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Published March 7, 2006 | Published
Journal Article Open

Electron trap for DNA-bound repair enzymes: A strategy for DNA-mediated signaling

Abstract

Despite a low copy number within the cell, base excision repair (BER) enzymes readily detect DNA base lesions and mismatches. These enzymes also contain [Fe4S4] clusters, yet a redox role for these iron cofactors had been unclear. Here, we provide evidence that BER proteins may use DNA-mediated redox chemistry as part of a signaling mechanism to detect base lesions. By using chemically modified bases, we show electron trapping on DNA in solution with bound BER enzymes by electron paramagnetic resonance (EPR) spectroscopy. We demonstrate electron transfer from two BER proteins, Endonuclease III (EndoIII) and MutY, to modified bases in DNA containing oxidized nitroxyl radical EPR probes. Electron trapping requires that the modified base is coupled to the DNA {pi}-stack, and trapping efficiency is increased when a noncleavable MutY substrate analogue is located distally to the trap. These results are consistent with DNA binding leading to the activation of the repair proteins toward oxidation. Significantly, these results support a mechanism for DNA repair that involves DNA-mediated charge transport.

Additional Information

© 2006 by The National Academy of Sciences of the USA Contributed by Jacqueline K. Barton, January 10, 2006. Published online before print February 27, 2006, 10.1073/pnas.0600239103 We thank A. Boal for preparation of EndoIII and E. Khamou for technical assistance. This work was supported by National Institutes of Health Grants GM49216 (to J.K.B.) and CA67985 (to S.S.D.). Author contributions: E.Y., E.D.A.S., S.S.D., and J.K.B. designed research; E.Y. performed research; V.L.O. and S.S.D. contributed new reagents/analytic tools; E.Y. and J.K.B. analyzed data; and E.Y., S.S.D., and J.K.B. wrote the paper. Conflict of interest statement: No conflicts declared.

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August 22, 2023
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