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TP53 missense allele predisposing to high risk of breast cancer but not pediatric cancers. | LitMetric

AI Article Synopsis

  • Pathogenic variants in the TP53 gene are linked to increased risks of early-onset breast cancer and other cancers associated with Li-Fraumeni syndrome (LFS), but the impact of certain less severe variants is still not well understood.
  • In a study involving Palestinian breast cancer patients, those carrying the TP53 p.R181C variant had a 50% risk of developing breast cancer by age 50 and an 81% risk by age 80.
  • The prevalence of pediatric cancers in relatives of these TP53 variant carriers was similar to those with no known cancer-related gene variants, indicating that genetic testing and cancer screening for children in these families may not be necessary.

Article Abstract

Pathogenic TP53 germline variants cause young-onset breast cancer and other cancers of the Li-Fraumeni syndrome (LFS) spectrum, but the clinical consequences of partial-loss-of function TP53 variants are incompletely understood. In the consecutive cohort of Palestinian breast cancer patients of the Middle East Breast Cancer Study (MEBCS), breast cancer risk among TP53 p. R181C heterozygotes was 50% by age 50 y and 81% by age 80 y. In contrast, prevalence of pediatric cancers in the MEBCS was similar among first degree relatives of TP53 p. R181C carriers (3/519 = 0.0058) and first degree relatives of MEBCS patients with no pathogenic germline variant in any known breast cancer gene (7/1082 = 0.0065; OR = 0.90, 95%CI [0.23,3.49], Fisher P = .90 (2-tailed)). This result suggests that in families harboring this TP53 allele, genetic testing in children is unwarranted, and screening children for LFS tumors is unnecessary. More generally, some TP53 missense alleles can predispose to very high risk of breast cancer without pleiotropic effects.

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Source
http://dx.doi.org/10.1093/jnci/djae334DOI Listing

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