首页> 美国卫生研究院文献>The Journal of Neuroscience >Serum Transthyretin Monomer as a Possible Marker of Blood-to-CSF Barrier Disruption
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Serum Transthyretin Monomer as a Possible Marker of Blood-to-CSF Barrier Disruption

机译:血清运甲状腺素蛋白单体可能是血脑脊液屏障破坏的标志物

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摘要

The CNS is shielded from systemic influences by two separate barriers, the blood–brain barrier (BBB) and the blood-to-CSF barrier. Failure of either barrier bears profound significance in the etiology and diagnosis of several neurological diseases. Furthermore, selective opening of BBB tight junctions provides an opportunity for delivery of otherwise BBB impermeant drugs. Peripheral assessment of BBB opening can be achieved by detection in blood of brain-specific proteins that extravasate when these endothelial junctions are breached. We developed a proteomic approach to discover clusters of CNS-specific proteins with extravasation into serum that correlates with BBB openings. Protein profiles from blood samples obtained from patients undergoing iatrogenic BBB disruption (BBBD) with intra-arterial hyperosmotic mannitol were compared with pre-BBB opening serum. A low molecular weight protein (14 kDa) identified by mass spectroscopy as transthyretin (TTR) consistently correlated with BBBD. Protein gel electrophoresis and immunodetection confirmed that TTR was indeed extravasated in its monomeric form when CNS barriers were breached. The time course of TTR extravasation was compared with release from the brain of another BBB integrity marker, S-100β (11 kDa). Kinetic analysis revealed that the appearance of S-100β, presumably originating from perivascular astrocytic end feet, preceded extravasation of TTR by several minutes. Because TTR is localized primarily in choroid plexus and, as a soluble monomer, in CSF, we concluded that although S-100β is a marker of BBB integrity, TTR instead may be a peripheral tracer of blood-to-cerebrospinal barrier.
机译:中枢神经系统通过两个独立的屏障,即血脑屏障(BBB)和血液对脑脊液屏障,免受系统性影响。任一障碍的失败对几种神经系统疾病的病因和诊断都具有深远的意义。此外,BBB紧密连接的选择性开放为其他BBB不渗透药物的输送提供了机会。通过在血液中检测这些内皮连接处被破坏时渗出的脑特异性蛋白,可以实现对血脑屏障开放性的外围评估。我们开发了一种蛋白质组学方法,以发现具有渗入血清的中枢神经系统特异性蛋白簇,这些蛋白与BBB开口有关。将来自患有动脉内高渗甘露醇的医源性BBB破坏(BBBD)患者的血液样品中的蛋白质谱与BBB前开放血清进行比较。被质谱鉴定为运甲状腺素蛋白(TTR)的低分子量蛋白质(14 kDa)与BBBD始终相关。蛋白质凝胶电泳和免疫检测证实,当突破CNS屏障时,TTR确实以其单体形式溢出。将TTR外渗的时间过程与另一种BBB完整性标志物S-100β(11 kDa)从大脑中释放进行了比较。动力学分析表明,S-100β的出现可能是由TTR外渗所致,而S-100β可能起源于血管周围的星形细胞末端脚。因为TTR主要位于脉络丛中,并且作为可溶性单体位于CSF中,所以我们得出结论,尽管S-100β是BBB完整性的标志物,但TTR可能是血脑屏障的外周示踪剂。

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