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1. Biologic subtypes of melanoma predict survival benefit of combination anti-PD1+anti-CTLA4 immune checkpoint inhibitors versus anti-PD1 monotherapy

Author

Deirdre Kelly, Anna Spreafico, Marcus O Butler, David Hogg, Danny Ghazarian, April A N Rose, Thiago Pimentel Muniz, Samuel D Saibil, Susan M Armstrong, Diana P Arteaga, Ian King, Zaid Saeed Kamil, and Kendra Ross

Subjects
Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Purpose Anti-programmed cell death protein 1 (PD1)±anti-cytotoxic T-lymphocyte associated protein 4 (CTLA4) immune checkpoint inhibitors (ICIs) are standard therapeutic options for metastatic melanoma. We assessed whether biologic subtype according to primary tumor type or genomic subtype can function as predictive biomarkers for anti-PD1±anti-CTLA4 ICI in patients with advanced melanoma.Methods We performed a single-center retrospective cohort analysis of patients who received anti-PD1±anti-CTLA4 ICI for advanced melanoma between 2012 and 2019. Primary tumor type, BRAF and NRAS mutation status, and other covariates were abstracted from chart review. Log-rank tests and multivariable Cox regression models were used to assess differences in clinical progression-free (cPFS) and overall survival (OS).Results We identified 230 patients who received 249 lines of anti-PD1±anti-CTLA4 ICI for unresectable or metastatic disease. Of these patients, 74% were cutaneous, 11% mucosal, 8% unknown primary and 7% acral. BRAF and NRAS mutations were identified in 35% and 28% of patients, respectively. In multivariable analyses of the entire cohort, acral or mucosal primary tumor type, >3 metastatic sites, elevated LDH were predictive of shorter cPFS and OS. Combination ICI therapy was associated with longer cPFS (HR 0.57, 95% CI 0.38 to 0.86, p=0.007) and OS (HR 0.42, 95% CI 0.28 to 0.65, p

Published
2021
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2. Correction: Combination checkpoint blockade for metastatic cutaneous malignancies in kidney transplant recipients

Author

Lisa Zimmer, Serigne Lo, Caroline Robert, John Haanen, Ines Pires da Silva, Reinhard Dummer, Michael Manos, Joanna Mangana, Marcus O Butler, Richard D Carvajal, Alon Vaisman, Christian Posch, F Stephen Hodi, Paola Queirolo, Axel Hauschild, Christian U Blank, Maria Grazia Vitale, Karijn P M Suijkerbuijk, Alexander M Menzies, Aljosja Rogiers, Chiara Tentori, Joseph M Grimes, Megan H Trager, Sharon Nahm, Peter Bowling, Neha Papneja, April A N Rose, Jessica S W Borgers, Severine Roy, Thiago Pimentel Muniz, Tim Cooksley, Jeremy Lupu, Samuel D Saibil, Michael Erdmann, Laura Pala, Ryan J Sullivan, Wilson H Miller Jr, Osama E Rahma, and Paul C Lorigan

Subjects
Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Published
2021
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3. Clinical impact of COVID-19 on patients with cancer treated with immune checkpoint inhibition

Author

Dirk Schadendorf, Carola Berking, Lisa Zimmer, Serigne Lo, Caroline Robert, John Haanen, Ines Pires da Silva, Paolo Antonio Ascierto, Reinhard Dummer, Michael Manos, Joanna Mangana, Marcus O Butler, Richard D Carvajal, Georgina V Long, Alon Vaisman, Christian Posch, F Stephen Hodi, Paola Queirolo, Axel Hauschild, Christian U Blank, Maria Grazia Vitale, Carlo Alberto Tondini, Leyre Zubiri, Arielle Elkrief, Karijn P M Suijkerbuijk, Mario Mandala, Alexander M Menzies, Aljosja Rogiers, Chiara Tentori, Joseph M Grimes, Megan H Trager, Sharon Nahm, Peter Bowling, Neha Papneja, April A N Rose, Jessica S W Borgers, Severine Roy, Thiago Pimentel Muniz, Tim Cooksley, Jeremy Lupu, Samuel D Saibil, Matteo S Carlino, Michael Erdmann, Laura Pala, Ryan J Sullivan, Wilson H Miller Jr, Kerry L Reynolds, Osama E Rahma, and Paul C Lorigan

Subjects
Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Background Patients with cancer who are infected with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) are more likely to develop severe illness and die compared with those without cancer. The impact of immune checkpoint inhibition (ICI) on the severity of COVID-19 illness is unknown. The aim of this study was to investigate whether ICI confers an additional risk for severe COVID-19 in patients with cancer.Methods We analyzed data from 110 patients with laboratory-confirmed SARS-CoV-2 while on treatment with ICI without chemotherapy in 19 hospitals in North America, Europe and Australia. The primary objective was to describe the clinical course and to identify factors associated with hospital and intensive care (ICU) admission and mortality.Findings Thirty-five (32%) patients were admitted to hospital and 18 (16%) died. All patients who died had advanced cancer, and only four were admitted to ICU. COVID-19 was the primary cause of death in 8 (7%) patients. Factors independently associated with an increased risk for hospital admission were ECOG ≥2 (OR 39.25, 95% CI 4.17 to 369.2, p=0.0013), treatment with combination ICI (OR 5.68, 95% CI 1.58 to 20.36, p=0.0273) and presence of COVID-19 symptoms (OR 5.30, 95% CI 1.57 to 17.89, p=0.0073). Seventy-six (73%) patients interrupted ICI due to SARS-CoV-2 infection, 43 (57%) of whom had resumed at data cut-off.Interpretation COVID-19–related mortality in the ICI-treated population does not appear to be higher than previously published mortality rates for patients with cancer. Inpatient mortality of patients with cancer treated with ICI was high in comparison with previously reported rates for hospitalized patients with cancer and was due to COVID-19 in almost half of the cases. We identified factors associated with adverse outcomes in ICI-treated patients with COVID-19.

Published
2021
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4. Characterization of innate lymphoid cell subsets infiltrating melanoma and epithelial ovarian tumors

Author

Douglas C. Chung, Maryam Ghaedi, Kathrin Warner, Azin Sayad, Samuel D. Saibil, Marcus Q. Bernardini, Blaise A. Clarke, Patricia A. Shaw, Marcus O. Butler, Alexandra Easson, Sorana Morrissy, Ben X. Wang, Linh Nguyen, Pamela S. Ohashi, and Nicolas Jacquelot

Subjects
Epithelial ovarian cancer, innate lymphoid cells, LAG-3, melanoma, myeloid cells, NK cells, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

The innate lymphoid cell (ILC) family is composed of heterogeneous innate effector and helper immune cells that preferentially reside in tissues where they promote tissue homeostasis. In cancer, they have been implicated in driving both pro- and anti-tumor responses. This apparent dichotomy highlights the need to better understand differences in the ILC composition and phenotype within different tumor types that could drive seemingly opposite anti-tumor responses. Here, we characterized the frequency and phenotype of various ILC subsets in melanoma metastases and primary epithelial ovarian tumors. We observed high PD-1 expression on ILC subsets isolated from epithelial ovarian tumor samples, while ILC populations in melanoma samples express higher levels of LAG-3. In addition, we found that the frequency of cytotoxic ILCs and NKp46+ILC3 in tumors positively correlates with monocytic cells and conventional type 2 dendritic cells, revealing potentially new interconnected immune cell subsets in the tumor microenvironment. Consequently, these observations may have direct relevance to tumor microenvironment composition and how ILC subset may influence anti-tumor immunity.

