapeshifting malignancy, the characteristics and treatment vulnerabilities of each subtype, and promising drugs in clinical phases.

Published

2024

28. Salvage therapies including retreatment with BCMA-directed approaches after BCMA CAR-T relapses for multiple myeloma.

Author

Reyes, Kevin, Liu, Yen-Chun, Huang, Chiung-yu, Banerjee, Rahul, Martin, Thomas, Wong, Sandy, Wolf, Jeffrey, Arora, Shagun, Shah, Nina, Chari, Ajai, and Chung, Alfred

Subjects

Humans, B-Cell Maturation Antigen, Multiple Myeloma, Salvage Therapy, Male, Female, Middle Aged, Immunotherapy, Adoptive, Aged, Retrospective Studies, Retreatment, Adult, Treatment Outcome, Recurrence, Receptors, Chimeric Antigen

Abstract

For patients with relapsed/refractory multiple myeloma with a relapse after B-cell maturation antigen (BCMA)-directed chimeric antigen receptor T-cell therapy (CAR-T), optimal salvage treatment strategies remain unclear. BCMA-directed CAR-T and bispecific antibodies (BsAbs) are now commercially available, and the outcomes for retreatment with BCMA-directed approaches are not well studied. We performed a retrospective analysis of 68 patients with relapsed disease after BCMA-directed CAR-T to evaluate outcomes and responses to salvage therapies. With a median follow-up of 13.5 months, median overall survival from time of relapse until death was 18 months (95% confidence interval [CI], 13.2 to not reached [NR]). Fifty-eight patients received subsequent myeloma-directed therapies, with a total of 265 lines of therapy (LOTs). The overall response rate for firstline salvage therapy was 41% (95% CI, 28-55). Among all LOTs, high response rates were observed among those receiving another BCMA-directed CAR-T (89%), BCMA-directed BsAbs (60%), CD38-directed combinations (80% when combined with BsAb; 50% when combined with immunomodulatory drugs and/or proteasome inhibitors), and alkylator-combinations (50% overall; 69% with high-dose alkylators). Thirty-four patients received at least 1 line of salvage BCMA-directed therapy; median progression-free survival was 8.3 months (95% CI, 7.9 to NR), 3.6 months (95% CI, 1.4 to NR), and 1 month (95% CI, 0.9 to NR) with median duration of response (DOR) of 8 months, 4.4 months, and 2.8 months for subsequent BCMA-directed CAR-T, BsAb, and belantamab mafadotin, respectively. Retreatment with BCMA-directed CAR-T and BsAbs can be effective salvage options after BCMA-directed CAR-T relapse; however, DORs appear limited, and further studies with new combinations and alternative targets are warranted.

Published

2024

29. CHMP2A regulates broad immune cell-mediated antitumor activity in an immunocompetent in vivo head and neck squamous cell carcinoma model

Author

Yun, Jiyoung, Saddawi-Konefka, Robert, Goldenson, Benjamin, Al-Msari, Riyam, Bernareggi, Davide, Thangaraj, Jaya L, Tang, Shiqi, Patel, Sonam H, Luna, Sarah M, Gutkind, J Silvio, and Kaufman, Dan

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Dental/Oral and Craniofacial Disease, Immunotherapy, Rare Diseases, Genetics, Cancer, 2.1 Biological and endogenous factors, 5.1 Pharmaceuticals, Good Health and Well Being, Animals, Humans, Mice, Cell Line, Tumor, Disease Models, Animal, Head and Neck Neoplasms, Immunocompetence, Killer Cells, Natural, Squamous Cell Carcinoma of Head and Neck, Immunity, Innate, Immunotherapy, Adoptive, Myeloid-Derived Suppressor Cells, Oncology and carcinogenesis

Abstract

BackgroundNatural killer (NK) cells are key effector cells of antitumor immunity. However, tumors can acquire resistance programs to escape NK cell-mediated immunosurveillance. Identifying mechanisms that mediate this resistance enables us to define approaches to improve immune-mediate antitumor activity. In previous studies from our group, a genome-wide CRISPR-Cas9 screen identified Charged Multivesicular Body Protein 2A (CHMP2A) as a novel mechanism that mediates tumor intrinsic resistance to NK cell activity.MethodsHere, we use an immunocompetent mouse model to demonstrate that CHMP2A serves as a targetable regulator of not only NK cell-mediated immunity but also other immune cell populations. Using the recently characterized murine 4MOSC model system, a syngeneic, tobacco-signature murine head and neck squamous cell carcinoma model, we deleted mCHMP2A using CRISPR/Cas9-mediated knock-out (KO), following orthotopic transplantation into immunocompetent hosts.ResultsWe found that mCHMP2A KO in 4MOSC1 cells leads to more potent NK-mediated tumor cell killing in vitro in these tumor cells. Moreover, following orthotopic transplantation, KO of mCHMP2A in 4MOSC1 cells, but not the more immune-resistant 4MOSC2 cells enables both T cells and NK cells to better mediate antitumor activity compared with wild type (WT) tumors. However, there was no difference in tumor development between WT and mCHMP2A KO 4MOSC1 or 4MOSC2 tumors when implanted in immunodeficient mice. Mechanistically, we find that mCHMP2A KO 4MOSC1 tumors transplanted into the immunocompetent mice had significantly increased CD4+T cells, CD8+T cells. NK cell, as well as fewer myeloid-derived suppressor cells (MDSC).ConclusionsTogether, these studies demonstrate that CHMP2A is a targetable inhibitor of cellular antitumor immunity.

Published

2024

30. Does the Timing of Cytoreductive Nephrectomy Impact Outcomes? Analysis of REMARCC Registry Data for Patients Receiving Tyrosine Kinase Inhibitor Versus Immune Checkpoint Inhibitor Therapy.

