Your search keyword '"David H Munn"' showing total 283 results

1. Indomethacin-induced oxidative stress enhances death receptor 5 signaling and sensitizes tumor cells to adoptive T-cell therapy

Author

Gang Zhou, David H Munn, Zhi-Chun Ding, Marco L Davila, Hongyan Xu, Nada S Aboelella, Caitlin Brandle, Ogacheko Okoko, Md Yeashin Gazi, Gregory Gorman, Roni Bollag, Locke J Bryan, and Gary A Piazza

Subjects

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

Abstract

Background Adoptive cell therapy (ACT) using genetically modified T cells has evolved into a promising treatment option for patients with cancer. However, even for the best-studied and clinically validated CD19-targeted chimeric antigen receptor (CAR) T-cell therapy, many patients face the challenge of lack of response or occurrence of relapse. There is increasing need to improve the efficacy of ACT so that durable, curative outcomes can be achieved in a broad patient population.Methods Here, we investigated the impact of indomethacin (indo), a non-steroidal anti-inflammatory drug (NSAID), on the efficacy of ACT in multiple preclinical models. Mice with established B-cell lymphoma received various combinations of preconditioning chemotherapy, infusion of suboptimal dose of tumor-reactive T cells, and indo administration. Donor T cells used in the ACT models included CD4+ T cells expressing a tumor-specific T cell receptor (TCR) and T cells engineered to express CD19CAR. Mice were monitored for tumor growth and survival. The effects of indo on donor T cell phenotype and function were evaluated. The molecular mechanisms by which indo may influence the outcome of ACT were investigated.Results ACT coupled with indo administration led to improved tumor growth control and prolonged mouse survival. Indo did not affect the activation status and tumor infiltration of the donor T cells. Moreover, the beneficial effect of indo in ACT did not rely on its inhibitory effect on the immunosuppressive cyclooxygenase 2 (COX2)/prostaglandin E2 (PGE2) axis. Instead, indo-induced oxidative stress boosted the expression of death receptor 5 (DR5) in tumor cells, rendering them susceptible to donor T cells expressing TNF-related apoptosis-inducing ligand (TRAIL). Furthermore, the ACT-potentiating effect of indo was diminished against DR5-deficient tumors, but was amplified by donor T cells engineered to overexpress TRAIL.Conclusion Our results demonstrate that the pro-oxidative property of indo can be exploited to enhance death receptor signaling in cancer cells, providing rationale for combining indo with genetically modified T cells to intensify tumor cell killing through the TRAIL-DR5 axis. These findings implicate indo administration, and potentially similar use of other NSAIDs, as a readily applicable and cost-effective approach to augment the efficacy of ACT.

Published

2022

2. p50 suppresses cytotoxic T lymphocyte effector function to regulate tumor immune escape and response to immunotherapy

Author

Jennifer L Waller, David H Munn, Chunwan Lu, Kebin Liu, John D Klement, Alyssa D Smith, Dafeng Yang, and Darren D Browning

Subjects

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

Abstract

Background NF-κB is a key link between inflammation and cancer. Previous studies of NF-κB have largely focused on tumor cells, and the intrinsic function of NF-κB in T cells in tumor development and response to immunotherapy is largely unknown. We aimed at testing the hypothesis that NF-κB1 (p50) activation in T cells underlies human colon cancer immune escape and human cancer non-response to anti-PD-1 immunotherapy.Methods We screened NF-κB activation in human colon carcinoma and used mouse models to determine p50 function in tumor cells and immune cells. RNA-Seq was used to identify p50 target genes. p50 binding to target gene promoters were determined by electrophoresis mobility shift assay and chromatin immunoprecipitation. A p50 activation score was generated from gene expression profiling and used to link p50 activation to T-cell activation and function pre-nivolumab and post-nivolumab immunotherapy in human patients with cancer.Results p50 is the dominant form of NF-κB that is highly activated in immune cells in the human colorectal carcinoma microenvironment and neighboring non-neoplastic colon epithelial cells. Tumor cell intrinsic p50 signaling and T-cell intrinsic p50 signaling exert opposing functions in tumor growth control in vivo. Deleting Nfkb1 in tumor cells increased whereas in T cells decreased tumor growth in preclinical mouse models. Gene expression profiling identified Gzmb as a p50 target in T cells. p50 binds directly to a previously uncharacterized κB sequence at the Gzmb promoter in T cells, resulting in repression of Gzmb expression in tumor-infiltrating cytotoxic T lymphocytes (CTLs) to induce a dysfunctional CTL phenotype to promote tumor immune escape. p50 activation is inversely correlated with both GZMB expression and T-cell tumor infiltration in human colorectal carcinoma. Furthermore, nivolumab immunotherapy decreased p50 activation and increased GZMB expression in human patients with melanoma.Conclusions Inflammation activates p50 that binds to the Gzmb promoter to repress granzyme B expression in T cells, resulting in CTL dysfunction to confer tumor immune escape and decreased response to anti-PD-1 immunotherapy.

Published

2020

3. Virus Infections Incite Pain Hypersensitivity by Inducing Indoleamine 2,3 Dioxygenase.

Author

Lei Huang, Rong Ou, Guilherme Rabelo de Souza, Thiago M Cunha, Henrique Lemos, Eslam Mohamed, Lingqian Li, Gabriela Pacholczyk, Janice Randall, David H Munn, and Andrew L Mellor

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Increased pain sensitivity is a comorbidity associated with many clinical diseases, though the underlying causes are poorly understood. Recently, chronic pain hypersensitivity in rodents treated to induce chronic inflammation in peripheral tissues was linked to enhanced tryptophan catabolism in brain mediated by indoleamine 2,3 dioxygenase (IDO). Here we show that acute influenza A virus (IAV) and chronic murine leukemia retrovirus (MuLV) infections, which stimulate robust IDO expression in lungs and lymphoid tissues, induced acute or chronic pain hypersensitivity, respectively. In contrast, virus-induced pain hypersensitivity did not manifest in mice lacking intact IDO1 genes. Spleen IDO activity increased markedly as MuLV infections progressed, while IDO1 expression was not elevated significantly in brain or spinal cord (CNS) tissues. Moreover, kynurenine (Kyn), a tryptophan catabolite made by cells expressing IDO, incited pain hypersensitivity in uninfected IDO1-deficient mice and Kyn potentiated pain hypersensitivity due to MuLV infection. MuLV infection stimulated selective IDO expression by a discreet population of spleen cells expressing both B cell (CD19) and dendritic cell (CD11c) markers (CD19+ DCs). CD19+ DCs were more susceptible to MuLV infection than B cells or conventional (CD19neg) DCs, proliferated faster than B cells from early stages of MuLV infection and exhibited mature antigen presenting cell (APC) phenotypes, unlike conventional (CD19neg) DCs. Moreover, interactions with CD4 T cells were necessary to sustain functional IDO expression by CD19+ DCs in vitro and in vivo. Splenocytes from MuLV-infected IDO1-sufficient mice induced pain hypersensitivity in uninfected IDO1-deficient recipient mice, while selective in vivo depletion of DCs alleviated pain hypersensitivity in MuLV-infected IDO1-sufficient mice and led to rapid reduction in splenomegaly, a hallmark of MuLV immune pathogenesis. These findings reveal critical roles for CD19+ DCs expressing IDO in host responses to MuLV infection that enhance pain hypersensitivity and cause immune pathology. Collectively, our findings support the hypothesis elevated IDO activity in non-CNS due to virus infections causes pain hypersensitivity mediated by Kyn. Previously unappreciated links between host immune responses to virus infections and pain sensitivity suggest that IDO inhibitors may alleviate heightened pain sensitivity during infections.

Published

2016

4. Indoleamine 2,3-dioxygenase 1 (ido1) is involved in the control of mouse caput epididymis immune environment.

Author

Aicha Jrad-Lamine, Joelle Henry-Berger, Christelle Damon-Soubeyrand, Fabrice Saez, Ayhan Kocer, Laurent Janny, Hanae Pons-Rejraji, David H Munn, Andrew L Mellor, Najoua Gharbi, Rémi Cadet, Rachel Guiton, Robert J Aitken, and Joël R Drevet

Subjects

Medicine, Science

Abstract

The epididymis maintains a state of immune tolerance towards spermatozoa while also protecting them and itself against infection and acute inflammation. The immunosuppressive enzyme indoleamine 2,3-dioxygenase 1 (Ido1) participates in this delicate local equilibrium. Using the mouse Ido1(-/-) model, we show here that the absence of IDO1 expression leads in the epididymis but not in serum to (1) an increase in the inflammatory state as evidenced by changes in the content of cytokines and chemokines, (2) the engagement of a Th1-driven inflammatory response as evidenced by changes in the Th17/Treg as well as Th1/Th2 equilibria, as well as (3) differences in the content of lipid intermediates classically involved in inflammation. Despite this more pronounced inflammatory state, Ido1(-/-) animals succeed in preserving the local epididymal immune situation due to the activation of compensatory mechanisms that are discussed.

Published

2013

5. Retinoic acid signaling acts as a rheostat to balance Treg function

Author

Govindarajan Thangavelu, Gabriela Andrejeva, Sara Bolivar-Wagers, Sujeong Jin, Michael C. Zaiken, Michael Loschi, Ethan G. Aguilar, Scott N. Furlan, Chrysothemis C. Brown, Yu-Chi Lee, Cameron McDonald Hyman, Colby J. Feser, Angela Panoskaltsis-Mortari, Keli L. Hippen, Kelli P. MacDonald, William J. Murphy, Ivan Maillard, Geoffrey R. Hill, David H. Munn, Robert Zeiser, Leslie S. Kean, Jeffrey C. Rathmell, Hongbo Chi, Randolph J. Noelle, and Bruce R. Blazar

Subjects

Mice, Infectious Diseases, Immunology, Immune Tolerance, Animals, Immunology and Allergy, Autoimmunity, Tretinoin, T-Lymphocytes, Regulatory, Article, Signal Transduction

Abstract

Regulatory T cells (Tregs) promote immune homeostasis by maintaining self-tolerance and regulating inflammatory responses. Under certain inflammatory conditions, Tregs can lose their lineage stability and function. Previous studies have reported that ex vivo exposure to retinoic acid (RA) enhances Treg function and stability. However, it is unknown how RA receptor signaling in Tregs influences these processes in vivo. Herein, we employed mouse models in which RA signaling is silenced by the expression of the dominant negative receptor (DN) RARα in all T cells. Despite the fact that DNRARα conventional T cells are hypofunctional, Tregs had increased CD25 expression, STAT5 pathway activation, mTORC1 signaling and supersuppressor function. Furthermore, DNRARα Tregs had increased inhibitory molecule expression, amino acid transporter expression, and metabolic fitness and decreased antiapoptotic proteins. Supersuppressor function was observed when wild-type mice were treated with a pharmacologic pan-RAR antagonist. Unexpectedly, Treg-specific expression of DNRARα resulted in distinct phenotypes, such that a single allele of DNRARα in Tregs heightened their suppressive function, and biallelic expression led to loss of suppression and autoimmunity. The loss of Treg function was not cell intrinsic, as Tregs that developed in a noninflammatory milieu in chimeric mice reconstituted with DNRARα and wild-type bone marrow maintained the enhanced suppressive capacity. Fate mapping suggested that maintaining Treg stability in an inflammatory milieu requires RA signaling. Our findings indicate that RA signaling acts as a rheostat to balance Treg function in inflammatory and noninflammatory conditions in a dose-dependent manner.

