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1. PemBla: A Phase 1 study of intravesical pembrolizumab in recurrent non‐muscle‐invasive bladder cancer

Author

Woodcock, VK, Chen, J-L, Purshouse, K, Butcher, C, Collins, L, Haddon, C, Verrall, G, Elhussein, L, Roberts, C, Tarlton, A, Rei, M, Napolitani, G, Salio, M, Middleton, MR, Cerundolo, V, Crew, J, and Protheroe, AS

Subjects
General Medicine
Abstract

Objectives: This study aimed to investigate the anti-PD-1 inhibitor pembrolizumab as a potential agent for use in non-muscle-invasive bladder cancer (NMIBC) by conducting a Phase 1 safety run-in study to assess the safety and tolerability of intravesical pembrolizumab after transurethral resection of the bladder tumour (TURBT). Patients and methods: Eligible patients had recurrent NMIBC for which adjuvant treatment post TURBT was a reasonable treatment option, Eastern Cooperative Oncology Group Performance Status (ECOG PS) 0–1 and adequate end-organ function. Pembrolizumab was administered by intravesical instillation once weekly for a total of six doses. Intra-patient dose escalation was performed in three paired patient cohorts with doses starting at 50 mg and increasing through 100 mg to a maximum of 200 mg. Adverse events (AEs) were assessed using Common Terminology Criteria for Adverse Events (CTCAE) v4.03 with dose limiting toxicity (DLT) defined as a clinically significant, drug-related, Grade 4 haematological or Grade 3 or higher non-haematological toxicity occurring within 7 days of administration of the first treatment at a given dose for that patient. Results: Six patients were treated with no DLTs seen during dose escalation. Drug-related AEs were of low grade and included dysuria and fatigue. All patients completed six doses of treatment as planned. Pharmacokinetic and pharmacodynamic assays did not detect any pembrolizumab in the serum following repeated intravesical administration, and no changes in peripheral immune cell populations were observed. Conclusions: Administration of intravesical pembrolizumab was well tolerated and did not raise any safety concerns in patients with NMIBC following TURBT. There was no evidence of systemic absorption or systemic immune effects following intravesical administration. Further studies are required to assess whether intravesical administration has anti-tumour activity.

Published
2023

2. Harnessing NKT Cells for Therapeutic Applications

Author

Cerundolo, V., Salio, M., Compans, R. W., editor, Cooper, M. D., editor, Honjo, T., editor, Koprowski, H., editor, Melchers, F., editor, Oldstone, M. B. A., editor, Olsnes, S., editor, Svanborg, C., editor, Vogt, P. K., editor, Wagner, H., editor, and Moody, D. Branch, editor

Published
2007
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3. Immune Monitoring in Cancer Immunotherapy

Author

Romero, P., Pittet, M. J., Valmori, D., Speiser, D. E., Cerundolo, V., Liénard, D., Lejeune, F., Cerottini, J.-C., Stock, G., editor, Lessl, M., editor, Walden, P., editor, Sterry, W., editor, and Hennekes, H., editor

Published
2000
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5. Precise tuning of gene expression levels in mammalian cells

Author

Michaels, Y, Barnkob, M, Barbosa, H, Baeumler, T, Thompson, M, Andre, V, Colin-York, H, Fritzsche, M, Gileadi, U, Sheppard, H, Knapp, D, Milne, T, Cerundolo, V, and Fulga, T

Subjects
Ovalbumin, Science, Genes, BRCA1, Melanoma, Experimental, High-Throughput Nucleotide Sequencing, Response Elements, Xenograft Model Antitumor Assays, Article, B7-H1 Antigen, Recombinant Proteins, Mice, Inbred C57BL, MicroRNAs, HEK293 Cells, Gene Expression Regulation, Genetic Techniques, Animals, Humans, lcsh:Q, CRISPR-Cas Systems, lcsh:Science, 3' Untranslated Regions
Abstract

Precise, analogue regulation of gene expression is critical for cellular function in mammals. In contrast, widely employed experimental and therapeutic approaches such as knock-in/out strategies are more suitable for binary control of gene activity. Here we report on a method for precise control of gene expression levels in mammalian cells using engineered microRNA response elements (MREs). First, we measure the efficacy of thousands of synthetic MRE variants under the control of an endogenous microRNA by high-throughput sequencing. Guided by this data, we establish a library of microRNA silencing-mediated fine-tuners (miSFITs) of varying strength that can be employed to precisely control the expression of user-specified genes. We apply this technology to tune the T-cell co-inhibitory receptor PD-1 and to explore how antigen expression influences T-cell activation and tumour growth. Finally, we employ CRISPR/Cas9 mediated homology directed repair to introduce miSFITs into the BRCA1 3′UTR, demonstrating that this versatile tool can be used to tune endogenous genes., Analogue regulation of gene expression is important for normal function in mammals but existing genetic technologies are designed to achieve ON/OFF control. Here the authors develop synthetic microRNA silencing-mediated fine-tuners (miSFITs) to precisely control target gene expression levels.