Author

Meagher, Margaret, Minervini, Andrea, Mir, Maria, Cerrato, Clara, Rebez, Giacomo, Autorino, Riccardo, Hampton, Lance, Campi, Riccardo, Kriegmair, Maximilian, Linares, Estefania, Hevia, Vital, Musquera, Maria, DAnna, Mauricio, Roussel, Eduard, Albersen, Maarten, Pavan, Nicola, Claps, Francesco, Antonelli, Alessandro, Marchioni, Michele, Paksoy, Nail, Erdem, Selcuk, and Derweesh, Ithaar

Subjects

Immunotherapy, Metastatic renal cell carcinoma, Nephrectomy, Survival, Tyrosine kinase inhibitor

Abstract

BACKGROUND AND OBJECTIVE: The role of cytoreductive nephrectomy (CN) in the treatment of metastatic renal cell carcinoma (mRCC) has been called into question on the basis of clinical trial data from the tyrosine kinase inhibitor (TKI) era. Comparative analyses of CN for patients treated with immuno-oncology (IO) versus TKI agents are sparse. Our objective was to compare CN timing and outcomes among patients who received TKI versus IO therapy. METHODS: This was a multicenter retrospective analysis of patients who underwent CN using data from the REMARCC (Registry of Metastatic RCC) database. The cohort was divided into TKI versus IO first-line therapy groups. The primary outcome was all-cause mortality (ACM). Secondary outcomes included cancer-specific mortality (CSM). Multivariable analysis was used to identify factors predictive for ACM and CSM. The Kaplan-Meier method was used to analyze 5-yr overall survival (OS) and cancer-specific survival (CSS) with stratification by primary systemic therapy and timing in relation to CN. KEY FINDINGS AND LIMITATIONS: We analyzed data for 189 patients (148 TKI + CN, 41 IO +CN; median follow-up 23.2 mo). Multivariable analysis revealed that a greater number of metastases (hazard ratio [HR] 1.06; p = 0.015), greater primary tumor size (HR 1.10; p = 0.043), TKI receipt (HR 2.36; p = 0.015), and initiation of systemic therapy after CN (HR 1.49; p = 0.039) were associated with worse ACM. A greater number of metastases at diagnosis (HR 1.07; p = 0.011), greater primary tumor size (HR 1.12; p = 0.018), TKI receipt (HR 5.43; p = 0.004), and initiation of systemic therapy after CN (HR 2.04; p

Published

2024

31. Epithelial Expressed B7-H4 Drives Differential Immunotherapy Response in Murine and Human Breast Cancer.

Author

Wescott, Elizabeth, Sun, Xiaopeng, Gonzalez-Ericsson, Paula, Hanna, Ann, Taylor, Brandie, Sanchez, Violeta, Bronzini, Juliana, Opalenik, Susan, Sanders, Melinda, Wulfkuhle, Julia, Gallagher, Rosa, Gomez, Henry, Isaacs, Claudine, Bharti, Vijaya, Wilson, John, Ballinger, Tarah, Santa-Maria, Cesar, Shah, Payal, Dees, Elizabeth, Lehmann, Brian, Abramson, Vandana, Brown Swigart, Lamorna, van ˈt Veer, Laura, Petricoin, Emanuel, Pietenpol, Jennifer, Balko, Justin, Esserman, Laura, and Hirst, Gillian

Subjects

V-Set Domain-Containing T-Cell Activation Inhibitor 1, Animals, Humans, Mice, Female, Cell Line, Tumor, Immunotherapy, Triple Negative Breast Neoplasms, Immune Checkpoint Inhibitors, Breast Neoplasms, B7-H1 Antigen, Epithelial Cells, Gene Expression Regulation, Neoplastic

Abstract

UNLABELLED: Combinations of immune checkpoint inhibitors (ICI, including anti-PD-1/PD-L1) and chemotherapy have been FDA approved for metastatic and early-stage triple-negative breast cancer (TNBC), but most patients do not benefit. B7-H4 is a B7 family ligand with proposed immunosuppressive functions being explored as a cancer immunotherapy target and may be associated with anti-PD-L1 resistance. However, little is known about its regulation and effect on immune cell function in breast cancers. We assessed murine and human breast cancer cells to identify regulation mechanisms of B7-H4 in vitro. We used an immunocompetent anti-PD-L1-sensitive orthotopic mammary cancer model and induced ectopic expression of B7-H4. We assessed therapy response and transcriptional changes at baseline and under treatment with anti-PD-L1. We observed B7-H4 was highly associated with epithelial cell status and transcription factors and found to be regulated by PI3K activity. EMT6 tumors with cell-surface B7-H4 expression were more resistant to immunotherapy. In addition, tumor-infiltrating immune cells had reduced immune activation signaling based on transcriptomic analysis. Paradoxically, in human breast cancer, B7-H4 expression was associated with survival benefit for patients with metastatic TNBC treated with carboplatin plus anti-PD-L1 and was associated with no change in response or survival for patients with early breast cancer receiving chemotherapy plus anti-PD-1. While B7-H4 induces tumor resistance to anti-PD-L1 in murine models, there are alternative mechanisms of signaling and function in human cancers. In addition, the strong correlation of B7-H4 to epithelial cell markers suggests a potential regulatory mechanism of B7-H4 independent of PD-L1. SIGNIFICANCE: This translational study confirms the association of B7-H4 expression with a cold immune microenvironment in breast cancer and offers preclinical studies demonstrating a potential role for B7-H4 in suppressing response to checkpoint therapy. However, analysis of two clinical trials with checkpoint inhibitors in the early and metastatic settings argue against B7-H4 as being a mechanism of clinical resistance to checkpoints, with clear implications for its candidacy as a therapeutic target.

Published

2024

32. Multi-omics Analysis Reveals Immune Features Associated with Immunotherapy Benefit in Patients with Squamous Cell Lung Cancer from Phase III Lung-MAP S1400I Trial.

