Neoantigen responses, immune correlates, and favorable outcomes after ipilimumab treatment of patients with prostate cancer

Sumit K. Subudhi; Luis Vence; Hao Zhao; Jorge Blando; Shalini S. Yadav; Qing Xiong; Alexandre Reuben; Ana Aparicio; Paul G. Corn; Brian F. Chapin; Louis L. Pisters; Patricia Troncoso; Rebecca Slack Tidwell; Peter Thall; Chang Jiun Wu; Jianhua Zhang; Christopher L. Logothetis; Andrew Futreal; James P. Allison; Padmanee Sharma

doi:10.1126/scitranslmed.aaz3577

Neoantigen responses, immune correlates, and favorable outcomes after ipilimumab treatment of patients with prostate cancer

Sumit K. Subudhi, Luis Vence, Hao Zhao, Jorge Blando, Shalini S. Yadav, Qing Xiong, Alexandre Reuben, Ana Aparicio, Paul G. Corn, Brian F. Chapin, Louis L. Pisters, Patricia Troncoso, Rebecca Slack Tidwell, Peter Thall, Chang Jiun Wu, Jianhua Zhang, Christopher L. Logothetis, Andrew Futreal, James P. Allison, Padmanee Sharma

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102 Scopus citations

Abstract

Tumors with high mutational burden (TMB) tend to be responsive to immune checkpoint blockade (ICB) because there are neoantigens available for targeting by reinvigorated T cells, whereas those with low TMB demonstrate limited clinical responses. To determine whether antigen-specific T cell responses can be elicited after treatment with ICB in cancers that have a low TMB, we conducted a clinical trial with ipilimumab in 30 patients with metastatic castration-resistant prostate cancer. We identified two distinct cohorts by survival and progression times: “favorable” (n = 9) and “unfavorable” (n = 10). Patients in the favorable cohort had high intratumoral CD8 T cell density and IFN-γ response gene signature and/or antigen-specific T cell responses. Two patients with a relatively low TMB had T cell responses against unique neoantigens. Moreover, six of nine patients in the favorable group are still alive at the time of analysis, with survival ranging from 33 to 54 months after treatment. All 10 patients in the unfavorable cohort have succumbed to their disease and had survival ranging from 0.6 to 10.3 months. Collectively, our data indicate that immunological correlates associated with effector T cell responses are observed in patients with metastatic prostate cancer who benefit from ICB.

Original language	English (US)
Article number	eaaz3577
Journal	Science translational medicine
Volume	12
Issue number	537
DOIs	https://doi.org/10.1126/scitranslmed.aaz3577
State	Published - Apr 1 2020

ASJC Scopus subject areas

General Medicine

MD Anderson CCSG core facilities

Advanced Technology Genomics Core
Biostatistics Resource Group
Tissue Biospecimen and Pathology Resource
Clinical Trials Office

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Subudhi, S. K., Vence, L., Zhao, H., Blando, J., Yadav, S. S., Xiong, Q., Reuben, A., Aparicio, A., Corn, P. G., Chapin, B. F., Pisters, L. L., Troncoso, P., Tidwell, R. S., Thall, P., Wu, C. J., Zhang, J., Logothetis, C. L., Futreal, A., Allison, J. P., & Sharma, P. (2020). Neoantigen responses, immune correlates, and favorable outcomes after ipilimumab treatment of patients with prostate cancer. Science translational medicine, 12(537), Article eaaz3577. https://doi.org/10.1126/scitranslmed.aaz3577

Subudhi, SK, Vence, L, Zhao, H, Blando, J, Yadav, SS, Xiong, Q, Reuben, A , Aparicio, A , Corn, PG , Chapin, BF , Pisters, LL , Troncoso, P , Tidwell, RS , Thall, P, Wu, CJ, Zhang, J, Logothetis, CL , Futreal, A , Allison, JP & Sharma, P 2020, 'Neoantigen responses, immune correlates, and favorable outcomes after ipilimumab treatment of patients with prostate cancer', Science translational medicine, vol. 12, no. 537, eaaz3577. https://doi.org/10.1126/scitranslmed.aaz3577

