Targeting T cell checkpoints 41BB and LAG3 and myeloid cell CXCR1/CXCR2 results in antitumor immunity and durable response in pancreatic cancer

Pat Gulhati; Aislyn Schalck; Shan Jiang; Xiaoying Shang; Chang Jiun Wu; Pingping Hou; Sharia Hernandez Ruiz; Luisa Solis Soto; Edwin Parra; Haoqiang Ying; Jincheng Han; Prasenjit Dey; Jun Li; Pingna Deng; Emi Sei; Dean Y. Maeda; John A. Zebala; Denise J. Spring; Michael Kim; Huamin Wang; Anirban Maitra; Dirk Moore; Karen Clise-Dwyer; Y. Alan Wang; Nicholas E. Navin; Ronald A. DePinho

doi:10.1038/s43018-022-00500-z

Targeting T cell checkpoints 41BB and LAG3 and myeloid cell CXCR1/CXCR2 results in antitumor immunity and durable response in pancreatic cancer

Pat Gulhati, Aislyn Schalck, Shan Jiang, Xiaoying Shang, Chang Jiun Wu, Pingping Hou, Sharia Hernandez Ruiz, Luisa Solis Soto, Edwin Parra, Haoqiang Ying, Jincheng Han, Prasenjit Dey, Jun Li, Pingna Deng, Emi Sei, Dean Y. Maeda, John A. Zebala, Denise J. Spring, Michael Kim, Huamin WangAnirban Maitra, Dirk Moore, Karen Clise-Dwyer, Y. Alan Wang, Nicholas E. Navin, Ronald A. DePinho

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27 Scopus citations

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is considered non-immunogenic, with trials showing its recalcitrance to PD1 and CTLA4 immune checkpoint therapies (ICTs). Here, we sought to systematically characterize the mechanisms underlying de novo ICT resistance and to identify effective therapeutic options for PDAC. We report that agonist 41BB and antagonist LAG3 ICT alone and in combination, increased survival and antitumor immunity, characterized by modulating T cell subsets with antitumor activity, increased T cell clonality and diversification, decreased immunosuppressive myeloid cells and increased antigen presentation/decreased immunosuppressive capability of myeloid cells. Translational analyses confirmed the expression of 41BB and LAG3 in human PDAC. Since single and dual ICTs were not curative, T cell-activating ICTs were combined with a CXCR1/2 inhibitor targeting immunosuppressive myeloid cells. Triple therapy resulted in durable complete responses. Given similar profiles in human PDAC and the availability of these agents for clinical testing, our findings provide a testable hypothesis for this lethal disease.

Original language	English (US)
Pages (from-to)	62-80
Number of pages	19
Journal	Nature Cancer
Volume	4
Issue number	1
DOIs	https://doi.org/10.1038/s43018-022-00500-z
State	Published - Jan 2023

ASJC Scopus subject areas

Oncology
Cancer Research

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Gulhati, P., Schalck, A., Jiang, S., Shang, X., Wu, C. J., Hou, P., Ruiz, S. H., Soto, L. S., Parra, E., Ying, H., Han, J., Dey, P., Li, J., Deng, P., Sei, E., Maeda, D. Y., Zebala, J. A., Spring, D. J., Kim, M., ... DePinho, R. A. (2023). Targeting T cell checkpoints 41BB and LAG3 and myeloid cell CXCR1/CXCR2 results in antitumor immunity and durable response in pancreatic cancer. Nature Cancer, 4(1), 62-80. https://doi.org/10.1038/s43018-022-00500-z

Gulhati, P, Schalck, A, Jiang, S, Shang, X, Wu, CJ, Hou, P, Ruiz, SH , Soto, LS , Parra, E , Ying, H, Han, J, Dey, P, Li, J, Deng, P, Sei, E, Maeda, DY, Zebala, JA, Spring, DJ, Kim, M , Wang, H , Maitra, A, Moore, D, Clise-Dwyer, K, Wang, YA, Navin, NE & DePinho, RA 2023, 'Targeting T cell checkpoints 41BB and LAG3 and myeloid cell CXCR1/CXCR2 results in antitumor immunity and durable response in pancreatic cancer', Nature Cancer, vol. 4, no. 1, pp. 62-80. https://doi.org/10.1038/s43018-022-00500-z