Published
2019

7. PLGA Nanoparticles Co-encapsulating NY-ESO-1 Peptides and IMM60 Induce Robust CD8 and CD4 T Cell and B Cell Responses

Author

Dolen, Y., Gileadi, U., Chen, J.L., Valente, M.C., Creemers, J.H.A., Dinther, E.A.W. van, Riessen, N.K. van, Jäger, E., Hruby, M., Cerundolo, V., Diken, M., Figdor, C.G., Vries, I.J.M. de, Dolen, Y., Gileadi, U., Chen, J.L., Valente, M.C., Creemers, J.H.A., Dinther, E.A.W. van, Riessen, N.K. van, Jäger, E., Hruby, M., Cerundolo, V., Diken, M., Figdor, C.G., and Vries, I.J.M. de

Abstract

Contains fulltext : 232076.pdf (Publisher’s version ) (Open Access), Tumor-specific neoantigens can be highly immunogenic, but their identification for each patient and the production of personalized cancer vaccines can be time-consuming and prohibitively expensive. In contrast, tumor-associated antigens are widely expressed and suitable as an off the shelf immunotherapy. Here, we developed a PLGA-based nanoparticle vaccine that contains both the immunogenic cancer germline antigen NY-ESO-1 and an α-GalCer analog IMM60, as a novel iNKT cell agonist and dendritic cell transactivator. Three peptide sequences (85-111, 117-143, and 157-165) derived from immunodominant regions of NY-ESO-1 were selected. These peptides have a wide HLA coverage and were efficiently processed and presented by dendritic cells via various HLA subtypes. Co-delivery of IMM60 enhanced CD4 and CD8 T cell responses and antibody levels against NY-ESO-1 in vivo. Moreover, the nanoparticles have negligible systemic toxicity in high doses, and they could be produced according to GMP guidelines. Together, we demonstrated the feasibility of producing a PLGA-based nanovaccine containing immunogenic peptides and an iNKT cell agonist, that is activating DCs to induce antigen-specific T cell responses.

Published
2021

10. Results of a randomized, double-blind phase II clinical trial of NY-ESO-1 vaccine with ISCOMATRIX adjuvant versus ISCOMATRIX alone in participants with high-risk resected melanoma

Author

Cebon, JS, Gore, M, Thompson, JF, Davis, ID, McArthur, GA, Walpole, E, Smithers, M, Cerundolo, V, Dunbar, PR, MacGregor, D, Fisher, C, Millward, M, Nathan, P, Findlay, MPN, Hersey, P, Evans, TRJ, Ottensmeier, CH, Marsden, J, Dalgleish, AG, Corrie, PG, Maria, M, Brimble, M, Williams, G, Winkler, S, Jackson, HM, Endo-Munoz, L, Tutuka, CSA, Venhaus, R, Old, LJ, Haack, D, Maraskovsky, E, Behren, A, Chen, W, Cebon, JS, Gore, M, Thompson, JF, Davis, ID, McArthur, GA, Walpole, E, Smithers, M, Cerundolo, V, Dunbar, PR, MacGregor, D, Fisher, C, Millward, M, Nathan, P, Findlay, MPN, Hersey, P, Evans, TRJ, Ottensmeier, CH, Marsden, J, Dalgleish, AG, Corrie, PG, Maria, M, Brimble, M, Williams, G, Winkler, S, Jackson, HM, Endo-Munoz, L, Tutuka, CSA, Venhaus, R, Old, LJ, Haack, D, Maraskovsky, E, Behren, A, and Chen, W

