Search

Your search keyword '"Sayers, Thomas J."' showing total 266 results
Start Over Author "Sayers, Thomas J."
266 results on '"Sayers, Thomas J."'

1. Bortezomib Improves Adoptive T-cell Therapy by Sensitizing Cancer Cells to FasL Cytotoxicity

Author

Shanker, Anil, Pellom, Samuel T, Dudimah, Duafalia F, Thounaojam, Menaka C, de Kluyver, Rachel L, Brooks, Alan D, Yagita, Hideo, McVicar, Daniel W, Murphy, William J, Longo, Dan L, and Sayers, Thomas J

Subjects
Immunization, Rare Diseases, Vaccine Related, Cancer, 1.1 Normal biological development and functioning, 5.2 Cellular and gene therapies, Development of treatments and therapeutic interventions, Underpinning research, Animals, Antineoplastic Agents, Bortezomib, Combined Modality Therapy, Cytotoxicity, Immunologic, Fas Ligand Protein, Flow Cytometry, Humans, Immunoblotting, Immunohistochemistry, Immunotherapy, Adoptive, Kidney Neoplasms, Melanoma, Mice, Mice, Inbred BALB C, Mice, Knockout, T-Lymphocytes, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

Cancer immunotherapy shows great promise but many patients fail to show objective responses, including in cancers that can respond well, such as melanoma and renal adenocarcinoma. The proteasome inhibitor bortezomib sensitizes solid tumors to apoptosis in response to TNF-family death ligands. Because T cells provide multiple death ligands at the tumor site, we investigated the effects of bortezomib on T-cell responses in immunotherapy models involving low-avidity antigens. Bortezomib did not affect lymphocyte or tissue-resident CD11c(+)CD8(+) dendritic cell counts in tumor-bearing mice, did not inhibit dendritic cell expression of costimulatory molecules, and did not decrease MHC class I/II-associated antigen presentation to cognate T cells. Rather, bortezomib activated NF-κB p65 in CD8(+) T cells, stabilizing expression of T-cell receptor CD3ζ and IL2 receptor-α, while maintaining IFNγ secretion to improve FasL-mediated tumor lysis. Notably, bortezomib increased tumor cell surface expression of Fas in mice as well as human melanoma tissue from a responsive patient. In renal tumor-bearing immunodeficient Rag2(-/-) mice, bortezomib treatment after adoptive T-cell immunotherapy reduced lung metastases and enhanced host survival. Our findings highlight the potential of proteasome inhibitors to enhance antitumor T-cell function in the context of cancer immunotherapy.

Published
2015

2. NK Cells Preferentially Target Tumor Cells with a Cancer Stem Cell Phenotype

Author

Ames, Erik, Canter, Robert J, Grossenbacher, Steven K, Mac, Stephanie, Chen, Mingyi, Smith, Rachel C, Hagino, Takeshi, Perez-Cunningham, Jessica, Sckisel, Gail D, Urayama, Shiro, Monjazeb, Arta M, Fragoso, Ruben C, Sayers, Thomas J, and Murphy, William J

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Rare Diseases, Stem Cell Research - Nonembryonic - Human, Stem Cell Research, Digestive Diseases, Pancreatic Cancer, Cancer, Orphan Drug, 2.1 Biological and endogenous factors, 5.2 Cellular and gene therapies, Animals, Antigens, CD, Cell Line, Tumor, Female, Humans, Immunity, Cellular, Killer Cells, Natural, Mice, Mice, Inbred NOD, Neoplasms, Neoplastic Stem Cells, Biochemistry and cell biology
Abstract

Increasing evidence supports the hypothesis that cancer stem cells (CSCs) are resistant to antiproliferative therapies, able to repopulate tumor bulk, and seed metastasis. NK cells are able to target stem cells as shown by their ability to reject allogeneic hematopoietic stem cells but not solid tissue grafts. Using multiple preclinical models, including NK coculture (autologous and allogeneic) with multiple human cancer cell lines and dissociated primary cancer specimens and NK transfer in NSG mice harboring orthotopic pancreatic cancer xenografts, we assessed CSC viability, CSC frequency, expression of death receptor ligands, and tumor burden. We demonstrate that activated NK cells are capable of preferentially killing CSCs identified by multiple CSC markers (CD24(+)/CD44(+), CD133(+), and aldehyde dehydrogenase(bright)) from a wide variety of human cancer cell lines in vitro and dissociated primary cancer specimens ex vivo. We observed comparable effector function of allogeneic and autologous NK cells. We also observed preferential upregulation of NK activation ligands MICA/B, Fas, and DR5 on CSCs. Blocking studies further implicated an NKG2D-dependent mechanism for NK killing of CSCs. Treatment of orthotopic human pancreatic cancer tumor-bearing NSG mice with activated NK cells led to significant reductions in both intratumoral CSCs and tumor burden. Taken together, these data from multiple preclinical models, including a strong reliance on primary human cancer specimens, provide compelling preclinical evidence that activated NK cells preferentially target cancer cells with a CSC phenotype, highlighting the translational potential of NK immunotherapy as part of a combined modality approach for refractory solid malignancies.