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title = "Targeting T cell checkpoints 41BB and LAG3 and myeloid cell CXCR1/CXCR2 results in antitumor immunity and durable response in pancreatic cancer",

abstract = "Pancreatic ductal adenocarcinoma (PDAC) is considered non-immunogenic, with trials showing its recalcitrance to PD1 and CTLA4 immune checkpoint therapies (ICTs). Here, we sought to systematically characterize the mechanisms underlying de novo ICT resistance and to identify effective therapeutic options for PDAC. We report that agonist 41BB and antagonist LAG3 ICT alone and in combination, increased survival and antitumor immunity, characterized by modulating T cell subsets with antitumor activity, increased T cell clonality and diversification, decreased immunosuppressive myeloid cells and increased antigen presentation/decreased immunosuppressive capability of myeloid cells. Translational analyses confirmed the expression of 41BB and LAG3 in human PDAC. Since single and dual ICTs were not curative, T cell-activating ICTs were combined with a CXCR1/2 inhibitor targeting immunosuppressive myeloid cells. Triple therapy resulted in durable complete responses. Given similar profiles in human PDAC and the availability of these agents for clinical testing, our findings provide a testable hypothesis for this lethal disease.",

author = "Pat Gulhati and Aislyn Schalck and Shan Jiang and Xiaoying Shang and Wu, {Chang Jiun} and Pingping Hou and Ruiz, {Sharia Hernandez} and Soto, {Luisa Solis} and Edwin Parra and Haoqiang Ying and Jincheng Han and Prasenjit Dey and Jun Li and Pingna Deng and Emi Sei and Maeda, {Dean Y.} and Zebala, {John A.} and Spring, {Denise J.} and Michael Kim and Huamin Wang and Anirban Maitra and Dirk Moore and Karen Clise-Dwyer and Wang, {Y. Alan} and Navin, {Nicholas E.} and DePinho, {Ronald A.}",

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doi = "10.1038/s43018-022-00500-z",

language = "English (US)",

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AU - Gulhati, Pat

AU - Schalck, Aislyn

AU - Jiang, Shan

AU - Shang, Xiaoying

AU - Wu, Chang Jiun

AU - Hou, Pingping

AU - Ruiz, Sharia Hernandez

AU - Soto, Luisa Solis

AU - Parra, Edwin

AU - Ying, Haoqiang

AU - Han, Jincheng

AU - Dey, Prasenjit

AU - Li, Jun

AU - Deng, Pingna

AU - Sei, Emi

AU - Maeda, Dean Y.

AU - Zebala, John A.

AU - Spring, Denise J.

AU - Kim, Michael

AU - Wang, Huamin

AU - Maitra, Anirban

AU - Moore, Dirk

AU - Clise-Dwyer, Karen

AU - Wang, Y. Alan

AU - Navin, Nicholas E.

AU - DePinho, Ronald A.

PY - 2023/1

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N2 - Pancreatic ductal adenocarcinoma (PDAC) is considered non-immunogenic, with trials showing its recalcitrance to PD1 and CTLA4 immune checkpoint therapies (ICTs). Here, we sought to systematically characterize the mechanisms underlying de novo ICT resistance and to identify effective therapeutic options for PDAC. We report that agonist 41BB and antagonist LAG3 ICT alone and in combination, increased survival and antitumor immunity, characterized by modulating T cell subsets with antitumor activity, increased T cell clonality and diversification, decreased immunosuppressive myeloid cells and increased antigen presentation/decreased immunosuppressive capability of myeloid cells. Translational analyses confirmed the expression of 41BB and LAG3 in human PDAC. Since single and dual ICTs were not curative, T cell-activating ICTs were combined with a CXCR1/2 inhibitor targeting immunosuppressive myeloid cells. Triple therapy resulted in durable complete responses. Given similar profiles in human PDAC and the availability of these agents for clinical testing, our findings provide a testable hypothesis for this lethal disease.

AB - Pancreatic ductal adenocarcinoma (PDAC) is considered non-immunogenic, with trials showing its recalcitrance to PD1 and CTLA4 immune checkpoint therapies (ICTs). Here, we sought to systematically characterize the mechanisms underlying de novo ICT resistance and to identify effective therapeutic options for PDAC. We report that agonist 41BB and antagonist LAG3 ICT alone and in combination, increased survival and antitumor immunity, characterized by modulating T cell subsets with antitumor activity, increased T cell clonality and diversification, decreased immunosuppressive myeloid cells and increased antigen presentation/decreased immunosuppressive capability of myeloid cells. Translational analyses confirmed the expression of 41BB and LAG3 in human PDAC. Since single and dual ICTs were not curative, T cell-activating ICTs were combined with a CXCR1/2 inhibitor targeting immunosuppressive myeloid cells. Triple therapy resulted in durable complete responses. Given similar profiles in human PDAC and the availability of these agents for clinical testing, our findings provide a testable hypothesis for this lethal disease.

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Targeting T cell checkpoints 41BB and LAG3 and myeloid cell CXCR1/CXCR2 results in antitumor immunity and durable response in pancreatic cancer

Abstract

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MD Anderson CCSG core facilities

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