Affiliation:
1. Department of Breast Oncology NHO Kyushu Cancer Center Fukuoka Japan
2. Department of Chemistry, Faculty of Science Fukuoka University Fukuoka Japan
3. Cancer Genetics Laboratory, Clinical Research Institute NHO Kyushu Cancer Center Fukuoka Japan
4. Cancer Genetics and Genomics NHO Kyushu Cancer Center Fukuoka Japan
5. Department of Biostatistics Yamaguchi University Graduate School of Medicine Ube Japan
Abstract
AbstractAnnotating genomic sequence alterations is sometimes a difficult decision, particularly in missense variants with uncertain pathogenic significance and also in those presumed as germline pathogenic variants. We here suggest that mutation spectrum may also be useful for judging them. From the public databases, 982 BRCA1/1861 BRCA2 germline missense variants and 294 BRCA1/420 BRCA2 somatic missense variants were obtained. We then compared their mutation spectra, i.e., the frequencies of two transition‐ and four transversion‐type mutations, in each category. Intriguingly, in BRCA1 variants, A:T to C:G transversion, which was relatively frequent in the germline, was extremely rare in somatic, particularly breast cancer, cells (p = .03). Conversely, A:T to T:A transversion was most infrequent in the germline, but not rare in somatic cells. Thus, BRCA1 variants with A:T to T:A transversion may be suspected as somatic, and those with A:T to C:G as being in the germline. These tendencies of mutation spectrum may also suggest the biological and chemical origins of the base alterations. On the other hand, unfortunately, variants of uncertain significance (VUS) were not distinguishable by mutation spectrum. Our findings warrant further and more detailed studies.
Funder
Japan Society for the Promotion of Science