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雄烯二醇调节小鼠对致命感染的全身抵抗力。

Androstenediol regulates systemic resistance against lethal infections in mice.

作者信息

Loria R M, Padgett D A

机构信息

Department of Microbiology and Immunology, Medical College of Virginia, Virginia Commonwealth University, Richmond.

出版信息

Arch Virol. 1992;127(1-4):103-15. doi: 10.1007/BF01309578.

Abstract

We previously reported that subcutaneous injection of DHEA (5-androsten-3 beta-ol-17-one, dehydroepiandrosterone) protected mice from lethal infection. This included both a lethal herpes virus type 2 encephalitis and a lethal systemic coxsackievirus B4 (CB4) infection. Androstenediol (5-androsten-3 beta-17 beta-diol, AED), a metabolic product of DHEA is up to 100 x more effective in regulating systemic resistance against lethal infection with CB 4 than its precursor DHEA. Compared to DHEA, treatment with AED was markedly superior in protecting mice against virus induced myocardiopathy, pancreopathy, and mortality. In addition to its protective effect, AED but not DHEA, induced a 3-4 fold proliferation of the spleen and thymus in virus infected animals; this effect of AED was only seen above a certain threshold dose. Neither steroid, however, has shown any significant direct antiviral effect in vitro; similarly, virus tissues titers in vivo are not affected by the hormones. Additionally, both DHEA and AED protected against a lethal infection with Enterococcus faecalis. These observations demonstrate that the steroid hormones DHEA and AED provide a novel approach for prevention and protection of the host from a variety of infectious diseases.

摘要

我们之前报道过,皮下注射脱氢表雄酮(5-雄烯-3β-醇-17-酮)可保护小鼠免受致死性感染。这包括致死性2型疱疹病毒性脑炎和致死性全身性柯萨奇病毒B4(CB4)感染。雄烯二醇(5-雄烯-3β-17β-二醇,AED)是脱氢表雄酮的一种代谢产物,在调节对CB4致死性感染的全身抵抗力方面,其效力比其前体脱氢表雄酮高100倍。与脱氢表雄酮相比,用AED治疗在保护小鼠免受病毒诱导的心肌病、胰腺炎和死亡方面明显更具优势。除了其保护作用外,AED而非脱氢表雄酮能使病毒感染动物的脾脏和胸腺增殖3至4倍;AED的这种作用仅在超过一定阈值剂量时才会出现。然而,这两种类固醇在体外均未显示出任何显著的直接抗病毒作用;同样,体内的病毒组织滴度也不受这些激素的影响。此外,脱氢表雄酮和AED都能保护小鼠免受粪肠球菌的致死性感染。这些观察结果表明,类固醇激素脱氢表雄酮和AED为预防和保护宿主免受多种传染病提供了一种新方法。

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