Coupling protein engineering with probe design to inhibit and image matrix metalloproteinases with controlled specificity.

نویسندگان

  • Montse Morell
  • Thinh Nguyen Duc
  • Amanda L Willis
  • Salahuddin Syed
  • Jiyoun Lee
  • Edgar Deu
  • Yang Deng
  • Junpeng Xiao
  • Benjamin E Turk
  • Jason R Jessen
  • Stephen J Weiss
  • Matthew Bogyo
چکیده

Matrix metalloproteinases (MMPs) are zinc endopeptidases that play roles in numerous pathophysiological processes and therefore are promising drug targets. However, the large size of this family and a lack of highly selective compounds that can be used for imaging or inhibition of specific MMPs members has limited efforts to better define their biological function. Here we describe a protein engineering strategy coupled with small-molecule probe design to selectively target individual members of the MMP family. Specifically, we introduce a cysteine residue near the active-site of a selected protease that does not alter its overall activity or function but allows direct covalent modification by a small-molecule probe containing a reactive electrophile. This specific engineered interaction between the probe and the target protease provides a means to both image and inhibit the modified protease with absolute specificity. Here we demonstrate the feasibility of the approach for two distinct MMP proteases, MMP-12 and MT1-MMP (or MMP-14).

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عنوان ژورنال:
  • Journal of the American Chemical Society

دوره 135 24  شماره 

صفحات  -

تاریخ انتشار 2013