Geospatial Immune Variability Illuminates Differential Evolution of Lung Adenocarcinoma

Overview

Journal Nat Med

Specialties General Medicine
Molecular Biology

Date 2020 May 29

PMID 32461698

Citations 108

Authors

Khalid AbdulJabbar

Shan E Ahmed Raza

Rachel Rosenthal

Mariam Jamal-Hanjani

Selvaraju Veeriah

Ayse Akarca

Tom Lund

David A Moore

Roberto Salgado

Maise Al Bakir

Luis Zapata

Crispin T Hiley

Leah Officer

Marco Sereno

Claire Rachel Smith

Sherene Loi

Allan Hackshaw

Teresa Marafioti

Sergio A Quezada

Nicholas McGranahan

John Le Quesne

Charles Swanton

Yinyin Yuan

Affiliations

Soon will be listed here.

Abstract

Remarkable progress in molecular analyses has improved our understanding of the evolution of cancer cells toward immune escape. However, the spatial configurations of immune and stromal cells, which may shed light on the evolution of immune escape across tumor geographical locations, remain unaddressed. We integrated multiregion exome and RNA-sequencing (RNA-seq) data with spatial histology mapped by deep learning in 100 patients with non-small cell lung cancer from the TRACERx cohort. Cancer subclones derived from immune cold regions were more closely related in mutation space, diversifying more recently than subclones from immune hot regions. In TRACERx and in an independent multisample cohort of 970 patients with lung adenocarcinoma, tumors with more than one immune cold region had a higher risk of relapse, independently of tumor size, stage and number of samples per patient. In lung adenocarcinoma, but not lung squamous cell carcinoma, geometrical irregularity and complexity of the cancer-stromal cell interface significantly increased in tumor regions without disruption of antigen presentation. Decreased lymphocyte accumulation in adjacent stroma was observed in tumors with low clonal neoantigen burden. Collectively, immune geospatial variability elucidates tumor ecological constraints that may shape the emergence of immune-evading subclones and aggressive clinical phenotypes.

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