HIV-1 Protease Uses Bi-Specific S2/S2′ Subsites to Optimize Cleavage of Two Classes of Target Sites

Marc Potempa; Sook Kyung Lee; Nese Kurt Yilmaz; Ellen A. Nalivaika; Amy Rogers; Ean Spielvogel; Charles W. Carter; Celia A. Schiffer; Ronald Swanstrom

doi:https://doi.org/10.1016/j.jmb.2018.10.022

doi.org/10.1016/j.jmb.2018.10.022

HIV-1 Protease Uses Bi-Specific S2/S2′ Subsites to Optimize Cleavage of Two Classes of Target Sites

,

,

..., Ronald Swanstrom

25

Journal of Molecular Biology5.60

Volume: 430, Issue: 24, Pages: 5182 - 5195

Published: Dec 1, 2018

Abstract

Retroviral proteases (PRs) have a unique specificity that allows cleavage of sites with or without a P1' proline. A P1' proline is required at the MA/CA cleavage site due to its role in a post-cleavage conformational change in the capsid protein. However, the HIV-1 PR prefers to have large hydrophobic amino acids flanking the scissile bond, suggesting that PR recognizes two different classes of substrate sequences. We analyzed the cleavage rate...

Paper Fields

Paper Details

Title

HIV-1 Protease Uses Bi-Specific S2/S2′ Subsites to Optimize Cleavage of Two Classes of Target Sites

DOI

doi.org/10.1016/j.jmb.2018.10.022

Published Date

Dec 1, 2018

Journal

Journal of Molecular Biology

Volume

430

Issue

24

Pages

5182 - 5195

Citation AnalysisPro

You’ll need to upgrade your plan to Pro

Looking to understand the true influence of a researcher’s work across journals & affiliations?

Scinapse’s Top 10 Citation Journals & Affiliations graph reveals the quality and authenticity of citations received by a paper.
Discover whether citations have been inflated due to self-citations, or if citations include institutional bias.

Learn more

Notes

History