Combined Analysis of Antigen Presentation and T-cell Recognition Reveals Restricted Immune Responses in Melanoma

Shelly Kalaora; Yochai Wolf; Tali Feferman; Eilon Barnea; Erez Greenstein; Dan Reshef; Itay Tirosh; Alexandre Reuben; Sushant Patkar; Ronen Levy; Juliane Quinkhardt; Tana Omokoko; Nouar Qutob; Ofra Golani; Jianhua Zhang; Xizeng Mao; Xingzhi Song; Chantale Bernatchez; Cara Haymaker; Marie-Andree Forget; Caitlin Creasy; Polina Greenberg; Brett W. Carter; Zachary A. Cooper; Steven A. Rosenberg; Michal Lotem; Ugur Sahin; Guy Shakhar; Eytan Ruppin; Jennifer A. Wargo; Nir Friedman; Arie Admon; Yardena Samuels

doi:10.1158/2159-8290.CD-17-1418

Combined Analysis of Antigen Presentation and T-cell Recognition Reveals Restricted Immune Responses in Melanoma

Shelly Kalaora, Yochai Wolf, Tali Feferman, Eilon Barnea, Erez Greenstein, Dan Reshef, Itay Tirosh, Alexandre Reuben, Sushant Patkar, Ronen Levy, Juliane Quinkhardt, Tana Omokoko, Nouar Qutob, Ofra Golani, Jianhua Zhang, Xizeng Mao, Xingzhi Song, Chantale Bernatchez, Cara Haymaker, Marie-Andree ForgetCaitlin Creasy, Polina Greenberg, Brett W. Carter, Zachary A. Cooper, Steven A. Rosenberg, Michal Lotem, Ugur Sahin, Guy Shakhar, Eytan Ruppin, Jennifer A. Wargo, Nir Friedman, Arie Admon, Yardena Samuels

Weizmann Institute of Science, Technion - Israel Institute of Technology

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

Abstract

The quest for tumor-associated antigens (TAA) and neoantigens is a major focus of cancer immunotherapy. Here, we combine a neoantigen prediction pipeline and human leukocyte antigen (HLA) peptidomics to identify TAAs and neoantigens in 16 tumors derived from seven patients with melanoma and characterize their interactions with their tumor-infiltrating lymphocytes (TIL). Our investigation of the antigenic and T-cell landscapes encompassing the TAA and neoantigen signatures, their immune reactivity, and their corresponding T-cell identities provides the first comprehensive analysis of cancer cell T-cell cosignatures, allowing us to discover remarkable antigenic and TIL similarities between metastases from the same patient. Furthermore, we reveal that two neoantigen-specific clonotypes killed 90% of autologous melanoma cells, both in vitro and in vivo, showing that a limited set of neoantigen-specific T cells may play a central role in melanoma tumor rejection. Our findings indicate that combining HLA peptidomics with neoantigen predictions allows robust identification of targetable neoantigens, which could successfully guide personalized cancer immunotherapies.

SIGNIFICANCE: As neoantigen targeting is becoming more established as a powerful therapeutic approach, investigating these molecules has taken center stage. Here, we show that a limited set of neoantigen-specific T cells mediates tumor rejection, suggesting that identifying just a few antigens and their corresponding T-cell clones could guide personalized immunotherapy. (c) 2018 AACR.

Original language	English
Pages (from-to)	1366-1375
Number of pages	10
Journal	Cancer Discovery
Volume	8
Issue number	11
DOIs	https://doi.org/10.1158/2159-8290.CD-17-1418
State	Published - Nov 2018

UN SDGs

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

SDG 3 Good Health and Well-being

All Science Journal Classification (ASJC) codes

Oncology

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Kalaora, S., Wolf, Y., Feferman, T., Barnea, E., Greenstein, E., Reshef, D., Tirosh, I., Reuben, A., Patkar, S., Levy, R., Quinkhardt, J., Omokoko, T., Qutob, N., Golani, O., Zhang, J., Mao, X., Song, X., Bernatchez, C., Haymaker, C., ... Samuels, Y. (2018). Combined Analysis of Antigen Presentation and T-cell Recognition Reveals Restricted Immune Responses in Melanoma. Cancer Discovery, 8(11), 1366-1375. https://doi.org/10.1158/2159-8290.CD-17-1418

