Memory T cells targeting oncogenic mutations detected in peripheral blood of epithelial cancer patients

Gal Cafri; Rami Yossef; Anna Pasetto; Drew C. Deniger; Yong Chen Lu; Maria Parkhurst; Jared J. Gartner; Li Jia; Satyajit Ray; Lien T. Ngo; Mohammad Jafferji; Abraham Sachs; Todd Prickett; Paul F. Robbins; Steven A. Rosenberg

doi:10.1038/s41467-019-08304-z

Memory T cells targeting oncogenic mutations detected in peripheral blood of epithelial cancer patients

Gal Cafri
, Rami Yossef
, Anna Pasetto
, Drew C. Deniger
, Yong Chen Lu
, Maria Parkhurst
, Jared J. Gartner
, Li Jia
, Satyajit Ray
, Lien T. Ngo
, Mohammad Jafferji
, Abraham Sachs
, Todd Prickett
, Paul F. Robbins
, Steven A. Rosenberg

Research output: Contribution to journal › Article › peer-review

148 Scopus citations

Abstract

T cells targeting shared oncogenic mutations can induce durable tumor regression in epithelial cancer patients. Such T cells can be detected in tumor infiltrating lymphocytes, but whether such cells can be detected in the peripheral blood of patients with the common metastatic epithelial cancer patients is unknown. Using a highly sensitive in vitro stimulation and cell enrichment of peripheral memory T cells from six metastatic cancer patients, we identified and isolated CD4⁺, and CD8⁺ memory T cells targeting the mutated KRAS^G12D and KRAS^G12V variants, respectively, in three patients. In an additional two metastatic colon cancer patients, we detected CD8⁺ neoantigen-specific cells targeting the mutated SMAD5 and MUC4 proteins. Therefore, memory T cells targeting unique as well as shared somatic mutations can be detected in the peripheral blood of epithelial cancer patients and can potentially be used for the development of effective personalized T cell-based cancer immunotherapy across multiple patients.

Original language	English
Article number	449
Journal	Nature Communications
Volume	10
Issue number	1
DOIs	https://doi.org/10.1038/s41467-019-08304-z
State	Published - 1 Dec 2019
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

ASJC Scopus subject areas

General Chemistry
General Biochemistry, Genetics and Molecular Biology
General
General Physics and Astronomy

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10.1038/s41467-019-08304-z

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Cafri, G., Yossef, R., Pasetto, A., Deniger, D. C., Lu, Y. C., Parkhurst, M., Gartner, J. J., Jia, L., Ray, S., Ngo, L. T., Jafferji, M., Sachs, A., Prickett, T., Robbins, P. F., & Rosenberg, S. A. (2019). Memory T cells targeting oncogenic mutations detected in peripheral blood of epithelial cancer patients. Nature Communications, 10(1), Article 449. https://doi.org/10.1038/s41467-019-08304-z

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title = "Memory T cells targeting oncogenic mutations detected in peripheral blood of epithelial cancer patients",

abstract = "T cells targeting shared oncogenic mutations can induce durable tumor regression in epithelial cancer patients. Such T cells can be detected in tumor infiltrating lymphocytes, but whether such cells can be detected in the peripheral blood of patients with the common metastatic epithelial cancer patients is unknown. Using a highly sensitive in vitro stimulation and cell enrichment of peripheral memory T cells from six metastatic cancer patients, we identified and isolated CD4+, and CD8+ memory T cells targeting the mutated KRASG12D and KRASG12V variants, respectively, in three patients. In an additional two metastatic colon cancer patients, we detected CD8+ neoantigen-specific cells targeting the mutated SMAD5 and MUC4 proteins. Therefore, memory T cells targeting unique as well as shared somatic mutations can be detected in the peripheral blood of epithelial cancer patients and can potentially be used for the development of effective personalized T cell-based cancer immunotherapy across multiple patients.",

author = "Gal Cafri and Rami Yossef and Anna Pasetto and Deniger, \{Drew C.\} and Lu, \{Yong Chen\} and Maria Parkhurst and Gartner, \{Jared J.\} and Li Jia and Satyajit Ray and Ngo, \{Lien T.\} and Mohammad Jafferji and Abraham Sachs and Todd Prickett and Robbins, \{Paul F.\} and Rosenberg, \{Steven A.\}",

note = "Publisher Copyright: {\textcopyright} 2019, This is a U.S. Government work and not under copyright protection in the US; foreign copyright protection may apply.",

year = "2019",

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doi = "10.1038/s41467-019-08304-z",

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AU - Cafri, Gal

AU - Yossef, Rami

AU - Pasetto, Anna

AU - Deniger, Drew C.

AU - Lu, Yong Chen

AU - Parkhurst, Maria

AU - Gartner, Jared J.

AU - Jia, Li

AU - Ray, Satyajit

AU - Ngo, Lien T.

AU - Jafferji, Mohammad

AU - Sachs, Abraham

AU - Prickett, Todd

AU - Robbins, Paul F.

AU - Rosenberg, Steven A.

PY - 2019/12/1

Y1 - 2019/12/1

N2 - T cells targeting shared oncogenic mutations can induce durable tumor regression in epithelial cancer patients. Such T cells can be detected in tumor infiltrating lymphocytes, but whether such cells can be detected in the peripheral blood of patients with the common metastatic epithelial cancer patients is unknown. Using a highly sensitive in vitro stimulation and cell enrichment of peripheral memory T cells from six metastatic cancer patients, we identified and isolated CD4+, and CD8+ memory T cells targeting the mutated KRASG12D and KRASG12V variants, respectively, in three patients. In an additional two metastatic colon cancer patients, we detected CD8+ neoantigen-specific cells targeting the mutated SMAD5 and MUC4 proteins. Therefore, memory T cells targeting unique as well as shared somatic mutations can be detected in the peripheral blood of epithelial cancer patients and can potentially be used for the development of effective personalized T cell-based cancer immunotherapy across multiple patients.

AB - T cells targeting shared oncogenic mutations can induce durable tumor regression in epithelial cancer patients. Such T cells can be detected in tumor infiltrating lymphocytes, but whether such cells can be detected in the peripheral blood of patients with the common metastatic epithelial cancer patients is unknown. Using a highly sensitive in vitro stimulation and cell enrichment of peripheral memory T cells from six metastatic cancer patients, we identified and isolated CD4+, and CD8+ memory T cells targeting the mutated KRASG12D and KRASG12V variants, respectively, in three patients. In an additional two metastatic colon cancer patients, we detected CD8+ neoantigen-specific cells targeting the mutated SMAD5 and MUC4 proteins. Therefore, memory T cells targeting unique as well as shared somatic mutations can be detected in the peripheral blood of epithelial cancer patients and can potentially be used for the development of effective personalized T cell-based cancer immunotherapy across multiple patients.

UR - https://www.scopus.com/pages/publications/85060555999

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JO - Nature Communications

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M1 - 449

ER -

Memory T cells targeting oncogenic mutations detected in peripheral blood of epithelial cancer patients

Abstract

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ASJC Scopus subject areas

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