Published

2022

6. Supplementary Tables 1 through 5 from Promoter Methylation Modulates Indoleamine 2,3-Dioxygenase 1 Induction by Activated T Cells in Human Breast Cancers

Author

Huidong Shi, David H. Munn, Shou-Ching Tang, Stefan Ambs, Arun Sreekumar, Muthusamy Thangaraju, Shuang Huang, Hong-Bo Xin, Libin Deng, Hasan Korkaya, Tim H.M. Huang, Katie Chiou, Jiseok Choi, Fang Shi, Ravindra Kolhe, Pei-Yin Hsu, Lirong Pei, Austin Y. Shull, Maria Ouzounova, Jaejik Kim, Qimei Han, Jeong-Hyeon Choi, Eun-Joon Lee, Franklin Gu, and Satish K. Noonepalle

Abstract

Supplementary Table 1: List of primers used for quantitative real time PCR. Supplementary Table. 2: List of primers used for construction of pGL2 and pMIR reporter plasmids. Supplementary Table. 3: List of primers used to generate PCR amplicons for pyrosequencing analysis. Supplementary Table. 4: Sequencing primers used for pyrosequencing. Supplementary Table. 5: Primers used for qPCR analysis in ChIP assay.

Published

2023

7. Data from Antigen-Specific Bacterial Vaccine Combined with Anti-PD-L1 Rescues Dysfunctional Endogenous T Cells to Reject Long-Established Cancer

Author

Hans Schreiber, Donald A. Rowley, David H. Munn, Robert M. Hoffman, Ming Zhao, Christian Idel, Byron Burnette, Theodore Karrison, Yang-Xin Fu, James M. Slauch, Ping Yu, Ainhoa Arina, Boris Engels, and David C. Binder

Abstract

Immunogenic tumors grow progressively even when heavily infiltrated by CD8+ T cells. We investigated how to rescue CD8+ T-cell function in long-established immunogenic melanomas that contained a high percentage of endogenous PD-1+ tumor-specific CD8+ T cells that were dysfunctional. Treatment with αPD-L1– and αCTLA-4–blocking antibodies did not prevent tumors from progressing rapidly. We then tested exogenous tumor-specific antigen delivery into tumors using Salmonella Typhimurium A1-R (A1-R) to increase antigen levels and generate a proinflammatory tumor microenvironment. Antigen-producing A1-R rescued the endogenous tumor-specific CD8+ T-cell response: Proliferation was induced in the lymphoid organs and effector function was recovered in the tumor. Treatment with antigen-producing A1-R led to improved mouse survival and resulted in 32% rejection of long-established immunogenic melanomas. Following treatment with antigen-producing A1-R, the majority of tumor-specific CD8+ T cells still expressed a high level of PD-1 in the tumor. Combining antigen-producing A1-R with αPD-L1-blocking antibody enhanced the expansion of tumor-specific CD8+ T cells and resulted in 80% tumor rejection. Collectively, these data show a powerful new therapeutic approach to rescue dysfunctional endogenous tumor-specific CD8+ T cells and eradicate advanced immunogenic tumors. Cancer Immunol Res; 1(2); 123–33. ©2013 AACR.

Published

2023

8. Supplementary Figure S2 from Promoter Methylation Modulates Indoleamine 2,3-Dioxygenase 1 Induction by Activated T Cells in Human Breast Cancers

Author

Huidong Shi, David H. Munn, Shou-Ching Tang, Stefan Ambs, Arun Sreekumar, Muthusamy Thangaraju, Shuang Huang, Hong-Bo Xin, Libin Deng, Hasan Korkaya, Tim H.M. Huang, Katie Chiou, Jiseok Choi, Fang Shi, Ravindra Kolhe, Pei-Yin Hsu, Lirong Pei, Austin Y. Shull, Maria Ouzounova, Jaejik Kim, Qimei Han, Jeong-Hyeon Choi, Eun-Joon Lee, Franklin Gu, and Satish K. Noonepalle

Abstract

A subset of primary breast tumors expresses a 308-gene signature that correlated with gene signatures specifically expressed in immune cells.

Published

2023

9. Supplementary Figures 1 - 3 from Antigen-Specific Bacterial Vaccine Combined with Anti-PD-L1 Rescues Dysfunctional Endogenous T Cells to Reject Long-Established Cancer

Author

Hans Schreiber, Donald A. Rowley, David H. Munn, Robert M. Hoffman, Ming Zhao, Christian Idel, Byron Burnette, Theodore Karrison, Yang-Xin Fu, James M. Slauch, Ping Yu, Ainhoa Arina, Boris Engels, and David C. Binder

Abstract

PDF file - 291K, Figure S1. A1-R SIINF preferentially accumulates in established B16-OVA tumors. Figure S2. A1-R SIINF induces systemic SIINF-specific CD8+ T cell proliferation. Figure S3. Weekly A1-R SIINF treatment leads to rejection of established B16-OVA tumors. Figure S4. The majority of intratumoral SIINF-specific CD8+ T cells still express a high level of PD-1 following A1-R OVA treatment.

Published

2023

10. Supplementary Methods, Figure Legend from Antigen-Specific Bacterial Vaccine Combined with Anti-PD-L1 Rescues Dysfunctional Endogenous T Cells to Reject Long-Established Cancer

Author

Hans Schreiber, Donald A. Rowley, David H. Munn, Robert M. Hoffman, Ming Zhao, Christian Idel, Byron Burnette, Theodore Karrison, Yang-Xin Fu, James M. Slauch, Ping Yu, Ainhoa Arina, Boris Engels, and David C. Binder

Abstract

PDF file - 122K

Published

2023

11. Data from Promoter Methylation Modulates Indoleamine 2,3-Dioxygenase 1 Induction by Activated T Cells in Human Breast Cancers

Author

Huidong Shi, David H. Munn, Shou-Ching Tang, Stefan Ambs, Arun Sreekumar, Muthusamy Thangaraju, Shuang Huang, Hong-Bo Xin, Libin Deng, Hasan Korkaya, Tim H.M. Huang, Katie Chiou, Jiseok Choi, Fang Shi, Ravindra Kolhe, Pei-Yin Hsu, Lirong Pei, Austin Y. Shull, Maria Ouzounova, Jaejik Kim, Qimei Han, Jeong-Hyeon Choi, Eun-Joon Lee, Franklin Gu, and Satish K. Noonepalle

Abstract

Triple-negative breast cancer (TNBC) cells are modulated in reaction to tumor-infiltrating lymphocytes. However, their specific responses to this immune pressure are unknown. In order to address this question, we first used mRNA sequencing to compare the immunophenotype of the TNBC cell line MDA-MB-231 and the luminal breast cancer cell line MCF7 after both were cocultured with activated human T cells. Despite similarities in the cytokine-induced immune signatures of the two cell lines, MDA-MD-231 cells were able to transcribe more IDO1 than MCF7 cells. The two cell lines had similar upstream JAK/STAT1 signaling and IDO1 mRNA stability. However, using a series of breast cancer cell lines, IFNγ stimulated IDO1 protein expression and enzymatic activity only in ER−, not ER+, cell lines. Treatment with 5-aza-deoxycytidine reversed the suppression of IDO1 expression in MCF7 cells, suggesting that DNA methylation was potentially involved in IDO1 induction. By analyzing several breast cancer datasets, we discovered subtype-specific mRNA and promoter methylation differences in IDO1, with TNBC/basal subtypes exhibiting lower methylation/higher expression and ER+/luminal subtypes exhibiting higher methylation/lower expression. We confirmed this trend of IDO1 methylation by bisulfite pyrosequencing breast cancer cell lines and an independent cohort of primary breast tumors. Taken together, these findings suggest that IDO1 promoter methylation regulates anti-immune responses in breast cancer subtypes and could be used as a predictive biomarker for IDO1 inhibitor–based immunotherapy. Cancer Immunol Res; 5(4); 330–44. ©2017 AACR.

Published

2023

12. Supplementary Figure Legends from Promoter Methylation Modulates Indoleamine 2,3-Dioxygenase 1 Induction by Activated T Cells in Human Breast Cancers

Author

Huidong Shi, David H. Munn, Shou-Ching Tang, Stefan Ambs, Arun Sreekumar, Muthusamy Thangaraju, Shuang Huang, Hong-Bo Xin, Libin Deng, Hasan Korkaya, Tim H.M. Huang, Katie Chiou, Jiseok Choi, Fang Shi, Ravindra Kolhe, Pei-Yin Hsu, Lirong Pei, Austin Y. Shull, Maria Ouzounova, Jaejik Kim, Qimei Han, Jeong-Hyeon Choi, Eun-Joon Lee, Franklin Gu, and Satish K. Noonepalle

Abstract

Figure Legends for Supplementary Figures 1-6

Published

2023

13. Supplementary Figure 2 from Advanced Age Increases Immunosuppression in the Brain and Decreases Immunotherapeutic Efficacy in Subjects with Glioblastoma

Author

Derek A. Wainwright, David H. Munn, George C. Prendergast, Ursula Grohmann, Judith Campisi, Graham Pawelec, Changyou Zhou, Min Wei, Craig Horbinski, Rimas V. Lukas, Karan Dixit, Jeffrey J. Raizer, Priya Kumthekar, Robert M. Prins, Aaron Y. Mochizuki, Leonidas C. Platanias, Joseph R. Podojil, Jennifer D. Wu, Bin Zhang, Masha Kocherginsky, Jiahui Xu, April Bell, Kristen L. Lauing, Lijie Zhai, and Erik Ladomersky

Abstract

Supplemental Figure 2. Glioblastoma patient overall survival.

Published

2023

14. Supplementary Figure 5 from Advanced Age Increases Immunosuppression in the Brain and Decreases Immunotherapeutic Efficacy in Subjects with Glioblastoma

Author

Derek A. Wainwright, David H. Munn, George C. Prendergast, Ursula Grohmann, Judith Campisi, Graham Pawelec, Changyou Zhou, Min Wei, Craig Horbinski, Rimas V. Lukas, Karan Dixit, Jeffrey J. Raizer, Priya Kumthekar, Robert M. Prins, Aaron Y. Mochizuki, Leonidas C. Platanias, Joseph R. Podojil, Jennifer D. Wu, Bin Zhang, Masha Kocherginsky, Jiahui Xu, April Bell, Kristen L. Lauing, Lijie Zhai, and Erik Ladomersky

Abstract

Supplemental Figure 5. Confirmation of gut microbiota depletion.

