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Literature DB >> 24742668

The role of select subtype polymorphisms on HIV-1 protease conformational sampling and dynamics.

Xi Huang¹, Manuel D Britto¹, Jamie L Kear-Scott¹, Christopher D Boone², James R Rocca³, Carlos Simmerling⁴, Robert Mckenna², Michael Bieri⁵, Paul R Gooley⁵, Ben M Dunn², Gail E Fanucci⁶.

Abstract

HIV-1 protease is an essential enzyme for viral particle maturation and is a target in the fight against HIV-1 infection worldwide. Several natural polymorphisms are also associated with drug resistance. Here, we utilized both pulsed electron double resonance, also called double electron-electron resonance, and NMR (15)N relaxation measurements to characterize equilibrium conformational sampling and backbone dynamics of an HIV-1 protease construct containing four specific natural polymorphisms commonly found in subtypes A, F, and CRF_01 A/E. Results show enhanced backbone dynamics, particularly in the flap region, and the persistence of a novel conformational ensemble that we hypothesize is an alternative flap orientation of a curled open state or an asymmetric configuration when interacting with inhibitors.

Entities: Disease Species

Keywords: Electron Paramagnetic Resonance (EPR); Electron Spin-Label; Flap; HIV-1 Protease; Natural Occurring Polymorphism; Protein Dynamic; Protein Stability; Protein Structure; Pulsed Electron Double Resonance; Salt Bridge

Mesh：

Substances：
HIV Protease

Year: 2014 PMID： 24742668 PMCID： PMC4059161 DOI： 10.1074/jbc.M114.571836

Source DB: PubMed Journal: J Biol Chem ISSN： 0021-9258 Impact factor: 5.157

60 in total

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