PLoS ONE (Jan 2012)

Core site-moiety maps reveal inhibitors and binding mechanisms of orthologous proteins by screening compound libraries.

  • Kai-Cheng Hsu,
  • Wen-Chi Cheng,
  • Yen-Fu Chen,
  • Hung-Jung Wang,
  • Ling-Ting Li,
  • Wen-Ching Wang,
  • Jinn-Moon Yang

DOI
https://doi.org/10.1371/journal.pone.0032142
Journal volume & issue
Vol. 7, no. 2
p. e32142

Abstract

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Members of protein families often share conserved structural subsites for interaction with chemically similar moieties despite low sequence identity. We propose a core site-moiety map of multiple proteins (called CoreSiMMap) to discover inhibitors and mechanisms by profiling subsite-moiety interactions of immense screening compounds. The consensus anchor, the subsite-moiety interactions with statistical significance, of a CoreSiMMap can be regarded as a "hot spot" that represents the conserved binding environments involved in biological functions. Here, we derive the CoreSiMMap with six consensus anchors and identify six inhibitors (IC(50)<8.0 µM) of shikimate kinases (SKs) of Mycobacterium tuberculosis and Helicobacter pylori from the NCI database (236,962 compounds). Studies of site-directed mutagenesis and analogues reveal that these conserved interacting residues and moieties contribute to pocket-moiety interaction spots and biological functions. These results reveal that our multi-target screening strategy and the CoreSiMMap can increase the accuracy of screening in the identification of novel inhibitors and subsite-moiety environments for elucidating the binding mechanisms of targets.