Published

2023

15. Data from Zinc Protoporphyrin IX Stimulates Tumor Immunity by Disrupting the Immunosuppressive Enzyme Indoleamine 2,3-Dioxygenase

Author

George C. Prendergast, Mario Mautino, Alexander J. Muller, David H. Munn, Sonja Rust, James B. DuHadaway, and Richard Metz

Abstract

The tryptophan catabolic enzyme indoleamine 2,3-dioxygenase (IDO) has emerged as an important driver of immune escape in a growing number of cancers and cancer-associated chronic infections. In this study, we define novel immunotherapeutic applications for the heme precursor compound zinc protoporphyrin IX (ZnPP) based on our discovery that it is a potent small-molecule inhibitor of IDO. Inhibitory activity was determined using in vitro and in-cell enzyme assays as well as a novel in vivo pharmacodynamic system. An irreversible mechanism of inhibition was documented, consistent with competition for heme binding in newly synthesized cellular protein. siRNA methodology and an IDO-deficient mouse strain were used to verify the specificity of ZnPP as an IDO inhibitor. In a preclinical model of melanoma, ZnPP displayed antitumor properties that relied on T-cell function and IDO integrity. ZnPP also phenocopied the known antitumor properties of IDO inhibitors in preclinical models of skin and breast carcinoma. Our results suggest clinical evaluation of ZnPP as an adjuvant immunochemotherapy in chronic infections and cancers in which there is emerging recognition of a pathophysiologic role for IDO dysregulation. Mol Cancer Ther; 9(6); 1864–71. ©2010 AACR.

Published

2023

16. Supplementary Data from Advanced Age Increases Immunosuppression in the Brain and Decreases Immunotherapeutic Efficacy in Subjects with Glioblastoma

Author

Derek A. Wainwright, David H. Munn, George C. Prendergast, Ursula Grohmann, Judith Campisi, Graham Pawelec, Changyou Zhou, Min Wei, Craig Horbinski, Rimas V. Lukas, Karan Dixit, Jeffrey J. Raizer, Priya Kumthekar, Robert M. Prins, Aaron Y. Mochizuki, Leonidas C. Platanias, Joseph R. Podojil, Jennifer D. Wu, Bin Zhang, Masha Kocherginsky, Jiahui Xu, April Bell, Kristen L. Lauing, Lijie Zhai, and Erik Ladomersky

Abstract

Supplementary Materials and Methods

Published

2023

17. Supplementary Figure 6 from Advanced Age Increases Immunosuppression in the Brain and Decreases Immunotherapeutic Efficacy in Subjects with Glioblastoma

Author

Derek A. Wainwright, David H. Munn, George C. Prendergast, Ursula Grohmann, Judith Campisi, Graham Pawelec, Changyou Zhou, Min Wei, Craig Horbinski, Rimas V. Lukas, Karan Dixit, Jeffrey J. Raizer, Priya Kumthekar, Robert M. Prins, Aaron Y. Mochizuki, Leonidas C. Platanias, Joseph R. Podojil, Jennifer D. Wu, Bin Zhang, Masha Kocherginsky, Jiahui Xu, April Bell, Kristen L. Lauing, Lijie Zhai, and Erik Ladomersky

Abstract

Supplemental Figure 6. Characterization of the potent clinical-grade IDO enzyme inhibitor, BGB-7204.

Published

2023

18. Supplementary Figure 1 from Advanced Age Increases Immunosuppression in the Brain and Decreases Immunotherapeutic Efficacy in Subjects with Glioblastoma

Author

Derek A. Wainwright, David H. Munn, George C. Prendergast, Ursula Grohmann, Judith Campisi, Graham Pawelec, Changyou Zhou, Min Wei, Craig Horbinski, Rimas V. Lukas, Karan Dixit, Jeffrey J. Raizer, Priya Kumthekar, Robert M. Prins, Aaron Y. Mochizuki, Leonidas C. Platanias, Joseph R. Podojil, Jennifer D. Wu, Bin Zhang, Masha Kocherginsky, Jiahui Xu, April Bell, Kristen L. Lauing, Lijie Zhai, and Erik Ladomersky

Abstract

Supplemental Figure 1. Inclusion and exclusion criteria for the analysis of human subjects diagnosed with glioblastoma (GBM).

Published

2023

19. Supplementary Figure 7 from Advanced Age Increases Immunosuppression in the Brain and Decreases Immunotherapeutic Efficacy in Subjects with Glioblastoma

Author

Derek A. Wainwright, David H. Munn, George C. Prendergast, Ursula Grohmann, Judith Campisi, Graham Pawelec, Changyou Zhou, Min Wei, Craig Horbinski, Rimas V. Lukas, Karan Dixit, Jeffrey J. Raizer, Priya Kumthekar, Robert M. Prins, Aaron Y. Mochizuki, Leonidas C. Platanias, Joseph R. Podojil, Jennifer D. Wu, Bin Zhang, Masha Kocherginsky, Jiahui Xu, April Bell, Kristen L. Lauing, Lijie Zhai, and Erik Ladomersky

Abstract

Supplemental Figure 7. Bioluminescent imaging.

Published

2023

20. Supplementary Data from Zinc Protoporphyrin IX Stimulates Tumor Immunity by Disrupting the Immunosuppressive Enzyme Indoleamine 2,3-Dioxygenase

Author

George C. Prendergast, Mario Mautino, Alexander J. Muller, David H. Munn, Sonja Rust, James B. DuHadaway, and Richard Metz

Abstract

Supplementary Data from Zinc Protoporphyrin IX Stimulates Tumor Immunity by Disrupting the Immunosuppressive Enzyme Indoleamine 2,3-Dioxygenase

Published

2023

21. Data from Advanced Age Increases Immunosuppression in the Brain and Decreases Immunotherapeutic Efficacy in Subjects with Glioblastoma

Author

Derek A. Wainwright, David H. Munn, George C. Prendergast, Ursula Grohmann, Judith Campisi, Graham Pawelec, Changyou Zhou, Min Wei, Craig Horbinski, Rimas V. Lukas, Karan Dixit, Jeffrey J. Raizer, Priya Kumthekar, Robert M. Prins, Aaron Y. Mochizuki, Leonidas C. Platanias, Joseph R. Podojil, Jennifer D. Wu, Bin Zhang, Masha Kocherginsky, Jiahui Xu, April Bell, Kristen L. Lauing, Lijie Zhai, and Erik Ladomersky

Abstract

Purpose:Wild-type isocitrate dehydrogenase–expressing glioblastoma (GBM) is the most common and aggressive primary brain tumor with a median age at diagnosis of ≥65 years. It accounts for approximately 90% of all GBMs and has a median overall survival (OS) of Experimental Design:(i) Clinical data: GBM patient datasets from The Cancer Genome Atlas, Northwestern Medicine Enterprise Data Warehouse, and clinical studies evaluating ICB were stratified by age and compared for OS. (ii) Animal models: young, middle-aged, and older adult wild-type and indoleamine 2,3 dioxygenase (IDO)-knockout syngeneic mice were intracranially engrafted with CT-2A or GL261 glioma cell lines and treated with or without CTLA-4/PD-L1 mAbs, or radiation, anti–PD-1 mAb, and/or a pharmacologic IDO enzyme inhibitor.Results:Advanced age was associated with decreased GBM patient survival regardless of treatment with ICB. The advanced age–associated increase of brain IDO expression was linked to the suppression of immunotherapeutic efficacy and was not reversed by IDO enzyme inhibitor treatment.Conclusions:Immunosuppression increases in the brain during advanced age and inhibits antiglioma immunity in older adults. Going forward, it will be important to fully understand the factors and mechanisms in the elderly brain that contribute to the decreased survival of older patients with GBM during treatment with ICB.

Published

2023

22. Supplementary Figure 4 from Advanced Age Increases Immunosuppression in the Brain and Decreases Immunotherapeutic Efficacy in Subjects with Glioblastoma

Author

Derek A. Wainwright, David H. Munn, George C. Prendergast, Ursula Grohmann, Judith Campisi, Graham Pawelec, Changyou Zhou, Min Wei, Craig Horbinski, Rimas V. Lukas, Karan Dixit, Jeffrey J. Raizer, Priya Kumthekar, Robert M. Prins, Aaron Y. Mochizuki, Leonidas C. Platanias, Joseph R. Podojil, Jennifer D. Wu, Bin Zhang, Masha Kocherginsky, Jiahui Xu, April Bell, Kristen L. Lauing, Lijie Zhai, and Erik Ladomersky

Abstract

Supplemental Figure 4. Confirmatory analysis of T cell depletion method.

Published

2023

23. Supplementary Figure Legends from Immunosuppressive Myeloid Cells Induced by Chemotherapy Attenuate Antitumor CD4+ T-Cell Responses through the PD-1–PD-L1 Axis

Author

Gang Zhou, David H. Munn, Andrew L. Mellor, Bruce R. Blazar, Matthias Mack, Antoni Krasinski, Matthew Walters, Kebin Liu, Phillip Chandler, Lei Huang, Henrique Lemos, Miao Yu, Xiaoyun Lu, and Zhi-Chun Ding

Abstract

PDF file - 30KB

Published

2023

24. Supplementary Figure S5 from β-Catenin Promotes Regulatory T-cell Responses in Tumors by Inducing Vitamin A Metabolism in Dendritic Cells

Author

Santhakumar Manicassamy, David H. Munn, Andrew L. Mellor, Balaji Manicassamy, Pandelakis A. Koni, Melinda L. Angus-Hill, Tanmay Majumdar, Amol Suryawanshi, Indumathi Manoharan, and Yuan Hong

Abstract

Supplementary Figure S5. Therapeutic effect of blocking the β-catenin pathway against established tumors.

Published

2023

25. Supplementary Figures 1 - 8 from Immunosuppressive Myeloid Cells Induced by Chemotherapy Attenuate Antitumor CD4+ T-Cell Responses through the PD-1–PD-L1 Axis

Author

Gang Zhou, David H. Munn, Andrew L. Mellor, Bruce R. Blazar, Matthias Mack, Antoni Krasinski, Matthew Walters, Kebin Liu, Phillip Chandler, Lei Huang, Henrique Lemos, Miao Yu, Xiaoyun Lu, and Zhi-Chun Ding

Abstract

PDF file - 133KB, Immunofluorescence staining (IF) of CD11b+ myeloid cells on spleen and tumor samples (S1). CTX+CD4 AT therapy induces an inflammatory immune milieu (S2). Chemoimmunotherapy leads to myeloid cell expansion in mice with lung metastasis of CT26HA colon cancer (S3). Therapy-induced monocytes can suppress CD4+ T cell activation in response to either antigen-specific or nonspecific stimulation (S4). Dose effect of CTX on myeloid cell induction (S5). Monocytic myeloid suppressor cells can be induced by doxorubicin and melphalan (S6). Low dose gemcitabine following CTX+CD4 AT therapy confers long-term survival benefit to mice with lung metastasis of CT26HA colon cancer (S7). Low dose 5-fluorouracil (5-FU) reduces therapy-induced monocytes (S8).

Published

2023

26. Supplementary Figure Legend from β-Catenin Promotes Regulatory T-cell Responses in Tumors by Inducing Vitamin A Metabolism in Dendritic Cells

Author

Santhakumar Manicassamy, David H. Munn, Andrew L. Mellor, Balaji Manicassamy, Pandelakis A. Koni, Melinda L. Angus-Hill, Tanmay Majumdar, Amol Suryawanshi, Indumathi Manoharan, and Yuan Hong

Abstract

Supplementary Figure Legend. Legend for Supplementary Figures S1-S5.

