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奥司他韦膦酸酯类似物的开发作为抗流感药物。

Development of oseltamivir phosphonate congeners as anti-influenza agents.

机构信息

The Genomics Research Center, Academia Sinica , No. 128, Sec. 2, Academia Road, Taipei 11529, Taiwan.

出版信息

J Med Chem. 2012 Oct 25;55(20):8657-70. doi: 10.1021/jm3008486. Epub 2012 Oct 12.

Abstract

Oseltamivir phosphonic acid (tamiphosphor, 3a), its monoethyl ester (3c), guanidino-tamiphosphor (4a), and its monoethyl ester (4c) are potent inhibitors of influenza neuraminidases. They inhibit the replication of influenza viruses, including the oseltamivir-resistant H275Y strain, at low nanomolar to picomolar levels, and significantly protect mice from infection with lethal doses of influenza viruses when orally administered with 1 mg/kg or higher doses. These compounds are stable in simulated gastric fluid, liver microsomes, and human blood and are largely free from binding to plasma proteins. Pharmacokinetic properties of these inhibitors are thoroughly studied in dogs, rats, and mice. The absolute oral bioavailability of these compounds was lower than 12%. No conversion of monoester 4c to phosphonic acid 4a was observed in rats after intravenous administration, but partial conversion of 4c was observed with oral administration. Advanced formulation may be investigated to develop these new anti-influenza agents for better therapeutic use.

摘要

奥司他韦膦酸(他拉米夫定,3a)、单乙酯(3c)、胍基他拉米夫定(4a)及其单乙酯(4c)是强效的流感神经氨酸酶抑制剂。它们在纳摩尔至皮摩尔的低浓度下就能抑制流感病毒的复制,包括对奥司他韦耐药的 H275Y 株,当以 1 毫克/千克或更高剂量口服给药时,能显著保护小鼠免受致死剂量流感病毒的感染。这些化合物在模拟胃液、肝微粒体和人血液中稳定,并且与血浆蛋白的结合率低。这些抑制剂的药代动力学特性在狗、大鼠和小鼠中得到了深入研究。这些化合物的绝对口服生物利用度低于 12%。在大鼠体内静脉注射后,未观察到单酯 4c 向膦酸 4a 的转化,但口服给药时观察到部分转化。可能会研究先进的制剂来开发这些新的抗流感药物,以更好地用于治疗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ff15/3492761/bce4aa670ee3/nihms411891f1.jpg

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