Literature DB >> 30809901

Pharmacokinetic stability of macrocyclic peptide triazole HIV-1 inactivators alone and in liposomes.

Rachna Aneja1, Antonella Grigoletto2, Aakansha Nangarlia1,3, Adel A Rashad1, Steven Wrenn4, Jeffrey M Jacobson5, Gianfranco Pasut2, Irwin Chaiken1.   

Abstract

Previously, we reported the discovery of macrocyclic peptide triazoles (cPTs) that bind to HIV-1 Env gp120, inhibit virus cell infection with nanomolar potencies, and cause irreversible virion inactivation. Given the appealing virus-killing activity of cPTs and resistance to protease cleavage observed in vitro, we here investigated in vivo pharmacokinetics of the cPT AAR029b. AAR029b was investigated both alone and encapsulated in a PEGylated liposome formulation that was designed to slowly release inhibitor. Pharmacokinetic analysis in rats showed that the half-life of FITC-AAR029b was substantial both alone and liposome-encapsulated, 2.92 and 8.87 hours, respectively. Importantly, liposome-encapsulated FITC-AAR029b exhibited a 15-fold reduced clearance rate from serum compared with the free FITC-cPT. This work thus demonstrated both the in vivo stability of cPT alone and the extent of pharmacokinetic enhancement via liposome encapsulation. The results obtained open the way to further develop cPTs as long-acting HIV-1 inactivators against HIV-1 infection.
© 2019 European Peptide Society and John Wiley & Sons, Ltd.

Entities:  

Keywords:  HIV-1; liposomes; macrocyclic peptide triazole; pharmacokinetic stability

Mesh:

Substances:

Year:  2019        PMID: 30809901      PMCID: PMC6467816          DOI: 10.1002/psc.3155

Source DB:  PubMed          Journal:  J Pept Sci        ISSN: 1075-2617            Impact factor:   1.905


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