Published

2023

27. Supplementary Materials from Immunosuppressive Myeloid Cells Induced by Chemotherapy Attenuate Antitumor CD4+ T-Cell Responses through the PD-1–PD-L1 Axis

Author

Gang Zhou, David H. Munn, Andrew L. Mellor, Bruce R. Blazar, Matthias Mack, Antoni Krasinski, Matthew Walters, Kebin Liu, Phillip Chandler, Lei Huang, Henrique Lemos, Miao Yu, Xiaoyun Lu, and Zhi-Chun Ding

Abstract

PDF file - 27KB

Published

2023

28. Data from Inhibition of Indoleamine 2,3-Dioxygenase in Dendritic Cells by Stereoisomers of 1-Methyl-Tryptophan Correlates with Antitumor Responses

Author

David H. Munn, George C. Prendergast, Andrew L. Mellor, Maribeth Johnson, Tinku Banerjee, James DuHadaway, Madhav D. Sharma, Alexander J. Muller, and De-Yan Hou

Abstract

Indoleamine 2,3-dioxygenase (IDO) is an immunosuppressive enzyme that contributes to tolerance in a number of biological settings. In cancer, IDO activity may help promote acquired tolerance to tumor antigens. The IDO inhibitor 1-methyl-tryptophan is being developed for clinical trials. However, 1-methyl-tryptophan exists in two stereoisomers with potentially different biological properties, and it has been unclear which isomer might be preferable for initial development. In this study, we provide evidence that the d and l stereoisomers exhibit important cell type–specific variations in activity. The l isomer was the more potent inhibitor of IDO activity using the purified enzyme and in HeLa cell–based assays. However, the d isomer was significantly more effective in reversing the suppression of T cells created by IDO-expressing dendritic cells, using both human monocyte–derived dendritic cells and murine dendritic cells isolated directly from tumor-draining lymph nodes. In vivo, the d isomer was more efficacious as an anticancer agent in chemo-immunotherapy regimens using cyclophosphamide, paclitaxel, or gemcitabine, when tested in mouse models of transplantable melanoma and transplantable and autochthonous breast cancer. The d isomer of 1-methyl-tryptophan specifically targeted the IDO gene because the antitumor effect of d-1-methyl-tryptophan was completely lost in mice with a disruption of the IDO gene (IDO-knockout mice). Taken together, our findings support the suitability of d-1-methyl-tryptophan for human trials aiming to assess the utility of IDO inhibition to block host-mediated immunosuppression and enhance antitumor immunity in the setting of combined chemo-immunotherapy regimens. [Cancer Res 2007;67(2):792–801]

Published

2023

29. Repurposing a novel anti-cancer RXR agonist to attenuate murine acute GVHD and maintain graft-versus-leukemia responses

Author

Randolph J. Noelle, Roshantha A.S. Chandraratna, Amanda Janesick, Ethan G. Aguilar, Kelli P. A. MacDonald, Asim Saha, Bruce R. Blazar, Keli L. Hippen, Michael Loschi, Govindarajan Thangavelu, Kazutoshi Aoyama, Geoffrey R. Hill, Angela Panoskaltsis-Mortari, Vijay K. Kuchroo, Yosef Refaeli, Bruce Blumberg, Chrysothemis C. Brown, Scott N. Furlan, William J. Murphy, David H. Munn, Jonathan S. Serody, Cameron McDonald-Hyman, Chao Wang, Ivan Maillard, Leslie S. Kean, Robert Zeiser, and Mark J. Osborn

Subjects

Agonist, medicine.drug_class, Chemistry, Immunology, FOXP3, chemical and pharmacologic phenomena, Cell Biology, Hematology, Retinoid X receptor, medicine.disease, Mixed lymphocyte reaction, Biochemistry, Proinflammatory cytokine, Leukemia, Graft-versus-host disease, medicine, Cancer research, Receptor

Abstract

The nuclear receptor (NR) subclass, retinoid X receptors (RXRs), exert immunomodulatory functions that control inflammation and metabolism via homodimers and heterodimers, with several other NRs, including retinoic acid receptors. IRX4204 is a novel, highly specific RXR agonist in clinical trials that potently and selectively activates RXR homodimers, but not heterodimers. In this study, in vivo IRX4204 compared favorably with FK506 in abrogating acute graft-versus-host disease (GVHD), which was associated with inhibiting allogeneic donor T-cell proliferation, reducing T-helper 1 differentiation, and promoting regulatory T-cell (Treg) generation. Recipient IRX4204 treatment reduced intestinal injury and decreased IFN-γ and TNF-α serum levels. Transcriptional analysis of donor T cells isolated from intestines of GVHD mice treated with IRX4204 revealed significant decreases in transcripts regulating proinflammatory pathways. In vitro, inducible Treg differentiation from naive CD4 T cells was enhanced by IRX4204. In vivo, IRX4204 increased the conversion of donor Foxp3 T cells into peripheral Foxp3 Tregs in GVHD mice. Using Foxp3 lineage-tracer mice in which both the origin and current FoxP3 expression of Tregs can be tracked, we demonstrated that IRX4204 supports Treg stability. Despite favoring Tregs and reducing Th1 differentiation, IRX4204-treated recipients maintained graft-versus-leukemia responses against both leukemia and lymphoma cells. Notably, IRX4204 reduced in vitro human T-cell proliferation and enhanced Treg generation in mixed lymphocyte reaction cultures. Collectively, these beneficial effects indicate that targeting RXRs with IRX4204 could be a novel approach to preventing acute GVHD in the clinic. Key Points: • A novel RXR agonist attenuates acute GVHD, while retaining graft-versus-leukemia responses. • The RXR agonist enhances Treg generation and stabilizes Foxp3, even in a highly inflammatory environment.

Published

2021

30. Antigen-presenting dendritic cells as targets for cancer immunotherapy

Author

Rafal Pacholczyk, Madhav D. Sharma, and David H. Munn

Subjects

Antigen, Cancer immunotherapy, business.industry, medicine.medical_treatment, Cancer research, medicine, business

Published

2021

31. Delayed Akt suppression in the lipopolysaccharide-induced acute lung injury promotes resolution that is associated with enhanced effector regulatory T cells

Author

Sandeep Artham, Mir S Adil, Payaningal R. Somanath, David H. Munn, Abdulrahman Alwhaibi, Arti Verma, and Santhakumar Manicassamy

Subjects

Lipopolysaccharides, Male, 0301 basic medicine, Pulmonary and Respiratory Medicine, Lipopolysaccharide, Neutrophils, Physiology, Acute Lung Injury, Pulmonary Edema, chemical and pharmacologic phenomena, Inflammation, Lung injury, T-Lymphocytes, Regulatory, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Antigens, CD, Physiology (medical), Animals, Medicine, Lung, Protein kinase B, Mice, Knockout, business.industry, Effector, FOXP3, Forkhead Transcription Factors, hemic and immune systems, Cell Biology, Pulmonary edema, medicine.disease, Acquired immune system, Adoptive Transfer, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, CD4 Antigens, Cancer research, Female, medicine.symptom, business, Integrin alpha Chains, Proto-Oncogene Proteins c-akt, Spleen, Research Article

Abstract

The adaptive immune response could play a major role in the resolution of lung injury. Although regulatory T cells (Tregs) have been implicated in promoting the resolution of lung injury, therapeutic strategies to enhance Treg quantity and activity at the site of injury need further exploration. In the current study, Akt inhibition using triciribine (TCBN), given 48 h after lipopolysaccharide (LPS) administration, increased Tregs-promoted resolution of acute lung injury (ALI). TCBN treatment enhanced the resolution of LPS-induced ALI on day 7 by reducing pulmonary edema and neutrophil activity associated with an increased number of CD4+/FoxP3+/CD103+ and CTLA4+ effector Tregs, specifically in the injured lungs and not in the spleen. Treatment of EL-4 T-lymphocytes with two Akt inhibitors (TCBN and MK-2206) for 72 h resulted in increased FoxP3 expression in vitro. On the other end, Treg-specific PTEN knockout (PTENTreg KO) mice that have a higher Akt activity in its Tregs exhibited a significant impairment in ALI resolution, increased edema, and neutrophil activity associated with a reduced number of CD4+/FoxP3+/CD103+ and CTLA4+ effector Tregs as compared with the control group. In conclusion, our study identifies a potential target for the treatment of late-stage ALI by promoting resolution through effector Treg-mediated suppression of inflammation.

Published

2020

32. Indomethacin-induced oxidative stress enhances death receptor 5 signaling and sensitizes tumor cells to adoptive T-cell therapy

Author

Nada S Aboelella, Caitlin Brandle, Ogacheko Okoko, Md Yeashin Gazi, Zhi-Chun Ding, Hongyan Xu, Gregory Gorman, Roni Bollag, Marco L Davila, Locke J Bryan, David H Munn, Gary A Piazza, and Gang Zhou

Subjects

Pharmacology, Cancer Research, Immunology, Anti-Inflammatory Agents, Non-Steroidal, Indomethacin, Cell- and Tissue-Based Therapy, TNF-Related Apoptosis-Inducing Ligand, Mice, Oxidative Stress, Receptors, TNF-Related Apoptosis-Inducing Ligand, Oncology, Molecular Medicine, Immunology and Allergy, Animals, Humans, Neoplasm Recurrence, Local

Abstract

BackgroundAdoptive cell therapy (ACT) using genetically modified T cells has evolved into a promising treatment option for patients with cancer. However, even for the best-studied and clinically validated CD19-targeted chimeric antigen receptor (CAR) T-cell therapy, many patients face the challenge of lack of response or occurrence of relapse. There is increasing need to improve the efficacy of ACT so that durable, curative outcomes can be achieved in a broad patient population.MethodsHere, we investigated the impact of indomethacin (indo), a non-steroidal anti-inflammatory drug (NSAID), on the efficacy of ACT in multiple preclinical models. Mice with established B-cell lymphoma received various combinations of preconditioning chemotherapy, infusion of suboptimal dose of tumor-reactive T cells, and indo administration. Donor T cells used in the ACT models included CD4+ T cells expressing a tumor-specific T cell receptor (TCR) and T cells engineered to express CD19CAR. Mice were monitored for tumor growth and survival. The effects of indo on donor T cell phenotype and function were evaluated. The molecular mechanisms by which indo may influence the outcome of ACT were investigated.ResultsACT coupled with indo administration led to improved tumor growth control and prolonged mouse survival. Indo did not affect the activation status and tumor infiltration of the donor T cells. Moreover, the beneficial effect of indo in ACT did not rely on its inhibitory effect on the immunosuppressive cyclooxygenase 2 (COX2)/prostaglandin E2 (PGE2) axis. Instead, indo-induced oxidative stress boosted the expression of death receptor 5 (DR5) in tumor cells, rendering them susceptible to donor T cells expressing TNF-related apoptosis-inducing ligand (TRAIL). Furthermore, the ACT-potentiating effect of indo was diminished against DR5-deficient tumors, but was amplified by donor T cells engineered to overexpress TRAIL.ConclusionOur results demonstrate that the pro-oxidative property of indo can be exploited to enhance death receptor signaling in cancer cells, providing rationale for combining indo with genetically modified T cells to intensify tumor cell killing through the TRAIL-DR5 axis. These findings implicate indo administration, and potentially similar use of other NSAIDs, as a readily applicable and cost-effective approach to augment the efficacy of ACT.

