Integrated Proteogenomic Deep Sequencing and Analytics Accurately Identify Non-canonical Peptides in Tumor Immunopeptidomes

Overview

Journal Nat Commun

Specialty Biology

Date 2020 Mar 12

PMID 32157095

Citations 145

Authors

Chloe Chong

Markus Muller

HuiSong Pak

Dermot Harnett

Florian Huber

Delphine Grun

Marion Leleu

Aymeric Auger

Marion Arnaud

Brian J Stevenson

Justine Michaux

Ilija Bilic

Antje Hirsekorn

Lorenzo Calviello

Laia Simo-Riudalbas

Evarist Planet

Jan Lubinski

Marta Bryskiewicz

Maciej Wiznerowicz

Ioannis Xenarios

Lin Zhang

Didier Trono

Alexandre Harari

Uwe Ohler

George Coukos

Michal Bassani-Sternberg

Affiliations

Soon will be listed here.

Abstract

Efforts to precisely identify tumor human leukocyte antigen (HLA) bound peptides capable of mediating T cell-based tumor rejection still face important challenges. Recent studies suggest that non-canonical tumor-specific HLA peptides derived from annotated non-coding regions could elicit anti-tumor immune responses. However, sensitive and accurate mass spectrometry (MS)-based proteogenomics approaches are required to robustly identify these non-canonical peptides. We present an MS-based analytical approach that characterizes the non-canonical tumor HLA peptide repertoire, by incorporating whole exome sequencing, bulk and single-cell transcriptomics, ribosome profiling, and two MS/MS search tools in combination. This approach results in the accurate identification of hundreds of shared and tumor-specific non-canonical HLA peptides, including an immunogenic peptide derived from an open reading frame downstream of the melanoma stem cell marker gene ABCB5. These findings hold great promise for the discovery of previously unknown tumor antigens for cancer immunotherapy.

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