AI Article Synopsis
- The XRCC3 variant T241M is linked to a higher risk of certain cancers, while the D213N variant does not show this association.
- Both variants lead to increased centrosome numbers and binucleated cells, but only the D213N variant results in higher spontaneous apoptosis levels.
- The T241M variant's lack of apoptotic response to defective cells may increase cancer risk, unlike the D213N variant, which effectively eliminates such cells.
Article Abstract
The XRCC3 variant T241M, but not D213N, has been reported to be associated with an increased risk of some cancers. XRCC3 is one out of five RAD51 paralogues and is involved in homologous recombination, as are the BRCA1 and BRCA2 proteins. However, in contrast to mutations in BRCA1 and BRCA2, the XRCC3(T241M) protein is proficient in homologous recombination and reverts sensitivity to mitomycin C found in XRCC3-deficient cells, whereas XRCC3(D213N) is defective in homologous recombination. Here, we report that both the XRCC3 D213N and T241M alleles are associated with an increase in centrosome number and binucleated cells. However, only the D213N allele gives an increase in spontaneous levels of apoptosis. We suggest that the inability of XRCC3 T241M to apoptotically eliminate aberrant cells with mitotic defects could increase cancer susceptibility in individuals carrying this variant. In contrast, cells carrying the XRCC3 D213N variant are able to eliminate aberrant cells by apoptosis, and consistent with this observation, this variant does not seem to be associated with cancer susceptibility.
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| http://dx.doi.org/10.1093/hmg/ddl037 | DOI Listing |
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