Evidence for Breast Cancer As an Integral Part of Lynch Syndrome

Overview

Journal Genes Chromosomes Cancer

Specialties Molecular Biology
Oncology

Date 2011 Oct 29

PMID 22034109

Citations 28

Authors

Nicole Buerki

Lucienne Gautier

Michal Kovac

Giancarlo Marra

Mauro Buser

Hansjakob Mueller

Karl Heinimann

Affiliations

Soon will be listed here.

Abstract

Lynch syndrome, an autosomal dominant cancer predisposition caused by mutations in DNA mismatch repair (MMR) genes, mainly mainly mutL homolog 1, OMIM 120436 (MLH1) and mutS homolog 2, OMIM 609309 (MSH2), encompasses a tumor spectrum including primarily gastrointestinal, endometrial, and ovarian cancer. This study aimed at clarifying the heavily debated issue of breast cancer being part of Lynch syndrome. Detailed clinical data on cancer occurrence in Swiss female MLH1/MSH2 mutation carriers were gathered, all available breast cancer specimens assessed for molecular evidence for MMR deficiency (i.e., microsatellite instability (MSI), MMR protein expression, and somatic (epi)genetic MMR gene alterations) and compiled with the scarce molecular data available from the literature. Seventy unrelated Swiss Lynch syndrome families were investigated comprising 632 female family members at risk of which 92 were genetically verified mutation carriers (52 MLH1 and 40 MSH2). On contrast to endometrial and ovarian cancer, which occurred significantly more often and at younger age in MLH1/MSH2 mutation carriers (median 50.5 and 49.0 years; P < 0.00001), overall cumulative breast cancer incidence closely mirrored the one in the Swiss population (56.5 years). Six (85.7%) of seven breast cancer specimens available for molecular investigations displayed the hallmarks of MMR deficiency. Combined with data from the literature, MSI was present in 26 (70.3%) of 37 and altered MMR protein expression in 16 (72.7%) of 22 breast cancer specimens from MLH1/MSH2 mutation carriers. These findings, thus, provide strong molecular evidence for a pivotal role of MMR deficiency in breast cancer development in Lynch syndrome.

Citing Articles

Prevalence of Variants of Uncertain Significance in Patients Undergoing Genetic Testing for Hereditary Breast and Ovarian Cancer and Lynch Syndrome.

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Lynch Syndrome Biopathology and Treatment: The Potential Role of microRNAs in Clinical Practice.

Ascrizzi S, Arillotta G, Grillone K, Carida G, Signorelli S, Ali A Cancers (Basel). 2023; 15(15).

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Cancer surveillance for transgender and gender diverse patients with Lynch syndrome: a practice resource of the Collaborative Group of the Americas on Inherited Gastrointestinal Cancer.

Hodan R, Rodgers-Fouche L, Chittenden A, Dominguez-Valentin M, Ferriss J, Gima L Fam Cancer. 2023; 22(4):437-448.

PMID: 37341816 DOI: 10.1007/s10689-023-00341-4.

Mismatch repair is a double-edged sword in the battle against microsatellite instability.

Miller C, Usdin K Expert Rev Mol Med. 2022; 24:e32.

PMID: 36059110 PMC: 9884765. DOI: 10.1017/erm.2022.16.

Clinical relevance of pathogenic germline variants in mismatch repair genes in Chinese breast cancer patients.

Hu L, Sun J, Li Z, Qu Z, Liu Y, Wan Q NPJ Breast Cancer. 2022; 8(1):52.

PMID: 35449176 PMC: 9023502. DOI: 10.1038/s41523-022-00417-x.