Author

Parra, Edwin, Zhang, Jiexin, Duose, Dzifa, Gonzalez-Kozlova, Edgar, Redman, Mary, Chen, Hong, Manyam, Ganiraju, Kumar, Gayatri, Zhang, Jianhua, Song, Xingzhi, Lazcano, Rossana, Marques-Piubelli, Mario, Laberiano-Fernandez, Caddie, Rojas, Frank, Zhang, Baili, Taing, Len, Jhaveri, Aashna, Geisberg, Jacob, Altreuter, Jennifer, Michor, Franziska, Provencher, James, Yu, Joyce, Cerami, Ethan, Moravec, Radim, Kannan, Kasthuri, Luthra, Rajyalakshmi, Alatrash, Gheath, Huang, Hsin-Hui, Xie, Hui, Patel, Manishkumar, Nie, Kai, Harris, Jocelyn, Argueta, Kimberly, Lindsay, James, Biswas, Roshni, Van Nostrand, Stephen, Kim-Schulze, Seunghee, Gray, Jhanelle, Herbst, Roy, Wistuba, Ignacio, Gettinger, Scott, Kelly, Karen, Bazhenova, Lyudmila, Gnjatic, Sacha, Lee, J, Zhang, Jianjun, and Haymaker, Cara

Subjects

Humans, Nivolumab, Lung Neoplasms, Multiomics, Antineoplastic Combined Chemotherapy Protocols, Carcinoma, Non-Small-Cell Lung, Carcinoma, Squamous Cell, Immunotherapy, Lung, Epithelial Cells, Ipilimumab, Tumor Microenvironment

Abstract

PURPOSE: Identifying molecular and immune features to guide immune checkpoint inhibitor (ICI)-based regimens remains an unmet clinical need. EXPERIMENTAL DESIGN: Tissue and longitudinal blood specimens from phase III trial S1400I in patients with metastatic squamous non-small cell carcinoma (SqNSCLC) treated with nivolumab monotherapy (nivo) or nivolumab plus ipilimumab (nivo+ipi) were subjected to multi-omics analyses including multiplex immunofluorescence (mIF), nCounter PanCancer Immune Profiling Panel, whole-exome sequencing, and Olink. RESULTS: Higher immune scores from immune gene expression profiling or immune cell infiltration by mIF were associated with response to ICIs and improved survival, except regulatory T cells, which were associated with worse overall survival (OS) for patients receiving nivo+ipi. Immune cell density and closer proximity of CD8+GZB+ T cells to malignant cells were associated with superior progression-free survival and OS. The cold immune landscape of NSCLC was associated with a higher level of chromosomal copy-number variation (CNV) burden. Patients with LRP1B-mutant tumors had a shorter survival than patients with LRP1B-wild-type tumors. Olink assays revealed soluble proteins such as LAMP3 increased in responders while IL6 and CXCL13 increased in nonresponders. Upregulation of serum CXCL13, MMP12, CSF-1, and IL8 were associated with worse survival before radiologic progression. CONCLUSIONS: The frequency, distribution, and clustering of immune cells relative to malignant ones can impact ICI efficacy in patients with SqNSCLC. High CNV burden may contribute to the cold immune microenvironment. Soluble inflammation/immune-related proteins in the blood have the potential to monitor therapeutic benefit from ICI treatment in patients with SqNSCLC.

Published

2024

33. Neoadjuvant followed by adjuvant pembrolizumab in melanoma: time biases in the data analysis of the SWOG S1801 trial.

Author

Olivier, Timothée and Prasad, Vinayak

Subjects

Immunotherapy, Informative censoring, Melanoma, Neoadjuvant

Abstract

The SWOG S1801 trial investigated the role of pembrolizumab, an anti-PD1 immune checkpoint inhibitor, in the perioperative setting of stage III or IV melanoma. This phase 2 trial compared two groups: one receiving pembrolizumab both before and after surgery (neoadjuvant-adjuvant), and another receiving it only post-surgery (adjuvant-only), with event-free survival (EFS) as the primary endpoint. Neoadjuvant strategies, involving pre-surgical drug administration, potentially offer rapid tumor control and a unique opportunity to assess tumor response. However, they may expose to toxicity and delay or preclude surgery. The study met its primary endpoint, with a 72 % EFS rate in the neoadjuvant-adjuvant group, and 49 % in the adjuvant group. Here, we question the results applicability with three potential limitations. Key concerns include an arbitrary rule in event assignment, possibly affecting the event distribution over time. Second, different rates of early censoring between groups introduce the possibility of informative censoring, which could have led to an artefactual benefit in EFS. Lastly, phase 2 trial results, by definition, carry risk of fluke results, and should be confirmed in phase 3 trial before wide adoption. Collectively, these factors must be integrated into a careful interpretation of the SWOG S1801 trial outcomes. More robust data are needed to fully appraise strengths and limitations of neoadjuvant pembrolizumab in melanoma treatment.

Published

2024

34. Phase 1 study combining elotuzumab with autologous stem cell transplant and lenalidomide for multiple myeloma.

Author

Coffey, David, Osman, Keren, Aleman, Adolfo, Bekri, Selma, Kats, Simone, Dhadwal, Amishi, Catamero, Donna, Kim-Schulze, Seunghee, Gnjatic, Sacha, Chari, Ajai, Parekh, Samir, Jagannath, Sundar, and Cho, Hearn

Subjects

hematologic neoplasms, immunotherapy, transplantation immunology, tumor microenvironment, Humans, Lenalidomide, Multiple Myeloma, Hematopoietic Stem Cell Transplantation, Leukocytes, Mononuclear, Transplantation, Autologous, Stem Cell Transplantation, Tumor Microenvironment, Antibodies, Monoclonal, Humanized

Abstract

BACKGROUND: Autologous stem cell transplantation (ASCT) after induction therapy improves disease-free survival for patients with multiple myeloma (MM). While the goal of ASCT is to render a minimal disease state, it is also associated with eradication of immunosuppressive cells, and we hypothesize that early introduction of immunotherapy post-ASCT may provide a window of opportunity to boost treatment efficacy. METHODS: We conducted a phase 1 clinical trial to investigate the application of autologous lymphocyte infusion and anti-SLAMF7 monoclonal antibody, elotuzumab, after ASCT in patients with newly diagnosed MM previously treated with induction therapy. In addition to CD34+ stem cells, peripheral blood mononuclear cells were harvested prior to transplant and infused on day 3 after stem cell infusion to accelerate immune reconstitution and provide autologous natural killer (NK) cells that are essential to the mechanism of elotuzumab. Elotuzumab was administered starting on day 4 and then every 28 days after until 1 year post-ASCT. Cycles 4-12 were administered with standard-of-care lenalidomide maintenance. RESULTS: All subjects were evaluated for safety, and 13 of 15 subjects completed the treatment protocol. At 1 year post-ASCT, the disease status of enrolled subjects was as follows: five stringent complete responses, one complete response, six very good partial responses, one partial response, and two progressive diseases. The treatment plan was well tolerated, with most grade 3 and 4 AEs being expected hematologic toxicities associated with ASCT. Correlative analysis of the immune microenvironment demonstrated a trend toward reduced regulatory T cells during the first 3 months post-transplant followed by an increase in NK cells and monocytes in patients achieving a complete remission. CONCLUSIONS: This phase 1 clinical trial demonstrates that early introduction of immunotherapy after ASCT is well tolerated and shows promising disease control in patients with MM, accompanied by favorable changes in the immune microenvironment. TRIAL REGISTRATION NUMBER: NCT02655458.