@article{8036906c42614df4bbafa533a4deb292,

title = "Combined Analysis of Antigen Presentation and T-cell Recognition Reveals Restricted Immune Responses in Melanoma",

abstract = "The quest for tumor-associated antigens (TAA) and neoantigens is a major focus of cancer immunotherapy. Here, we combine a neoantigen prediction pipeline and human leukocyte antigen (HLA) peptidomics to identify TAAs and neoantigens in 16 tumors derived from seven patients with melanoma and characterize their interactions with their tumor-infiltrating lymphocytes (TIL). Our investigation of the antigenic and T-cell landscapes encompassing the TAA and neoantigen signatures, their immune reactivity, and their corresponding T-cell identities provides the first comprehensive analysis of cancer cell T-cell cosignatures, allowing us to discover remarkable antigenic and TIL similarities between metastases from the same patient. Furthermore, we reveal that two neoantigen-specific clonotypes killed 90\% of autologous melanoma cells, both in vitro and in vivo, showing that a limited set of neoantigen-specific T cells may play a central role in melanoma tumor rejection. Our findings indicate that combining HLA peptidomics with neoantigen predictions allows robust identification of targetable neoantigens, which could successfully guide personalized cancer immunotherapies.SIGNIFICANCE: As neoantigen targeting is becoming more established as a powerful therapeutic approach, investigating these molecules has taken center stage. Here, we show that a limited set of neoantigen-specific T cells mediates tumor rejection, suggesting that identifying just a few antigens and their corresponding T-cell clones could guide personalized immunotherapy. (c) 2018 AACR.",

author = "Shelly Kalaora and Yochai Wolf and Tali Feferman and Eilon Barnea and Erez Greenstein and Dan Reshef and Itay Tirosh and Alexandre Reuben and Sushant Patkar and Ronen Levy and Juliane Quinkhardt and Tana Omokoko and Nouar Qutob and Ofra Golani and Jianhua Zhang and Xizeng Mao and Xingzhi Song and Chantale Bernatchez and Cara Haymaker and Marie-Andree Forget and Caitlin Creasy and Polina Greenberg and Carter, \{Brett W.\} and Cooper, \{Zachary A.\} and Rosenberg, \{Steven A.\} and Michal Lotem and Ugur Sahin and Guy Shakhar and Eytan Ruppin and Wargo, \{Jennifer A.\} and Nir Friedman and Arie Admon and Yardena Samuels",

note = "Publisher Copyright: {\textcopyright}2018 American Association for Cancer Research.",

year = "2018",

month = nov,

doi = "10.1158/2159-8290.CD-17-1418",

language = "الإنجليزيّة",

volume = "8",

pages = "1366--1375",

journal = "Cancer Discovery",

issn = "2159-8274",

publisher = "John Wiley and Sons Inc.",

number = "11",

}

Kalaora, S, Wolf, Y, Feferman, T, Barnea, E, Greenstein, E, Reshef, D, Tirosh, I, Reuben, A, Patkar, S, Levy, R, Quinkhardt, J, Omokoko, T, Qutob, N, Golani, O, Zhang, J, Mao, X, Song, X, Bernatchez, C, Haymaker, C, Forget, M-A, Creasy, C, Greenberg, P, Carter, BW, Cooper, ZA, Rosenberg, SA, Lotem, M, Sahin, U, Shakhar, G, Ruppin, E, Wargo, JA, Friedman, N, Admon, A & Samuels, Y 2018, 'Combined Analysis of Antigen Presentation and T-cell Recognition Reveals Restricted Immune Responses in Melanoma', Cancer Discovery, vol. 8, no. 11, pp. 1366-1375. https://doi.org/10.1158/2159-8290.CD-17-1418

TY - JOUR

T1 - Combined Analysis of Antigen Presentation and T-cell Recognition Reveals Restricted Immune Responses in Melanoma

AU - Kalaora, Shelly

AU - Wolf, Yochai

AU - Feferman, Tali

AU - Barnea, Eilon

AU - Greenstein, Erez

AU - Reshef, Dan

AU - Tirosh, Itay

AU - Reuben, Alexandre

AU - Patkar, Sushant

AU - Levy, Ronen

AU - Quinkhardt, Juliane

AU - Omokoko, Tana

AU - Qutob, Nouar

AU - Golani, Ofra

AU - Zhang, Jianhua

AU - Mao, Xizeng

AU - Song, Xingzhi

AU - Bernatchez, Chantale

AU - Haymaker, Cara

AU - Forget, Marie-Andree

AU - Creasy, Caitlin

AU - Greenberg, Polina

AU - Carter, Brett W.

