A study of somatic BRCA variants and their putative effect on protein properties in malignant mesothelioma

Author:

Krishnamurthy Kritika1ORCID,Oh Kei Shing2,Alghamdi Sarah23,Sriganeshan Vathany23,Poppiti Robert23

Affiliation:

1. Department of Pathology , Montefiore Medical Center, Albert Einstein College of Medicine , Bronx , NY , USA

2. AM Rywlin Department of Pathology , Mount Sinai Medical Center , Miami Beach , FL , USA

3. Pathology , FIU/Herbert Werthein College of Medicine , Miami , FL , USA

Abstract

Abstract Objectives The aim of this study is to analyze the prevalence of somatic mutations in BRCA1 and BRCA2 in malignant mesothelioma and their putative impact on protein properties. Methods Eighteen cases of malignant mesothelioma were retrieved from the archives and for next generation sequencing analysis of BRCA1 and BRCA2 genes. Variants were analyzed using Ensembl VEP17, Polyphen 2.0 software, SIFT software, MutpredV2, and SWISS-MODEL homology-modeling pipeline server. Results BRCA2 variants were found in significantly higher percentage (22%) of cases (p=0.02). Five missense variants were identified. These were p.A2351P, p.T2250A, p.A895V, pG1771D, and p.R2034C. The SIFT scores of all except one were ≥ 0.03. The Polyphen scores of these four alterations were ≤0.899. In case of p.A2315, the SIFT score was 0.01, while the Polyphen 2 score was 0.921. MutPred2 scores were ≤0.180 for all. Loss of intrinsic disorder was predicted (Pr=0.32, p=0.07) for p.R2034C, while gain of intrinsic disorder was predicted for p.A2351P (Pr=0.36, p=0.01) and p.G1771D (Pr=0.34, p=0.02). Conclusions BRCA2 somatic variants were identified in 22% cases of malignant mesotheliomas in this study. The variants localize more frequently to the disordered regions of the protein and are predicted to affect the level of disorder.

Publisher

Walter de Gruyter GmbH

Subject

Internal Medicine

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