Abstract

BACKGROUND: To compare the clinical efficacy of New York Esophageal squamous cell carcinoma-1 (NY-ESO-1) vaccine with ISCOMATRIX adjuvant versus ISCOMATRIX alone in a randomized, double-blind phase II study in participants with fully resected melanoma at high risk of recurrence. METHODS: Participants with resected stage IIc, IIIb, IIIc and IV melanoma expressing NY-ESO-1 were randomized to treatment with three doses of NY-ESO-1/ISCOMATRIX or ISCOMATRIX adjuvant administered intramuscularly at 4-week intervals, followed by a further dose at 6 months. Primary endpoint was the proportion free of relapse at 18 months in the intention-to-treat (ITT) population and two per-protocol populations. Secondary endpoints included relapse-free survival (RFS) and overall survival (OS), safety and NY-ESO-1 immunity. RESULTS: The ITT population comprised 110 participants, with 56 randomized to NY-ESO-1/ISCOMATRIX and 54 to ISCOMATRIX alone. No significant toxicities were observed. There were no differences between the study arms in relapses at 18 months or for median time to relapse; 139 vs 176 days (p=0.296), or relapse rate, 27 (48.2%) vs 26 (48.1%) (HR 0.913; 95% CI 0.402 to 2.231), respectively. RFS and OS were similar between the study arms. Vaccine recipients developed strong positive antibody responses to NY-ESO-1 (p≤0.0001) and NY-ESO-1-specific CD4+ and CD8+ responses. Biopsies following relapse did not demonstrate differences in NY-ESO-1 expression between the study populations although an exploratory study demonstrated reduced (NY-ESO-1)+/Human Leukocyte Antigen (HLA) class I+ double-positive cells in biopsies from vaccine recipients performed on relapse in 19 participants. CONCLUSIONS: The vaccine was well tolerated, however, despite inducing antigen-specific immunity, it did not affect survival endpoints. Immune escape through the downregulation of NY-ESO-1 and/or HLA class I molecules on tumor may have contributed to relapse.

Published
2020

11. Ligand-dependent downregulation of MR1 cell surface expression

Author

Salio, M, Awad, W, Veerapen, N, Gonzalez-Lopez, C, Kulicke, C, Waithe, D, Martens, AWJ, Lewinsohn, DM, Hobrath, JV, Cox, LR, Rossjohn, J, Besra, GS, Cerundolo, V, Salio, M, Awad, W, Veerapen, N, Gonzalez-Lopez, C, Kulicke, C, Waithe, D, Martens, AWJ, Lewinsohn, DM, Hobrath, JV, Cox, LR, Rossjohn, J, Besra, GS, and Cerundolo, V

Abstract

The antigen-presenting molecule MR1 presents riboflavin-based metabolites to Mucosal-Associated Invariant T (MAIT) cells. While MR1 egress to the cell surface is ligand-dependent, the ability of small-molecule ligands to impact on MR1 cellular trafficking remains unknown. Arising from an in silico screen of the MR1 ligand-binding pocket, we identify one ligand, 3-([2,6-dioxo-1,2,3,6-tetrahydropyrimidin-4-yl]formamido)propanoic acid, DB28, as well as an analog, methyl 3-([2,6-dioxo-1,2,3,6-tetrahydropyrimidin-4-yl]formamido)propanoate, NV18.1, that down-regulate MR1 from the cell surface and retain MR1 molecules in the endoplasmic reticulum (ER) in an immature form. DB28 and NV18.1 compete with the known MR1 ligands, 5-OP-RU and acetyl-6-FP, for MR1 binding and inhibit MR1-dependent MAIT cell activation. Crystal structures of the MAIT T cell receptor (TCR) complexed with MR1-DB28 and MR1-NV18.1, show that these two ligands reside within the A'-pocket of MR1. Neither ligand forms a Schiff base with MR1 molecules; both are nevertheless sequestered by a network of hydrophobic and polar contacts. Accordingly, we define a class of compounds that inhibits MR1 cellular trafficking.

Published
2020

16. Investigating tumour immune microenvironment effects of hypofractionated radiotherapy +/- immune checkpoint blockade in immunocompetent pre-clinical prostate cancer models

Author

Philippou, Y, primary, Sjoberg, H., additional, Murphy, E., additional, Alyacoubi, S., additional, Jones, K., additional, Gordon-Weeks, A.N., additional, Lamb, A.D., additional, McKenna, W.G., additional, Gileadi, U., additional, Cerundolo, V., additional, Mills, I.G., additional, Hamdy, F.C., additional, Muschel, R.J., additional, and Bryant, R.J., additional

Published
2020
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24. TAP deficiency syndrome

Author

GADOLA, S D, MOINS-TEISSERENC, H T, TROWSDALE, J, GROSS, W L, and CERUNDOLO, V

Published
2000

30. Presentation of viral antigen controlled by a gene in the major histocompatibility complex

Author

Cerundolo, V., Alexander, J., Anderson, K., Lamb, C., Cresswell, P., McMichael, A., Gotch, F., and Townsend, A.