Published

2022

33. Abstract LB200: Indoximod or ibrutinib/indoximod based clinical chemo-immunotherapy drives conversion of extra-tumoral circulating stem-like precursor CD8+ T cells into clonally expanded, rejuvenated effector cells

Author

Theodore S. Johnson, Rafal Pacholczyk, Zuzana Berrong, Chenbin Huang, Eugene P. Kennedy, Eric Ring, Ramses F. Sadek, Sarthak Satpathy, Beena E. Thomas, Tobey J. MacDonald, Manoj Bhasin, and David H. Munn

Subjects

Cancer Research, Oncology

Abstract

Increasing evidence suggests that many of the effector CD8+ T cells reactivated (‘rejuvenated”) by immunotherapy come from outside the tumor, derived from a circulating pool of “stem-like” memory or “precursor-exhausted” (TPEX) cells. These cells have been characterized in mice, but, despite their importance, circulating counterparts in humans have not yet been identified for study. We hypothesized that immunotherapy designed to enhance immunogenic antigen-presentation during chemotherapy might produce extensive reactivation of these precursor T cells. While the antigen-presentation step occurs in tissues, homing of the rejuvenated T cells to the tumor is via the circulation; thus, we hypothesized that they would be visible in blood. Informative patients were selected from two ongoing clinical trials of children with brain tumors treated with the IDO-inhibitor drug indoximod: a Phase 2 trial (NCT04049669) of indoximod plus chemotherapy; and a Phase 1 trial (NCT05106296) of indoximod, chemotherapy and the BTK-inhibitor ibrutinib, which synergistically destabilizes IDO (Immunity 54:2354-2371, 2021). Patient selection criteria included either (i) massive clonal expansion of activated CD8+ T cells on therapy (expanded clones reaching 16-25% of total CD8+ T cells); or (ii) complete radiographic tumor response (CR) on treatment; or (iii) both. Longitudinal blood samples (4-10 samples per patient) were obtained over a period of 6-24 months and analyzed by single-cell RNA-sequencing (scRNA-seq) with paired single-cell T cell receptor sequencing (scTCR-seq). TCR clonotypes of interest were identified based on robust clonal expansion on-treatment; then each clonotype was traced back through earlier samples to the pre-treatment baseline, or the earliest sample in which that clone could be detected. Clones were pooled, subjected to UMAP clustering, and differential gene-expression and trajectory analysis performed. At earliest appearance, each clonotype was enriched for a phenotype dominated by early transcription factors TCF7 and IKZF2 (Helios). These cells expressed little PDCD1 (PD-1) but showed a “hybrid” combination of genes associated with immaturity/arrest (BACH2, DUSP2, LTB, IL7R, CD160) and effector/memory (NKG7, GZMK, GZMA). Within each responding clone, this “precursor” phenotype could be observed to progressively transition into a mature cytotoxic/effector phenotype (PRF1, GZMB, GZMH, FGFBP2, KLRB1, IFNG). Trajectory analysis of this maturation sequence allowed us to analyze key gene-regulatory networks and transcription factor profiles at each stage. To our knowledge, this is the first study in humans to identify this key stem-like precursor population in circulation, allowing us to sequentially follow the molecular changes in these cells during rejuvenation. Citation Format: Theodore S. Johnson, Rafal Pacholczyk, Zuzana Berrong, Chenbin Huang, Eugene P. Kennedy, Eric Ring, Ramses F. Sadek, Sarthak Satpathy, Beena E. Thomas, Tobey J. MacDonald, Manoj Bhasin, David H. Munn. Indoximod or ibrutinib/indoximod based clinical chemo-immunotherapy drives conversion of extra-tumoral circulating stem-like precursor CD8+ T cells into clonally expanded, rejuvenated effector cells [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 2 (Clinical Trials and Late-Breaking Research); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(8_Suppl):Abstract nr LB200.

Published

2023

34. Ablation of the endoplasmic reticulum stress kinase PERK induces paraptosis and type I interferon to promote anti-tumor T cell responses

Author

Jessica K. Mandula, Shiun Chang, Eslam Mohamed, Rachel Jimenez, Rosa A. Sierra-Mondragon, Darwin C. Chang, Alyssa N. Obermayer, Carlos M. Moran-Segura, Satyajit Das, Julio A. Vazquez-Martinez, Karol Prieto, Ann Chen, Keiran S.M. Smalley, Brian Czerniecki, Peter Forsyth, Richard C. Koya, Brian Ruffell, Juan R. Cubillos-Ruiz, David H. Munn, Timothy I. Shaw, Jose R. Conejo-Garcia, and Paulo C. Rodriguez

Subjects

Cancer Research, Mice, eIF-2 Kinase, Oncology, Neoplasms, T-Lymphocytes, Interferon Type I, Unfolded Protein Response, Animals, Endoplasmic Reticulum Stress, Signal Transduction

Abstract

Activation of unfolded protein responses (UPRs) in cancer cells undergoing endoplasmic reticulum (ER) stress promotes survival. However, how UPR in tumor cells impacts anti-tumor immune responses remains poorly described. Here, we investigate the role of the UPR mediator pancreatic ER kinase (PKR)-like ER kinase (PERK) in cancer cells in the modulation of anti-tumor immunity. Deletion of PERK in cancer cells or pharmacological inhibition of PERK in melanoma-bearing mice incites robust activation of anti-tumor T cell immunity and attenuates tumor growth. PERK elimination in ER-stressed malignant cells triggers SEC61β-induced paraptosis, thereby promoting immunogenic cell death (ICD) and systemic anti-tumor responses. ICD induction in PERK-ablated tumors stimulates type I interferon production in dendritic cells (DCs), which primes CCR2-dependent tumor trafficking of common-monocytic precursors and their intra-tumor commitment into monocytic-lineage inflammatory Ly6C

Published

2022

35. Tumor PD-L1 engages myeloid PD-1 to suppress type I interferon to impair cytotoxic T lymphocyte recruitment

Author

John D. Klement, Priscilla S. Redd, Chunwan Lu, Alyssa D. Merting, Dakota B. Poschel, Dafeng Yang, Natasha M. Savage, Gang Zhou, David H. Munn, Padraic G. Fallon, and Kebin Liu

Subjects

Cancer Research, Oncology

Published

2023

36. BET-bromodomain and EZH2 inhibitor-treated chronic GVHD mice have blunted germinal centers with distinct transcriptomes

Author

Michael C. Zaiken, Ryan Flynn, Katelyn G. Paz, Stephanie Y. Rhee, Sujeong Jin, Fathima A. Mohamed, Asim Saha, Govindarajan Thangavelu, Paul M. C. Park, Matthew L. Hemming, Peter T. Sage, Arlene H. Sharpe, Michel DuPage, Jeffrey A. Bluestone, Angela Panoskaltsis-Mortari, Corey S. Cutler, John Koreth, Joseph H. Antin, Robert J. Soiffer, Jerome Ritz, Leo Luznik, Ivan Maillard, Geoffrey R. Hill, Kelli P. A. MacDonald, David H. Munn, Jonathan S. Serody, William J. Murphy, Leslie S. Kean, Yi Zhang, James E. Bradner, Jun Qi, and Bruce R. Blazar

Subjects

B-Lymphocytes, Immunology, Graft vs Host Disease, Proteins, Cell Biology, Hematology, Germinal Center, Biochemistry, Mice, hemic and lymphatic diseases, Chronic Disease, Animals, Humans, Enhancer of Zeste Homolog 2 Protein, Enzyme Inhibitors, Transcriptome, Bronchiolitis Obliterans

Abstract

Despite advances in the field, chronic graft-versus-host-disease (cGVHD) remains a leading cause of morbidity and mortality following allogenic hematopoietic stem cell transplant. Because treatment options remain limited, we tested efficacy of anticancer, chromatin-modifying enzyme inhibitors in a clinically relevant murine model of cGVHD with bronchiolitis obliterans (BO). We observed that the novel enhancer of zeste homolog 2 (EZH2) inhibitor JQ5 and the BET-bromodomain inhibitor JQ1 each improved pulmonary function; impaired the germinal center (GC) reaction, a prerequisite in cGVHD/BO pathogenesis; and JQ5 reduced EZH2-mediated H3K27me3 in donor T cells. Using conditional EZH2 knockout donor cells, we demonstrated that EZH2 is obligatory for the initiation of cGVHD/BO. In a sclerodermatous cGVHD model, JQ5 reduced the severity of cutaneous lesions. To determine how the 2 drugs could lead to the same physiological improvements while targeting unique epigenetic processes, we analyzed the transcriptomes of splenic GCB cells (GCBs) from transplanted mice treated with either drug. Multiple inflammatory and signaling pathways enriched in cGVHD/BO GCBs were reduced by each drug. GCBs from JQ5- but not JQ1-treated mice were enriched for proproliferative pathways also seen in GCBs from bone marrow-only transplanted mice, likely reflecting their underlying biology in the unperturbed state. In conjunction with in vivo data, these insights led us to conclude that epigenetic targeting of the GC is a viable clinical approach for the treatment of cGVHD, and that the EZH2 inhibitor JQ5 and the BET-bromodomain inhibitor JQ1 demonstrated clinical potential for EZH2i and BETi in patients with cGVHD/BO.

Published

2021

37. CD73 on cancer-associated fibroblasts enhanced by the A2B-mediated feedforward circuit enforces an immune checkpoint

Author

Lei Huang, Ningchun Xu, Paulo C. Rodriguez, Madison Canning, Gang Guo, Yan Cui, Ali S. Arbab, Chang Sheng Chang, Bhagelu R. Achyut, Miao Yu, Huidong Shi, David H. Munn, Libin Deng, Roni J. Bollag, and Andrew L. Mellor

Subjects

0301 basic medicine, Science, Population, General Physics and Astronomy, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, NT5E, 0302 clinical medicine, Immune system, Downregulation and upregulation, Medicine, Receptor, education, lcsh:Science, Tumor microenvironment, education.field_of_study, Multidisciplinary, business.industry, fungi, food and beverages, General Chemistry, Immune checkpoint, 3. Good health, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer research, Cancer-Associated Fibroblasts, lcsh:Q, business

Abstract

CD73, an ecto-5′-nucleotidase (NT5E), serves as an immune checkpoint by generating adenosine (ADO), which suppresses immune activation through the A2A receptor. Elevated CD73 levels in tumor tissues correlate with poor clinical outcomes. However, the crucial source of CD73 activity within the tumor microenvironment remains unspecified. Here, we demonstrate that cancer-associated fibroblasts (CAFs) constitute the prominent CD73hi population in human colorectal cancers (CRCs) and two CD73− murine tumor models, including a modified CRC. Clinically, high CAF abundancy in CRC tissues correlates strongly with elevated CD73 activity and poor prognosis. Mechanistically, CAF-CD73 expression is enhanced via an ADO-A2B receptor-mediated feedforward circuit triggered by tumor cell death, which enforces the CD73-checkpoint. Simultaneous inhibition of A2A and A2B pathways with CD73-neutralization synergistically enhances antitumor immunity in CAF-rich tumors. Therefore, the strategic and effective targeting of both the A2B-mediated ADO-CAF-CD73 feedforward circuit and A2A-mediated immune suppression is crucial for improving therapeutic outcomes.

