Functional characterisation guides classification of novel BAP1 germline variants

Author:

Hong Jing HanORCID,Chong Siao Ting,Lee Po-Hsien,Tan Jing,Heng Hong Lee,Ishak Nur Diana Binte,Chan Sock HoaiORCID,Teh Bin TeanORCID,Ngeow JoanneORCID

Abstract

AbstractWe have identified six patients harbouring distinct germline BAP1 mutations. In this study, we functionally characterise known BAP1 pathogenic and likely benign germline variants out of these six patients to aid in the evaluation and classification of unknown BAP1 germline variants. We found that pathogenic germline variants tend to encode truncated proteins, show diminished expression of epithelial-mesenchymal transition (EMT) markers, are localised in the cytosol and have reduced deubiquitinase capabilities. We show that these functional assays are useful for BAP1 variant curation and may be added in the American College of Medical Genetics and Genomics (ACMG) criteria for BAP1 variant classification. This will allow clinicians to distinguish between BAP1 pathogenic and likely benign variants reliably and may aid to quickly benchmark newly identified BAP1 germline variants. Classification of novel BAP1 germline variants allows clinicians to inform predisposed patients and relevant family members regarding potential cancer risks, with appropriate clinical interventions implemented if required.

Funder

MOH | National Medical Research Council

LKC Start-Up Grant. Also partially funded by NCC Research Fund, NCC Cancer Fund, Terry Fox and Lee Foundation supporting funds

Duke-NUS Khoo Postdoctoral Fellowship Award

NRF-NSFC Joint Research Grant (Data Science)

Publisher

Springer Science and Business Media LLC

Subject

Genetics(clinical),Genetics,Molecular Biology

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