PLoS Computational Biology (Feb 2017)

ALKBH7 Variant Related to Prostate Cancer Exhibits Altered Substrate Binding.

  • Alice R Walker,
  • Pavel Silvestrov,
  • Tina A Müller,
  • Robert H Podolsky,
  • Gregory Dyson,
  • Robert P Hausinger,
  • Gerardo Andrés Cisneros

DOI
https://doi.org/10.1371/journal.pcbi.1005345
Journal volume & issue
Vol. 13, no. 2
p. e1005345

Abstract

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The search for prostate cancer biomarkers has received increased attention and several DNA repair related enzymes have been linked to this dysfunction. Here we report a targeted search for single nucleotide polymorphisms (SNPs) and functional impact characterization of human ALKBH family dioxygenases related to prostate cancer. Our results uncovered a SNP of ALKBH7, rs7540, which is associated with prostate cancer disease in a statistically significantly manner in two separate cohorts, and maintained in African American men. Comparisons of molecular dynamics (MD) simulations on the wild-type and variant protein structures indicate that the resulting alteration in the enzyme induces a significant structural change that reduces ALKBH7's ability to bind its cosubstrate. Experimental spectroscopy studies with purified proteins validate our MD predictions and corroborate the conclusion that this cancer-associated mutation affects productive cosubstrate binding in ALKBH7.