Neoantigen Immunogenicity Landscapes and Evolution of Tumor Ecosystems During Immunotherapy with Nivolumab

Overview

Journal Nat Med

Specialties General Medicine
Molecular Biology

Date 2024 Sep 30

PMID 39349627

Authors

Tyler J Alban

Nadeem Riaz

Prerana Parthasarathy

Vladimir Makarov

Sviatoslav Kendall

Seong-Keun Yoo

Rachna Shah

Nils Weinhold

Raghvendra Srivastava

Xiaoxiao Ma

Chirag Krishna

Juk Yee Mok

Wim J E van Esch

Edward Garon

Wallace Akerley

Benjamin Creelan

Nivedita Aanur

Diego Chowell

William J Geese

Naiyer A Rizvi

Timothy A Chan

Affiliations

Soon will be listed here.

Abstract

Neoantigen immunoediting drives immune checkpoint blockade efficacy, yet the molecular features of neoantigens and how neoantigen immunogenicity shapes treatment response remain poorly understood. To address these questions, 80 patients with non-small cell lung cancer were enrolled in the biomarker cohort of CheckMate 153 (CA209-153), which collected radiographic guided biopsy samples before treatment and during treatment with nivolumab. Early loss of mutations and neoantigens during therapy are both associated with clinical benefit. We examined 1,453 candidate neoantigens, including many of which that had reduced cancer cell fraction after treatment with nivolumab, and identified 196 neopeptides that were recognized by T cells. Mapping these neoantigens to clonal dynamics, evolutionary trajectories and clinical response revealed a strong selection against immunogenic neoantigen-harboring clones. We identified position-specific amino acid and physiochemical features related to immunogenicity and developed an immunogenicity score. Nivolumab-induced microenvironmental evolution in non-small cell lung cancer shared some similarities with melanoma, yet critical differences were apparent. This study provides unprecedented molecular portraits of neoantigen landscapes underlying nivolumab's mechanism of action.

Citing Articles

Dynamic profiling of immune microenvironment during anti-PD-1 immunotherapy for head and neck squamous cell carcinoma: the IPRICE study.

Helene C, Conrad O, Pflumio C, Borel C, Voegelin M, Bernard A BMC Cancer. 2023; 23(1):1209.

PMID: 38066522 PMC: 10704641. DOI: 10.1186/s12885-023-11672-x.

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