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Discovery of GS-9131: Design, synthesis and optimization of amidate prodrugs of the novel nucleoside phosphonate HIV reverse transcriptase (RT) inhibitor GS-9148
Richard L. Mackman ,
Adrian S. Ray ,
Hon C. Hui ,
Lijun Zhang ,
Gabriel Birkus ,
Constantine G. Boojamra ,
Manoj C. Desai ,
Janet L. Douglas ,
Ying Gao ,
Deborah Grant ,
Genevieve Laflamme ,
Kuei-Ying Lin ,
David Y. Markevitch ,
Ruchika Mishra ,
Martin McDermott ,
Rowchanak Pakdaman ,
Oleg V. Petrakovsky ,
Jennifer E. Vela ,
Tomas Cihlar
May 2010
May 2010
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Abstract
GS-9148 [(5-(6-amino-purin-9-yl)-4-fluoro-2,5-dihydro-furan-2-yloxymethyl)phosphonic
acid] 4 is a novel nucleoside phosphonate HIV-1 reverse transcriptase (RT) inhibitor
with a unique resistance profile toward N(t)RTI resistance mutations. To effectively
deliver 4 and its active phosphorylated metabolite 15 into target cells, a series
of amidate prodrugs were designed as substrates of cathepsin A, an intracellular lysosomal
carboxypeptidase highly expressed in peripheral blood mononuclear cells (PBMCs). The
ethylalaninyl phosphonamidate prodrug 5 (GS-9131) demonstrated favorable cathepsin
A substrate properties, in addition to favorable in vitro intestinal and hepatic stabilities.
Following oral dosing (3mg/kg) in Beagle dogs, high levels (>9.0microM) of active
metabolite 15 were observed in PBMCs, validating the prodrug design process and leading
to the nomination of 5 as a clinical candidate.