Subjects
HLA histocompatibility antigens -- Genetic aspects, Cellular immunity -- Research, HLA class II antigens -- Genetic aspects, Immune response -- Research, Antigens -- Research, Environmental issues, Science and technology, Zoology and wildlife conservation
Abstract

For antigens to be recognized by T cells, they must be presented in association with major histocompatibility (MHC) antigens, so that an immune response can be initiated. A B lymphocyte cell line, known as LBL 721.174, which has been mutated (changed genetically), is defective in that it cannot assemble or express class I MHC molecules on the cell surface. These cells were examined for defects in antigen presentation. The study showed that the cells could no longer present a viral antigen that is normally found inside of the virus which causes influenza, yet they could present a peptide that is normally found outside of the cell. Cells that expressed the class I antigens and cells that do not express the class I antigens were fused together and the characteristics of the progeny cells and the genes that were inherited by the progeny were studied. It was shown that the defect in antigen presentation was located on chromosome 6, where the MHC antigens are located. The gene involved in antigen presentation is different from the genes that code for the MHC antigens. The understanding of how antigen presentation occurs and the role of the molecules involved in the initiation of an immune response will allow further understanding and perhaps manipulation of the immune response so that an effective immune response may be induced against various foreign molecules, including viruses. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1990

31. The impact of vaccination and prior exposure on stool shedding of Salmonella Typhi and Salmonella Paratyphi in 6 controlled human infection studies

Author

Gibani, M.M., Voysey, M., Jin, C., Jones, C., Thomaides-Brears, H., Jones, E., Baker, P., Morgan, M., Simmons, A., Gordon, M.A., Cerundolo, V., Pitzer, V.E., Angus, B., Levine, M.M., Darton, T.C., and Pollard, A.J.

Subjects
Immunology, CHILDREN, TOXOID CONJUGATE VACCINE, IMMUNOGENICITY, Microbiology, Salmonella Typhi, complex mixtures, Feces, fluids and secretions, FEVER, Paratyphoid Fever, Humans, Typhoid Fever, Articles and Commentaries, indirect effects, 11 Medical and Health Sciences, Bacterial Shedding, Science & Technology, Typhoid-Paratyphoid Vaccines, GLOBAL BURDEN, 06 Biological Sciences, EFFICACY, MODEL, Infectious Diseases, stool shedding, Salmonella paratyphi A, Vi-polysaccharide vaccine, bacteria, TRIAL, typhoid conjugate vaccine, Life Sciences & Biomedicine
Abstract

Six Salmonella Typhi or Paratyphi human challenge studies were conducted, and daily stool cultures performed. Vi-containing vaccines reduced bacterial shedding, Ty21a or an experimental vaccine did not. Higher Vi immunoglobulin G titers were associated with reduced shedding., Background Shedding of Salmonella Typhi or Paratyphi in the stool or urine leads to contamination of food or water, which is a prerequisite for transmission of enteric fever. Currently, there are limited data on the effect of vaccination or prior exposure on stool shedding. Methods Six Salmonella Typhi or Paratyphi human challenge studies were conducted between 2011 and 2017. Participants were either unvaccinated or vaccinated with 1 of 4 vaccines: Vi-polysaccharide (Vi-PS), Vi-tetanus-toxoid conjugate vaccine (Vi-TT), live oral Ty21a vaccine, or an experimental vaccine (M01ZH09). Daily stool cultures were collected for 14 days after challenge. Results There were 4934 stool samples collected from 430 volunteers. Participants who received Vi-PS or Vi-TT shed less than unvaccinated participants (odds ratio [OR], 0.34; 95% confidence interval [CI], 0.15–0.77; P = .010 and OR, 0.41; 95% CI, 0.19–0.91, P = .029 for Vi-PS and Vi-TT, respectively). Higher anti-Vi immunoglobulin G titers were associated with less shedding of S. Typhi (P < .0001). A nonsignificant reduction in shedding was associated with Ty21a vaccine (OR, 0.57; 95% CI, 0.27–1.20; P = .140). Individuals previously exposed to S. Typhi shed less than previously unexposed individuals (OR, 0.30; 95% CI, 0.1–0.8; P = .016). Shedding of S. Typhi was more common than S. Paratyphi. Conclusions Prior vaccination with Vi vaccines, or natural infection, reduces onward transmission of S. Typhi. Field trials of Vi-TT should be designed to detect indirect protection, reflecting the consequence of reduced stool shedding observed in the human challenge model.

Published
2018

32. Somatic POLE exonuclease domain mutations are early events in sporadic endometrial and colorectal carcinogenesis, determining driver mutational landscape, clonal neoantigen burden and immune response

Author

Temko, D., Gool, I.C. van, Rayner, E., Glaire, M., Makino, S., Brown, M., Chegwidden, L., Palles, C., Depreeuw, J., Beggs, A., Stathopoulou, C., Mason, J., Baker, A.M., Williams, M., Cerundolo, V., Rei, M., Taylor, J.C., Schuh, A., Ahmed, A., Amant, F., Lambrechts, D., Smit, V.T.H.B.M., Bosse, T., Graham, T.A., Church, D.N., Tomlinson, I., Obstetrics and Gynaecology, and Amsterdam Reproduction & Development (AR&D)

