Synthesis and stability studies of phosphonoformate–amino acid conjugates: a new class of slowly releasing foscarnet prodrugs

Prodrugs of phosphonoformic acid (PFA), an anti-viral agent used clinically as the trisodium salt (foscarnet), are of interest due to the low bioavailability of the parent drug, which severely limits its utility. Neutral PFA triesters are known to be susceptible to P–C bond cleavage under hydrolytic...

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Bibliographic Details
Published in:Bioorganic & medicinal chemistry letters 2004-04, Vol.14 (7), p.1787-1790
Main Authors: Marma, Mong S, Kashemirov, Boris A, McKenna, Charles E
Format: Article
Language:English
Subjects:
Amino Acids - chemical synthesis
Amino Acids - pharmacokinetics
Antibiotics. Antiinfectious agents. Antiparasitic agents
Antiviral agents
Biological and medical sciences
Chemistry
Delayed-Action Preparations - chemical synthesis
Delayed-Action Preparations - pharmacokinetics
Drug Stability
Exact sciences and technology
Foscarnet - chemical synthesis
Foscarnet - pharmacokinetics
Medical sciences
Organic chemistry
Organometalloidal and organometallic compounds
P derivatives
Pharmacology. Drug treatments
Preparations and properties
Prodrugs - chemical synthesis
Prodrugs - pharmacokinetics
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Summary:Prodrugs of phosphonoformic acid (PFA), an anti-viral agent used clinically as the trisodium salt (foscarnet), are of interest due to the low bioavailability of the parent drug, which severely limits its utility. Neutral PFA triesters are known to be susceptible to P–C bond cleavage under hydrolytic de-esterification conditions, and it was previously found that P,C-dimethyl PFA P–N conjugates with amino acid ethyl esters did not release PFA at pH 7, and could not be fully deprotected under either acid or basic conditions, which led, respectively, to premature cleavage of the P–N linkage (with incomplete deprotection of the PFA ester moiety), or to P–C cleavage. Here we report that novel, fully deprotected PFA-amino acid P–N conjugates 4 can be prepared via coupling of C-methyl PFA dianion 2 with C-ethyl-protected amino acids using aqueous EDC, which gives a stable monoanionic intermediate 3 that resists P–C cleavage during subsequent alkaline deprotection of the two carboxylate ester groups. At 37 °C, the resulting new PFA-amino acid (Val, Leu, Phe) conjugates ( 4a– c) undergo P–N cleavage near neutral pH, cleanly releasing PFA. A kinetic investigation of 4a hydrolysis at pH values 6.7, 7.2, and 8.5 showed that PFA release was first-order in [ 4a] with respective t 1/2 values of 1.4, 3.8, and 10.6 h. A new class of foscarnet prodrug has been prepared. The prodrugs slowly release foscarnet at physiological pH and temperature.
ISSN:0960-894X
1464-3405
DOI:10.1016/j.bmcl.2004.01.016