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Familial Cancer
Published in: Familial Cancer 3/2017

01-07-2017 | Original Article

Correlation between germline mutations in MMR genes and microsatellite instability in ovarian cancer specimens

Authors: Mohammad R. Akbari, Shiyu Zhang, Deborah Cragun, Ji-Hyun Lee, Domenico Coppola, John McLaughlin, Harvey A. Risch, Barry Rosen, Patricia Shaw, Thomas A. Sellers, Joellen Schildkraut, Steven A. Narod, Tuya Pal

Published in: Familial Cancer | Issue 3/2017

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Abstract

A high proportion of ovarian cancers from women who carry germline mutations in mismatch repair (MMR) genes demonstrate microsatellite instability (MSI). The utility of pre-screening ovarian cancer specimens for MSI to identify potential patients for germline screening for MMR mutations is uncertain. 656 women with malignant ovarian cancer underwent both MSI testing and germline mutation testing for large rearrangements in three MMR genes, MLH1, MSH2 and MSH6. Germline DNA sequencing data for the same genes was available. Among the 656 women, only four (0.6%) carried a clearly pathogenic MMR mutation. All four cancers from patients with mutations had loss of two or more microsatellite markers (MSI-high). Eighty-four of 652 (13.0%) women without a mutation had MSI-high ovarian cancers. Using MSI-high as a prescreening criterion, the sensitivity of MSI testing to identify germline MMR gene mutations was 100% and the positive predictive value was 4.5%. Germline mutations in MLH1, MSH2 and MSH6 are rare among unselected cases of ovarian cancer. Patients with germline mutations often will have MSI-positive cancers and pre-screening of ovarian cancer specimens may be an efficient way of identifying patients with Lynch syndrome.
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Metadata
Title
Correlation between germline mutations in MMR genes and microsatellite instability in ovarian cancer specimens
Authors
Mohammad R. Akbari
Shiyu Zhang
Deborah Cragun
Ji-Hyun Lee
Domenico Coppola
John McLaughlin
Harvey A. Risch
Barry Rosen
Patricia Shaw
Thomas A. Sellers
Joellen Schildkraut
Steven A. Narod
Tuya Pal
Publication date
01-07-2017
Publisher
Springer Netherlands
Published in
Familial Cancer / Issue 3/2017
Print ISSN: 1389-9600
Electronic ISSN: 1573-7292
DOI
https://doi.org/10.1007/s10689-017-9973-1

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