Pulsed EPR characterization of HIV-1 protease conformational sampling and inhibitor-induced population shifts.

نویسندگان

  • Zhanglong Liu
  • Thomas M Casey
  • Mandy E Blackburn
  • Xi Huang
  • Linh Pham
  • Ian Mitchelle S de Vera
  • Jeffrey D Carter
  • Jamie L Kear-Scott
  • Angelo M Veloro
  • Luis Galiano
  • Gail E Fanucci
چکیده

The conformational landscape of HIV-1 protease (PR) can be experimentally characterized by pulsed-EPR double electron-electron resonance (DEER). For this characterization, nitroxide spin labels are attached to an engineered cysteine residue in the flap region of HIV-1 PR. DEER distance measurements from spin-labels contained within each flap of the homodimer provide a detailed description of the conformational sampling of apo-enzyme as well as induced conformational shifts as a function of inhibitor binding. The distance distribution profiles are further interpreted in terms of a conformational ensemble scheme that consists of four unique states termed "curled/tucked", "closed", "semi-open" and "wide-open" conformations. Reported here are the DEER results for a drug-resistant variant clinical isolate sequence, V6, in the presence of FDA approved protease inhibitors (PIs) as well as a non-hydrolyzable substrate mimic, CaP2. Results are interpreted in the context of the current understanding of the relationship between conformational sampling, drug resistance, and kinetic efficiency of HIV-1PR as derived from previous DEER and kinetic data for a series of HIV-1PR constructs that contain drug-pressure selected mutations or natural polymorphisms. Specifically, these collective results support the notion that inhibitor-induced closure of the flaps correlates with inhibitor efficiency and drug resistance. This body of work also suggests DEER as a tool for studying conformational sampling in flexible enzymes as it relates to function.

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عنوان ژورنال:
  • Physical chemistry chemical physics : PCCP

دوره 18 8  شماره 

صفحات  -

تاریخ انتشار 2016