Published
2024
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5. Supplementary Figures and Tables from IL6 Induces an IL22+ CD8+ T-cell Subset with Potent Antitumor Function

Author

Pamela S. Ohashi, Trevor J. Pugh, Benjamin Haibe-Kains, Linh T. Nguyen, Marcus Q. Bernardini, Blaise A. Clarke, Patricia A. Shaw, Sarah Rachel Katz, Michael Zon, Céline Robert-Tissot, Kavita Israni-Winger, Alisha R. Elford, Carlos R. Garcia-Batres, David T. Mulder, Azin Sayad, SeongJun Han, Scott C. Lien, Samuel D. Saibil, and Michael St. Paul

Abstract

Supplemental Figures 1-9 and Supplementary Tables 1-3

Published
2023

6. Data from IL6 Induces an IL22+ CD8+ T-cell Subset with Potent Antitumor Function

Author

Pamela S. Ohashi, Trevor J. Pugh, Benjamin Haibe-Kains, Linh T. Nguyen, Marcus Q. Bernardini, Blaise A. Clarke, Patricia A. Shaw, Sarah Rachel Katz, Michael Zon, Céline Robert-Tissot, Kavita Israni-Winger, Alisha R. Elford, Carlos R. Garcia-Batres, David T. Mulder, Azin Sayad, SeongJun Han, Scott C. Lien, Samuel D. Saibil, and Michael St. Paul

Abstract

CD8+ T cells can be polarized into several different subsets as defined by the cytokines they produce and the transcription factors that govern their differentiation. Here, we identified the polarizing conditions to induce an IL22-producing CD8+ Tc22 subset, which is dependent on IL6 and the aryl hydrocarbon receptor transcription factor. Further characterization showed that this subset was highly cytolytic and expressed a distinct cytokine profile and transcriptome relative to other subsets. In addition, polarized Tc22 were able to control tumor growth as well as, if not better than, the traditional IFNγ-producing Tc1 subset. Tc22s were also found to infiltrate the tumors of human patients with ovarian cancer, comprising up to approximately 30% of expanded CD8+ tumor-infiltrating lymphocytes (TIL). Importantly, IL22 production in these CD8+ TILs correlated with improved recurrence-free survival. Given the antitumor properties of Tc22 cells, it may be prudent to polarize T cells to the Tc22 lineage when using chimeric antigen receptor (CAR)-T or T-cell receptor (TCR) transduction–based immunotherapies.

Published
2023

9. Data from Activation of Peroxisome Proliferator-Activated Receptors α and δ Synergizes with Inflammatory Signals to Enhance Adoptive Cell Therapy

Author

Pamela S. Ohashi, Linh T. Nguyen, Russell G. Jones, Dominic G. Roy, Céline Robert-Tissot, Natasha Grimshaw, Alisha R. Elford, Kavita Israni-Winger, Carlos R. Garcia-Batres, Robert C. Laister, Michael St. Paul, and Samuel D. Saibil

Abstract

Memory CD8+ T cells (Tmem) are superior mediators of adoptive cell therapy (ACT) compared with effector CD8+ T cells (Teff) due to increased persistence in vivo. Underpinning Tmem survival is a shift in cellular metabolism away from aerobic glycolysis towards fatty acid oxidation (FAO). Here we investigated the impact of the peroxisome proliferator-activated receptor (PPAR) agonist GW501516 (GW), an agent known to boost FAO in other tissues, on CD8+ T-cell metabolism, function, and efficacy in a murine ACT model. Via activation of both PPARα and PPARδ/β, GW treatment increased expression of carnitine palmitoyl transferase 1a, the rate-limiting enzyme of FAO, in activated CD8+ T cells. Using a metabolomics approach, we demonstrated that GW increased the abundance of multiple different acylcarnitines, consistent with enhanced FAO. T cells activated in the presence of GW and inflammatory signals, either mature dendritic cells or IL12, also demonstrated enhanced production of IFNγ and expression of T-bet. Despite high expression of T-bet, a characteristic of short-lived effector cells, GW-treated cells demonstrated enhanced persistence in vivo and superior efficacy in a model of ACT. Collectively, these data identify combined PPARα and PPARδ/β agonists as attractive candidates for further studies and rapid translation into clinical trials of ACT.Significance:Dual activation of peroxisome proliferator-activated receptors α and δ improves the efficacy of adoptive cell therapy by reprogramming T-cell metabolism and cytokine expression.

Published
2023

11. Turnaround Times in Melanoma BRAF Testing and the Impact on the Initiation of Systemic Therapy at a Single Tertiary Care Cancer Center

Author

Diana P. Arteaga, Zaid Saeed-Kamil, Ian King, Tracy Stockley, Diane Liu, Thiago P. Muniz, Samuel D. Saibil, David Hogg, Anna Spreafico, and Marcus O. Butler

Subjects
Adult, Proto-Oncogene Proteins B-raf, Skin Neoplasms, Oncology, Oncology (nursing), Tertiary Healthcare, Health Policy, Humans, neoplasms, Melanoma, Retrospective Studies
Abstract

PURPOSE: The identification of BRAF mutations in melanoma enables targeted therapy and improves patient outcomes. Barriers to BRAF molecular testing affect the quality of care and therapeutic options. METHODS: This retrospective study mapped BRAF testing timelines in adult patients with melanoma at the Princess Margaret Cancer Centre to identify obstacles to timely BRAF reporting and its impact on the initiation of therapy. RESULTS: Sixty-six cases were included. The median time between BRAF request and result was 12 days (95% CI, 8 to 15) when the BRAF test was ordered by pathology, compared with 20 days (95% CI, 16 to 23) if the test was requested by another specialist ( P < .001). When the BRAF test and biopsy were performed within the same institution, the BRAF median turnaround time (TAT) was 13 days (95% CI, 6 to 19) compared with 19 days (95% CI, 16 to 21) if the sample was transferred from another institution ( P = .02). Forty-seven patients received systemic therapy, and 20 had metastatic disease. In the metastatic subgroup, if the BRAF result was available at the first medical oncology visit, the initiation of treatment was 20 days (95% CI, 9.6 to 30.3), but was delayed to 31 days (95% CI, 10.8 to 51.1) if the BRAF result was not available ( P = .03). CONCLUSION: This study showed variations in BRAF test results in TAT. One factor affecting this timeline is the transfer time, which can be streamlined by pathology reflex testing. Delays in TAT affect the timing and type of therapeutic intervention, especially in patients with stage IV disease.

