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Literature DB >> 18312292

Inhibition of HIV-2 protease by HIV-1 protease inhibitors in clinical use.

Evan T Brower¹, Usman M Bacha, Yuko Kawasaki, Ernesto Freire.

Abstract

Over the past 10 years, protease inhibitors have been a key component in antiretroviral therapies for HIV/AIDS. While the vast majority of HIV/AIDS cases in the world are due to HIV-1, HIV-2 infection must also be addressed. HIV-2 is endemic to Western Africa, and has also appeared in European countries such as Portugal, Spain, and Estonia. Current protease inhibitors have not been optimized for treatment of HIV-2 infection; therefore, it is important to assess the effectiveness of currently FDA-approved protease inhibitors against the HIV-2 protease, which shares only 50% sequence identity with the HIV-1 protease. Kinetic inhibition assays were performed to measure the inhibition constants (K(i)) of the HIV-1 protease inhibitors indinavir, nelfinavir, saquinavir, ritonavir, amprenavir, lopinavir, atazanavir, tipranavir, and darunavir against the HIV-2 protease. Lopinavir, saquinavir, tipranavir, and darunavir exhibit the highest potency with K(i) values of 0.7, 0.6, 0.45, and 0.17 nm, respectively. These K(i) values are 84, 2, 24, and 17 times weaker than the corresponding values against the HIV-1 protease. In general, inhibitors show K(i) ratios ranging between 2 and 80 for the HIV-2 and HIV-1 proteases. The relative drop in potency is proportional to the affinity of the inhibitor against the HIV-1 protease and is related to specific structural characteristics of the inhibitors. In particular, the potency drop is high when the maximum cap size of the inhibitors consists of very few atoms. Caps are groups located at the periphery of the molecule that are added to core structures to increase the specificity of the inhibitor to its target. The caps positioned on the HIV-1 protease inhibitors affect selectivity through interactions with distinct regions of the binding pocket. The flexibility and adaptability imparted by the higher number of rotatable bonds in large caps enables an inhibitor to accommodate changes in binding pocket geometry between HIV-1 and HIV-2 protease.

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Year: 2008 PMID： 18312292 DOI： 10.1111/j.1747-0285.2008.00647.x

Source DB: PubMed Journal: Chem Biol Drug Des ISSN： 1747-0277 Impact factor: 2.817

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Cited

45 in total

1. Saquinavir inhibits early events associated with establishment of HIV-1 infection: potential role for protease inhibitors in prevention.

Authors: Martha Stefanidou; Carolina Herrera; Naomi Armanasco; Robin J Shattock
Journal: Antimicrob Agents Chemother Date: 2012-06-04 Impact factor: 5.191

2. Revealing the dimer dissociation and existence of a folded monomer of the mature HIV-2 protease.

Authors: John M Louis; Rieko Ishima; Annie Aniana; Jane M Sayer
Journal: Protein Sci Date: 2009-12 Impact factor: 6.725

3. Inhibition of autoprocessing of natural variants and multidrug resistant mutant precursors of HIV-1 protease by clinical inhibitors.

Authors: John M Louis; Annie Aniana; Irene T Weber; Jane M Sayer
Journal: Proc Natl Acad Sci U S A Date: 2011-05-16 Impact factor: 11.205

4. How much binding affinity can be gained by filling a cavity?

Authors: Yuko Kawasaki; Eduardo E Chufan; Virginie Lafont; Koushi Hidaka; Yoshiaki Kiso; L Mario Amzel; Ernesto Freire
Journal: Chem Biol Drug Des Date: 2009-12-17 Impact factor: 2.817

Review 5. Highly resistant HIV-1 proteases and strategies for their inhibition.

Authors: Irene T Weber; Daniel W Kneller; Andres Wong-Sam
Journal: Future Med Chem Date: 2015 Impact factor: 3.808

6. Complex patterns of protease inhibitor resistance among antiretroviral treatment-experienced HIV-2 patients from Senegal: implications for second-line therapy.

Authors: Dana N Raugi; Robert A Smith; Selly Ba; Macoumba Toure; Fatou Traore; Fatima Sall; Charlotte Pan; Lindsey Blankenship; Alexandra Montano; Julia Olson; Ndeye Mery Dia Badiane; James I Mullins; Nancy B Kiviat; Stephen E Hawes; Papa Salif Sow; Geoffrey S Gottlieb
Journal: Antimicrob Agents Chemother Date: 2013-04-09 Impact factor: 5.191

Review 7. Bacterial proteases: targets for diagnostics and therapy.

Authors: W E Kaman; J P Hays; H P Endtz; F J Bikker
Journal: Eur J Clin Microbiol Infect Dis Date: 2014-02-18 Impact factor: 3.267

8. Interactions of different inhibitors with active-site aspartyl residues of HIV-1 protease and possible relevance to pepsin.

Authors: Jane M Sayer; John M Louis
Journal: Proteins Date: 2009-05-15

9. Emergence of multiclass drug-resistance in HIV-2 in antiretroviral-treated individuals in Senegal: implications for HIV-2 treatment in resouce-limited West Africa.

Authors: Geoffrey S Gottlieb; Ndeye Mery Dia Badiane; Stephen E Hawes; Louise Fortes; Macoumba Toure; Cheikh T Ndour; Alison K Starling; Fatou Traore; Fatima Sall; Kim G Wong; Stephen L Cherne; Donovan J Anderson; Stefanie A Dye; Robert A Smith; James I Mullins; Nancy B Kiviat; Papa Salif Sow
Journal: Clin Infect Dis Date: 2009-02-15 Impact factor: 9.079

Review 10. Atazanavir: its role in HIV treatment.

Authors: Robin Wood
Journal: Expert Rev Anti Infect Ther Date: 2008-12 Impact factor: 5.091