| Literature DB >> 31089269 |
Andromachi Vagena1,2, Myrto Papamentzelopoulou1, Despoina Kalfakakou1, Panagoula Kollia2, Christos Papadimitriou3, Amanda Psyrri4, Paraskevi Apostolou1, George Fountzilas5, Irene Konstantopoulou1, Drakoulis Yannoukakos1, Florentia Fostira6.
Abstract
PALB2 loss-of-function variants play an important role in breast, pancreatic and possibly, ovarian and gastric cancer susceptibility. Their frequency can be influenced by founder effects, already described in some populations. Herein, we have assessed the possible founder effect of PALB2 c.2257C>T (p.Arg753*) truncating variant among Greek breast cancer patients, while investigating possible correlations with cancer diagnoses. Following a lead deriving from a background study of highly selected Greek breast cancer patients, a total of 2496 breast and 697 ovarian cancer patients were directly genotyped for the PALB2 c.2257C>T truncating variant. Consequently, haplotype analysis was conducted on identified carriers, using seven microsatellite markers. The prevalence of the PALB2 variant was 0.24% (6/2496) and 0.14% (1/697) among breast and ovarian cases, respectively. Family history seems to be an important factor for the variant identification, although not reaching statistical significance. Microsatellite analysis on 12 carriers revealed a common shared haplotype, spanning a chromosomal region of ~1.2 Mb; the variant was possibly introduced in the Greek population ~1600 years ago. The variant confers high breast cancer risk, as illustrated by comparison with publicly available control groups. Genetic testing for PALB2, especially for the Greek founder c.2257C>T truncating variant, should be seriously considered in Greek breast cancer cases, since such findings could assist appropriate clinical management for the patients and their families.Entities:
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Year: 2019 PMID: 31089269 DOI: 10.1038/s10038-019-0612-6
Source DB: PubMed Journal: J Hum Genet ISSN: 1434-5161 Impact factor: 3.172