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1,5-二氨基蒽醌的抗病毒及诱导干扰素特性

Antiviral and interferon-inducing properties of 1,5-diamino anthraquinones.

作者信息

Stringfellow D A, Weed S D, Underwood G E

出版信息

Antimicrob Agents Chemother. 1979 Jan;15(1):111-8. doi: 10.1128/AAC.15.1.111.

Abstract

A series of anthraquinones with amino substituents at the 1,5 positions were found to induce interferon in mice. A prototype compound, 1,5-bis[(3-morpholinopropyl)amino]-anthraquinone (Ia), was an effective antiviral agent when administered either orally or parenterally. Peak interferon titers were found 12 to 24 h after drug treatment. The minimum oral dose of Ia required to induce serum interferon or to protect mice against a lethal virus infection was 62 mg/kg. Mice tolerated an oral dose of at least 30 times this minimum effective dose. A single dose of Ia given up to 6 days prior to infection had significant protective activity. Biological properties of Ia were compared with those of three other 1,5-diamino anthraquinones, which also induced interferon and demonstrated antiviral activity in mice. The most active compound was 1,5-bis[[2-(diethylamino)ethyl]amino]-anthraquinone (Ib), which protected mice against virus infection at a dose as low as 8 mg/kg (less than 1/60 its maximum tolerated dose). Mice developed hyporeactivity to interferon induction if the same inducer was injected daily, although by alternating between different inducers the loss of interferon responsiveness could be avoided.

摘要

发现一系列在1,5位带有氨基取代基的蒽醌能在小鼠体内诱导产生干扰素。一种原型化合物,1,5-双[(3-吗啉丙基)氨基]-蒽醌(Ia),经口服或非肠道给药时是一种有效的抗病毒剂。在药物治疗后12至24小时发现干扰素滴度达到峰值。诱导血清干扰素或保护小鼠免受致命病毒感染所需的Ia最小口服剂量为62毫克/千克。小鼠能耐受至少是该最小有效剂量30倍的口服剂量。在感染前6天内给予单次剂量的Ia具有显著的保护活性。将Ia的生物学特性与其他三种1,5-二氨基蒽醌的特性进行了比较,这三种蒽醌也能诱导干扰素并在小鼠体内显示出抗病毒活性。活性最高的化合物是1,5-双[[2-(二乙氨基)乙基]氨基]-蒽醌(Ib),它能以低至8毫克/千克的剂量(不到其最大耐受剂量的1/60)保护小鼠免受病毒感染。如果每天注射相同的诱导剂,小鼠会对干扰素诱导产生低反应性,不过通过交替使用不同的诱导剂可以避免干扰素反应性的丧失。

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