Genomic-Transcriptomic Evolution in Lung Cancer and Metastasis

Authors

Carlos Martínez-Ruiz
James R M Black
Clare Puttick
Mark S Hill
Jonas Demeulemeester
Elizabeth Larose Cadieux
Kerstin Thol
Thomas P Jones
Selvaraju Veeriah
Cristina Naceur-Lombardelli
Antonia Toncheva
Paulina Prymas
Andrew Rowan
Sophia Ward
Laura Cubitt
Foteini Athanasopoulou
Oriol Pich
Takahiro Karasaki
David A Moore
Roberto Salgado
Emma Colliver
Carla Castignani
Michelle Dietzen
Ariana Huebner
Maise Al Bakir
Miljana Tanić
Thomas B K Watkins
Emilia L Lim
Ali M Al-Rashed
Danny Lang
James Clements
Daniel E Cook
Rachel Rosenthal
Gareth A Wilson
Alexander M Frankell
Sophie de Carné Trécesson
Philip East
Nnennaya Kanu
Kevin Litchfield
Nicolai J Birkbak
Allan Hackshaw
Stephan Beck
Peter Van Loo
Mariam Jamal-Hanjani
Charles Swanton
Nicholas McGranahan

Publication Date

4-1-2023

Journal

Nature

Abstract

Intratumour heterogeneity (ITH) fuels lung cancer evolution, which leads to immune evasion and resistance to therapy1. Here, using paired whole-exome and RNA sequencing data, we investigate intratumour transcriptomic diversity in 354 non-small cell lung cancer tumours from 347 out of the first 421 patients prospectively recruited into the TRACERx study2,3. Analyses of 947 tumour regions, representing both primary and metastatic disease, alongside 96 tumour-adjacent normal tissue samples implicate the transcriptome as a major source of phenotypic variation. Gene expression levels and ITH relate to patterns of positive and negative selection during tumour evolution. We observe frequent copy number-independent allele-specific expression that is linked to epigenomic dysfunction. Allele-specific expression can also result in genomic-transcriptomic parallel evolution, which converges on cancer gene disruption. We extract signatures of RNA single-base substitutions and link their aetiology to the activity of the RNA-editing enzymes ADAR and APOBEC3A, thereby revealing otherwise undetected ongoing APOBEC activity in tumours. Characterizing the transcriptomes of primary-metastatic tumour pairs, we combine multiple machine-learning approaches that leverage genomic and transcriptomic variables to link metastasis-seeding potential to the evolutionary context of mutations and increased proliferation within primary tumour regions. These results highlight the interplay between the genome and transcriptome in influencing ITH, lung cancer evolution and metastasis.

Keywords

Humans, Carcinoma, Non-Small-Cell Lung, Genomics, Lung Neoplasms, Mutation, Neoplasm Metastasis, Transcriptome, Evolution, Molecular, Alleles, Machine Learning, Genome, Human, Cancer genomics, Non-small-cell lung cancer, Transcriptomics, Tumour heterogeneity, Epigenomics

Comments

Trial registration: ClinicalTrials.gov NCT01888601.

Associated Data

PMID: 37046093