A Highly Conserved Region in BRCA2 Suppresses the RAD51-Interaction Activity of BRC Repeats

Simple Summary Mammary tumors are the most common tumor type in female dogs and one of the major problems in veterinary oncology. Breast cancer 2, early onset (BRCA2) mutations are associated with tumorigenesis in humans and dogs. BRCA2 is a DNA damage repair protein that interacts with RAD51, another DNA-damage-repair protein, to preserve DNA stability. Tumors, such as mammary tumors, are developed when their function or interaction is lost. It is currently unclear how the interaction activity of BRCA2 and RAD51 is regulated. We focused on a highly conserved region (HCR) near the BRC repeats, which are RAD51-interacting domains in BRCA2. We demonstrated that HCR regulated the RAD51-interaction activity of BRC repeats. In addition, we looked for HCR mutations in canine mammary tumors and discovered I1110M mutations. The effect of four HCR mutations, including I1110M, on the RAD51-interaction activity of BRC repeats was investigated. Three HCR mutations (A1108G, S1114P, and T1115P) found in canine mammary tumors or human breast cancers influenced the RAD51-interaction activity of BRC repeats. According to this study, HCR regulated the RAD51-interacting activity of BRC repeats, and HCR mutations may be related to tumorigenesis in both dogs and humans. Mammary tumors are the most prevalent type of tumors in female dogs. Breast cancer 2, early onset (BRCA2) malignant mutations are associated with tumorigenesis in humans and dogs. BRCA2 plays a pivotal role in homologous recombination repair by recruiting RAD51 recombinase to DNA damage sites to maintain genome stability. To recruit RAD51, BRCA2 must interact with RAD51 via BRC repeats, but the regulation of this interaction has been unclear. In this study, we focused on a highly conserved region (HCR) near BRC repeats. Using co-immunoprecipitation and mammalian two-hybrid assay, we found that HCR suppressed the RAD51-interaction activity of BRC repeats and that substitutions of HCR phosphorylation sites affected it. In canine tumor samples, we found ten mutations, including a novel HCR mutation (I1110M) from canine tumor samples. The effect of four HCR mutations, including I1110M, on the RAD51-interaction activity of BRC repeats was tested. One of the HCR mutations found in canine mammary tumors increased the interaction, but the two mutations found in human breast cancers decreased it. This study suggested that the HCR regulated the RAD51-interacting activity of BRC repeats through HCR phosphorylation and that mutations in HCR may be related to tumorigenesis in both dogs and humans.