Published
2015

3. Anti-proliferative but not anti-angiogenic tyrosine kinase inhibitors enrich for cancer stem cells in soft tissue sarcoma

Author

Canter, Robert J, Ames, Erik, Mac, Stephanie, Grossenbacher, Steven K, Chen, Mingyi, Li, Chin-Shang, Borys, Dariusz, Smith, Rachel C, Tellez, Joe, Sayers, Thomas J, Monjazeb, Arta M, and Murphy, William J

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Stem Cell Research - Nonembryonic - Human, Stem Cell Research, Rare Diseases, Stem Cell Research - Nonembryonic - Non-Human, Clinical Research, Cancer, Aldehyde Dehydrogenase 1 Family, Angiogenesis Inhibitors, Animals, Antigens, CD, Cell Line, Tumor, Cell Proliferation, Cell Survival, Female, Humans, Indazoles, Isoenzymes, Liver Neoplasms, Lung Neoplasms, Mice, Inbred NOD, Neoadjuvant Therapy, Neoplastic Stem Cells, Niacinamide, Phenylurea Compounds, Protein Kinase Inhibitors, Pyrimidines, Retinal Dehydrogenase, Sarcoma, Sorafenib, Sulfonamides, Tissue Array Analysis, Xenograft Model Antitumor Assays, Soft tissue sarcoma, Cancer stem cells, Tyrosine kinase inhibitors, Pazopanib, Regorafenib, ALDH, Public Health and Health Services, Oncology & Carcinogenesis, Oncology and carcinogenesis, Epidemiology
Abstract

BackgroundIncreasing studies implicate cancer stem cells (CSCs) as the source of resistance and relapse following conventional cytotoxic therapies. Few studies have examined the response of CSCs to targeted therapies, such as tyrosine kinase inhibitors (TKIs). We hypothesized that TKIs would have differential effects on CSC populations depending on their mechanism of action (anti-proliferative vs. anti-angiogenic).MethodsWe exposed human sarcoma cell lines to sorafenib, regorafenib, and pazopanib and assessed cell viability and expression of CSC markers (ALDH, CD24, CD44, and CD133). We evaluated survival and CSC phenotype in mice harboring sarcoma metastases after TKI therapy. We exposed dissociated primary sarcoma tumors to sorafenib, regorafenib, and pazopanib, and we used tissue microarray (TMA) and primary sarcoma samples to evaluate the frequency and intensity of CSC markers after neoadjuvant therapy with sorafenib and pazopanib. Parametric and non-parametric statistical analyses were performed as appropriate.ResultsAfter functionally validating the CSC phenotype of ALDHbright sarcoma cells, we observed that sorafenib and regorafenib were cytotoxic to sarcoma cell lines (P < 0.05), with a corresponding 1.4 - 2.8 fold increase in ALDHbright cells from baseline (P < 0.05). In contrast, we observed negligible effects on viability and CSC sub-populations with pazopanib. At low doses, there was progressive CSC enrichment in vitro after longer term exposure to sorafenib although the anti-proliferative effects were attenuated. In vivo, sorafenib improved median survival by 11 days (P < 0.05), but enriched ALDHbright cells 2.5 - 2.8 fold (P < 0.05). Analysis of primary human sarcoma samples revealed direct cytotoxicity following exposure to sorafenib and regorafenib with a corresponding increase in ALDHbright cells (P < 0.05). Again, negligible effects from pazopanib were observed. TMA analysis of archived specimens from sarcoma patients treated with sorafenib demonstrated significant enrichment for ALDHbright cells in the post-treatment resection specimen (P < 0.05), whereas clinical specimens obtained longitudinally from a patient treated with pazopanib showed no enrichment for ALDHbright cells (P > 0.05).ConclusionsAnti-proliferative TKIs appear to enrich for sarcoma CSCs while anti-angiogenic TKIs do not. The rational selection of targeted therapies for sarcoma patients may benefit from an awareness of the differential impact of TKIs on CSC populations.

