A mosaic pathogenic variant in MSH6 causes MSH6-deficient colorectal and endometrial cancer in a patient classified as suspected Lynch syndrome: a case report

Author:

Walker Romy1,Clendenning Mark1,Joo Jihoon E.1,Xue Jessie1,Mahmood Khalid1,Georgeson Peter1,Como Julia1,Joseland Sharelle1,Preston Susan G.1,Chan James M.1,Jenkins Mark A.1,Rosty Christophe2,Macrae Finlay A.3,Palma Stephanie Di4,Campbell Ainsley4,Winship Ingrid M.3,Buchanan Daniel D.1

Affiliation:

1. University of Melbourne

2. Envoi Specialist Pathologists

3. Royal Melbourne Hospital

4. Austin Health

Abstract

Abstract Germline pathogenic variants in the DNA mismatch (MMR) repair genes (Lynch syndrome) predispose to colorectal (CRC) and endometrial (EC) cancer. However, mosaic variants in the MMR genes have been rarely described. We identified a likely de novo mosaic MSH6:c.1135_1139del p.Arg379* pathogenic variant in a patient diagnosed with suspected Lynch syndrome/Lynch-like syndrome. The patient developed MSH6-deficient EC and CRC at 54 and 58 years of age, respectively, without a detectable germline MMR pathogenic variant. Multigene panel sequencing of tumor and blood-derived DNA identified an MSH6 somatic mutation (MSH6:c.1135_1139del p.Arg379*) common to both the EC and CRC, raising suspicion of mosaicism. A droplet digital polymerase chain reaction (ddPCR) assay detected the MSH6 variant at 5.34% frequency in normal colonic tissue, 3.49% in saliva and 1.64% in blood DNA, demonstrating the presence of the MSH6 variant in all three germ layers. This study highlights the utility of tumor sequencing to guide sensitive ddPCR testing to detect low-level mosaicism in the MMR genes. Further investigation of the prevalence of MMR mosaicism is needed to inform routine diagnostic approaches and genetic counselling.

Publisher

Research Square Platform LLC

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