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Structure of the recA protein–ADP complex

Nature volume 355pages 374–376 (1992)Cite this article

Abstract

THE recA protein catalyses the ATP-driven homologous pairing and strand exchange of DNA molecules1–3. It is an allosteric enzyme: the ATPase activity is DNA-dependent4,5, and ATP-bound recA protein has a high affinity for DNA, whereas the ADP-bound form has a low affinity6. In the absence of ATP hydrolysis, recA protein can still promote homologous pairing, apparently through the formation of a triple-stranded intermediate1,7–9. The exact role of ATP hydrolysis is not clear, but it presumably drives the triplex intermediate towards products1,9,10. Here we determine the position of bound ADP diffused into the recA crystal. We show that only the phosphates are bound in the same way as in other NTPases containing the G/AXXXXGKT/S motif. We propose that recA protein may change its conformation upon ATP hydrolysis in a manner analogous to one such protein, the p21 protein from theras oncogene. A model is presented to account for the allosteric stimulation of DNA binding by ATP. The mechanism by which nucleoside triphosphate hydrolysis is coupled to the binding of another ligand in recA protein and p21 may be typical of the large class of NTPases containing this conserved motif.

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Authors and Affiliations

  1. Department of Molecular Biophysics and Biochemistry, Department of Chemistry, and Howard Hughes Medical Institute at Yale University, New Haven, Connecticut, 06511, USA

    Randall M. Story & Thomas A. Steitz

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  1. Randall M. Story
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  2. Thomas A. Steitz
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Story, R., Steitz, T. Structure of the recA protein–ADP complex. Nature 355, 374–376 (1992). https://doi.org/10.1038/355374a0

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