AUTHOR=Hu Zhe-Yu , Liu Liping , Xie Ning , Lu Jun , Liu Zhentian , Tang Yu , Wang Yikai , Yang Jianbo , Ouyang Quchang 

TITLE=Germline PALB2 Mutations in Cancers and Its Distinction From Somatic PALB2 Mutations in Breast Cancers

JOURNAL=Frontiers in Genetics

VOLUME=11

YEAR=2020

URL=https://www.frontiersin.org/journals/genetics/articles/10.3389/fgene.2020.00829

DOI=10.3389/fgene.2020.00829

ISSN=1664-8021

ABSTRACT=<p><italic>PALB2</italic> is an important BRCAx candidate for familial breast cancers (FBC). <italic>PALB2</italic> pathogenic variants (PVs) may not to conform to “two hit” paradigm. However, a recent study demonstrates that in the majority <italic>PALB2</italic> germline mutant breast cancers, the loss of heterozygosity (LOH) and somatic point mutations are the “second hit.” This study aimed to investigate the second hits in germline <italic>PALB2</italic> mutations in breast cancers. We screened out 28 germline <italic>PALB2-</italic>mutation carriers among 480 familial cancer patients (including 143 FBC patients) in Geneplus database pool. Of the 143 patients with FBC, 10 had mono-allelic <italic>PALB2</italic> germline mutations. All these germline <italic>PALB2</italic> mutations were high-risk stop-gain, frameshift, or splicing mutations that concentrated in EX5–EX9 and might led to truncated proteins, severe functional defects and malignant phenotype. The hotspots were c.1057A[3 &gt; 2] and c.3114-1G &gt; A. Other mutations included c.389delA, c.2068C &gt; T, c.2167_2168delAT, c.2629delT and c.2968G &gt; T. Only one FBC patient has <italic>PALB2</italic> somatic mutation and two patients had LOH of <italic>PALB2</italic>. All germline <italic>PALB2</italic> mutations were high-risk mutations, whereas the somatic <italic>PALB2</italic> mutations were moderate-risk missense mutations. We also distinguished PALB2 “novel mutations” from “reported mutations.” In conclusion, germline <italic>PALB2</italic> mutation should be put into the context of future screening.</p>