Published

2024

35. Targeting pathogenic CD8+ tissue-resident T cells with chimeric antigen receptor therapy in murine autoimmune cholangitis.

Author

Zhu, Hao-Xian, Yang, Shu-Han, Gao, Cai-Yue, Bian, Zhen-Hua, Chen, Xiao-Min, Huang, Rong-Rong, Meng, Qian-Li, Li, Xin, Jin, Haosheng, Tsuneyama, Koichi, Han, Ying, Li, Liang, Zhao, Zhi-Bin, Gershwin, M, and Lian, Zhe-Xiong

Subjects

Mice, Animals, Liver Cirrhosis, Biliary, Immunotherapy, Adoptive, Programmed Cell Death 1 Receptor, CD8-Positive T-Lymphocytes, Cholangitis, Autoimmune Diseases

Abstract

Primary biliary cholangitis (PBC) is a cholestatic autoimmune liver disease characterized by autoreactive T cell response against intrahepatic small bile ducts. Here, we use Il12b-/-Il2ra-/- mice (DKO mice) as a model of autoimmune cholangitis and demonstrate that Cd8a knockout or treatment with an anti-CD8α antibody prevents/reduces biliary immunopathology. Using single-cell RNA sequencing analysis, we identified CD8+ tissue-resident memory T (Trm) cells in the livers of DKO mice, which highly express activation- and cytotoxicity-associated markers and induce apoptosis of bile duct epithelial cells. Liver CD8+ Trm cells also upregulate the expression of several immune checkpoint molecules, including PD-1. We describe the development of a chimeric antigen receptor to target PD-1-expressing CD8+ Trm cells. Treatment of DKO mice with PD-1-targeting CAR-T cells selectively depleted liver CD8+ Trm cells and alleviated autoimmune cholangitis. Our work highlights the pathogenic role of CD8+ Trm cells and the potential therapeutic usage of PD-1-targeting CAR-T cells.

Published

2024

36. Preclinical evaluation and first-in-dog clinical trials of PBMC-expanded natural killer cells for adoptive immunotherapy in dogs with cancer

Author

Razmara, Aryana M, Farley, Lauren E, Harris, Rayna M, Judge, Sean J, Lammers, Marshall, Iranpur, Khurshid R, Johnson, Eric G, Dunai, Cordelia, Murphy, William J, Brown, C Titus, Rebhun, Robert B, Kent, Michael S, and Canter, Robert J

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Clinical Trials and Supportive Activities, Vaccine Related, Biotechnology, Genetics, Clinical Research, Immunization, Immunotherapy, Rare Diseases, Cancer, 5.2 Cellular and gene therapies, Dogs, Animals, Humans, Immunotherapy, Adoptive, Leukocytes, Mononuclear, Cytotoxicity, Immunologic, Killer Cells, Natural, Osteosarcoma, Bone Neoplasms, Cytokines, killer cells, natural, immunotherapy, adoptive, computational biology, clinical trials as topic, adoptive cell therapy, Oncology and carcinogenesis

Abstract

BackgroundNatural killer (NK) cells are cytotoxic cells capable of recognizing heterogeneous cancer targets without prior sensitization, making them promising prospects for use in cellular immunotherapy. Companion dogs develop spontaneous cancers in the context of an intact immune system, representing a valid cancer immunotherapy model. Previously, CD5 depletion of peripheral blood mononuclear cells (PBMCs) was used in dogs to isolate a CD5dim-expressing NK subset prior to co-culture with an irradiated feeder line, but this can limit the yield of the final NK product. This study aimed to assess NK activation, expansion, and preliminary clinical activity in first-in-dog clinical trials using a novel system with unmanipulated PBMCs to generate our NK cell product.MethodsStarting populations of CD5-depleted cells and PBMCs from healthy beagle donors were co-cultured for 14 days, phenotype, cytotoxicity, and cytokine secretion were measured, and samples were sequenced using the 3'-Tag-RNA-Seq protocol. Co-cultured human PBMCs and NK-isolated cells were also sequenced for comparative analysis. In addition, two first-in-dog clinical trials were performed in dogs with melanoma and osteosarcoma using autologous and allogeneic NK cells, respectively, to establish safety and proof-of-concept of this manufacturing approach.ResultsCalculated cell counts, viability, killing, and cytokine secretion were equivalent or higher in expanded NK cells from canine PBMCs versus CD5-depleted cells, and immune phenotyping confirmed a CD3-NKp46+ product from PBMC-expanded cells at day 14. Transcriptomic analysis of expanded cell populations confirmed upregulation of NK activation genes and related pathways, and human NK cells using well-characterized NK markers closely mirrored canine gene expression patterns. Autologous and allogeneic PBMC-derived NK cells were successfully expanded for use in first-in-dog clinical trials, resulting in no serious adverse events and preliminary efficacy data. RNA sequencing of PBMCs from dogs receiving allogeneic NK transfer showed patient-unique gene signatures with NK gene expression trends in response to treatment.ConclusionsOverall, the use of unmanipulated PBMCs appears safe and potentially effective for canine NK immunotherapy with equivalent to superior results to CD5 depletion in NK expansion, activation, and cytotoxicity. Our preclinical and clinical data support further evaluation of this technique as a novel platform for optimizing NK immunotherapy in dogs.

