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转甲状腺素蛋白对小鼠脑脊液中甲状腺素和β-淀粉样蛋白清除的影响。

Effects of transthyretin on thyroxine and β-amyloid removal from cerebrospinal fluid in mice.

作者信息

Chen Ruoli, Chen Carl P, Preston Jane E

机构信息

Institute of Pharmaceutical Science, King's College London, London, UK.

Institute of Science and Technology of Medicine, School of Pharmacy, Keele University, Staffordshire, UK.

出版信息

Clin Exp Pharmacol Physiol. 2016 Sep;43(9):844-50. doi: 10.1111/1440-1681.12598.

Abstract

Transthyretin (TTR) is a binding protein for the thyroid hormone thyroxine (T4 ), retinol and β-amyloid peptide. TTR aids the transfer of T4 from the blood to the cerebrospinal fluid (CSF), but also prevents T4 loss from the blood-CSF barrier. It is, however, unclear whether TTR affects the clearance of β-amyloid from the CSF. This study aimed to investigate roles of TTR in β-amyloid and T4 efflux from the CSF. Eight-week-old 129sv male mice were anaesthetized and their lateral ventricles were cannulated. Mice were infused with artificial CSF containing (125) I-T4 /(3) H-mannitol, or (125) I-Aβ40/(3) H-inulin, in the presence or absence of TTR. Mice were decapitated at 2, 4, 8, 16, 24 minutes after injection. The whole brain was then removed and divided into different regions. The radioactivities in the brain were determined by liquid scintillation counting. At baseline, the net uptake of (125) I-T4 into the brain was significantly higher than that of (125) I-Aβ40, and the half time for efflux was shorter ((125) I-T4 , 5.16; (3) H-mannitol, 7.44; (125) I-Aβ40, 8.34; (3) H-inulin, 10.78 minutes). The presence of TTR increased the half time for efflux of (125) I-T4 efflux, and caused a noticeable increase in the uptake of (125) I-T4 and (125) I-Aβ40 in the choroid plexus, whilst uptakes of (3) H-mannitol and (3) H-inulin remained similar to control experiments. This study indicates that thyroxine and amyloid peptide effuse from the CSF using different transporters. TTR binds to thyroxine and amyloid peptide to prevent the loss of thyroxine from the brain and redistribute amyloid peptide to the choroid plexus.

摘要

转甲状腺素蛋白(TTR)是甲状腺激素甲状腺素(T4)、视黄醇和β-淀粉样肽的结合蛋白。TTR有助于T4从血液转移至脑脊液(CSF),同时也能防止T4从血脑屏障流失。然而,目前尚不清楚TTR是否会影响脑脊液中β-淀粉样蛋白的清除。本研究旨在探究TTR在脑脊液中β-淀粉样蛋白和T4流出过程中的作用。将8周龄的129sv雄性小鼠麻醉后,在其侧脑室插入套管。在有或没有TTR的情况下,给小鼠输注含有(125)I-T4/(3)H-甘露醇或(125)I-Aβ40/(3)H-菊粉的人工脑脊液。注射后2、4、8、16、24分钟将小鼠断头。然后取出整个大脑并分成不同区域。通过液体闪烁计数法测定脑中的放射性。在基线时,(125)I-T4进入大脑的净摄取量显著高于(125)I-Aβ40,流出的半衰期较短((125)I-T4为5.16;(3)H-甘露醇为7.44;(125)I-Aβ40为8.34;(3)H-菊粉为10.78分钟)。TTR的存在增加了(125)I-T4流出的半衰期,并导致脉络丛中(125)I-T4和(125)I-Aβ40的摄取显著增加,而(3)H-甘露醇和(3)H-菊粉的摄取与对照实验相似。本研究表明,甲状腺素和淀粉样肽通过不同的转运体从脑脊液中流出。TTR与甲状腺素和淀粉样肽结合,以防止甲状腺素从大脑中流失,并将淀粉样肽重新分布到脉络丛。

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