Preexisting Skin-Resident CD8 and γδ T-cell Circuits Mediate Immune Response in Merkel Cell Carcinoma and Predict Immunotherapy Efficacy.

Creator(s)

Zachary Z. Reinstein
Yue Zhang
Oscar E. Ospina
Matt D. Nichols
Victoria A. Chu
Alvaro de Mingo Pulido
Karol Prieto
Jonathan V. Nguyen
Rui Yin
Carlos Moran Segura
Ahmed Usman
Brittney Sell
Spencer Ng
Janis V. de la Iglesia
Sunandana Chandra
Jeffrey A. Sosman
Raymond J. Cho
Jeffrey B. Cheng
Ellie Ivanova
Sergei B. Koralov
Robbert J C Slebos
Christine H. Chung
Nikhil I. Khushalani
Jane L. Messina
Amod A. Sarnaik
Jonathan S. Zager
Vernon K. Sondak
Charles Vaske
Sungjune Kim
Andrew S. Brohl
Xinlei Mi
Brian G. Pierce
Xuefeng Wang
Brooke L. Fridley, Children's Mercy Kansas CityFollow
Kenneth Y. Tsai
Jaehyuk Choi

Document Type

Article

Publication Date

9-4-2024

Abstract

Merkel cell carcinoma (MCC) is an aggressive neuroendocrine skin cancer with a ∼50% response rate to immune checkpoint blockade (ICB) therapy. To identify predictive biomarkers, we integrated bulk and single-cell RNA sequencing (RNA-seq) with spatial transcriptomics from a cohort of 186 samples from 116 patients, including bulk RNA-seq from 14 matched pairs pre- and post-ICB. In nonresponders, tumors show evidence of increased tumor proliferation, neuronal stem cell markers, and IL1. Responders have increased type I/II interferons and preexisting tissue resident (Trm) CD8 or Vδ1 γδ T cells that functionally converge with overlapping antigen-specific transcriptional programs and clonal expansion of public T-cell receptors. Spatial transcriptomics demonstrated colocalization of T cells with B and dendritic cells, which supply chemokines and costimulation. Lastly, ICB significantly increased clonal expansion or recruitment of Trm and Vδ1 cells in tumors specifically in responders, underscoring their therapeutic importance. These data identify potential clinically actionable biomarkers and therapeutic targets for MCC. Significance: MCC serves as a model of ICB response. We utilized the largest-to-date, multimodal MCC dataset (n = 116 patients) to uncover unique tumor-intrinsic properties and immune circuits that predict response. We identified CD8 Trm and Vδ1 T cells as clinically actionable mediators of ICB response in major histocompatibility complex-high and -low MCCs, respectively.

Journal Title

Cancer Discov

Volume

14

Issue

9

First Page

1631

Last Page

1652

MeSH Keywords

Humans; Carcinoma, Merkel Cell; CD8-Positive T-Lymphocytes; Skin Neoplasms; Immunotherapy; Immune Checkpoint Inhibitors

Keywords

Carcinoma, Merkel Cell; CD8-Positive T-Lymphocytes; Skin Neoplasms; Immunotherapy; Immune Checkpoint Inhibitors

Comments

Grants and funding

• 2019 AOA Carolyn E Kuckein Fellowship/Alpha Omega Alpha Honor Medical Society (AOA)
• P30-CA076292/National Cancer Institute (NCI)
• T32 CA009560/CA/NCI NIH HHS/United States
• DP2 OD024475-01/National Cancer Institute (NCI)
• R35 GM144083/GM/NIGMS NIH HHS/United States
• 1377-21/Leukemia and Lymphoma Society (LLS)
• T2021-019/V Foundation for Cancer Research (VFCR)
• NCCN-YIA 2019/National Comprehensive Cancer Network
• T32CA233399/National Cancer Institute (NCI)

Recommended Citation

Reinstein ZZ, Zhang Y, Ospina OE, et al. Preexisting Skin-Resident CD8 and γδ T-cell Circuits Mediate Immune Response in Merkel Cell Carcinoma and Predict Immunotherapy Efficacy. Cancer Discov. 2024;14(9):1631-1652. doi:10.1158/2159-8290.CD-23-0798