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Gene fusions during the early evolution of mesothelioma correlate with impaired DNA repair and Hippo pathways

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posted on 2024-03-21, 15:47 authored by Maymun Jama, Min Zhang, Charlotte Poile, Apostolos Nakas, Annabel Sharkey, Joanna Dzialo, Alan Dawson, Kudazyi Kutywayo, Dean A Fennell, Ed HolloxEd Hollox

Malignant pleural mesothelioma (MPM), a rare cancer a long latency period (up to 40 years) between asbestos exposure and disease presentation. The mechanisms coupling asbestos to recurrent somatic alterations are poorly defined. Gene fusions arising through genomic instability may create novel drivers during early MPM evolution. We explored the gene fusions that occurred early in the evolutionary history of the tumor. We conducted multiregional whole exome sequencing (WES) of 106 samples from 20 patients undergoing pleurectomy decortication and identified 24 clonal nonrecurrent gene fusions, three of which were novel (FMO9P‐OR2W5, GBA3, and SP9). The number of early gene fusion events detected varied from zero to eight per tumor, and presence of gene fusions was associated with clonal losses involving the Hippo pathway genes and homologous recombination DNA repair genes. Fusions involved known tumor suppressors BAP1, MTAP, and LRP1B, and a clonal oncogenic fusion involving CACNA1D‐ERC2, PARD3B‐NT5DC2, and STAB2‐NT5DC2 fusions were also identified as clonal fusions. Gene fusions events occur early during MPM evolution. Individual fusions are rare as no recurrent truncal fusions event were found. This suggests the importance of early disruption of these pathways in generating genomic rearrangements resulting in potentially oncogenic gene fusions.

Funding

British Lung Foundation-Mesothelioma UK grant MESOUK17-8

PhD studentship from the University of Leicester College of Life Sciences

History

Author affiliation

College of Life Sciences/Genetics & Genome Biology

Version

  • VoR (Version of Record)

Published in

Genes, Chromosomes and Cancer

Volume

63

Issue

1

Pagination

e23189

Publisher

Wiley

issn

1045-2257

eissn

1098-2264

Copyright date

2024

Available date

2024-03-21

Spatial coverage

United States

Language

en

Deposited by

Professor Ed Hollox

Deposit date

2024-03-20

Data Access Statement

Data for figure 5 and Supplementary table 5 are available at DOI: 10.25392/leicester.data.22360534 The exome sequencing data are available from the NCBI Sequence Read Archive under accession number PRJNA649889 All other data available from the corresponding author on request.

Rights Retention Statement

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