Frequency of the TP53 R337H variant in sporadic breast cancer and its impact on genomic instability

Author:

Mathias Carolina,Bortoletto Stéfanne,Centa Ariana,Komechen Heloisa,Lima Rubens S.,Fonseca Aline S.,Sebastião Ana Paula,Urban Cícero A.,Soares Emerson W. S.,Prando Carolina,Figueiredo Bonald C.,Cavalli Iglenir J.,Cavalli Luciane R.,Ribeiro Enilze M. F. S.

Abstract

AbstractThe R337H is a TP53 germline pathogenic variant that has been associated with several types of cancers, including breast cancer. Our main objective was to determine the frequency of the R337H variant in sporadic breast cancer patients from Paraná state, South Brazil, its association with prognosis and its impact in genomic instability. The genotyping of 805 breast cancer tissues revealed a genotypic and allelic frequency of the R337H variant of 2.36% and 1.18%, respectively. In these R337H+ cases a lower mean age at diagnosis was observed when compared to the R337H-cases. Array-CGH analysis showed that R337H+ patients presented a higher number of copy number alterations (CNAs), compared to the R337H−. These CNAs affected genes and miRNAs that regulate critical cancer signaling pathways; a number of these genes were associated with survival after querying the KMplot database. Furthermore, homozygous (R337H+/R337H+) fibroblasts presented increased levels of copy number variants when compared to heterozygous or R337H− cells. In conclusion, the R337H variant may contribute to 2.36% of the breast cancer cases without family cancer history in Paraná. Among other mechanisms, R337H increases the level of genomic instability, as evidenced by a higher number of CNAs in the R337H+ cases compared to the R337H−.

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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