Subjects
Male, colorectal cancer, Adenocarcinoma, CD8-Positive T-Lymphocytes, Genomic Instability, Lymphocytes, Tumor-Infiltrating, Antigens, Neoplasm, Databases, Genetic, Tumor Microenvironment, Humans, Genetic Predisposition to Disease, Poly-ADP-Ribose Binding Proteins, Neoplasm Staging, Original Paper, Whole Genome Sequencing, Gene Expression Profiling, precursor lesion, DNA Polymerase II, Middle Aged, Original Papers, Endometrial Neoplasms, Gene Expression Regulation, Neoplastic, Cell Transformation, Neoplastic, Phenotype, POLE, endometrial cancer, Female, Neoplasm Grading, polymerase proofreading, mutation, Colorectal Neoplasms
Abstract

Genomic instability, which is a hallmark of cancer, is generally thought to occur in the middle to late stages of tumourigenesis, following the acquisition of permissive molecular aberrations such as TP53 mutation or whole genome doubling. Tumours with somatic POLE exonuclease domain mutations are notable for their extreme genomic instability (their mutation burden is among the highest in human cancer), distinct mutational signature, lymphocytic infiltrate, and excellent prognosis. To what extent these characteristics are determined by the timing of POLE mutations in oncogenesis is unknown. Here, we have shown that pathogenic POLE mutations are detectable in non-malignant precursors of endometrial and colorectal cancer. Using genome and exome sequencing, we found that multiple driver mutations in POLE-mutant cancers show the characteristic POLE mutational signature, including those in genes conventionally regarded as initiators of tumourigenesis. In POLE-mutant cancers, the proportion of monoclonal predicted neoantigens was similar to that in other cancers, but the absolute number was much greater. We also found that the prominent CD8+ T-cell infiltrate present in POLE-mutant cancers was evident in their precursor lesions. Collectively, these data indicate that somatic POLE mutations are early, quite possibly initiating, events in the endometrial and colorectal cancers in which they occur. The resulting early onset of genomic instability may account for the striking immune response and excellent prognosis of these tumours, as well as their early presentation. © 2018 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland.

Published
2018

33. Generation of a double binary transgenic zebrafish model to study myeloid gene regulation in response to oncogene activation in melanocytes

Author

Kenyon, A, Gavriouchkina, D, Zorman, J, Chong-Morrison, V, Napolitani, G, Cerundolo, V, and Sauka-Spengler, T

Subjects
Transcription, Genetic, Macrophage, Neutrophils, Biotagging, lcsh:Medicine, Animals, Genetically Modified, Melanocyte, lcsh:Pathology, Animals, Myeloid Cells, Resource Article, Cell Shape, Melanoma, Oncogene, Zebrafish, Cell Line, Transformed, Cell Proliferation, Gene Expression Profiling, lcsh:R, Neutrophil, Oncogenes, Mifepristone, Genes, ras, Gene Expression Regulation, Models, Animal, Melanocytes, lcsh:RB1-214
Abstract

A complex network of inflammatory genes is closely linked to somatic cell transformation and malignant disease. Immune cells and their associated molecules are responsible for detecting and eliminating cancer cells as they establish themselves as the precursors of a tumour. By the time a patient has a detectable solid tumour, cancer cells have escaped the initial immune response mechanisms. Here, we describe the development of a double binary zebrafish model that enables regulatory programming of the myeloid cells as they respond to oncogene-activated melanocytes to be explored, focussing on the initial phase when cells become the precursors of cancer. A hormone-inducible binary system allows for temporal control of expression of different Ras oncogenes (NRasQ61K, HRasG12V and KRasG12V) in melanocytes, leading to proliferation and changes in morphology of the melanocytes. This model was coupled to binary cell-specific biotagging models allowing in vivo biotinylation and subsequent isolation of macrophage or neutrophil nuclei for regulatory profiling of their active transcriptomes. Nuclear transcriptional profiling of neutrophils, performed as they respond to the earliest precursors of melanoma in vivo, revealed an intricate landscape of regulatory factors that may promote progression to melanoma, including Serpinb1l4, Fgf1, Fgf6, Cathepsin H, Galectin 1 and Galectin 3. The model presented here provides a powerful platform to study the myeloid response to the earliest precursors of melanoma., Summary: The authors present an innovative double binary zebrafish model for exploring regulatory mechanisms that govern the myeloid response at the onset of melanoma.

