Integrating Tumor Sequencing Into Clinical Practice for Patients With Mismatch Repair-Deficient Lynch Syndrome Spectrum Cancers. Issue 8 (16th August 2021)

Record Type:: Journal Article
Title:: Integrating Tumor Sequencing Into Clinical Practice for Patients With Mismatch Repair-Deficient Lynch Syndrome Spectrum Cancers. Issue 8 (16th August 2021)
Main Title:: Integrating Tumor Sequencing Into Clinical Practice for Patients With Mismatch Repair-Deficient Lynch Syndrome Spectrum Cancers
Authors:: Dixon, Katherine
Asrat, Mary-Jill
Bedard, Angela C.
Binnington, Kristin
Compton, Katie
Cremin, Carol
Heidary, Nili
Lohn, Zoe
Lovick, Niki
McCullum, Mary
Mindlin, Allison
O'Loughlin, Melanie
Petersen, Tammy
Portigal-Todd, Cheryl
Scott, Jenna
St-Martin, Genevieve
Thompson, Jennifer
Turnbull, Ruth
Mung, Sze Wing
Hong, Quan
Bezeau, Marjorie
Bosdet, Ian
Tucker, Tracy
Young, Sean
Yip, Stephen
Aubertin, Gudrun
Blood, Katherine A.
Nuk, Jennifer
Sun, Sophie
Schrader, Kasmintan A.
Abstract:: Abstract : INTRODUCTION: Uninformative germline genetic testing presents a challenge to clinical management for patients suspected to have Lynch syndrome, a cancer predisposition syndrome caused by germline variants in the mismatch repair (MMR) genes or EPCAM . METHODS: Among a consecutive series of MMR-deficient Lynch syndrome spectrum cancers identified through immunohistochemistry-based tumor screening, we investigated the clinical utility of tumor sequencing for the molecular diagnosis and management of suspected Lynch syndrome families. MLH1-deficient colorectal cancers were prescreened for BRAF V600E before referral for genetic counseling. Microsatellite instability, MLH1 promoter hypermethylation, and somatic and germline genetic variants in the MMR genes were assessed according to an established clinical protocol. RESULTS: Eighty-four individuals with primarily colorectal (62%) and endometrial (31%) cancers received tumor-normal sequencing as part of routine clinical genetic assessment. Overall, 27% received a molecular diagnosis of Lynch syndrome. Most of the MLH1-deficient tumors were more likely of sporadic origin, mediated by MLH1 promoter hypermethylation in 54% and double somatic genetic alterations in MLH1 (17%). MSH2-deficient, MSH6-deficient, and/or PMS2-deficient tumors could be attributed to pathogenic germline variants in 37% and double somatic events in 28%. Notably, tumor sequencing could explain 49% of cases without causal germline variants, somatic … (more)
Is Part Of:: Clinical and translational gastroenterology. Volume 12:Issue 8(2021)
Journal:: Clinical and translational gastroenterology
Issue:: Volume 12:Issue 8(2021)
Issue Display:: Volume 12, Issue 8 (2021)
Year:: 2021
Volume:: 12
Issue:: 8
Issue Sort Value:: 2021-0012-0008-0000
Page Start:: e00397
Page End:
Publication Date:: 2021-08-16
Subjects:: Stomach -- Diseases -- Periodicals
Intestines -- Diseases -- Periodicals
Gastroenterology
Gastrointestinal Diseases
Liver Diseases
Intestines -- Diseases
Stomach -- Diseases
Periodical
Periodicals
Fulltext
Internet Resources
Periodicals
Electronic journals
616.33
Journal URLs:: http://bibpurl.oclc.org/web/52768 ↗
http://www.nature.com/ctg ↗
http://www.ncbi.nlm.nih.gov/pmc/journals/1564/ ↗
https://journals.lww.com/ctg/pages/default.aspx ↗
http://www.nature.com/ ↗
DOI:: 10.14309/ctg.0000000000000397 ↗
Languages:: English
ISSNs:: 2155-384X
Deposit Type:: Legaldeposit
View Content:: Available online (eLD content is only available in our Reading Rooms) ↗
Physical Locations:: British Library DSC - BLDSS-3PM
British Library HMNTS - ELD Digital store
Ingest File:: 24092.xml