Published
2022

12. IL6 Induces an IL22+ CD8+ T-cell Subset with Potent Antitumor Function

Author

Benjamin Haibe-Kains, Linh T. Nguyen, Blaise A. Clarke, SeongJun Han, Michael Zon, David Mulder, Pamela S. Ohashi, Alisha R. Elford, Celine Robert-Tissot, Carlos Garcia-Batres, Sarah Rachel Katz, Michael St. Paul, Azin Sayad, Samuel D. Saibil, Patricia Shaw, Marcus Q. Bernardini, Kavita Israni-Winger, Scott C. Lien, and Trevor J. Pugh

Subjects
Cancer Research, biology, Chemistry, medicine.medical_treatment, Immunology, T-cell receptor, Immunotherapy, Aryl hydrocarbon receptor, Chimeric antigen receptor, 3. Good health, 03 medical and health sciences, 0302 clinical medicine, Antigen, 030220 oncology & carcinogenesis, Cancer research, medicine, biology.protein, Cytotoxic T cell, Transcription factor, CD8, 030215 immunology
Abstract

CD8+ T cells can be polarized into several different subsets as defined by the cytokines they produce and the transcription factors that govern their differentiation. Here, we identified the polarizing conditions to induce an IL22-producing CD8+ Tc22 subset, which is dependent on IL6 and the aryl hydrocarbon receptor transcription factor. Further characterization showed that this subset was highly cytolytic and expressed a distinct cytokine profile and transcriptome relative to other subsets. In addition, polarized Tc22 were able to control tumor growth as well as, if not better than, the traditional IFNγ-producing Tc1 subset. Tc22s were also found to infiltrate the tumors of human patients with ovarian cancer, comprising up to approximately 30% of expanded CD8+ tumor-infiltrating lymphocytes (TIL). Importantly, IL22 production in these CD8+ TILs correlated with improved recurrence-free survival. Given the antitumor properties of Tc22 cells, it may be prudent to polarize T cells to the Tc22 lineage when using chimeric antigen receptor (CAR)-T or T-cell receptor (TCR) transduction–based immunotherapies.

Published
2020

13. CANDIED: A Pan-Canadian Cohort of Immune Checkpoint Inhibitor-Induced Insulin-Dependent Diabetes Mellitus

Author

Thiago P. Muniz, Daniel V. Araujo, Kerry J. Savage, Tina Cheng, Moumita Saha, Xinni Song, Sabrina Gill, Jose G. Monzon, Debjani Grenier, Sofia Genta, Michael J. Allen, Diana P. Arteaga, Samuel D. Saibil, Marcus O. Butler, Anna Spreafico, and David Hogg

Subjects
Cancer Research, anti-PD-L1, immune checkpoint inhibitor, diabetes mellitus, immune-related adverse event, anti-PD1, anti-CTLA4, survival, Oncology, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Article, RC254-282
Abstract

Simple Summary Immune checkpoint inhibitor-induced insulin-dependent diabetes mellitus (ICI-induced IDDM) is an emerging form of autoimmune diabetes. We describe the characteristics of 34 patients who developed ICI-induced IDDM across five Canadian cancer centres. We observed that presentation with hyperglycemic crisis is common and that patients treated with combination immunotherapy regimens develop ICI-induced IDDM earlier than those treated with monotherapy. Our results suggest that ICI-induced IDDM is irreversible but is associated with high tumor response rates and prolonged survival. The data generated by this study may help clinicians manage ICI-induced IDDM. Abstract Immune checkpoint inhibitor (ICI)-induced insulin-dependent diabetes mellitus (IDDM) is a rare but potentially fatal immune-related adverse event (irAE). In this multicentre retrospective cohort study, we describe the characteristics of ICI-induced IDDM in patients treated across five Canadian cancer centres, as well as their tumor response rates and survival. In 34 patients identified, 25 (74%) were male and 19 (56%) had melanoma. All patients received anti-programed death 1 (anti-PD1) or anti-programmed death ligand-1 (anti-PD-L1)-based therapy. From ICI initiation, median time to onset of IDDM was 2.4 months (95% CI 1.1–3.6). Patients treated with anti-PD1/PD-L1 in combination with an anti-cytotoxic T lymphocyte antigen 4 antibody developed IDDM earlier compared with patients on monotherapy (1.4 vs. 3.9 months, p = 0.05). Diabetic ketoacidosis occurred in 21 (62%) patients. Amongst 30 patients evaluable for response, 10 (33%) had a complete response and another 10 (33%) had a partial response. Median overall survival was not reached (95% CI NE; median follow-up 31.7 months). All patients remained insulin-dependent at the end of follow-up. We observed that ICI-induced IDDM is an irreversible irAE and may be associated with a high response rate and prolonged survival.

Published
2021
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14. Pre-encoded responsiveness to type I interferon in the peripheral immune system defines outcome of PD1 blockade therapy

Author

Giselle M. Boukhaled, Ramy Gadalla, Heidi J. Elsaesser, Diala Abd-Rabbo, Rene Quevedo, S. Y. Cindy Yang, Mengdi Guo, Ben X. Wang, Babak Noamani, Diana Gray, Sally C. M. Lau, Kirsty Taylor, Kyaw Aung, Anna Spreafico, Aaron R. Hansen, Samuel D. Saibil, Naoto Hirano, Cynthia Guidos, Trevor J. Pugh, Tracy L. McGaha, Pamela S. Ohashi, Adrian G. Sacher, Marcus O. Butler, and David G. Brooks

Subjects
Inflammation, T-Lymphocytes, Immunology, Interferon Type I, Immunology and Allergy, Humans, Immunotherapy
Abstract

Type I interferons (IFN-Is) are central regulators of anti-tumor immunity and responses to immunotherapy, but they also drive the feedback inhibition underlying therapeutic resistance. In the present study, we developed a mass cytometry approach to quantify IFN-I-stimulated protein expression across immune cells and used multi-omics to uncover pre-therapy cellular states encoding responsiveness to inflammation. Analyzing peripheral blood cells from multiple cancer types revealed that differential responsiveness to IFN-Is before anti-programmed cell death protein 1 (PD1) treatment was highly predictive of long-term survival after therapy. Unexpectedly, IFN-I hyporesponsiveness efficiently predicted long-term survival, whereas high responsiveness to IFN-I was strongly associated with treatment failure and diminished survival time. Peripheral IFN-I responsive states were not associated with tumor inflammation, identifying a disconnect between systemic immune potential and 'cold' or 'hot' tumor states. Mechanistically, IFN-I responsiveness was epigenetically imprinted before therapy, poising cells for differential inflammatory responses and dysfunctional T cell effector programs. Thus, we identify physiological cell states with clinical importance that can predict success and long-term survival of PD1-blocking immunotherapy.

