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Torpor: The Rise and Fall of 3-Monoiodothyronamine from Brain to Gut—From Gut to Brain?

机译:托普尔:3-单硫代乙胺从脑到肠的兴衰-从肠到脑?

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摘要

3-Monoiodothyronamine (T1AM), first isolated from rat brain, is reported to be an endogenous, rapidly acting metabolite of thyroxine. One of its numerous effects is the induction of a “torpor-like” state in experimental animals. A critical analysis of T1AM, to serve as an endogenous cryogen, is given. The proposed biosynthetic pathway for formation of T1AM, which includes deiodinases and ornithine decarboxylase in the upper intestinum, is an unusual one. To reach the brain via systemic circulation, enterohepatic recycling and passage through the liver may occur. The possible role of gut microbiota is discussed. T1AM concentrations in human serum, measured by a specific monoclonal assay are up to three orders of magnitude higher compared to values obtained by MS/MS technology. The difference is explained by the presence of a high-affinity binder for T1AM (Apolipoprotein B-100) in serum, which permits the immunoassay to measure the total concentration of the analyte but limits MS/MS technology to detect only the unbound (free) analyte, a view, which is contested here.
机译:据报道,最早从大鼠大脑中分离出的 3-单硫代胸腺嘧啶(T1AM)是甲状腺素的内源性,作用迅速的代谢产物。其众多作用之一是在实验动物中诱发“ torpor-like”状态。给出了用作内源性冷冻剂的T1AM的临界分析。拟议的T1AM形成的生物合成途径是一种不寻常的途径,其中包括上小肠中的碘化酶和鸟氨酸脱羧酶。为了通过全身循环到达大脑,可能会发生肝肠循环和通过肝脏。讨论了肠道菌群的可能作用。与通过MS / MS技术获得的值相比,通过特定的单克隆测定法测量的人血清中的T1AM浓度高出三个数量级。差异可以通过血清中T1AM(载脂蛋白B-100)的高亲和力结合剂来解释,该结合剂可以进行免疫测定来测量分析物的总浓度,但限制了MS / MS技术只能检测未结合的(游离)分析物,一种观点,在这里引起争议。

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