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The evolution of transthyretin synthesis in the choroid plexus.

机译:脉络丛中运甲状腺素蛋白合成的演变。

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摘要

Choroid plexus has the highest concentration of transthyretin (TTR) mRNA in the body, 4.4 microg TTR mRNA/g wet weight tissue, compared with 0.39 microg in the liver. The proportion of TTR to total protein synthesis in choroid plexus is 12%. All newly synthesized TTR is secreted towards the ventricles. Net transfer of T4 occurs only towards the ventricle and depends on ongoing protein synthesis. Thyroxine-binding globulin (TBG), TTR and albumin form a "buffering" system for plasma [T4] because of their overlapping affinities and on/off rates for L-thyroxine (T4)-binding. The individual components of this network determining T4 distribution are functionally highly redundant. Absence of TBG (humans), or TTR (mice), or albumin (humans, rats) is not associated with hypothyroidism. Natural selection is based on small, inheritable alterations improving function. The study of these alterations can identify function. TTR genes were cloned and sequenced for a large number of vertebrate species. Systematic, stepwise changes during evolution occurred only in the N-terminal region, which became shorter and more hydrophilic. Simultaneously, a change in function occurred: TTR affinities for T4 are higher in mammals than in reptiles and birds. L-triiodothyronine (T3) affinities show the opposite trend. This favors site-specific regulation of thyroid hormones by tissue-specific deiodinases in the brain.
机译:脉络丛中的甲状腺素转运蛋白(TTR)mRNA浓度最高,为4.4微克TTR mRNA / g湿重组织,而肝脏为0.39微克。脉络丛中TTR与总蛋白合成的比例为12%。所有新合成的TTR都向心室分泌。 T4的净转移仅发生在脑室,并取决于正在进行的蛋白质合成。甲状腺素结合球蛋白(TBG),TTR和白蛋白形成血浆[T4]的“缓冲”系统,因为它们的亲和力和L-甲状腺素(T4)结合的开/关速率都很高。该网络中确定T4分布的各个组件在功能上是高度冗余的。缺乏TBG(人类)或TTR(小鼠)或白蛋白(人类,大鼠)与甲状腺功能减退无关。自然选择是基于小的,可继承的改进功能。对这些变化的研究可以确定功能。克隆了大量的脊椎动物物种的TTR基因并进行了测序。进化过程中的系统性,逐步变化仅发生在N末端区域,该区域变得更短且更具亲水性。同时,功能发生了变化:哺乳动物的TTR对T4的亲和力高于爬行动物和鸟类。 L-triiodothyronine(T3)亲和力显示相反的趋势。这有利于大脑中组织特异性脱碘酶对甲状腺激素的位点特异性调节。

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