Published
2021

15. Development of a Metastatic Uveal Melanoma Prognostic Score (MUMPS) for Use in Patients Receiving Immune Checkpoint Inhibitors

Author

Danny Ghazarian, Daniel Vilarim Araujo, Marco Iafolla, Ian King, Zaid Saeed Kamil, John Waldron, April A. N. Rose, Anna Spreafico, Marcus O. Butler, Deirdre Kelly, David Hogg, Kendra Ross, Hatem Krema, Thiago Pimentel Muniz, Normand Laperriere, and Samuel D. Saibil

Subjects
0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Prognostic variable, immune checkpoint inhibitor, Disease, Article, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Prospective cohort study, RC254-282, CTLA4, Proportional hazards model, business.industry, Melanoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Retrospective cohort study, predictive score, medicine.disease, PD1, 030104 developmental biology, 030220 oncology & carcinogenesis, Cohort, immunotherapy, uveal melanoma, business, prognostic, Rare disease
Abstract

Metastatic uveal melanoma (mUM) is a rare disease. There are limited data on prognostic clinical factors for overall survival (OS) in patients with mUM treated with immune checkpoint inhibitors (ICI). Retrospective and non-randomized prospective studies have reported response rates of 0–17% for anti-PD1/L1 ± anti-CTLA4 ICI in mUM, indicating a potential benefit only in a subset of patients. This study evaluates the characteristics associated with ICI benefit in patients with mUM. We performed a single-center retrospective cohort study of patients with mUM who received anti-PD1/L1 ± anti-CTLA4 ICI between 2014–2019. Clinical and genomic characteristics were collected from a chart review. Treatment response and clinical progression were determined by physician assessment. Multivariable Cox regression models and Kaplan–Meier log-rank tests were used to assess differences in clinical progression-free survival (cPFS) and OS between groups and identify clinical variables associated with ICI outcomes. We identified 71 mUM patients who received 75 lines of ICI therapy. Of these, 54 received anti-PD1/L1 alone, and 21 received anti-PD1/L1 + anti-CTLA4. Patient characteristics were: 53% female, 48% were 65 or older, 72% received one or fewer lines of prior therapy. Within our cohort, 53% of patients had developed metastatic disease &lt, 2 years after their initial diagnosis. Bone metastases were present in 12% of patients. The median cPFS was 2.7 months, and the median OS was 10.0 months. In multivariable analyses for both cPFS and OS, the following variables were associated with a good prognosis: ≥2 years from the initial diagnosis to metastatic disease (n = 25), LDH &lt, 1.5 × ULN (n = 45), and absence of bone metastases (n = 66). We developed a Metastatic Uveal Melanoma Prognostic Score (MUMPS). Patients were divided into 3 MUMPS groups based on the number of the above-mentioned prognostic variables: Poor prognosis (0–1), Intermediate prognosis (2) and Good prognosis (3). Good prognosis patients experienced longer cPFS (6.0 months) and OS (34.5 months) than patients with intermediate (2.3 months cPFS, 9.4 months OS) and poor prognosis disease (1.8 months cPFS, 3.9 months OS), p &lt, 0.0001. We developed MUMPS—a prognostic score based on retrospective data that is comprised of 3 readily available clinical variables (time to metastatic diagnosis, presence of bone metastases, and LDH). This MUMPS score has a potential prognostic value. Further validation in independent datasets is warranted to determine the role of this MUMPS score in selecting ICI treatment management for mUM.

Published
2021

16. Development of a Metastatic Uveal Melanoma Prognostic risk Score (MUMPS) for use in patients receiving immune checkpoint inhibitors

Author

John Waldron, Marco Iafolla, Ian King, Thiago Pimentel Muniz, April A.N. Rose, Kendra Ross, Normand Laperriere, Hatem Krema, Marcus O. Butler, David Hogg, Anna Spreafico, Samuel D. Saibil, Danny Ghazarian, Daniel Vilarim Araujo, Deirdre Kelly, and Zaid Saeed Kamil

Subjects
Oncology, Prognostic variable, medicine.medical_specialty, Framingham Risk Score, Proportional hazards model, business.industry, Melanoma, Retrospective cohort study, Disease, medicine.disease, Internal medicine, Cohort, medicine, business, Prospective cohort study
Abstract

BackgroundMetastatic uveal melanoma (mUM) is a rare disease for which no systemic therapy has demonstrated overall survival (OS) benefit. There are no robust data on prognostic factors for OS in patients with mUM treated with immune checkpoint inhibitors (ICI).Retrospective and non-randomized prospective studies have reported response rates of 0-37% for anti-PD1/L1 +/-anti-CTLA4 ICI in mUM, indicating a potential benefit only in a subset of patients. This study evaluates the characteristics associated with ICI benefit in patients with mUM.MethodsWe performed a single-center retrospective cohort study of patients with mUM who received anti-PD1/L1 +/-anti-CTLA4 ICI between 2014–2019. Clinical and genomic characteristics were collected from chart review. Treatment response and clinical progression were determined by physician assessment. Multivariable Cox regression models and Kaplan-Meier log-rank tests were used to assess differences in clinical progression-free survival (cPFS) and OS between groups and to identify clinical variables associated with ICI outcomes.ResultsWe identified 71 mUM patients who received 75 lines of ICI therapy. Of these, 54 received anti-PD1/L1 alone, and 21 received anti-PD1/L1 + anti-CTLA4. Patient characteristics were: 53% female, 48% were 65 or older, 72% received one or fewer lines of prior therapy. Within our cohort, 53% of patients had developed stage IV disease < 2 years after their initial diagnosis. Bone metastases were present in 12% of patients. For the entire cohort, the median cPFS was 2.7 months and median OS was 10.0 months. In multivariable analyses for both cPFS and OS, the following variables were associated with good prognosis: ≥ 2yrs from initial diagnosis to stage IV (n=25), LDH Metastatic Uveal Melanoma Prognostic risk Score (MUMPS). Patients were divided into 3 MUMPS risk groups based on the number of the above-mentioned prognostic variables: Poor risk (0-1), Intermediate risk (2) and Good risk (3). Good risk patients experienced longer cPFS (6.0 months) and OS (34.5 months) than patients with intermediate (2.3 months cPFS, 9.4 months OS) and poor risk disease (1.8 months cPFS, 3.9 months OS); PConclusionWe developed a MUMPS risk score, based on retrospective data, that is comprised of 3 readily available clinical variables (time to stage IV diagnosis, presence of bone metastases, and LDH). This MUMPS risk score has potential prognostic value. Further validation in independent datasets is warranted to determine the role of this MUMPS risk score in selecting ICI treatment management for mUM.

Published
2021

17. Clinical impact of COVID-19 on patients with cancer treated with immune checkpoint inhibition

Author

Paolo A. Ascierto, Serigne Lo, Carlo Tondini, Richard D. Carvajal, Karijn P M Suijkerbuijk, Kerry L. Reynolds, Jessica S.W. Borgers, Jeremy Lupu, Christian U. Blank, Séverine Roy, Christian Posch, Michael Erdmann, Mario Mandalà, Ines Pires da Silva, Matteo S. Carlino, Maria Grazia Vitale, Tim Cooksley, F. Stephen Hodi, Megan H. Trager, Carola Berking, Leyre Zubiri, Laura Pala, Sharon Nahm, Dirk Schadendorf, Paola Queirolo, Alon Vaisman, Neha Papneja, Paul Lorigan, Joanna Mangana, Aljosja Rogiers, Alexander M. Menzies, Thiago Pimentel Muniz, Caroline Robert, Ryan J. Sullivan, John B. A. G. Haanen, Marcus O. Butler, Reinhard Dummer, Peter Bowling, Wilson H. Miller, Osama E. Rahma, Arielle Elkrief, Samuel D. Saibil, Chiara Tentori, Joseph M. Grimes, Michael Manos, Lisa Zimmer, Georgina V. Long, April A.N. Rose, and Axel Hauschild