Published

2024

37. Locoregional delivery of IL-13Rα2-targeting CAR-T cells in recurrent high-grade glioma: a phase 1 trial

Author

Brown, Christine E, Hibbard, Jonathan C, Alizadeh, Darya, Blanchard, M Suzette, Natri, Heini M, Wang, Dongrui, Ostberg, Julie R, Aguilar, Brenda, Wagner, Jamie R, Paul, Jinny A, Starr, Renate, Wong, Robyn A, Chen, Wuyang, Shulkin, Noah, Aftabizadeh, Maryam, Filippov, Aleksandr, Chaudhry, Ammar, Ressler, Julie A, Kilpatrick, Julie, Myers-McNamara, Paige, Chen, Mike, Wang, Leo D, Rockne, Russell C, Georges, Joseph, Portnow, Jana, Barish, Michael E, D’Apuzzo, Massimo, Banovich, Nicholas E, Forman, Stephen J, and Badie, Behnam

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Immunology, Neurosciences, Rare Diseases, Brain Cancer, Cancer, Clinical Research, Orphan Drug, Clinical Trials and Supportive Activities, Brain Disorders, Vaccine Related, 6.2 Cellular and gene therapies, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, T-Lymphocytes, Humans, Glioma, Glioblastoma, Neoplasm Recurrence, Local, Immunotherapy, Adoptive, Receptors, Chimeric Antigen, Medical and Health Sciences, Biomedical and clinical sciences, Health sciences

Abstract

Chimeric antigen receptor T cell (CAR-T) therapy is an emerging strategy to improve treatment outcomes for recurrent high-grade glioma, a cancer that responds poorly to current therapies. Here we report a completed phase I trial evaluating IL-13Rα2-targeted CAR-T cells in 65 patients with recurrent high-grade glioma, the majority being recurrent glioblastoma (rGBM). Primary objectives were safety and feasibility, maximum tolerated dose/maximum feasible dose and a recommended phase 2 dose plan. Secondary objectives included overall survival, disease response, cytokine dynamics and tumor immune contexture biomarkers. This trial evolved to evaluate three routes of locoregional T cell administration (intratumoral (ICT), intraventricular (ICV) and dual ICT/ICV) and two manufacturing platforms, culminating in arm 5, which utilized dual ICT/ICV delivery and an optimized manufacturing process. Locoregional CAR-T cell administration was feasible and well tolerated, and as there were no dose-limiting toxicities across all arms, a maximum tolerated dose was not determined. Probable treatment-related grade 3+ toxicities were one grade 3 encephalopathy and one grade 3 ataxia. A clinical maximum feasible dose of 200 × 106 CAR-T cells per infusion cycle was achieved for arm 5; however, other arms either did not test or achieve this dose due to manufacturing feasibility. A recommended phase 2 dose will be refined in future studies based on data from this trial. Stable disease or better was achieved in 50% (29/58) of patients, with two partial responses, one complete response and a second complete response after additional CAR-T cycles off protocol. For rGBM, median overall survival for all patients was 7.7 months and for arm 5 was 10.2 months. Central nervous system increases in inflammatory cytokines, including IFNγ, CXCL9 and CXCL10, were associated with CAR-T cell administration and bioactivity. Pretreatment intratumoral CD3 T cell levels were positively associated with survival. These findings demonstrate that locoregional IL-13Rα2-targeted CAR-T therapy is safe with promising clinical activity in a subset of patients. ClinicalTrials.gov Identifier: NCT02208362 .

Published

2024

38. Soluble immune checkpoint factors reflect exhaustion of antitumor immunity and response to PD-1 blockade.

Author

Kurosaki, Takashi, Togashi, Yosuke, Fukuoka, Kazuya, Goto, Megumi, Chiba, Yasutaka, Tomida, Shuta, Ota, Takayo, Haratani, Koji, Takahama, Takayuki, Tanizaki, Junko, Yoshida, Takeshi, Iwasa, Tsutomu, Tanaka, Kaoru, Takeda, Masayuki, Hirano, Tomoko, Yoshida, Hironori, Ozasa, Hiroaki, Sakamori, Yuichi, Sakai, Kazuko, Higuchi, Keiko, Uga, Hitoshi, Suminaka, Chihiro, Hirai, Toyohiro, Nishio, Kazuto, Nakagawa, Kazuhiko, Honjo, Tasuku, Hayashi, Hidetoshi, Chamoto, Kenji, and Hatae, Ryusuke

Subjects

Immunotherapy, Lung cancer, Oncology, T cells, Humans, B7-H1 Antigen, Carcinoma, Non-Small-Cell Lung, Immunologic Factors, Lung Neoplasms, Programmed Cell Death 1 Receptor, Immune Checkpoint Inhibitors

Abstract

BACKGROUNDPrecise stratification of patients with non-small cell lung cancer (NSCLC) is needed for appropriate application of PD-1/PD-L1 blockade therapy.METHODSWe measured soluble forms of the immune-checkpoint molecules PD-L1, PD-1, and CTLA-4 in plasma of patients with advanced NSCLC before PD-1/PD-L1 blockade. A prospective biomarker-finding trial (cohort A) included 50 previously treated patients who received nivolumab. A retrospective observational study was performed for patients treated with any PD-1/PD-L1 blockade therapy (cohorts B and C), cytotoxic chemotherapy (cohort D), or targeted therapy (cohort E). Plasma samples from all patients were assayed for soluble immune-checkpoint molecules with a highly sensitive chemiluminescence-based assay.RESULTSNonresponsiveness to PD-1/PD-L1 blockade therapy was associated with higher concentrations of these soluble immune factors among patients with immune-reactive (hot) tumors. Such an association was not apparent for patients treated with cytotoxic chemotherapy or targeted therapy. Integrative analysis of tumor size, PD-L1 expression in tumor tissue (tPD-L1), and gene expression in tumor tissue and peripheral CD8+ T cells revealed that high concentrations of the 3 soluble immune factors were associated with hyper or terminal exhaustion of antitumor immunity. The combination of soluble PD-L1 (sPD-L1) and sCTLA-4 efficiently discriminated responsiveness to PD-1/PD-L1 blockade among patients with immune-reactive tumors.CONCLUSIONCombinations of soluble immune factors might be able to identify patients unlikely to respond to PD-1/PD-L1 blockade as a result of terminal exhaustion of antitumor immunity. Our data suggest that such a combination better predicts, along with tPD-L1, for the response of patients with NSCLC.TRIAL REGISTRATIONUMIN000019674.FUNDINGThis study was funded by Ono Pharmaceutical Co. Ltd. and Sysmex Corporation.