Published
2014

4. Regulatory T Cells and Myeloid-Derived Suppressor Cells in the Tumor Microenvironment Undergo Fas-Dependent Cell Death during IL-2/αCD40 Therapy

Author

Weiss, Jonathan M, Subleski, Jeff J, Back, Tim, Chen, Xin, Watkins, Stephanie K, Yagita, Hideo, Sayers, Thomas J, Murphy, William J, and Wiltrout, Robert H

Subjects
Vaccine Related, Cancer, Clinical Research, Immunization, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Animals, Antineoplastic Agents, CD40 Antigens, CD8-Positive T-Lymphocytes, Cell Death, Cell Line, Tumor, Interleukin-2, Mice, Mice, Inbred BALB C, Mice, Knockout, Myeloid Cells, Neoplasms, Experimental, Proto-Oncogene Proteins c-bcl-2, T-Lymphocytes, Regulatory, Tumor Microenvironment, fas Receptor, Immunology
Abstract

Fas ligand expression in certain tumors has been proposed to contribute to immunosuppression and poor prognosis. However, immunotherapeutic approaches may elicit the Fas-mediated elimination of immunosuppressive regulatory T cells (Tregs) and myeloid-derived suppressor cells (MDSCs) within tumors that represent major obstacles for cancer immunotherapy. Previously, we showed that IL-2 and agonistic CD40 Ab (αCD40) elicited synergistic antitumor responses coincident with the efficient removal of Tregs and MDSCs. We demonstrate in this study in two murine tumor models that Treg and MDSC loss within the tumor microenvironment after IL-2/αCD40 occurs through a Fas-dependent cell death pathway. Among tumor-infiltrating leukocytes, CD8(+) T cells, neutrophils, and immature myeloid cells expressed Fas ligand after treatment. Fas was expressed by tumor-associated Tregs and immature myeloid cells, including MDSCs. Tregs and MDSCs in the tumor microenvironment expressed active caspases after IL-2/αCD40 therapy and, in contrast with effector T cells, Tregs significantly downregulated Bcl-2 expression. In contrast, Tregs and MDSCs proliferated and expanded in the spleen after treatment. Adoptive transfer of Fas-deficient Tregs or MDSCs into wild-type, Treg-, or MDSC-depleted hosts resulted in the persistence of Tregs or MDSCs and the loss of antitumor efficacy in response to IL-2/αCD40. These results demonstrate the importance of Fas-mediated Treg/MDSC removal for successful antitumor immunotherapy. Our results suggest that immunotherapeutic strategies that include exploiting Treg and MDSC susceptibility to Fas-mediated apoptosis hold promise for treatment of cancer.

Published
2014

8. Data from Small-Molecule Natural Product Physachenolide C Potentiates Immunotherapy Efficacy by Targeting BET Proteins

Author

Tewary, Poonam, primary, Brooks, Alan D., primary, Xu, Ya-Ming, primary, Wijeratne, E.M. Kithsiri, primary, Babyak, Ashley L., primary, Back, Timothy C., primary, Chari, Raj, primary, Evans, Christine N., primary, Henrich, Curtis J., primary, Meyer, Thomas J., primary, Edmondson, Elijah F., primary, de Aquino, Maria T. Prudente, primary, Kanagasabai, Thanigaivelan, primary, Shanker, Anil, primary, Gunatilaka, A.A. Leslie, primary, and Sayers, Thomas J., primary

Published
2023
Full Text
View/download PDF

9. Supplementary Data from Small-Molecule Natural Product Physachenolide C Potentiates Immunotherapy Efficacy by Targeting BET Proteins

Author

Tewary, Poonam, primary, Brooks, Alan D., primary, Xu, Ya-Ming, primary, Wijeratne, E.M. Kithsiri, primary, Babyak, Ashley L., primary, Back, Timothy C., primary, Chari, Raj, primary, Evans, Christine N., primary, Henrich, Curtis J., primary, Meyer, Thomas J., primary, Edmondson, Elijah F., primary, de Aquino, Maria T. Prudente, primary, Kanagasabai, Thanigaivelan, primary, Shanker, Anil, primary, Gunatilaka, A.A. Leslie, primary, and Sayers, Thomas J., primary

Published
2023
Full Text
View/download PDF

35. Small-Molecule Natural Product Physachenolide C Potentiates Immunotherapy Efficacy by Targeting BET Proteins

Author

Tewary, Poonam, primary, Brooks, Alan D., additional, Xu, Ya-Ming, additional, Wijeratne, E.M. Kithsiri, additional, Babyak, Ashley L., additional, Back, Timothy C., additional, Chari, Raj, additional, Evans, Christine N., additional, Henrich, Curtis J., additional, Meyer, Thomas J., additional, Edmondson, Elijah F., additional, de Aquino, Maria T. Prudente, additional, Kanagasabai, Thanigaivelan, additional, Shanker, Anil, additional, Gunatilaka, A.A. Leslie, additional, and Sayers, Thomas J., additional

Published
2021
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results