Subjects
Male, 0301 basic medicine, Cancer Research, viruses, Medizin, law.invention, Cohort Studies, 0302 clinical medicine, law, Neoplasms, Immunology and Allergy, Immune Checkpoint Inhibitors, RC254-282, Cause of death, Aged, 80 and over, Clinical/Translational Cancer Immunotherapy, education.field_of_study, Manchester Cancer Research Centre, Mortality rate, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, virus diseases, Middle Aged, Intensive care unit, ddc, Oncology, 030220 oncology & carcinogenesis, Molecular Medicine, Female, immunotherapy, Adult, medicine.medical_specialty, Immunology, Population, macromolecular substances, 03 medical and health sciences, Internal medicine, Intensive care, medicine, Humans, ddc:610, Ticilimumab, Risk factor, education, Aged, Retrospective Studies, Pharmacology, SARS-CoV-2, business.industry, ResearchInstitutes_Networks_Beacons/mcrc, COVID-19, Cancer, biochemical phenomena, metabolism, and nutrition, medicine.disease, Coronavirus, 030104 developmental biology, nervous system, business
Abstract

BackgroundPatients with cancer who are infected with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) are more likely to develop severe illness and die compared with those without cancer. The impact of immune checkpoint inhibition (ICI) on the severity of COVID-19 illness is unknown. The aim of this study was to investigate whether ICI confers an additional risk for severe COVID-19 in patients with cancer.MethodsWe analyzed data from 110 patients with laboratory-confirmed SARS-CoV-2 while on treatment with ICI without chemotherapy in 19 hospitals in North America, Europe and Australia. The primary objective was to describe the clinical course and to identify factors associated with hospital and intensive care (ICU) admission and mortality.FindingsThirty-five (32%) patients were admitted to hospital and 18 (16%) died. All patients who died had advanced cancer, and only four were admitted to ICU. COVID-19 was the primary cause of death in 8 (7%) patients. Factors independently associated with an increased risk for hospital admission were ECOG ≥2 (OR 39.25, 95% CI 4.17 to 369.2, p=0.0013), treatment with combination ICI (OR 5.68, 95% CI 1.58 to 20.36, p=0.0273) and presence of COVID-19 symptoms (OR 5.30, 95% CI 1.57 to 17.89, p=0.0073). Seventy-six (73%) patients interrupted ICI due to SARS-CoV-2 infection, 43 (57%) of whom had resumed at data cut-off.InterpretationCOVID-19–related mortality in the ICI-treated population does not appear to be higher than previously published mortality rates for patients with cancer. Inpatient mortality of patients with cancer treated with ICI was high in comparison with previously reported rates for hospitalized patients with cancer and was due to COVID-19 in almost half of the cases. We identified factors associated with adverse outcomes in ICI-treated patients with COVID-19.

Published
2021

18. Biologic subtypes of melanoma predict survival benefit of combination anti-PD1+anti-CTLA4 immune checkpoint inhibitors versus anti-PD1 monotherapy

Author

Susan M. Armstrong, Danny Ghazarian, Thiago Pimentel Muniz, Ian F. G. King, Zaid Saeed Kamil, Kendra Ross, Samuel D. Saibil, David Hogg, Anna Spreafico, Marcus O. Butler, Deirdre Kelly, April A.N. Rose, and Diana Paola Arteaga

Subjects
Oncology, Neuroblastoma RAS viral oncogene homolog, Male, Cancer Research, medicine.medical_treatment, GTP Phosphohydrolases, 0302 clinical medicine, Immunotherapy Biomarkers, Immunology and Allergy, 030212 general & internal medicine, Neoplasm Metastasis, Immune Checkpoint Inhibitors, RC254-282, Melanoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Drug Synergism, Primary tumor, Nivolumab, Treatment Outcome, 030220 oncology & carcinogenesis, Cohort, Molecular Medicine, Female, immunotherapy, Proto-Oncogene Proteins B-raf, medicine.medical_specialty, Immunology, programmed cell death 1 receptor, 03 medical and health sciences, Internal medicine, medicine, melanoma, Humans, Retrospective Studies, Pharmacology, Proportional hazards model, business.industry, Membrane Proteins, Retrospective cohort study, Immunotherapy, medicine.disease, Ipilimumab, Survival Analysis, Clinical trial, tumor biomarkers, Mutation, genetic markers, business
Abstract

PurposeAnti-programmed cell death protein 1 (PD1)±anti-cytotoxic T-lymphocyte associated protein 4 (CTLA4) immune checkpoint inhibitors (ICIs) are standard therapeutic options for metastatic melanoma. We assessed whether biologic subtype according to primary tumor type or genomic subtype can function as predictive biomarkers for anti-PD1±anti-CTLA4 ICI in patients with advanced melanoma.MethodsWe performed a single-center retrospective cohort analysis of patients who received anti-PD1±anti-CTLA4 ICI for advanced melanoma between 2012 and 2019. Primary tumor type, BRAF and NRAS mutation status, and other covariates were abstracted from chart review. Log-rank tests and multivariable Cox regression models were used to assess differences in clinical progression-free (cPFS) and overall survival (OS).ResultsWe identified 230 patients who received 249 lines of anti-PD1±anti-CTLA4 ICI for unresectable or metastatic disease. Of these patients, 74% were cutaneous, 11% mucosal, 8% unknown primary and 7% acral. BRAF and NRAS mutations were identified in 35% and 28% of patients, respectively. In multivariable analyses of the entire cohort, acral or mucosal primary tumor type, >3 metastatic sites, elevated LDH were predictive of shorter cPFS and OS. Combination ICI therapy was associated with longer cPFS (HR 0.57, 95% CI 0.38 to 0.86, p=0.007) and OS (HR 0.42, 95% CI 0.28 to 0.65, pNRAS (HR 0.24, 95% CI 0.10 to 0.62, p=0.003, n=69) and BRAF V600E/K (HR 0.47, 95% CI 0.24 to 0.90, p=0.024, n=86) mutant melanoma but not BRAF/NRAS wild-type (n=94) melanoma.ConclusionsIn our cohort, primary melanoma tumor type and genomic subtype were independent predictive markers of cPFS and OS for patients with metastatic melanoma receiving anti-PD1 ICI. Primary tumor type and genomic subtype—including NRAS—should be further evaluated in prospective clinical trials to determine their value as predictive markers. Biologic subtypes may facilitate clinical decision-making when recommending combination ICI treatment (anti-PD1±anti-CTLA4) versus anti-PD1 alone for patients with metastatic melanoma.