Published

2024

39. Engineering a Programmed Death-Ligand 1-Targeting Monobody Via Directed Evolution for SynNotch-Gated Cell Therapy.

Author

Zhu, Linshan, Man, Chi-Wei, Harrison, Reed, Wu, Zhuohang, Limsakul, Praopim, Peng, Qin, Hashimoto, Matthew, Mamaril, Anthony, Xu, Hongquan, Liu, Longwei, and Wang, Yingxiao

Subjects

CAR T cell therapy, Directed evolution, Monobody, PD-L1, SynNotch, Yeast surface display, Humans, Mice, Animals, Receptors, Antigen, T-Cell, B7-H1 Antigen, Ligands, Cell Line, Tumor, T-Lymphocytes, Immunotherapy, Adoptive

Abstract

Programmed death-ligand 1 (PD-L1) is a promising target for cancer immunotherapy due to its ability to inhibit T cell activation; however, its expression on various noncancer cells may cause on-target off-tumor toxicity when designing PD-L1-targeting Chimeric Antigen Receptor (CAR) T cell therapies. Combining rational design and directed evolution of the human fibronectin-derived monobody scaffold, PDbody was engineered to bind to PD-L1 with a preference for a slightly lower pH, which is typical in the tumor microenvironment. PDbody was further utilized as a CAR to target the PD-L1-expressing triple negative MDA-MB-231 breast cancer cell line. To mitigate on-target off-tumor toxicity associated with targeting PD-L1, a Cluster of Differentiation 19 (CD19)-recognizing SynNotch IF THEN gate was integrated into the system. This CD19-SynNotch PDbody-CAR system was then expressed in primary human T cells to target CD19-expressing MDA-MB-231 cancer cells. These CD19-SynNotch PDbody-CAR T cells demonstrated both specificity and efficacy in vitro, accurately eradicating cancer targets in cytotoxicity assays. Moreover, in an in vivo bilateral murine tumor model, they exhibited the capability to effectively restrain tumor growth. Overall, CD19-SynNotch PDbody-CAR T cells represent a distinct development over previously published designs due to their increased efficacy, proliferative capability, and mitigation of off-tumor toxicity for solid tumor treatment.

Published

2024

40. Outpatient COVID-19 convalescent plasma recipient antibody thresholds correlated to reduced hospitalizations within a randomized trial.

Author

Park, Han-Sol, Yin, Anna, Barranta, Caelan, Lee, John, Caputo, Christopher, Sachithanandham, Jaiprasath, Li, Maggie, Yoon, Steve, Sitaras, Ioannis, Jedlicka, Anne, Eby, Yolanda, Ram, Malathi, Fernandez, Reinaldo, Baker, Owen, Shenoy, Aarthi, Mosnaim, Giselle, Fukuta, Yuriko, Patel, Bela, Heath, Sonya, Levine, Adam, Meisenberg, Barry, Spivak, Emily, Anjan, Shweta, Huaman, Moises, Blair, Janis, Zand, Martin, Cachay, Edward, Raval, Jay, Kassaye, Seble, Marshall, Christi, Yarava, Anusha, Lane, Karen, McBee, Nichol, Gawad, Amy, Karlen, Nicky, Singh, Atika, Ford, Daniel, Jabs, Douglas, Appel, Lawrence, Shade, David, Lau, Bryan, Ehrhardt, Stephan, Baksh, Sheriza, Shapiro, Janna, Ou, Jiangda, Na, Yu, Knoll, Maria, Ornelas-Gatdula, Elysse, Arroyo-Curras, Netzahualcoyotl, Gniadek, Thomas, Caturegli, Patrizio, Wu, Jinke, Ndahiro, Nelson, Betenbaugh, Michael, Hanley, Daniel, Casadevall, Arturo, Shoham, Shmuel, Bloch, Evan, Gebo, Kelly, Tobian, Aaron, Laeyendecker, Oliver, Pekosz, Andrew, Klein, Sabra, Sullivan, David, Paxton, James, Gerber, Jonathan, Petrini, Joann, Broderick, Patrick, Rausch, William, Cordisco, Marie, Hammel, Jean, Greenblatt, Benjamin, Cluzet, Valerie, Cruser, Daniel, Oei, Kevin, Abinante, Matthew, Hammitt, Laura, Sutcliffe, Catherine, Currier, Judith, Forthal, Donald, and Ziman, Alyssa

Subjects

COVID-19, Immunoglobulins, Immunotherapy, Humans, COVID-19, COVID-19 Serotherapy, Antibodies, Viral, Immunization, Passive, Hospitalization, SARS-CoV-2, Male, Female, Middle Aged, Adult, Immunoglobulin G, Antibodies, Neutralizing, Double-Blind Method, Aged, Blood Donors, Outpatients

Abstract

BACKGROUNDCOVID-19 convalescent plasma (CCP) virus-specific antibody levels that translate into recipient posttransfusion antibody levels sufficient to prevent disease progression are not defined.METHODSThis secondary analysis correlated donor and recipient antibody levels to hospitalization risk among unvaccinated, seronegative CCP recipients within the outpatient, double-blind, randomized clinical trial that compared CCP to control plasma. The majority of COVID-19 CCP arm hospitalizations (15/17, 88%) occurred in this unvaccinated, seronegative subgroup. A functional cutoff to delineate recipient high versus low posttransfusion antibody levels was established by 2 methods: (i) analyzing virus neutralization-equivalent anti-Spike receptor-binding domain immunoglobulin G (anti-S-RBD IgG) responses in donors or (ii) receiver operating characteristic (ROC) curve analysis.RESULTSSARS-CoV-2 anti-S-RBD IgG antibody was volume diluted 21.3-fold into posttransfusion seronegative recipients from matched donor units. Virus-specific antibody delivered was approximately 1.2 mg. The high-antibody recipients transfused early (symptom onset within 5 days) had no hospitalizations. A CCP-recipient analysis for antibody thresholds correlated to reduced hospitalizations found a statistical significant association between early transfusion and high antibodies versus all other CCP recipients (or control plasma), with antibody cutoffs established by both methods-donor-based virus neutralization cutoffs in posttransfusion recipients (0/85 [0%] versus 15/276 [5.6%]; P = 0.03) or ROC-based cutoff (0/94 [0%] versus 15/267 [5.4%]; P = 0.01).CONCLUSIONIn unvaccinated, seronegative CCP recipients, early transfusion of plasma units in the upper 30% of study donors antibody levels reduced outpatient hospitalizations. High antibody level plasma units, given early, should be reserved for therapeutic use.TRIAL REGISTRATIONClinicalTrials.gov NCT04373460.FUNDINGDepartment of Defense (W911QY2090012); Defense Health Agency; Bloomberg Philanthropies; the State of Maryland; NIH (3R01AI152078-01S1, U24TR001609-S3, 1K23HL151826NIH); the Mental Wellness Foundation; the Moriah Fund; Octapharma; the Healthnetwork Foundation; the Shear Family Foundation; the NorthShore Research Institute; and the Rice Foundation.