Published

2020

38. Tumor PD-L1 selectively suppresses type I interferon in myeloid cells to suppress CTL recruitment to promote lung metastasis

Author

Dakota B. Poschel, Zhou G, Dafeng Yang, Priscilla S. Redd, David H. Munn, Alyssa D. Merting, Kebin Liu, Chunwan Lu, and John D. Klement

Subjects

Myeloid, business.industry, medicine.medical_treatment, T cell, Immunotherapy, medicine.disease, Primary tumor, CTL, medicine.anatomical_structure, Immune system, Interferon, Cancer research, Medicine, Cytotoxic T cell, business, medicine.drug

Abstract

The mechanism underlying tumor cell PD-L1 (tPD-L1) induction of immune suppression through T cell PD-1 is well-known, but the mechanism underlying tPD-L1 induction of immune suppression via an intermediate cell is incompletely understood. We report here that tPD-L1 does not suppress cytotoxic T lymphocyte (CTL) activation and lytic function when only tumor cells and CTLs are present. Strikingly, knocking out PD-L1 in tumor cells has no effect on primary tumor growth, but significantly decreases lung metastasis in a CTL-dependent manner. Depletion of myeloid cells impaired tPD-L1 promotion of lung metastasis. Single-cell RNA sequencing revealed that tPD-L1 engages myeloid PD-1 (mPD-1) to antagonize type I interferon (IFN-I) and STAT1 signaling to repress Cxcl9 and Cxcl10 expression to impair CTL recruitment to lung metastases. Human patient response to PD-1 blockade immunotherapy correlates with IFN-I response in myeloid cells. Our data determines that the tPD-L1/mPD-1/IFN-I/STAT1/Cxcl9/10 axis controls CTL tumor infiltration in lung metastasis.

Published

2021

39. Phase II trial of the IDO pathway inhibitor indoximod plus pembrolizumab for the treatment of patients with advanced melanoma

Author

Montaser Shaheen, Jiayi Yu, Charles J. Link, Yousef Zakharia, Ramses F. Sadek, Robert R. McWilliams, Mohammed M. Milhem, Lucinda Tennant, Joseph J. Drabick, Olivier Rixe, Kenneth F. Grossmann, Gabriela R. Rossi, Nicholas N. Vahanian, Erik L. Brincks, Eugene P. Kennedy, Ravindra Kolhe, David H. Munn, Steven S. Shen, Christopher M Smith, and Rafal Pacholczyk

Subjects

Oncology, Adult, Male, Cancer Research, medicine.medical_specialty, medicine.medical_treatment, Immunology, Population, Ipilimumab, Pembrolizumab, Antibodies, Monoclonal, Humanized, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, melanoma, Immunology and Allergy, Humans, education, RC254-282, Aged, Pharmacology, Aged, 80 and over, Clinical/Translational Cancer Immunotherapy, education.field_of_study, business.industry, Melanoma, Tryptophan, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cancer, Immunotherapy, Middle Aged, medicine.disease, Clinical trial, indoleamine-pyrrole 2, Dioxygenase, Molecular Medicine, Female, immunotherapy, Nivolumab, business, medicine.drug

Abstract

BackgroundThe indoleamine 2,3-dioxygenase (IDO) pathway is a key counter-regulatory mechanism that, in cancer, is exploited by tumors to evade antitumor immunity. Indoximod is a small-molecule IDO pathway inhibitor that reverses the immunosuppressive effects of low tryptophan (Trp) and high kynurenine (Kyn) that result from IDO activity. In this study, indoximod was used in combination with a checkpoint inhibitor (CPI) pembrolizumab for the treatment for advanced melanoma.MethodsPatients with advanced melanoma were enrolled in a single-arm phase II clinical trial evaluating the addition of indoximod to standard of care CPI approved for melanoma. Investigators administered their choice of CPI including pembrolizumab (P), nivolumab (N), or ipilimumab (I). Indoximod was administered continuously (1200 mg orally two times per day), with concurrent CPI dosed per US Food and Drug Administration (FDA)-approved label.ResultsBetween July 2014 and July 2017, 131 patients were enrolled. (P) was used more frequently (n=114, 87%) per investigator’s choice. The efficacy evaluable population consisted of 89 patients from the phase II cohort with non-ocular melanoma who received indoximod combined with (P).The objective response rate (ORR) for the evaluable population was 51% with confirmed complete response of 20% and disease control rate of 70%. Median progression-free survival was 12.4 months (95% CI 6.4 to 24.9). The ORR for Programmed Death-Ligand 1 (PD-L1)-positive patients was 70% compared with 46% for PD-L1-negative patients. The combination was well tolerated, and side effects were similar to what was expected from single agent (P).ConclusionIn this study, the combination of indoximod and (P) was well tolerated and showed antitumor efficacy that is worth further evaluation in selected patients with advanced melanoma.

Published

2021

40. Persistent STAT5 activation reprograms the epigenetic landscape in CD4 + T cells to drive polyfunctionality and antitumor immunity

Author

Richard A. McIndoe, Eun Jeong Park, David H. Munn, Nada S. Aboelella, Gary A. Piazza, Zhuoqi Liu, Hongyan Xu, Jiaqi Li, Lirong Pei, Kateryna Fesenkova, Bruce R. Blazar, Zhi-Chun Ding, Gang Zhou, and Huidong Shi

Subjects

CD4-Positive T-Lymphocytes, Male, Adoptive cell transfer, Lymphoma, T cell, medicine.medical_treatment, Primary Cell Culture, Immunology, Mice, Transgenic, Immunotherapy, Adoptive, Article, Epigenesis, Genetic, Mice, Single-cell analysis, Transduction, Genetic, Cell Line, Tumor, STAT5 Transcription Factor, medicine, Animals, Humans, RNA-Seq, Epigenetics, Receptors, Chimeric Antigen, Chemistry, General Medicine, Immunotherapy, Chimeric antigen receptor, Cell biology, Gene Expression Regulation, Neoplastic, Disease Models, Animal, medicine.anatomical_structure, Cell culture, Female, Single-Cell Analysis, CD8

Abstract

The presence of polyfunctional CD4(+) T cells is often associated with favorable antitumor immunity. We report here that persistent activation of signal transducer and activator of transcription 5 (STAT5) in tumor-specific CD4(+) T cells drives the development of polyfunctional T cells. We showed that ectopic expression of a constitutively active form of murine STAT5A (CASTAT5) enabled tumor-specific CD4(+) T cells to undergo robust expansion, infiltrate tumors vigorously and elicit antitumor CD8(+) T cell responses in a CD4(+) T-cell adoptive transfer model system. Integrated epigenomic and transcriptomic analysis revealed that CASTAT5 induced genome-wide chromatin remodeling in CD4(+) T cells and established a distinct epigenetic and transcriptional landscape. Single-cell RNA sequencing analysis further identified a subset of CASTAT5-transduced CD4(+) T cells with a molecular signature indicative of progenitor polyfunctional T cells. The therapeutic significance of CASTAT5 came from our finding that adoptive transfer of T cells engineered to co-express CD19-targeting chimeric antigen receptor (CAR) and CASTAT5 gave rise to polyfunctional CD4(+) CAR T cells in a mouse B-cell lymphoma model. Notably, the optimal therapeutic outcome was obtained when both CD4(+) and CD8(+) CAR T cells were transduced with CASTAT5, indicating that CASTAT5 facilitates productive CD4 help to CD8(+) T cells. Furthermore, we provide evidence that CASTAT5 is functional in primary human CD4(+) T cells, underscoring its potential clinical relevance. Our results implicate STAT5 as a valid candidate for T cell engineering to generate polyfunctional, exhaustion-resistant, and tumor-tropic antitumor CD4(+) T cells to potentiate adoptive T-cell therapy for cancer.

Published

2020

41. ER stress-induced mediator C/EBP homologous protein thwarts effector T cell activity in tumors through T-bet repression

Author

Yu Cao, Shikhar Mehrotra, Eslam Mohamed, David H. Munn, Anthony M. Magliocco, Ling Cen, Rosa A. Sierra, Jose R. Conejo-Garcia, Richard Klar, Carmen M. Anadon, Sven Michel, Juan R. Cubillos-Ruiz, Wenjie Dai, Jimena Trillo-Tinoco, Paulo C. Rodriguez, Douglas C. Marchion, Frank Jaschinski, Richard R. Reich, and Tara Lee Costich

Subjects

0301 basic medicine, Adoptive cell transfer, medicine.medical_treatment, General Physics and Astronomy, 02 engineering and technology, CD8-Positive T-Lymphocytes, Carcinoma, Ovarian Epithelial, CHOP, Mice, eIF-2 Kinase, hemic and lymphatic diseases, Tumor Microenvironment, RNA, Small Interfering, lcsh:Science, Mice, Knockout, Ovarian Neoplasms, Immunity, Cellular, Multidisciplinary, Effector, Chemistry, Endoplasmic Reticulum Stress, 021001 nanoscience & nanotechnology, Adoptive Transfer, Publisher Correction, 3. Good health, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Tumour immunology, Female, 0210 nano-technology, Science, T cell, chemical and pharmacologic phenomena, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Lymphocytes, Tumor-Infiltrating, Cell Line, Tumor, medicine, Animals, Humans, Tumor microenvironment, Immunosurveillance, General Chemistry, Immunotherapy, Activating Transcription Factor 4, Survival Analysis, Xenograft Model Antitumor Assays, 030104 developmental biology, Unfolded protein response, Cancer research, lcsh:Q, T-Box Domain Proteins, Transcription Factor CHOP, CD8

Abstract

Understanding the intrinsic mediators that render CD8+ T cells dysfunctional in the tumor microenvironment is a requirement to develop more effective cancer immunotherapies. Here, we report that C/EBP homologous protein (Chop), a downstream sensor of severe endoplasmic reticulum (ER) stress, is a major negative regulator of the effector function of tumor-reactive CD8+ T cells. Chop expression is increased in tumor-infiltrating CD8+ T cells, which correlates with poor clinical outcome in ovarian cancer patients. Deletion of Chop in T cells improves spontaneous antitumor CD8+ T cell immunity and boosts the efficacy of T cell-based immunotherapy. Mechanistically, Chop in CD8+ T cells is elevated primarily through the ER stress-associated kinase Perk and a subsequent induction of Atf4; and directly represses the expression of T-bet, a master regulator of effector T cell function. These findings demonstrate the primary role of Chop in tumor-induced CD8+ T cell dysfunction and the therapeutic potential of blocking Chop or ER stress to unleash T cell-mediated antitumor immunity., T-cell function impairment is one of the major determinants of tumour immune evasion. Here, the authors show that the hostile conditions in the tumour microenvironment lead to C/EBP homologous-protein upregulation in T cells via ER stress, resulting in repression of T-bet and consequent inhibition of CD8+ T cell function.”