Published
2021

19. Coenzyme A fuels T cell anti-tumor immunity

Author

Michael St. Paul, Samuel D. Saibil, SeongJun Han, Kavita Israni-Winger, Scott C. Lien, Rob C. Laister, Azin Sayad, Susanne Penny, Rodabe N. Amaria, Lauren E. Haydu, Carlos R. Garcia-Batres, Meghan Kates, David T. Mulder, Céline Robert-Tissot, Matthew J. Gold, Charles W. Tran, Alisha R. Elford, Linh T. Nguyen, Trevor J. Pugh, Devanand M. Pinto, Jennifer A. Wargo, and Pamela S. Ohashi

Subjects
Mice, T-Lymphocyte Subsets, Physiology, Animals, Humans, Cell Differentiation, Coenzyme A, Cell Biology, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Molecular Biology
Abstract

Metabolic programming is intricately linked to the anti-tumor properties of T cells. To study the metabolic pathways associated with increased anti-tumor T cell function, we utilized a metabolomics approach to characterize three different CD8

Published
2021

20. Glycogen Synthase Kinase-3 Modulates Cbl-b and Constrains T Cell Activation

Author

Kelly Tai, Mitchell G. Vainberg, Tak W. Mak, Han You, Josef M. Penninger, Michael E. Parsons, James R. Woodgett, Amy E. Lin, Sara R. Hamilton, Kristine M. Garza, Karl S. Lang, Alisha R. Elford, Kip Wigmore, Charles W. Tran, Thierry Le Bihan, Samuel D. Saibil, and Pamela S. Ohashi

Subjects
0301 basic medicine, T cell, Immunology, Medizin, Autoimmunity, Mice, Transgenic, macromolecular substances, Lymphocyte Activation, Glycogen Synthase Kinase 3, Mice, Phosphatidylinositol 3-Kinases, Phosphoserine, 03 medical and health sciences, 0302 clinical medicine, Species Specificity, T-Lymphocyte Subsets, GSK-3, Immune Tolerance, medicine, Animals, Protein Isoforms, Immunology and Allergy, Amino Acid Sequence, Proto-Oncogene Proteins c-cbl, Phosphorylation, Protein kinase A, Protein kinase B, Adaptor Proteins, Signal Transducing, Mice, Knockout, biology, T-cell receptor, CD28, Specific Pathogen-Free Organisms, Ubiquitin ligase, Cell biology, Enzyme Activation, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, biology.protein, Cancer research, Signal transduction, Protein Processing, Post-Translational, Proto-Oncogene Proteins c-akt, Sequence Alignment, Signal Transduction, 030215 immunology
Abstract

The decision between T cell activation and tolerance is governed by the spatial and temporal integration of diverse molecular signals and events occurring downstream of TCR and costimulatory or coinhibitory receptor engagement. The PI3K–protein kinase B (PKB; also known as Akt) signaling pathway is a central axis in mediating proximal signaling events of TCR and CD28 engagement in T cells. Perturbation of the PI3K–PKB pathway, or the loss of negative regulators of T cell activation, such as the E3 ubiquitin ligase Cbl-b, have been reported to lead to increased susceptibility to autoimmunity. In this study, we further examined the molecular pathway linking PKB and Cbl-b in murine models. Our data show that the protein kinase GSK-3, one of the first targets identified for PKB, catalyzes two previously unreported phosphorylation events at Ser476 and Ser480 of Cbl-b. GSK-3 inactivation by PKB abrogates phosphorylation of Cbl-b at these two sites and results in reduced Cbl-b protein levels. We further show that constitutive activation of PKB in vivo results in a loss of tolerance that is mediated through the downregulation of Cbl-b. Altogether, these data indicate that the PI3K–PKB–GSK-3 pathway is a novel regulatory axis that is important for controlling the decision between T cell activation and tolerance via Cbl-b.

Published
2017

21. IL6 Induces an IL22

Author

Michael, St Paul, Samuel D, Saibil, Scott C, Lien, SeongJun, Han, Azin, Sayad, David T, Mulder, Carlos R, Garcia-Batres, Alisha R, Elford, Kavita, Israni-Winger, Céline, Robert-Tissot, Michael, Zon, Sarah Rachel, Katz, Patricia A, Shaw, Blaise A, Clarke, Marcus Q, Bernardini, Linh T, Nguyen, Benjamin, Haibe-Kains, Trevor J, Pugh, and Pamela S, Ohashi

Subjects
Mice, Knockout, Ovarian Neoplasms, Interleukin-6, Interleukins, Melanoma, Experimental, Receptors, Antigen, T-Cell, Cell Polarity, Mice, Transgenic, T-Lymphocytes, Helper-Inducer, Immunotherapy, Adoptive, Mice, Inbred C57BL, Lymphocytes, Tumor-Infiltrating, Receptors, Aryl Hydrocarbon, T-Lymphocyte Subsets, Basic Helix-Loop-Helix Transcription Factors, Tumor Cells, Cultured, Animals, Humans, Female, T-Box Domain Proteins, Transcriptome, T-Lymphocytes, Cytotoxic
Abstract

CD8

Published
2019

22. Immune checkpoint inhibitors in cancer immunotherapy

Author

Samuel D. Saibil, Alexandra Saltman, and Megan E. Himmel

Subjects
medicine.medical_treatment, Immune checkpoint inhibitors, chemical and pharmacologic phenomena, 03 medical and health sciences, 0302 clinical medicine, Immune system, Cancer immunotherapy, Neoplasms, Programmed cell death 1, Humans, Medicine, Cytotoxic T cell, 030212 general & internal medicine, Receptor, Immune Checkpoint Inhibitors, Practice, biology, business.industry, General Medicine, Immunotherapy, Immune checkpoint, 030220 oncology & carcinogenesis, biology.protein, Cancer research, business
Abstract

Tumour cells can evade destruction by the immune system by triggering immune checkpoint receptors, such as cytotoxic T-lymphocyte–associated protein 4 (CTLA-4), programmed cell death protein 1 (PD-1) or programmed death-ligand 1 (PD-L1), that are expressed on T-cells and whose engagement inhibit T

Published
2020

23. ARIH2 is essential for embryogenesis, and its hematopoietic deficiency causes lethal activation of the immune system

Author

Simon Preston, Yongkai Ow, Jesse G. Toe, Amy E. Lin, Hamish W Scott, Andrew Wakeham, Tak W. Mak, James P Cooney, Gregor Ebert, Jennifer Silvester, Raymond H. Kim, Samuel D. Saibil, Pamela S. Ohashi, Annick You-Ten, Arda Shahinian, Marc Pellegrini, Masato Sasaki, Dilan Dissanayake, and Gordon S. Duncan

Subjects
Transcriptional Activation, Multiple Organ Failure, Ubiquitin-Protein Ligases, Immunology, Embryonic Development, Mice, Immune system, Ubiquitin, Transcription (biology), Animals, Humans, Immunology and Allergy, Molecular Targeted Therapy, Transcription factor, Cells, Cultured, Mice, Knockout, biology, NF-kappa B, Ubiquitination, Dendritic Cells, NFKB1, Hematopoiesis, Cell biology, Ubiquitin ligase, Mice, Inbred C57BL, Disease Models, Animal, Haematopoiesis, Immune System, biology.protein, Stem cell
Abstract

The E3 ligase ARIH2 has an unusual structure and mechanism of elongating ubiquitin chains. To understand its physiological role, we generated gene-targeted mice deficient in ARIH2. ARIH2 deficiency resulted in the embryonic death of C57BL/6 mice. On a mixed genetic background, the lethality was attenuated, with some mice surviving beyond weaning and then succumbing to an aggressive multiorgan inflammatory response. We found that in dendritic cells (DCs), ARIH2 caused degradation of the inhibitor IκBβ in the nucleus, which abrogated its ability to sequester, protect and transcriptionally coactivate the transcription factor subunit p65 in the nucleus. Loss of ARIH2 caused dysregulated activation of the transcription factor NF-κB in DCs, which led to lethal activation of the immune system in ARIH2-sufficent mice reconstituted with ARIH2-deficient hematopoietic stem cells. Our data have therapeutic implications for targeting ARIH2 function.

