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Genomic instability in early systemic sclerosis

Robert Gniadecki, Aishwarya Iyer, Dylan Hennessey, Lamia Khan, Sandra O’Keefe, Desiree Redmond, Jan Storek, Caylib Durand, Jan Willem Cohen-Tervaert, Mohammed Osman

2022Journal of Autoimmunity24 citationsDOIOpen Access PDF

Abstract

OBJECTIVES: Systemic sclerosis (SSc) is associated with secondary malignancies. Previous studies have suggested that mutated cancer proteins, such as RNA polymerase III, are autoantigens promoting an inflammatory response in SSc. However, it has never been previously investigated whether non-neoplastic tissue in SSc harbors mutations which may play a role in SSc pathogenesis. METHODS: Skin biopsies were obtained from 8 sequential patients with a progressive form of early stage SSc (with severe skin and/or lung involvement). Areas of dermal fibrosis were microdissected and analyzed with deep, whole exome sequencing. Gene mutation patterns were compared to autologous buccal mucosal cells as a control. RESULTS: base pairs. The mutational pattern in all samples exhibited a clock-like signature, which is ubiquitous in cancers and in senescent cells. Of the 1997 genes we identified which were mutated in at least two SSc patients, 39 genes represented cancer drivers (i.e. tumor suppressor genes or oncogenes) which are commonly found in gynecological, squamous and gastrointestinal cancer signatures. Of all the mutations, the most common mutated genes were important in regulating pathways related to epigenetic histone modifications, DNA repair and genome integrity. CONCLUSIONS: Somatic hypermutation occurs in fibrotic skin in patients with early progressive SSc. Cancer driver gene mutations may potentially play a fundamental role in the pathogenesis of SSc.

Topics & Concepts

BiologyCancer researchGenome instabilityCancerGeneGermline mutationPathogenesisSomatic cellMutationGeneticsDNA damageImmunologyDNASystemic Sclerosis and Related DiseasesInflammatory Myopathies and DermatomyositisSkin Diseases and Diabetes
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