Published

2019

42. Treg Destabilization and Reprogramming: Implications for Cancer Immunotherapy

Author

Madhav D. Sharma, Theodore S. Johnson, and David H. Munn

Subjects

0301 basic medicine, Cancer Research, medicine.medical_treatment, Receptors, Antigen, T-Cell, Down-Regulation, chemical and pharmacologic phenomena, Inflammation, T-Lymphocytes, Regulatory, Article, Proinflammatory cytokine, Translational Research, Biomedical, Interferon-gamma, 03 medical and health sciences, 0302 clinical medicine, Immune system, Cancer immunotherapy, Cell Line, Tumor, Neoplasms, Tumor Microenvironment, Animals, Humans, Medicine, Cell Lineage, Tumor microenvironment, Interleukin-6, business.industry, PTEN Phosphohydrolase, Cancer, hemic and immune systems, Immunotherapy, medicine.disease, Gene Expression Regulation, Neoplastic, Phenotype, 030104 developmental biology, Oncology, Immune System, 030220 oncology & carcinogenesis, Cancer research, medicine.symptom, business, Reprogramming

Abstract

Regulatory T cells (Tregs) are an important contributor to the immunosuppressive tumor microenvironment. To date, however, they have been difficult to target for therapy. One emerging new aspect of Treg biology is their apparent functional instability in the face of certain acute proinflammatory signals such as IL6 and IFNγ. Under the right conditions, these signals can cause a rapid loss of suppressor activity and reprogramming of the Tregs into a proinflammatory phenotype. In this review, we propose the hypothesis that this phenotypic modulation does not reflect infidelity to the Treg lineage, but rather represents a natural, physiologic response of Tregs during beneficial inflammation. In tumors, however, this inflammation-induced Treg destabilization is actively opposed by dominant stabilizing factors such as indoleamine 2,3-dioxygenase and the PTEN phosphatase pathway in Tregs. Under such conditions, tumor-associated Tregs remain highly suppressive and inhibit cross-presentation of tumor antigens released by dying tumor cells. Interrupting these Treg stabilizing pathways can render tumor-associated Tregs sensitive to rapid destabilization during immunotherapy, or during the wave of cell death following chemotherapy or radiation, thus enhancing antitumor immune responses. Understanding the emerging pathways of Treg stabilization and destabilization may reveal new molecular targets for therapy. Cancer Res; 78(18); 5191–9. ©2018 AACR.

Published

2018

43. The vimentin intermediate filament network restrains regulatory T cell suppression of graft-versus-host disease

Author

Jonathan S. Serody, Ameeta Kelekar, Brent H. Koehn, Brian T. Fife, Laurence A. Turka, Asim Saha, Govindarajan Thangavelu, Keli L. Hippen, Sudha Kumari, Angela Panoskaltsis-Mortari, Andrew Kemal Kirchmeier, Mark J. Osborn, Cameron McDonald-Hyman, David H. Munn, Jason S. Mitchell, Guoan Zhang, Bruce R. Blazar, Colby J. Feser, Michael Loschi, Michael L. Dustin, Jiqiang Lin, James E. Muller, Thomas A. Neubert, Hongbo Chi, Michelle J. Smith, and Dawn K. Reichenbach

Subjects

0301 basic medicine, Regulatory T cell, T cell, Cell, Intermediate Filaments, Antigen-Presenting Cells, Graft vs Host Disease, Priming (immunology), Mice, Transgenic, chemical and pharmacologic phenomena, Vimentin, Lymphocyte Activation, T-Lymphocytes, Regulatory, Mice, 03 medical and health sciences, medicine, Animals, Humans, Kinase activity, Protein kinase C, Mice, Inbred BALB C, biology, Chemistry, General Medicine, Acquired immune system, Cell biology, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Protein Kinase C-theta, biology.protein, Research Article

Abstract

Regulatory T cells (Tregs) are critical for maintaining immune homeostasis. However, current Treg immunotherapies do not optimally treat inflammatory diseases in patients. Understanding the cellular processes that control Treg function may allow for the augmentation of therapeutic efficacy. In contrast to activated conventional T cells, in which protein kinase C-θ (PKC-θ) localizes to the contact point between T cells and antigen-presenting cells, in human and mouse Tregs, PKC-θ localizes to the opposite end of the cell in the distal pole complex (DPC). Here, using a phosphoproteomic screen, we identified the intermediate filament vimentin as a PKC-θ phospho target and show that vimentin forms a DPC superstructure on which PKC-θ accumulates. Treatment of mouse Tregs with either a clinically relevant PKC-θ inhibitor or vimentin siRNA disrupted vimentin and enhanced Treg metabolic and suppressive activity. Moreover, vimentin-disrupted mouse Tregs were significantly better than controls at suppressing alloreactive T cell priming in graft-versus-host disease (GVHD) and GVHD lethality, using a complete MHC-mismatch mouse model of acute GVHD (C57BL/6 donor into BALB/c host). Interestingly, vimentin disruption augmented the suppressor function of PKC-θ-deficient mouse Tregs. This suggests that enhanced Treg activity after PKC-θ inhibition is secondary to effects on vimentin, not just PKC-θ kinase activity inhibition. Our data demonstrate that vimentin is a key metabolic and functional controller of Treg activity and provide proof of principle that disruption of vimentin is a feasible, translationally relevant method to enhance Treg potency.

Published

2018

44. Apoptotic cell–induced AhR activity is required for immunological tolerance and suppression of systemic lupus erythematosus in mice and humans

Author

Reema Deol, Tiago Medina, Rahul Shinde, Marie Jo Halaby, Yuriy Baglaenko, Zahi Touma, Sathi Babu Chodisetti, Kieran P. Manion, Haiyun Liu, Maria Eldh, Sara Lamorte, Kapil Chaudhary, Andreas Kloetgen, Drew Wallace, Kebria Hezaveh, Tracy L. McGaha, Ankur Chakravarthy, Aristotelis Tsirigos, David H. Munn, Joan E. Wither, Susanne Gabrielsson, Michael P. Madaio, Daniel D. De Carvalho, and Buvana Ravishankar

Subjects

0301 basic medicine, medicine.medical_treatment, Immunology, Cell, Apoptosis, Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immunity, Immune Tolerance, medicine, Animals, Humans, Lupus Erythematosus, Systemic, Immunology and Allergy, Transcription factor, Macrophages, Peripheral tolerance, TLR9, respiratory system, respiratory tract diseases, 3. Good health, 030104 developmental biology, Cytokine, medicine.anatomical_structure, Receptors, Aryl Hydrocarbon, Toll-Like Receptor 9, 030220 oncology & carcinogenesis, Signal Transduction

Abstract

The transcription factor AhR modulates immunity at multiple levels. Here we report that phagocytes exposed to apoptotic cells exhibited rapid activation of AhR, which drove production of the cytokine IL-10. Activation of AhR was dependent on interactions between apoptotic-cell DNA and the pattern-recognition receptor TLR9 that was required for the prevention of immune responses to DNA and histones in vivo. Moreover, disease progression in mouse systemic lupus erythematosus (SLE) correlated with strength of the AhR signal, and the disease course could be altered by modulation of AhR activity. Deletion of AhR in the myeloid lineage caused systemic autoimmunity in mice, and an enhanced AhR transcriptional signature correlated with disease in patients with SLE. Thus, AhR activity induced by apoptotic cell phagocytes maintains peripheral tolerance.

Published

2018

45. Immunosuppressive metabolites in tumoral immune evasion: redundancies, clinical efforts, and pathways forward

Author

Maria Rain Jennings, John Blazeck, and David H. Munn

Subjects

Cancer Research, medicine.medical_treatment, Immunology, Review, Bioinformatics, Immune system, Negatively associated, Neoplasms, medicine, Humans, Immunology and Allergy, RC254-282, Immune Evasion, Immunosuppression Therapy, Pharmacology, business.industry, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cancer, tumor escape, Immunotherapy, medicine.disease, Evasion (ethics), Phenotype, indoleamine-pyrrole 2,3-dioxygenase, Oncology, Tumor Escape, adenosine, Molecular Medicine, Signal transduction, metabolic networks and pathways, business

Abstract

Tumors accumulate metabolites that deactivate infiltrating immune cells and polarize them toward anti-inflammatory phenotypes. We provide a comprehensive review of the complex networks orchestrated by several of the most potent immunosuppressive metabolites, highlighting the impact of adenosine, kynurenines, prostaglandin E2, and norepinephrine and epinephrine, while discussing completed and ongoing clinical efforts to curtail their impact. Retrospective analyses of clinical data have elucidated that their activity is negatively associated with prognosis in diverse cancer indications, though there is a current paucity of approved therapies that disrupt their synthesis or downstream signaling axes. We hypothesize that prior lukewarm results may be attributed to redundancies in each metabolites’ synthesis or signaling pathway and highlight routes for how therapeutic development and patient stratification might proceed in the future.

Published

2021

46. Inhibition of the BTK-IDO-mTOR axis promotes differentiation of monocyte-lineage dendritic cells and enhances anti-tumor T cell immunity

Author

Roni J. Bollag, Huidong Shi, Eugene P. Kennedy, Ramses F. Sadek, Madhav D. Sharma, Jessica Mandula, Thomas Cash, Chang Sheng S. Chang, Tracy L. McGaha, Rafal Pacholczyk, Yousef Zakharia, David H. Munn, Ravindra Kolhe, Paulo C. Rodriguez, Zuzana Berrong, Bruce R. Blazar, Austin Greco, Theodore S. Johnson, and Sudharshan Eathiraj

Subjects

biology, medicine.medical_treatment, Monocyte, Immunology, hemic and immune systems, chemical and pharmacologic phenomena, Immunotherapy, mTORC1, Infectious Diseases, medicine.anatomical_structure, hemic and lymphatic diseases, Cancer research, medicine, biology.protein, Immunology and Allergy, Bruton's tyrosine kinase, Antigen-presenting cell, Indoleamine 2,3-dioxygenase, Tyrosine kinase, PI3K/AKT/mTOR pathway

Abstract

Summary Monocytic-lineage inflammatory Ly6c+CD103+ dendritic cells (DCs) promote antitumor immunity, but these DCs are infrequent in tumors, even upon chemotherapy. Here, we examined how targeting pathways that inhibit the differentiation of inflammatory myeloid cells affect antitumor immunity. Pharmacologic inhibition of Bruton’s tyrosine kinase (BTK) and the tryptophan-degrading enzyme indoleamine 2,3-dioxygenase (IDO) or deletion of Btk or Ido1 allowed robust differentiation of inflammatory Ly6c+CD103+ DCs during chemotherapy, promoting antitumor T cell responses and inhibiting tumor growth. Immature Ly6c+c-kit+ precursor cells had epigenetic profiles similar to conventional DC precursors; deletion of Btk or Ido1 promoted differentiation of these cells. Mechanistically, a BTK-IDO axis inhibited a tryptophan-sensitive differentiation pathway driven by GATOR2 and mTORC1, and disruption of the GATOR2 in monocyte-lineage precursors prevented differentiation into inflammatory DCs in vivo. IDO-expressing DCs and monocytic cells were present across a range of human tumors. Thus, a BTK-IDO axis represses differentiation of inflammatory DCs during chemotherapy, with implications for targeted therapies.

