Germline Mutation in MUS81 Resulting in Impaired Protein Stability is Associated with Familial Breast and Thyroid Cancer

Author:

Pinheiro MaisaORCID,Lupinacci Fernanda Cristina Sulla,Santiago Karina MirandaORCID,Drigo Sandra AparecidaORCID,Marchi Fabio Albuquerque,Fonseca-Alves Carlos EduardoORCID,Andrade Sonia Cristina da SilvaORCID,Aagaard Mads MalikORCID,Basso Tatiane Ramos,dos Reis Mariana Bisarro,Villacis Rolando André Rios,Roffé MartinORCID,Hajj Glaucia Noeli Maroso,Jurisica IgorORCID,Kowalski Luiz Paulo,Achatz Maria IsabelORCID,Rogatto Silvia ReginaORCID

Abstract

Multiple primary thyroid cancer (TC) and breast cancer (BC) are commonly diagnosed, and the lifetime risk for these cancers is increased in patients with a positive family history of both TC and BC. Although this phenotype is partially explained by TP53 or PTEN mutations, a significant number of patients are negative for these alterations. We judiciously recruited patients diagnosed with BC and/or TC having a family history of these tumors and assessed their whole-exome sequencing. After variant prioritization, we selected MUS81 c.1292G>A (p.R431H) for further investigation. This variant was genotyped in a healthy population and sporadic BC/TC tissues and investigated at the protein level and cellular models. MUS81 c.1292G>A was the most frequent variant (25%) and the strongest candidate due to its function of double-strand break repair. This variant was confirmed in four relatives from two families. MUS81 p.R431H protein exhibited lower expression levels in tumors from patients positive for the germline variant, compared with wild-type BC, and normal breast and thyroid tissues. Using cell line models, we showed that c.1292G>A induced protein instability and affected DNA damage response. We suggest that MUS81 is a novel candidate involved in familial BC/TC based on its low frequency in healthy individuals and proven effect in protein stability.

Funder

National Council for Scientific and Technological Development

Coordination for the Improvement of Higher Education Personnel

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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