Published
2012

24. c-Rel phenocopies PKCθ but not Bcl-10 in regulating CD8+T-cell activationversustolerance

Author

Tak W. Mak, Alisha R. Elford, Kiichi Murakami, Jürgen Ruland, Leslie Po, Samuel D. Saibil, Yong-Chen Lu, Laurence Chapatte, Pamela S. Ohashi, Steve Gerondakis, and Elissa K. Deenick

Subjects
P50, Blotting, Western, Immunology, Mice, Transgenic, CD8-Positive T-Lymphocytes, Biology, Lymphocyte Activation, Mice, Animals, Immunology and Allergy, Cytotoxic T cell, Transcription factor, Protein Kinase C, Adaptor Proteins, Signal Transducing, Clonal Anergy, NF-kappa B, NFAT, B-Cell CLL-Lymphoma 10 Protein, Phenotype, Proto-Oncogene Proteins c-rel, Cell biology, Isoenzymes, AP-1 transcription factor, Protein Kinase C-theta, REL, CD8, Signal Transduction
Abstract

Elucidating the signaling events that promote T-cell tolerance versus activation provides important insights for manipulating immunity in vivo. Previous studies have suggested that the absence of PKCtheta results in the induction of anergy and that the balance between the induction of the transcription factors NFAT, AP1 and NF-kappaB plays a key role in determining whether T-cell anergy or activation is induced. Here, we examine whether Bcl-10 and specific family members of NF-kappaB act downstream of PKCtheta to alter CD8(+) T-cell activation and/or anergy. We showed that T cells from mice deficient in c-Rel but not NF-kappaB1 (p50) have increased susceptibility to the induction of anergy, similar to T cells from PKCtheta-deficient mice. Surprisingly T cells from Bcl-10-deficient mice showed a strikingly different phenotype to the PKCtheta-deficient T cells, with a severe block in TCR-mediated activation. Furthermore, we have also shown that survival signals downstream of NF-kappaB, are uncoupled from signals that mediate T-cell anergy. These results suggest that c-Rel plays a critical role downstream of PKCtheta in controlling CD8(+) T-cell anergy induction.

Published
2010

25. CD4+ and CD8+ T Cell Survival Is Regulated Differentially by Protein Kinase Cθ, c-Rel, and Protein Kinase B

Author

Elissa K. Deenick, Mitchell G. Vainberg, Nicole Liadis, Pamela S. Ohashi, James R. Woodgett, Samuel D. Saibil, Heather Baerg, Steve Gerondakis, Alisha R. Elford, and Russell G. Jones

Subjects
CD4-Positive T-Lymphocytes, Cell Survival, T cell, Immunology, bcl-X Protein, CD8-Positive T-Lymphocytes, Biology, Lymphocyte Activation, TCIRG1, Mice, Interleukin 21, medicine, Animals, Immunology and Allergy, Cytotoxic T cell, IL-2 receptor, Protein Kinase C, Mice, Knockout, ZAP70, NF-kappa B p50 Subunit, CD28, Proto-Oncogene Proteins c-rel, Cell biology, Isoenzymes, medicine.anatomical_structure, Gene Expression Regulation, Protein Kinase C-theta, Interleukin-2, Proto-Oncogene Proteins c-akt, CD8, Signal Transduction
Abstract

An effective immune response requires the expansion and survival of a large number of activated T cells. This study compared the role of protein kinase C (PKC)θ and associated signaling molecules in the survival of activated primary CD4+ vs CD8+ murine T cells. We demonstrate that the absence of PKCθ resulted in a moderate survival defect in CD4+ T cells and a striking survival defect of CD8+ T lymphocytes. CD8+ T cells lacking the c-Rel, but not the NF-κB1/p50, member of the NF-κB family of transcription factors displayed a similar impairment in cell survival as PKCθ−/− CD8+ T lymphocytes. This implicates c-Rel as a key target of PKCθ-mediated survival signals in CD8+ T cells. In addition, both c-Rel−/− and PKCθ−/− T cells also displayed impaired expression of the antiapoptotic Bcl-xL protein upon activation. Changes in Bcl-xL expression, however, did not correlate with the survival of CD4+ or CD8+ lymphocytes. The addition of protein kinase B-mediated survival signals could restore partially CD4+ T cell viability, but did not dramatically influence CD8+ survival. Active protein kinase B was also unable to restore proliferative responses in CD8+ PKCθ−/− T cells. The survival of CD4+ and CD8+ T cells deficient in either PKCθ or c-Rel, however, was promoted by the addition of IL-2. Collectively, these data demonstrate that CD4+ and CD8+ T cell survival signals are differentially programmed.

Published
2007

26. DNA damage- and stress-induced apoptosis occurs independently of PIDD

Author

Samuel Benchimol, Andrea Jurisicova, Kiichi Murakami, Samuel D. Saibil, Wen Chen Yeh, Alisha R. Elford, Nien Jung Chen, Elzbieta Matysiak-Zablocki, Pamela S. Ohashi, Ira R. Kim, and Madeleine Bonnard

Subjects
Cancer Research, Death Domain Receptor Signaling Adaptor Proteins, DNA damage, Clinical Biochemistry, Caspase 2, Pharmaceutical Science, Apoptosis, Mice, Stress, Physiological, In Situ Nick-End Labeling, Animals, Receptor, Death domain, Pharmacology, biology, Biochemistry (medical), Gene targeting, Cell Biology, Cell biology, Gene Targeting, biology.protein, Signal transduction, Tumor Suppressor Protein p53, Carrier Proteins, Protein Processing, Post-Translational, Whole-Body Irradiation, DNA Damage, Signal Transduction
Abstract

The p53-induced protein with a death domain, PIDD, was identified as a p53 target gene whose main role is to execute apoptosis in a p53-dependent manner. To investigate the physiological role of PIDD in apoptosis, we generated PIDD-deficient mice. Here, we report that, although PIDD expression is inducible upon DNA damage, PIDD-deficient mice undergo apoptosis normally not only in response to DNA damage, but also in response to various p53-independent stress signals and to death receptor (DR) engagement. This indicates that PIDD is not required for DNA damage-, stress-, and DR-induced apoptosis. Also, in the absence of PIDD, both caspase-2 processing and activation occur in response to DNA damage. Our findings demonstrate that PIDD does not play an essential role for all p53-mediated or p53-independent apoptotic pathways.