Published

2021

47. Adjuvant IL-7 potentiates adoptive T cell therapy by amplifying and sustaining polyfunctional antitumor CD4+ T cells

Author

Locke J. Bryan, David H. Munn, Zhi-Chun Ding, Tsadik Habtetsion, Tao Li, Tingting Chen, Michal Kuczma, Chufeng Liu, Gang Zhou, Zhonglin Hao, and Yang Cao

Subjects

CD4-Positive T-Lymphocytes, 0301 basic medicine, Lymphoma, medicine.medical_treatment, T cell, lcsh:Medicine, Biology, Immunotherapy, Adoptive, Article, 03 medical and health sciences, Interleukin 21, Immune system, Adjuvants, Immunologic, medicine, Animals, IL-2 receptor, lcsh:Science, Mice, Inbred BALB C, Multidisciplinary, Interleukin-7, lcsh:R, Immunotherapy, Recombinant Proteins, 3. Good health, 030104 developmental biology, Cytokine, medicine.anatomical_structure, Immunology, lcsh:Q, Adjuvant, CD8

Abstract

Increased availability of homeostatic cytokines is considered a major mechanism by which lymphodepletion enhances the efficacy of adoptive T cell therapy (ACT). IL-7 is one such cytokine capable of augmenting the function of tumor-reactive CD8+ T cells. However, whether host-derived IL-7 plays a role in driving the proper function of CD4+ T cells in an ACT setting remains unclear. Here we report that lymphodepleting chemotherapy by cyclophosphamide (CTX) does not lead to increased availability of the endogenous IL-7 in mice. Despite of a paucity of IL-7 in the immune milieu, CTX preconditioning allowed adoptively transferred naïve tumor-specific CD4+ T cells to undergo effector differentiation and regain IL-7Rα expression, giving rise to IL-7-responsive polyfunctional CD4+ effector cells. Correspondingly, supplementation of exogenous recombinant IL-7 markedly amplified and sustained polyfunctional CD4+ effector cells, resulting in improved therapeutic outcome in a mouse lymphoma model. We further demonstrated that the immune-enhancing effects of IL-7 were also applicable to donor CD4+ T cells pre-activated under Th1 polarizing condition. These findings suggest caution in relying on the endogenous IL-7 to enhance donor T cell expansion and persistence after lymphodepleting chemotherapy, and highlight the usefulness of recombinant IL-7 as an adjuvant for adoptive immunotherapy.

Published

2017

48. Advanced Age Increases Immunosuppression in the Brain and Decreases Immunotherapeutic Efficacy in Subjects with Glioblastoma

Author

Craig Horbinski, Judith Campisi, David H. Munn, Kristen L. Lauing, Ursula Grohmann, George C. Prendergast, Karan Dixit, Aaron Mochizuki, Jeffrey Raizer, Jiahui Xu, Robert M. Prins, Derek A. Wainwright, April Bell, Changyou Zhou, Graham Pawelec, Priya Kumthekar, Jennifer D. Wu, Leonidas C. Platanias, Erik Ladomersky, Rimas V. Lukas, Joseph R. Podojil, Bin Zhang, Masha Kocherginsky, Lijie Zhai, and Min Wei

Subjects

Adult, Male, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, medicine.drug_class, medicine.medical_treatment, Brain tumor, Monoclonal antibody, Article, B7-H1 Antigen, 03 medical and health sciences, 0302 clinical medicine, Text mining, Older patients, Immunity, Internal medicine, medicine, Animals, Humans, Indoleamine-Pyrrole 2,3,-Dioxygenase, CTLA-4 Antigen, Immune Checkpoint Inhibitors, Cellular Senescence, Aged, Aged, 80 and over, Immunosuppression Therapy, Mice, Knockout, biology, business.industry, Age Factors, Brain, Immunosuppression, Middle Aged, medicine.disease, Isocitrate Dehydrogenase, Progression-Free Survival, Disease Models, Animal, 030104 developmental biology, Enzyme inhibitor, biology.protein, Female, Glioblastoma, business, 030217 neurology & neurosurgery

Abstract

Purpose: Wild-type isocitrate dehydrogenase–expressing glioblastoma (GBM) is the most common and aggressive primary brain tumor with a median age at diagnosis of ≥65 years. It accounts for approximately 90% of all GBMs and has a median overall survival (OS) of Experimental Design: (i) Clinical data: GBM patient datasets from The Cancer Genome Atlas, Northwestern Medicine Enterprise Data Warehouse, and clinical studies evaluating ICB were stratified by age and compared for OS. (ii) Animal models: young, middle-aged, and older adult wild-type and indoleamine 2,3 dioxygenase (IDO)-knockout syngeneic mice were intracranially engrafted with CT-2A or GL261 glioma cell lines and treated with or without CTLA-4/PD-L1 mAbs, or radiation, anti–PD-1 mAb, and/or a pharmacologic IDO enzyme inhibitor. Results: Advanced age was associated with decreased GBM patient survival regardless of treatment with ICB. The advanced age–associated increase of brain IDO expression was linked to the suppression of immunotherapeutic efficacy and was not reversed by IDO enzyme inhibitor treatment. Conclusions: Immunosuppression increases in the brain during advanced age and inhibits antiglioma immunity in older adults. Going forward, it will be important to fully understand the factors and mechanisms in the elderly brain that contribute to the decreased survival of older patients with GBM during treatment with ICB.

Published

2020

49. GCN2 drives macrophage and MDSC function and immunosuppression in the tumor microenvironment

Author

Marie Jo Halaby, Vincenzo Bronte, Andreas Kloetgen, Trevor J. Pugh, David G. Brooks, Kebria Hezaveh, M. Teresa Ciudad, Tracy L. McGaha, Daniel D. De Carvalho, Mengdi Guo, David H. Munn, Sara Lamorte, Aristotelis Tsirigos, Bethany L. MacLeod, Marcus O. Butler, Stefano Ugel, Tiago Medina, Ankur Chakravarthy, and Pamela S. Ohashi

Subjects

0301 basic medicine, Small interfering RNA, Myeloid, T cell, Immunology, Macrophage polarization, CD8-Positive T-Lymphocytes, Protein Serine-Threonine Kinases, Biology, Article, Proinflammatory cytokine, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, Tumor Microenvironment, medicine, Animals, Humans, Immunology, tumor Immunology, Melanoma, Transcription factor, Cells, Cultured, Tumor microenvironment, tumor Immunology, Macrophages, Myeloid-Derived Suppressor Cells, General Medicine, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cancer research

Abstract

General control nonderepressible 2 (GCN2) is an environmental sensor controlling transcription and translation in response to nutrient availability. Although GCN2 is a putative therapeutic target for immuno-oncology, its role in shaping the immune response to tumors is poorly understood. Here, we used mass cytometry, transcriptomics, and transcription factor-binding analysis to determine the functional impact of GCN2 on the myeloid phenotype and immune responses in melanoma. We found that myeloid-lineage deletion of GCN2 drives a shift in the phenotype of tumor-associated macrophages and myeloid-derived suppressor cells (MDSCs) that promotes antitumor immunity. Time-of-flight mass cytometry (CyTOF) and single-cell RNA sequencing showed that this was due to changes in the immune microenvironment with increased proinflammatory activation of macrophages and MDSCs and interferon-γ expression in intratumoral CD8+ T cells. Mechanistically, GCN2 altered myeloid function by promoting increased translation of the transcription factor CREB-2/ATF4, which was required for maturation and polarization of macrophages and MDSCs in both mice and humans, whereas targeting Atf4 by small interfering RNA knockdown reduced tumor growth. Last, analysis of patients with cutaneous melanoma showed that GCN2-dependent transcriptional signatures correlated with macrophage polarization, T cell infiltrates, and overall survival. Thus, these data reveal a previously unknown dependence of tumors on myeloid GCN2 signals for protection from immune attack.

Published

2019

50. Donor and host B7-H4 expression negatively regulates acute graft-versus-host disease lethality

Author

Xingxing Zang, Angela Panoskaltsis-Mortari, Patricia A. Taylor, Jonathan S. Serody, Yosef Refaeli, William J. Murphy, David H. Munn, Shuyu Huang, Marcel R.M. van den Brink, Ivan Maillard, Govindarajan Thangavelu, James P. Allison, Mark J. Osborn, Robert Zeiser, Christopher J. Lees, Chen Dong, Bruce R. Blazar, Geoffrey R. Hill, Asim Saha, Colby J. Feser, Wolfgang Melchinger, and Katharina Kreymborg

Subjects

0301 basic medicine, Lymphoma, T-Lymphocytes, Graft vs Host Disease, Inbred C57BL, Mice, 0302 clinical medicine, Lung, Inbred BALB C, Bone Marrow Transplantation, Mice, Knockout, Mice, Inbred BALB C, Tumor, General Medicine, Hematology, Tissue Donors, Haematopoiesis, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cytokines, Female, Metabolic Networks and Pathways, Research Article, Bone marrow transplantation, T cell, Knockout, Immunology, T cells, Biology, Proinflammatory cytokine, Cell Line, 03 medical and health sciences, Chimera (genetics), Oxygen Consumption, Rare Diseases, Cell Line, Tumor, medicine, Animals, Cell Proliferation, Transplantation, Animal, V-Set Domain-Containing T-Cell Activation Inhibitor 1, Stem Cell Research, Mice, Inbred C57BL, Gastrointestinal Tract, Cytolysis, Disease Models, Animal, 030104 developmental biology, Apoptosis, Disease Models, Cancer research, Transcriptome, Homing (hematopoietic)

Abstract

B7-H4 is a negative regulatory B7 family member. We investigated the role of host and donor B7-H4 in regulating acute graft-versus-host disease (GVHD). Allogeneic donor T cells infused into B7-H4(–/–) versus WT recipients markedly accelerated GVHD-induced lethality. Chimera studies pointed toward B7-H4 expression on host hematopoietic cells as more critical than parenchymal cells in controlling GVHD. Rapid mortality in B7-H4(–/–) recipients was associated with increased donor T cell expansion, gut T cell homing and loss of intestinal epithelial integrity, increased T effector function (proliferation, proinflammatory cytokines, cytolytic molecules), and reduced apoptosis. Higher metabolic demands of rapidly proliferating donor T cells in B7-H4(–/–) versus WT recipients required multiple metabolic pathways, increased extracellular acidification rates (ECARs) and oxygen consumption rates (OCRs), and increased expression of fuel substrate transporters. During GVHD, B7-H4 expression was upregulated on allogeneic WT donor T cells. B7-H4(–/–) donor T cells given to WT recipients increased GVHD mortality and had function and biological properties similar to WT T cells from allogeneic B7-H4(–/–) recipients. Graft-versus-leukemia responses were intact regardless as to whether B7-H4(–/–) mice were used as hosts or donors. Taken together, these data provide new insights into the negative regulatory processes that control GVHD and provide support for developing therapeutic strategies directed toward the B7-H4 pathway.

Published

2019