mRNA vaccine–induced neoantigen-specific T cell immunity in patients with gastrointestinal cancer

Gal Cafri; Jared J. Gartner; Tal Zaks; Kristen Hopson; Noam Levin; Biman C. Paria; Maria R. Parkhurst; Rami Yossef; Frank J. Lowery; Mohammad S. Jafferji; Todd D. Prickett; Stephanie L. Goff; Christine T. McGowan; Samantha Seitter; Mackenzie L. Shindorf; Anup Parikh; Praveen D. Chatani; Paul F. Robbins; Steven A. Rosenberg

doi:10.1172/JCI134915

mRNA vaccine–induced neoantigen-specific T cell immunity in patients with gastrointestinal cancer

Gal Cafri
, Jared J. Gartner
, Tal Zaks
, Kristen Hopson
, Noam Levin
, Biman C. Paria
, Maria R. Parkhurst
, Rami Yossef
, Frank J. Lowery
, Mohammad S. Jafferji
, Todd D. Prickett
, Stephanie L. Goff
, Christine T. McGowan
, Samantha Seitter
, Mackenzie L. Shindorf
, Anup Parikh
, Praveen D. Chatani
, Paul F. Robbins
, Steven A. Rosenberg

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

371 Scopus citations

Abstract

BACKGROUND. Therapeutic vaccinations against cancer have mainly targeted differentiation antigens, cancer-testis antigens, and overexpressed antigens and have thus far resulted in little clinical benefit. Studies conducted by multiple groups have demonstrated that T cells recognizing neoantigens are present in most cancers and offer a specific and highly immunogenic target for personalized vaccination. METHODS. We recently developed a process using tumor-infiltrating lymphocytes to identify the specific immunogenic mutations expressed in patients’ tumors. Here, validated, defined neoantigens, predicted neoepitopes, and mutations of driver genes were concatenated into a single mRNA construct to vaccinate patients with metastatic gastrointestinal cancer. RESULTS. The vaccine was safe and elicited mutation-specific T cell responses against predicted neoepitopes not detected before vaccination. Furthermore, we were able to isolate and verify T cell receptors targeting KRAS^G12D mutation. We observed no objective clinical responses in the 4 patients treated in this trial. CONCLUSION. This vaccine was safe, and potential future combination of such vaccines with checkpoint inhibitors or adoptive T cell therapy should be evaluated for possible clinical benefit in patients with common epithelial cancers.

Original language	English
Pages (from-to)	5976-5988
Number of pages	13
Journal	Journal of Clinical Investigation
Volume	130
Issue number	11
DOIs	https://doi.org/10.1172/JCI134915
State	Published - 2 Nov 2020
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 Medicine

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10.1172/JCI134915

Cite this

Cafri, G., Gartner, J. J., Zaks, T., Hopson, K., Levin, N., Paria, B. C., Parkhurst, M. R., Yossef, R., Lowery, F. J., Jafferji, M. S., Prickett, T. D., Goff, S. L., McGowan, C. T., Seitter, S., Shindorf, M. L., Parikh, A., Chatani, P. D., Robbins, P. F., & Rosenberg, S. A. (2020). mRNA vaccine–induced neoantigen-specific T cell immunity in patients with gastrointestinal cancer. Journal of Clinical Investigation, 130(11), 5976-5988. https://doi.org/10.1172/JCI134915

@article{2e25ec7274a14427a4932b0612543102,

title = "mRNA vaccine–induced neoantigen-specific T cell immunity in patients with gastrointestinal cancer",

abstract = "BACKGROUND. Therapeutic vaccinations against cancer have mainly targeted differentiation antigens, cancer-testis antigens, and overexpressed antigens and have thus far resulted in little clinical benefit. Studies conducted by multiple groups have demonstrated that T cells recognizing neoantigens are present in most cancers and offer a specific and highly immunogenic target for personalized vaccination. METHODS. We recently developed a process using tumor-infiltrating lymphocytes to identify the specific immunogenic mutations expressed in patients{\textquoteright} tumors. Here, validated, defined neoantigens, predicted neoepitopes, and mutations of driver genes were concatenated into a single mRNA construct to vaccinate patients with metastatic gastrointestinal cancer. RESULTS. The vaccine was safe and elicited mutation-specific T cell responses against predicted neoepitopes not detected before vaccination. Furthermore, we were able to isolate and verify T cell receptors targeting KRASG12D mutation. We observed no objective clinical responses in the 4 patients treated in this trial. CONCLUSION. This vaccine was safe, and potential future combination of such vaccines with checkpoint inhibitors or adoptive T cell therapy should be evaluated for possible clinical benefit in patients with common epithelial cancers.",

author = "Gal Cafri and Gartner, \{Jared J.\} and Tal Zaks and Kristen Hopson and Noam Levin and Paria, \{Biman C.\} and Parkhurst, \{Maria R.\} and Rami Yossef and Lowery, \{Frank J.\} and Jafferji, \{Mohammad S.\} and Prickett, \{Todd D.\} and Goff, \{Stephanie L.\} and McGowan, \{Christine T.\} and Samantha Seitter and Shindorf, \{Mackenzie L.\} and Anup Parikh and Chatani, \{Praveen D.\} and Robbins, \{Paul F.\} and Rosenberg, \{Steven A.\}",