AU - Cooper, Zachary A.

AU - Rosenberg, Steven A.

AU - Lotem, Michal

AU - Sahin, Ugur

AU - Shakhar, Guy

AU - Ruppin, Eytan

AU - Wargo, Jennifer A.

AU - Friedman, Nir

AU - Admon, Arie

AU - Samuels, Yardena

PY - 2018/11

Y1 - 2018/11

N2 - The quest for tumor-associated antigens (TAA) and neoantigens is a major focus of cancer immunotherapy. Here, we combine a neoantigen prediction pipeline and human leukocyte antigen (HLA) peptidomics to identify TAAs and neoantigens in 16 tumors derived from seven patients with melanoma and characterize their interactions with their tumor-infiltrating lymphocytes (TIL). Our investigation of the antigenic and T-cell landscapes encompassing the TAA and neoantigen signatures, their immune reactivity, and their corresponding T-cell identities provides the first comprehensive analysis of cancer cell T-cell cosignatures, allowing us to discover remarkable antigenic and TIL similarities between metastases from the same patient. Furthermore, we reveal that two neoantigen-specific clonotypes killed 90% of autologous melanoma cells, both in vitro and in vivo, showing that a limited set of neoantigen-specific T cells may play a central role in melanoma tumor rejection. Our findings indicate that combining HLA peptidomics with neoantigen predictions allows robust identification of targetable neoantigens, which could successfully guide personalized cancer immunotherapies.SIGNIFICANCE: As neoantigen targeting is becoming more established as a powerful therapeutic approach, investigating these molecules has taken center stage. Here, we show that a limited set of neoantigen-specific T cells mediates tumor rejection, suggesting that identifying just a few antigens and their corresponding T-cell clones could guide personalized immunotherapy. (c) 2018 AACR.

AB - The quest for tumor-associated antigens (TAA) and neoantigens is a major focus of cancer immunotherapy. Here, we combine a neoantigen prediction pipeline and human leukocyte antigen (HLA) peptidomics to identify TAAs and neoantigens in 16 tumors derived from seven patients with melanoma and characterize their interactions with their tumor-infiltrating lymphocytes (TIL). Our investigation of the antigenic and T-cell landscapes encompassing the TAA and neoantigen signatures, their immune reactivity, and their corresponding T-cell identities provides the first comprehensive analysis of cancer cell T-cell cosignatures, allowing us to discover remarkable antigenic and TIL similarities between metastases from the same patient. Furthermore, we reveal that two neoantigen-specific clonotypes killed 90% of autologous melanoma cells, both in vitro and in vivo, showing that a limited set of neoantigen-specific T cells may play a central role in melanoma tumor rejection. Our findings indicate that combining HLA peptidomics with neoantigen predictions allows robust identification of targetable neoantigens, which could successfully guide personalized cancer immunotherapies.SIGNIFICANCE: As neoantigen targeting is becoming more established as a powerful therapeutic approach, investigating these molecules has taken center stage. Here, we show that a limited set of neoantigen-specific T cells mediates tumor rejection, suggesting that identifying just a few antigens and their corresponding T-cell clones could guide personalized immunotherapy. (c) 2018 AACR.

UR - http://www.scopus.com/inward/record.url?scp=85055912571&partnerID=8YFLogxK

U2 - 10.1158/2159-8290.CD-17-1418

DO - 10.1158/2159-8290.CD-17-1418

M3 - مقالة

SN - 2159-8274

VL - 8

SP - 1366

EP - 1375

JO - Cancer Discovery

JF - Cancer Discovery

IS - 11

ER -

Combined Analysis of Antigen Presentation and T-cell Recognition Reveals Restricted Immune Responses in Melanoma

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