Characterisation of Clinical Response and Transcriptional Profiling of Proliferating CD8 T Cells in the Blood of Cancer Patients After PD-1 Monotherapy or Combination Therapy

Overview

Journal BMJ Oncol

Date 2025 Jan 31

PMID 39886145

Authors

Rebecca C Obeng

Tahseen H Nasti

Kylee Martens

Peng Li

Annapaola Mariniello

Daniel Y Chang

Christiane S Eberhardt

Donald McGuire

Haydn Kissick

Candace Daugherty

Yuzi Zhang

Andreas Wieland

Zhengjia Chen

Jeffrey M Switchenko

Rathi Pillai

Alice O Kamphorst

Warren J Leonard

Rafi Ahmed

Suresh S Ramalingam

Affiliations

Soon will be listed here.

Abstract

Objective: Immune checkpoint inhibitors (ICI) that block the programmed cell death 1 (PD-1) pathway have shown promise with limited benefit. We and others have shown in small patient cohorts that an early proliferative CD8 T-cell response in the blood may be predictive of clinical response. However, these studies lack detailed analyses and comparisons between monotherapy and combination therapies.

Methods And Analysis: We analysed longitudinal blood samples from 103 patients with cancer who received αPD-1 monotherapy or combined with anti-cytotoxic T lymphocyte-associated protein 4 (αCTLA-4) or chemotherapy. Transcriptional analysis of CD8 T cells after the first treatment cycle with effector cells generated following yellow fever virus (YFV-17D) vaccine-induced infection was also compared.

Results: An early proliferative (Ki-67) CD8 T-cell response was observed after cycle 1 in 60 patients (58.3%). Patients with early-and-sustained proliferative responses (cycle 1 and beyond) had better clinical responses and survival than patients with an early-but-limited response (p=0.02). The proliferating cells had an effector-like phenotype. The transcriptional profiles of the effector-like CD8 T cells were similar irrespective of treatment type or clinical response but distinct from that of YFV-specific effector CD8 T cells.

Conclusions: Our data suggest that early proliferative CD8 T-cell response in the blood is predictive, and that an early-and-sustained proliferative response may further identify patients with prolonged survival. The ICI-induced effector-like CD8 T cells are transcriptionally distinct from highly functional YFV-specific cells, suggesting opportunities for improved T-cell effector function with combination therapies for better clinical outcome.

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