Institute of Organic Chemistry and Biochemistry, Academy of Sciences of the Czech Republic, v.v.i., 166 10 Prague, Czech Republic.
Johns Hopkins Drug Discovery, Johns Hopkins University , Baltimore, Maryland 21205, United States.
J Med Chem. 2016 Mar 24;59(6):2810-9. doi: 10.1021/acs.jmedchem.6b00062. Epub 2016 Mar 10.
2-Phosphonomethylpentanedioic acid (1, 2-PMPA) is a potent inhibitor of glutamate carboxypeptidase II which has demonstrated robust neuroprotective efficacy in many neurological disease models. However, 1 is highly polar containing a phosphonate and two carboxylates, severely limiting its oral bioavailability. We strategized to mask the polar groups via a prodrug approach, increasing the likelihood of passive oral absorption. Our initial strategy was to cover the phosphonate with hydrophobic moieties such as pivaloyloxymethyl (POM) and isopropyloxycarbonyloxymethyl (POC) while keeping the α- and γ-carboxylates unsubstituted. This attempt was unsuccessful due to the chemical instability of the bis-POC/POM derivatives. Addition of α,γ-diesters and α-monoesters enhanced chemical stability and provided excellent oral exposure in mice, but these mixed esters were too stable in vivo, resulting in minimal release of 1. By introducing POC groups on both the phosphonate and α-carboxylate, we synthesized Tris-POC-2-PMPA (21b), which afforded excellent release of 1 following oral administration in both mice and dog.
2-膦酸基甲基戊二酸(1,2-PMPA)是一种有效的谷氨酸羧肽酶 II 抑制剂,在许多神经疾病模型中显示出强大的神经保护作用。然而,1 具有很强的极性,含有一个膦酸酯和两个羧酸盐,严重限制了其口服生物利用度。我们通过前药策略来掩蔽极性基团,增加被动口服吸收的可能性。我们的初始策略是用疏水分子,如特戊酰氧甲基(POM)和异丙氧羰氧甲基(POC)覆盖膦酸酯,同时保持α-和γ-羧酸盐未取代。由于双 POC/POM 衍生物的化学不稳定性,这一尝试失败了。添加α,γ-二酯和α-单酯提高了化学稳定性,并在小鼠中提供了优异的口服暴露量,但这些混合酯在体内太稳定,导致 1 的释放量极小。通过在膦酸酯和α-羧酸盐上都引入 POC 基团,我们合成了 Tris-POC-2-PMPA(21b),在小鼠和狗中口服给药后,1 能够得到极好的释放。
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