Published
2009

27. RIP2 contributes to Nod signaling but is not essential for T cell proliferation, T helper differentiation or TLR responses

Author

Margareta Wilhelm, Richard A. Flavell, Pamela S. Ohashi, Tak W. Mak, Samuel D. Saibil, and Håkan Hall

Subjects
Cellular differentiation, T cell, Immunology, Blotting, Western, Nod, Biology, Lymphocyte Activation, Mice, Immune system, Receptor-Interacting Protein Serine-Threonine Kinase 2, medicine, Immunology and Allergy, Macrophage, Animals, Arenaviridae Infections, Lymphocytic choriomeningitis virus, Cell Proliferation, Mice, Knockout, Innate immune system, Cell growth, Toll-Like Receptors, Cell Differentiation, T-Lymphocytes, Helper-Inducer, Cell biology, Mice, Inbred C57BL, Nod Signaling Adaptor Proteins, medicine.anatomical_structure, Receptor-Interacting Protein Serine-Threonine Kinases, Cytokines
Abstract

Receptor-interacting protein 2 (RIP2), also known as CARDIAK and RICK, has been reported to play a role in both adaptive T cell responses and innate immunity as a mediator in TLR signaling and nucleotide-binding oligomerization domain (Nod) signaling. Because initial reports remain controversial, we have further examined both innate and adaptive immune responses in RIP2-deficient mice on the C57BL/6 background. Despite the up-regulation of RIP2 after T cell activation, we could not detect any defect in T cell proliferation or Th1/Th2 responses in RIP2-KO mice. Furthermore, we found that TLR responses in RIP2-deficient macrophages were normal. However, our analysis showed that Nod signaling was impaired in macrophages from RIP2-deficient mice. In conclusion, our data demonstrate a critical role for RIP2 in Nod signaling, while T cell proliferation, T helper differentiation and TLR responses were unaffected by the absence of RIP2.

Published
2007

28. The sound of silence: modulating anergy in T lymphocytes

Author

Elissa K. Deenick, Samuel D. Saibil, and Pamela S. Ohashi

Subjects
Cell signaling, Diacylglycerol Kinase, T cell, T-Lymphocytes, Immunology, Receptors, Antigen, T-Cell, Biology, B7-H1 Antigen, Antigens, CD, medicine, Immune Tolerance, Immunology and Allergy, Cytotoxic T cell, Animals, Humans, Protein Isoforms, Adaptor Proteins, Signal Transducing, Clonal Anergy, Effector, T-cell receptor, Membrane Proteins, Cell biology, medicine.anatomical_structure, Second messenger system, Signal transduction, Lipid modification, Cyclin-Dependent Kinase Inhibitor p27, Signal Transduction
Abstract

Understanding the intercellular and intracellular mechanisms that maintain anergy and prevent the induction of full effector function is one avenue that may allow us to manipulate immune responses. Recent studies of T cell receptor (TCR)-proximal signaling events in different models of T cell unresponsiveness have suggested that biochemically distinct forms of anergy may exist in vivo. T cell responsiveness can be altered through the control of the intracellular pool of key second messengers, such as diacylglycerol (DAG) or the lipid modification of signaling molecules, such as the Linker for activated T cells (LAT). Studies on the molecule programmed death-1 (PD-1) and its ligands have revealed that tissue-resident signals are essential in the maintenance of T cell unresponsiveness. Thus, the emerging view is that T cell anergy is a dynamic state whose establishment and maintenance can be influenced by numerous different signaling pathways.

Published
2007

29. Weak agonist self-peptides promote selection and tuning of virus-specific T cells

Author

Toshiaki Ohteki, Brian H. Barber, Samuel D. Saibil, Josef M. Penninger, J. Shabanowitz, Arsen Zakarian, Hiroshi Nishina, Forest M. White, Patrice Hugo, Pamela S. Ohashi, Alisha R. Elford, Mark A. Luscher, and Donald F. Hunt

Subjects
Transgene, T cell, T-Lymphocytes, Immunology, Molecular Sequence Data, Receptors, Antigen, T-Cell, Peptide, Dopamine beta-Hydroxylase, Biology, Lymphocyte Activation, Clonal deletion, Mice, medicine, Immunology and Allergy, Animals, Lymphocytic choriomeningitis virus, Amino Acid Sequence, Histocompatibility Antigen H-2D, chemistry.chemical_classification, T-cell receptor, H-2 Antigens, In vitro, Peptide Fragments, Fetal Thymic Organ Culture, Cell biology, ErbB Receptors, medicine.anatomical_structure, chemistry, Signal transduction
Abstract

Recent progress has begun to define the interactions and signaling pathways that are triggered during positive selection. To identify and further examine self-peptides that can mediate positive selection, we searched a protein-database to find peptides that have minimal homology with the viral peptide (p33) that activates a defined P14 transgenic TCR. We identified four peptides that could bind the restriction element H-2D(b) and induce proliferation of P14 transgenic splenocytes at high concentration. Two of the four peptides (DBM and RPP) were able to positively select the virus-specific TCR in fetal thymic organ culture but were unable to induce clonal deletion. Reverse-phase HPLC and mass spectrometry demonstrated that these peptides were presented by H-2D(b) molecules on thymic epithelial cell lines. We also examined whether the selecting ligands altered T cell responsiveness in vitro. DBM-selected T cells lost their ability to respond to the positively selecting ligand DBM, whereas RPP-selected T cells only retained their ability to respond to high concentrations of RPP. These results demonstrate that self-peptides that mediate positive selection can differentially "tune" the activation threshold of T cells and alter the functional repertoire of T cells.

Published
2003

30. Marked induction of the IAP family antiapoptotic proteins survivin and XIAP by VEGF in vascular endothelial cells

Author

Samuel D. Saibil, Jennifer Tran, Janusz Rak, Eric C. LaCasse, Capucine Sheehan, Robert G. Korneluk, and Robert S. Kerbel

Subjects
Vascular Endothelial Growth Factor A, Angiogenesis, Survivin, Biophysics, Apoptosis, X-Linked Inhibitor of Apoptosis Protein, Endothelial Growth Factors, Vascular endothelial growth inhibitor, Biochemistry, Inhibitor of Apoptosis Proteins, chemistry.chemical_compound, Vasculogenesis, Humans, Receptors, Growth Factor, Molecular Biology, Lymphokines, Vascular Endothelial Growth Factors, Proteins, Receptor Protein-Tyrosine Kinases, Cell Biology, Cell biology, Neoplasm Proteins, Up-Regulation, Vascular endothelial growth factor, Vascular endothelial growth factor B, Vascular endothelial growth factor A, Receptors, Vascular Endothelial Growth Factor, chemistry, Vascular endothelial growth factor C, Protein Biosynthesis, Endothelium, Vascular, Microtubule-Associated Proteins
Abstract

Vascular endothelial growth factor (VEGF) is a potent angiogenic factor that has been shown to act as an endothelial cell mitogen as well as a vascular permeability factor. Several recent reports have also implicated VEGF as a major survival factor for endothelial cells during angiogenesis and vasculogenesis along with other growth factors such as bFGF and angiopoietin-1. VEGF has been shown to mediate this additional function, at least in part through the induction of bcl-2 and the activation of the PI3 kinase-Akt/PKB signaling pathway. We report here that VEGF can also mediate the induction/upregulation of members of a newly discovered family of antiapoptotic proteins, namely the Inhibitors of Apoptosis (IAP), in vascular endothelial cells. We show that VEGF(165) leads to the induction of XIAP (2.9-fold) and survivin (19.1-fold) protein in human umbilical vein endothelial cells (HUVECs). In contrast, bFGF had little effect on XIAP expression, but produced approximately a 10-fold induction on survivin. VEGF-dependent upregulation of survivin could be prevented by cell cycle arrest in the G1 and S phases. These findings implicate that the survival and mitotic functions of VEGF in an angiogenic context may be more intrinsically related than previously anticipated. Moreover, they also raise the possibility of therapeutically targeting XIAP or survivin in antiangiogenic therapy as a means of suppressing tumor growth, in addition to directly targeting tumor cells which express these survival proteins.

Published
1999

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