note = "Publisher Copyright: Copyright: {\textcopyright} 2020, American Society for Clinical Investigation.",

year = "2020",

month = nov,

day = "2",

doi = "10.1172/JCI134915",

language = "English",

volume = "130",

pages = "5976--5988",

journal = "Journal of Clinical Investigation",

issn = "0021-9738",

publisher = "American Society for Clinical Investigation",

number = "11",

}

Cafri, G, Gartner, JJ, Zaks, T, Hopson, K, Levin, N, Paria, BC, Parkhurst, MR, Yossef, R, Lowery, FJ, Jafferji, MS, Prickett, TD, Goff, SL, McGowan, CT, Seitter, S, Shindorf, ML, Parikh, A, Chatani, PD, Robbins, PF & Rosenberg, SA 2020, 'mRNA vaccine–induced neoantigen-specific T cell immunity in patients with gastrointestinal cancer', Journal of Clinical Investigation, vol. 130, no. 11, pp. 5976-5988. https://doi.org/10.1172/JCI134915

TY - JOUR

T1 - mRNA vaccine–induced neoantigen-specific T cell immunity in patients with gastrointestinal cancer

AU - Cafri, Gal

AU - Gartner, Jared J.

AU - Zaks, Tal

AU - Hopson, Kristen

AU - Levin, Noam

AU - Paria, Biman C.

AU - Parkhurst, Maria R.

AU - Yossef, Rami

AU - Lowery, Frank J.

AU - Jafferji, Mohammad S.

AU - Prickett, Todd D.

AU - Goff, Stephanie L.

AU - McGowan, Christine T.

AU - Seitter, Samantha

AU - Shindorf, Mackenzie L.

AU - Parikh, Anup

AU - Chatani, Praveen D.

AU - Robbins, Paul F.

AU - Rosenberg, Steven A.

PY - 2020/11/2

Y1 - 2020/11/2

N2 - BACKGROUND. Therapeutic vaccinations against cancer have mainly targeted differentiation antigens, cancer-testis antigens, and overexpressed antigens and have thus far resulted in little clinical benefit. Studies conducted by multiple groups have demonstrated that T cells recognizing neoantigens are present in most cancers and offer a specific and highly immunogenic target for personalized vaccination. METHODS. We recently developed a process using tumor-infiltrating lymphocytes to identify the specific immunogenic mutations expressed in patients’ tumors. Here, validated, defined neoantigens, predicted neoepitopes, and mutations of driver genes were concatenated into a single mRNA construct to vaccinate patients with metastatic gastrointestinal cancer. RESULTS. The vaccine was safe and elicited mutation-specific T cell responses against predicted neoepitopes not detected before vaccination. Furthermore, we were able to isolate and verify T cell receptors targeting KRASG12D mutation. We observed no objective clinical responses in the 4 patients treated in this trial. CONCLUSION. This vaccine was safe, and potential future combination of such vaccines with checkpoint inhibitors or adoptive T cell therapy should be evaluated for possible clinical benefit in patients with common epithelial cancers.

AB - BACKGROUND. Therapeutic vaccinations against cancer have mainly targeted differentiation antigens, cancer-testis antigens, and overexpressed antigens and have thus far resulted in little clinical benefit. Studies conducted by multiple groups have demonstrated that T cells recognizing neoantigens are present in most cancers and offer a specific and highly immunogenic target for personalized vaccination. METHODS. We recently developed a process using tumor-infiltrating lymphocytes to identify the specific immunogenic mutations expressed in patients’ tumors. Here, validated, defined neoantigens, predicted neoepitopes, and mutations of driver genes were concatenated into a single mRNA construct to vaccinate patients with metastatic gastrointestinal cancer. RESULTS. The vaccine was safe and elicited mutation-specific T cell responses against predicted neoepitopes not detected before vaccination. Furthermore, we were able to isolate and verify T cell receptors targeting KRASG12D mutation. We observed no objective clinical responses in the 4 patients treated in this trial. CONCLUSION. This vaccine was safe, and potential future combination of such vaccines with checkpoint inhibitors or adoptive T cell therapy should be evaluated for possible clinical benefit in patients with common epithelial cancers.

UR - https://www.scopus.com/pages/publications/85094955425

U2 - 10.1172/JCI134915

DO - 10.1172/JCI134915

M3 - Article

C2 - 33016924

AN - SCOPUS:85094955425

SN - 0021-9738

VL - 130

SP - 5976

EP - 5988

JO - Journal of Clinical Investigation

JF - Journal of Clinical Investigation

IS - 11

ER -

mRNA vaccine–induced neoantigen-specific T cell immunity in patients with gastrointestinal cancer

Abstract

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ASJC Scopus subject areas

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