Published

2024

41. Metastatic melanoma to small bowel: metastasectomy is supported in the era of immunotherapy and checkpoint inhibitors.

Author

Wong, Paul, Wisneski, Andrew, Tsai, Katy, Chang, Tammy, Hirose, Kenzo, Nakakura, Eric, Daud, Adil, Maker, Ajay, and Corvera, Carlos

Subjects

Checkpoint Inhibitors, Immunotherapy, Melanoma, Metastasectomy, Small Bowel Resection, Humans, Male, Female, Adult, Middle Aged, Aged, Aged, 80 and over, Melanoma, Metastasectomy, Quality of Life, Immunotherapy, Intestine, Small, Retrospective Studies

Abstract

BACKGROUND: Metastatic melanoma to the small bowel is an aggressive disease often accompanied by obstruction, abdominal pain, and gastrointestinal bleeding. With advancements in melanoma treatment, the role for metastasectomy continues to evolve. Inclusion of novel immunotherapeutic agents, such as checkpoint inhibitors, into standard treatment regimens presents potential survival benefits for patients receiving metastasectomy. CASE PRESENTATION: We report an institutional experience of 15 patients (12 male, 3 female) between 2014-2022 that underwent small bowel metastasectomy for metastatic melanoma and received perioperative systemic treatment. Median age of patients was 64 years (range: 35-83 years). No patients died within 30 days of their surgery, and the median hospital length of stay was 5 days. Median overall survival in these patients was 30.1 months (range: 2-115 months). Five patients died from disease (67 days, 252 days, 426 days, 572 days, 692 days postoperatively), one patient died of non-disease related causes (1312 days postoperatively), six patients are alive with disease, and three remain disease free. CONCLUSIONS: This case series presents an updated perspective of the utility of metastasectomy for small bowel metastasis in the age of novel immunotherapeutic agents as standard systemic treatment. Small bowel metastasectomy for advanced melanoma performed in conjunction with perioperative systemic therapy is safe and appears to promote long-term survival and enhanced quality of life.

Published

2024

42. Disentangling tau: One protein, many therapeutic approaches

Author

Lane-Donovan, Courtney and Boxer, Adam L

Subjects

Biomedical and Clinical Sciences, Biological Psychology, Neurosciences, Psychology, Pharmacology and Pharmaceutical Sciences, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Frontotemporal Dementia (FTD), Aging, Rare Diseases, Neurodegenerative, Alzheimer's Disease, Dementia, Brain Disorders, Acquired Cognitive Impairment, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Aetiology, 2.1 Biological and endogenous factors, Neurological, Humans, tau Proteins, Alzheimer Disease, Tauopathies, Supranuclear Palsy, Progressive, Neurodegenerative Diseases, Tau, Neurodegeneration, Alzheimer's disease, Progressive supranuclear palsy, Immunotherapy, Clinical trials, Public Health and Health Services, Neurology & Neurosurgery, Pharmacology and pharmaceutical sciences, Biological psychology

Abstract

The tauopathies encompass over 20 adult neurodegenerative diseases and are characterized by the dysfunction and accumulation of insoluble tau protein. Among them, Alzheimer's disease, frontotemporal dementia, and progressive supranuclear palsy collectively impact millions of patients and their families worldwide. Despite years of drug development using a variety of mechanisms of action, no therapeutic directed against tau has been approved for clinical use. This raises important questions about our current model of tau pathology and invites thoughtful consideration of our approach to nonclinical models and clinical trial design. In this article, we review what is known about the biology and genetics of tau, placing it in the context of current and failed clinical trials. We highlight potential reasons for the lack of success to date and offer suggestions for new pathways in therapeutic development. Overall, our viewpoint to the future is optimistic for this important group of neurodegenerative diseases.

Published

2024

43. Suppressive effects of obesity on NK cells: is it time to incorporate obesity as a clinical variable for NK cell-based cancer immunotherapy regimens?

Author

Canter, Robert J, Judge, Sean J, Collins, Craig P, Yoon, Daniel Jaeho, and Murphy, William J

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Killer Cells, Natural, Humans, Neoplasms, Obesity, Immunotherapy, Clinical Trials as Topic, Oncology and carcinogenesis

Abstract

Abstract:

Published

2024

44. INCUBATING BUSINESS: Raleigh's NovaQuest expands beyond financing drug trials to startup investing

Author

Roush, Chris

Subjects

Immunotherapy, Government aid, Government funding, Company financing, Business, Business, regional

Abstract

Ramin Karimpour, the CEO of agriculture-tech startup Targan, had been funding the company with a variety of government grants and even his 2015 $1 million dollar ticket. But he was [...]

