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From strand exchange to branch migration; bypassing of non-homologous sequences by human Rad51 and Rad54
Authors:Urena Damian E  Zhang Zhaoqing  Tsai Yu-Cheng  Wang Yu-Zhen  Chen Junghuei
Affiliation:
  • 1 Department of Chemistry and Biochemistry, University of Delaware, Newark, DE 19716, USA
  • 2 SABioscience Corp., 6951 Executive Way Frederick, MD 21703, USA
  • Abstract:Rad51 and Rad54 play crucial roles during homologous recombination. The biochemical activities of human Rad51 (hRad51) and human Rad54 (hRad54) and their interactions with each other are well documented. However, it is not known how these two proteins work together to bypass heterologous sequences; i.e. mismatched base pairs, during homologous recombination. In this study, we used a fluorescence resonance energy transfer assay to monitor homologous recombination processes in real time so that the interactions between hRad54 and hRad51 during DNA strand exchange and branch migration, which are two core steps of homologous recombination, could be characterized. Our results indicate that hRad54 can facilitate hRad51-promoted strand exchange through various degrees of mismatching. We propose that the main roles of hRad51 in homologous recombination is to initiate the homology recognition and strand-exchange steps and those of hRad54 are to promote efficient branch migration, bypass potential mismatches and facilitate long-range strand exchanges through branch migration of Holliday junctions.
    Keywords:homologous recombination   DNA mismatches   human Rad51   human Rad54   Holliday junctions
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