Published
2018

34. A phase I study to assess the safety and tolerability of intravesical pembrolizumab in recurrent non-muscle invasive bladder cancer (NMIBC)

Author

Purshouse, K., primary, Woodcock, V.K., additional, Butcher, C., additional, Haddon, C., additional, Verrall, G., additional, Elhussein, L., additional, Salio, M., additional, Middleton, M.R., additional, Cerundolo, V., additional, Kwok, J., additional, Blagden, S., additional, Protheroe, A.S., additional, and Crew, J., additional

Published
2019
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36. Harnessing the Power of Invariant Natural Killer T Cells in Cancer Immunotherapy

Author

Bedard, M, Salio, M, and Cerundolo, V

Subjects
lcsh:Immunologic diseases. Allergy, CD1d molecules, Immunology, innate immune response, invariant natural killer T cells, Immunology and Allergy, chemical and pharmacologic phenomena, Review, tumor immunology, lcsh:RC581-607, lipid antigens
Abstract

Invariant natural killer T (iNKT) cells are a distinct subset of innate-like lymphocytes bearing an invariant T-cell receptor, through which they recognize lipid antigens presented by monomorphic CD1d molecules. Upon activation, iNKT cells are capable of not only having a direct effector function but also transactivating NK cells, maturing dendritic cells, and activating B cells, through secretion of several cytokines and cognate TCR-CD1d interaction. Endowed with the ability to orchestrate an all-encompassing immune response, iNKT cells are critical in shaping immune responses against pathogens and cancer cells. In this review, we examine the critical role of iNKT cells in antitumor responses from two perspectives: (i) how iNKT cells potentiate antitumor immunity and (ii) how CD1d+ tumor cells may modulate their own expression of CD1d molecules. We further explore hypotheses to explain iNKT cell activation in the context of cancer and how the antitumor effects of iNKT cells can be exploited in different forms of cancer immunotherapy, including their role in the development of cancer vaccines.

Published
2017
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38. Clonal analysis of Salmonella-specific effector T cells reveals serovar-specific and cross-reactive T cell responses

Author

Napolitani, G., Kurupati, P., Teng, K.W.W., Gibani, M.M., Rei, M., Aulicino, A., Preciado-Llanes, L., Wong, M.T., Becht, E., Howson, L., Haas, P. de, Salio, M., Blohmke, C.J., Olsen, L.R., Pinto, D.M.S., Scifo, L., Jones, C., Dobinson, H., Campbell, D., Juel, H.B., Thomaides-Brears, H., Pickard, D., Bumann, D., Baker, S., Dougan, G., Simmons, A., Gordon, M.A., Newell, E.W., Pollard, A.J., Cerundolo, V., Napolitani, G., Kurupati, P., Teng, K.W.W., Gibani, M.M., Rei, M., Aulicino, A., Preciado-Llanes, L., Wong, M.T., Becht, E., Howson, L., Haas, P. de, Salio, M., Blohmke, C.J., Olsen, L.R., Pinto, D.M.S., Scifo, L., Jones, C., Dobinson, H., Campbell, D., Juel, H.B., Thomaides-Brears, H., Pickard, D., Bumann, D., Baker, S., Dougan, G., Simmons, A., Gordon, M.A., Newell, E.W., Pollard, A.J., and Cerundolo, V.

Abstract

Item does not contain fulltext, To tackle the complexity of cross-reactive and pathogen-specific T cell responses against related Salmonella serovars, we used mass cytometry, unbiased single-cell cloning, live fluorescence barcoding, and T cell-receptor sequencing to reconstruct the Salmonella-specific repertoire of circulating effector CD4(+) T cells, isolated from volunteers challenged with Salmonella enterica serovar Typhi (S. Typhi) or Salmonella Paratyphi A (S. Paratyphi). We describe the expansion of cross-reactive responses against distantly related Salmonella serovars and of clonotypes recognizing immunodominant antigens uniquely expressed by S. Typhi or S. Paratyphi A. In addition, single-amino acid variations in two immunodominant proteins, CdtB and PhoN, lead to the accumulation of T cells that do not cross-react against the different serovars, thus demonstrating how minor sequence variations in a complex microorganism shape the pathogen-specific T cell repertoire. Our results identify immune-dominant, serovar-specific, and cross-reactive T cell antigens, which should aid in the design of T cell-vaccination strategies against Salmonella.