Published

2024

45. Alteraciones neoplásicas en personas con enfermedad renal crónica en hemodiálisis: un análisis retrospectivo

Author

Pardo-Vicastillo, Vanesa, Andrino-Llorente, María Teresa, Marks-Álvarez, Marta, and Quiroga-Gili, Borja

Published

2024

46. Melanoma medicine: New drugs for melanoma and the role of the general practitioner

Author

Boutros, Andrea, Carlino, Matteo S, and Menzies, Alexander M

Published

2024

47. Expert consensus guidelines on management and best practices for tumor-infiltrating lymphocyte cell therapy.

Author

Betof Warner, Allison, Hamid, Omid, Komanduri, Krishna, Amaria, Rodabe, Butler, Marcus, Haanen, John, Nikiforow, Sarah, Puzanov, Igor, Sarnaik, Amod, Bishop, Michael, and Schoenfeld, Adam

Subjects

Adoptive cell therapy - ACT, Infusion, Skin Cancer, T cell, Tumor infiltrating lymphocyte - TIL, United States, Humans, Immunotherapy, Adoptive, Lymphocytes, Tumor-Infiltrating, Melanoma, Combined Modality Therapy, Cell- and Tissue-Based Therapy

Abstract

Adoptive cell therapy with autologous, ex vivo-expanded, tumor-infiltrating lymphocytes (TILs) is being investigated for treatment of solid tumors and has shown robust responses in clinical trials. Based on the encouraging efficacy, tolerable safety profile, and advancements in a central manufacturing process, lifileucel is now the first US Food and Drug Administration (FDA)-approved TIL cell therapy product. To this end, treatment management and delivery practice guidance is needed to ensure successful integration of this modality into clinical care. This review includes clinical and toxicity management guidelines pertaining to the TIL cell therapy regimen prepared by the TIL Working Group, composed of internationally recognized hematologists and oncologists with expertize in TIL cell therapy, and relates to patient care and operational aspects. Expert consensus recommendations for patient management, including patient eligibility, screening tests, and clinical and toxicity management with TIL cell therapy, including tumor tissue procurement surgery, non-myeloablative lymphodepletion, TIL infusion, and IL-2 administration, are discussed in the context of potential standard of care TIL use. These recommendations provide practical guidelines for optimal clinical management during administration of the TIL cell therapy regimen, and recognition of subsequent management of toxicities. These guidelines are focused on multidisciplinary teams of physicians, nurses, and stakeholders involved in the care of these patients.

Published

2024

48. Synergistic combination therapy using cowpea mosaic virus intratumoral immunotherapy and Lag-3 checkpoint blockade.

Author

Karan, Sweta, Jung, Eunkyeong, Boone, Christine, and Steinmetz, Nicole

Subjects

Checkpoint therapy, Cowpea mosaic virus, Intratumoral immunotherapy, Lag-3, Humans, Animals, Mice, Comovirus, Combined Modality Therapy, Immunotherapy, Disease Models, Animal, Melanoma

Abstract

Immune checkpoint therapy (ICT) for cancer can yield dramatic clinical responses; however, these may only be observed in a minority of patients. These responses can be further limited by subsequent disease recurrence and resistance. Combination immunotherapy strategies are being developed to overcome these limitations. We have previously reported enhanced efficacy of combined intratumoral cowpea mosaic virus immunotherapy (CPMV IIT) and ICT approaches. Lymphocyte-activation gene-3 (LAG-3) is a next-generation inhibitory immune checkpoint with broad expression across multiple immune cell subsets. Its expression increases on activated T cells and contributes to T cell exhaustion. We observed heightened efficacy of a combined CPMV IIT and anti-LAG-3 treatment in a mouse model of melanoma. Further, LAG-3 expression was found to be increased within the TME following intratumoral CPMV administration. The integration of CPMV IIT with LAG-3 inhibition holds significant potential to improve treatment outcomes by concurrently inducing a comprehensive anti-tumor immune response, enhancing local immune activation, and mitigating T cell exhaustion.

Published

2024

49. Enhancing cancer immunotherapy via inhibition of soluble epoxide hydrolase

Author

Kelly, Abigail G, Wang, Weicang, Rothenberger, Eva, Yang, Jun, Gilligan, Molly M, Kipper, Franciele C, Attaya, Ahmed, Gartung, Allison, Hwang, Sung Hee, Gillespie, Michael J, Bayer, Rachel L, Quinlivan, Katherine M, Torres, Kimberly L, Huang, Sui, Mitsiades, Nicholas, Yang, Haixia, Hammock, Bruce D, and Panigrahy, Dipak

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Complementary and Integrative Health, Dietary Supplements, Immunotherapy, Nutrition, Cancer, 5.1 Pharmaceuticals, 2.1 Biological and endogenous factors, Development of treatments and therapeutic interventions, Aetiology, Mice, Humans, Animals, Epoxide Hydrolases, Fatty Acids, Inflammation, Neoplasms, Tumor Microenvironment, immunonutrition, omega-3 fatty acids, eicosanoid, soluble epoxide hydrolase, inflammation resolution

Abstract

Cancer therapy, including immunotherapy, is inherently limited by chronic inflammation-induced tumorigenesis and toxicity within the tumor microenvironment. Thus, stimulating the resolution of inflammation may enhance immunotherapy and improve the toxicity of immune checkpoint inhibition (ICI). As epoxy-fatty acids (EpFAs) are degraded by the enzyme soluble epoxide hydrolase (sEH), the inhibition of sEH increases endogenous EpFA levels to promote the resolution of cancer-associated inflammation. Here, we demonstrate that systemic treatment with ICI induces sEH expression in multiple murine cancer models. Dietary omega-3 polyunsaturated fatty acid supplementation and pharmacologic sEH inhibition, both alone and in combination, significantly enhance anti-tumor activity of ICI in these models. Notably, pharmacological abrogation of the sEH pathway alone or in combination with ICI counter-regulates an ICI-induced pro-inflammatory and pro-tumorigenic cytokine storm. Thus, modulating endogenous EpFA levels through dietary supplementation or sEH inhibition may represent a unique strategy to enhance the anti-tumor activity of paradigm cancer therapies.

Published

2024

50. CAR-T cell manufacturing: Major process parameters and next-generation strategies.

Author

Ayala Ceja, Melanie, Khericha, Mobina, Harris, Caitlin, Puig-Saus, Cristina, and Chen, Yvonne

Subjects

Humans, Autoimmune Diseases, Immunotherapy, Adoptive, T-Lymphocytes

Abstract

Chimeric antigen receptor (CAR)-T cell therapies have demonstrated strong curative potential and become a critical component in the array of B-cell malignancy treatments. Successful deployment of CAR-T cell therapies to treat hematologic and solid cancers, as well as other indications such as autoimmune diseases, is dependent on effective CAR-T cell manufacturing that impacts not only product safety and efficacy but also overall accessibility to patients in need. In this review, we discuss the major process parameters of autologous CAR-T cell manufacturing, as well as regulatory considerations and ongoing developments that will enable the next generation of CAR-T cell therapies.

Published

2024