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title = "Neoantigen responses, immune correlates, and favorable outcomes after ipilimumab treatment of patients with prostate cancer",

abstract = "Tumors with high mutational burden (TMB) tend to be responsive to immune checkpoint blockade (ICB) because there are neoantigens available for targeting by reinvigorated T cells, whereas those with low TMB demonstrate limited clinical responses. To determine whether antigen-specific T cell responses can be elicited after treatment with ICB in cancers that have a low TMB, we conducted a clinical trial with ipilimumab in 30 patients with metastatic castration-resistant prostate cancer. We identified two distinct cohorts by survival and progression times: “favorable” (n = 9) and “unfavorable” (n = 10). Patients in the favorable cohort had high intratumoral CD8 T cell density and IFN-γ response gene signature and/or antigen-specific T cell responses. Two patients with a relatively low TMB had T cell responses against unique neoantigens. Moreover, six of nine patients in the favorable group are still alive at the time of analysis, with survival ranging from 33 to 54 months after treatment. All 10 patients in the unfavorable cohort have succumbed to their disease and had survival ranging from 0.6 to 10.3 months. Collectively, our data indicate that immunological correlates associated with effector T cell responses are observed in patients with metastatic prostate cancer who benefit from ICB.",

author = "Subudhi, {Sumit K.} and Luis Vence and Hao Zhao and Jorge Blando and Yadav, {Shalini S.} and Qing Xiong and Alexandre Reuben and Ana Aparicio and Corn, {Paul G.} and Chapin, {Brian F.} and Pisters, {Louis L.} and Patricia Troncoso and Tidwell, {Rebecca Slack} and Peter Thall and Wu, {Chang Jiun} and Jianhua Zhang and Logothetis, {Christopher L.} and Andrew Futreal and Allison, {James P.} and Padmanee Sharma",

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doi = "10.1126/scitranslmed.aaz3577",

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AU - Subudhi, Sumit K.

AU - Vence, Luis

AU - Zhao, Hao

AU - Blando, Jorge

AU - Yadav, Shalini S.

AU - Xiong, Qing

AU - Reuben, Alexandre

AU - Aparicio, Ana

AU - Corn, Paul G.

AU - Chapin, Brian F.

AU - Pisters, Louis L.

AU - Troncoso, Patricia

AU - Tidwell, Rebecca Slack

AU - Thall, Peter

AU - Wu, Chang Jiun

AU - Zhang, Jianhua

AU - Logothetis, Christopher L.

AU - Futreal, Andrew

AU - Allison, James P.

AU - Sharma, Padmanee

PY - 2020/4/1

Y1 - 2020/4/1

N2 - Tumors with high mutational burden (TMB) tend to be responsive to immune checkpoint blockade (ICB) because there are neoantigens available for targeting by reinvigorated T cells, whereas those with low TMB demonstrate limited clinical responses. To determine whether antigen-specific T cell responses can be elicited after treatment with ICB in cancers that have a low TMB, we conducted a clinical trial with ipilimumab in 30 patients with metastatic castration-resistant prostate cancer. We identified two distinct cohorts by survival and progression times: “favorable” (n = 9) and “unfavorable” (n = 10). Patients in the favorable cohort had high intratumoral CD8 T cell density and IFN-γ response gene signature and/or antigen-specific T cell responses. Two patients with a relatively low TMB had T cell responses against unique neoantigens. Moreover, six of nine patients in the favorable group are still alive at the time of analysis, with survival ranging from 33 to 54 months after treatment. All 10 patients in the unfavorable cohort have succumbed to their disease and had survival ranging from 0.6 to 10.3 months. Collectively, our data indicate that immunological correlates associated with effector T cell responses are observed in patients with metastatic prostate cancer who benefit from ICB.

AB - Tumors with high mutational burden (TMB) tend to be responsive to immune checkpoint blockade (ICB) because there are neoantigens available for targeting by reinvigorated T cells, whereas those with low TMB demonstrate limited clinical responses. To determine whether antigen-specific T cell responses can be elicited after treatment with ICB in cancers that have a low TMB, we conducted a clinical trial with ipilimumab in 30 patients with metastatic castration-resistant prostate cancer. We identified two distinct cohorts by survival and progression times: “favorable” (n = 9) and “unfavorable” (n = 10). Patients in the favorable cohort had high intratumoral CD8 T cell density and IFN-γ response gene signature and/or antigen-specific T cell responses. Two patients with a relatively low TMB had T cell responses against unique neoantigens. Moreover, six of nine patients in the favorable group are still alive at the time of analysis, with survival ranging from 33 to 54 months after treatment. All 10 patients in the unfavorable cohort have succumbed to their disease and had survival ranging from 0.6 to 10.3 months. Collectively, our data indicate that immunological correlates associated with effector T cell responses are observed in patients with metastatic prostate cancer who benefit from ICB.

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Neoantigen responses, immune correlates, and favorable outcomes after ipilimumab treatment of patients with prostate cancer

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MD Anderson CCSG core facilities

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