Published
2018

39. M1-like monocytes are a major immunological determinant of severity in previously healthy adults with life-threatening influenza

Author

Cole, SL, Dunning, J, Kok, WL, Benam, KH, Benlahrech, A, Repapi, E, Martinez, FO, Drumright, L, Powell, TJ, Bennett, M, Elderfield, R, Thomas, C, MOSAIC investigators, Dong, T, McCauley, J, Liew, FY, Taylor, S, Zambon, M, Barclay, W, Cerundolo, V, Openshaw, PJ, McMichael, AJ, Ho, LP, Wellcome Trust, Medical Research Council (MRC), Imperial College Healthcare NHS Trust- BRC Funding, National Institute for Health Research, and Commission of the European Communities

Abstract

In each influenza season, a distinct group of young, otherwise healthy individuals with no risk factors succumbs to life-threatening infection. To better understand the cause for this, we analyzed a broad range of immune responses in blood from a unique cohort of patients, comprising previously healthy individuals hospitalized with and without respiratory failure during one influenza season, and infected with one specific influenza A strain. This analysis was compared with similarly hospitalized influenza patients with known risk factors (total of n = 60 patients recruited). We found a sustained increase in a specific subset of proinflammatory monocytes, with high TNF-α expression and an M1-like phenotype (independent of viral titers), in these previously healthy patients with severe disease. The relationship between M1-like monocytes and immunopathology was strengthened using murine models of influenza, in which severe infection generated using different models (including the high-pathogenicity H5N1 strain) was also accompanied by high levels of circulating M1-like monocytes. Additionally, a raised M1/M2 macrophage ratio in the lungs was observed. These studies identify a specific subtype of monocytes as a modifiable immunological determinant of disease severity in this subgroup of severely ill, previously healthy patients, offering potential novel therapeutic avenues.

Published
2017

40. M1-like monocytes are a major immunological determinant of severity in previously healthy adults with life-threatening influenza

Author

Cole, S, Dunning, J, Kok, W, Benam, K, Benlahrech, A, Repapi, E, Martinez, F, Drumright, L, Powell, T, Bennett, M, Elderfield, R, Thomas, C, Dong, T, McCauley, J, Liew, F, Taylor, S, Zambon, M, Barclay, W, Cerundolo, V, Openshaw, P, McMichael, A, and Ho, L

Subjects
Adult, Male, Influenza A Virus, H5N1 Subtype, Tumor Necrosis Factor-alpha, Macrophages, Middle Aged, Viral Load, Monocytes, Mice, Inbred C57BL, Mice, Young Adult, Phenotype, Influenza, Human, Animals, Humans, Female, Lung, Research Article, Aged
Abstract

In each influenza season, a distinct group of young, otherwise healthy individuals with no risk factors succumbs to life-threatening infection. To better understand the cause for this, we analyzed a broad range of immune responses in blood from a unique cohort of patients, comprising previously healthy individuals hospitalized with and without respiratory failure during one influenza season, and infected with one specific influenza A strain. This analysis was compared with similarly hospitalized influenza patients with known risk factors (total of n = 60 patients recruited). We found a sustained increase in a specific subset of proinflammatory monocytes, with high TNF-α expression and an M1-like phenotype (independent of viral titers), in these previously healthy patients with severe disease. The relationship between M1-like monocytes and immunopathology was strengthened using murine models of influenza, in which severe infection generated using different models (including the high-pathogenicity H5N1 strain) was also accompanied by high levels of circulating M1-like monocytes. Additionally, a raised M1/M2 macrophage ratio in the lungs was observed. These studies identify a specific subtype of monocytes as a modifiable immunological determinant of disease severity in this subgroup of severely ill, previously healthy patients, offering potential novel therapeutic avenues., In a cohort of influenza patients, previously healthy and young patients who succumbed to life-threatening disease were defined by high levels of circulating M1-like, TNF-αhi monocytes.

Published
2017

41. Discussion

Author

Pollard, J, Caux, C, Strieter, R, Brennan, F, Cerundolo, V, Pepper, MS, Gallimore, A, Blankenstein, T, Oppenheim, J, Feldmann, M, Balkwill, F, and Gordon, S

Published
2016

43. T cells work together to fight cancer

Author

Cerundolo, V

Subjects
TheoryofComputation_ANALYSISOFALGORITHMSANDPROBLEMCOMPLEXITY
Abstract

Recent studies have identified new melanoma antigens that are recognised by CD4+ T cells. Analysis of tumour-specific CD4+ T-cell responses may lead to the development of optimal anti-cancer vaccines that can induce an orchestrated effort of tumour-specific CD4+ and CD8+ T cells in the fight against cancer.

Published
2016

45. Peripheral burst of tumor-specific cytotoxic T lymphocytes and infiltration of metastatic lesions by memory CD8+ T cells in melanoma patients receiving interleukin 12

Author

Mortarini, R, Borri, A, Tragni, G, Bersani, I, Vegetti, C, Bajetta, E, Pilotti, S, Cerundolo, V, and Anichini, A

Abstract

Systemic effects on T-cell-mediated antitumor immunity, on expression of T-cell adhesion/homing receptors, and on the promotion of T-cell infiltration of neoplastic tissue may represent key steps for the efficacy of immunological therapies of cancer. In this study, we investigated whether these processes can be promoted by s.c. administration of low-dose (0.5 microg/kg) recombinant human interleukin-12 (rHuIL-12) to metastatic melanoma patients. A striking burst of HLA-restricted CTL precursors (CTLp) directed to autologous tumor was documented in peripheral blood by a high-efficiency limiting dilution analysis technique within a few days after rHuIL-12 injection. A similar burst in peripheral CTLp frequency was observed even when looking at response to a single tumor-derived peptide, as documented by an increase in Melan-A/Mart-1(27-35)-specific CTLp in two HLA-A*0201+ patients by limiting dilution analysis and by staining peripheral blood lymphocytes (PBLs) with HLA-A*0201-melanoma antigen-A/melanoma antigen recognized by T cells (Melan-A/Mart)-1 tetrameric complexes. The CTLp burst was associated, in PBLs, with enhanced expression of T-cell adhesion/homing receptors CD11a/CD18, CD49d, CD44, and with increased proportion of cutaneous lymphocyte antigen (CLA)-positive T cells. This was matched by a marked increase, in serum, of soluble forms of the endothelial cell adhesion molecules E-selectin, vascular cell adhesion molecules (VCAM)-1 and intercellular adhesion molecules (ICAM)-1. Infiltration of neoplastic tissue by CDS+ T cells with a memory and cytolytic phenotype was found by immunohistochemistry in eight of eight posttreatment metastatic lesions but not in five of five pretreatment metastatic lesions from three patients. Increased tumor necrosis and/or fibrosis were also found in several posttherapy lesions of two of three patients in comparison with pretherapy metastases. These results provide the first evidence that rHuIL-12 can boost the frequency of circulating antitumor CTLp in tumor patients, enhances expression of ligand receptor pairs contributing to the lymphocyte function-associated antigen-1/ICAM-1, very late antigen-4/VCAM-1, and CLA/E-selectin adhesion pathways, and promotes infiltration of neoplastic lesions by CD8+ memory T cells in a clinical setting.

Published
2016

46. An antigen-targeted approach to adoptive transfer therapy of cancer

Author

Valmori, D., Pittet, M. J., Rimoldi, D., Liénard, D., Rod Dunbar, Cerundolo, V., Lejeune, F., Cerottini, J. -C, and Romero, P.

Abstract

Previous attempts to treat human malignancies by adoptive transfer of tumor-specific CTLs have been limited by the difficulty of isolating T cells of defined antigen specificity. The recent development of MHC class I/antigenic peptide tetrameric complexes that allow direct identification of antigen-specific T cells has opened new possibilities for the isolation and in vitro expansion of tumor-specific T cells. In the present study, we have derived polyclonal monospecific cell lines from circulating Melan-A-specific CTL precursors of HLA-A*0201+ melanoma patients by combining stimulation with recently identified peptide analogues of the immunodominant epitope from the melanoma-associated antigen Melan-A with staining with fluorescent HLA-A*0201/Melan-A peptide tetramers. In vitro expansion of antigen-specific CD8+ T cells was monitored by flow cytometry with the fluorescent tetramers and anti-CD8 monoclonal antibody. This analysis revealed that Melan-A 26-35 peptide analogues were much more efficient than the parental peptides in stimulating a rapid in vitro expansion of antigen-specific CD8+ T cells. These cells were then isolated by tetramer-guided cell sorting and subsequently expanded in vitro by mitogen stimulation. The resulting polyclonal but monospecific CTLs fully cross-recognized the parental peptides and were able to efficiently lyse Melan-A-expressing tumor cells. Altogether, these results pave the way to a molecularly defined approach to antigen-specific adoptive transfer therapy of cancer.

Published
2016

49. Plasma cell antibody repertoire analysis following administration of meningococcal polysaccharide and protein-polysaccharide conjugate vaccines: evidence of distinct patterns of B cell activation

Author

Galson, JD, Clutterbuck, EA, Trueck, J, Muenz, M, Fowler, A, Cerundolo, V, Pollard, AJ, Lunter, G, and Kelly, DF

Abstract

Vaccines against N.meningitidis have been developed from the plain capsular polysaccharide, (T-independent antigen), and by covalently linking the polysaccharide to a protein carrier to from a polysaccharide-protein conjugate (T-dependent antigen). To investigate differences in the immune response to these two vaccine types, plasma cells were isolated 7 days following administration of meningococcal serogroup ACWY polysaccharide and conjugate vaccines. Additionally, naïve, marginal zone, IgM memory and IgG memory B cell subsets were isolated at baseline. Next-generation sequencing was used to obtain B cell receptor sequence data from all populations.

Published
2016

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