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羊瘙痒症:一种病毒诱导的脑淀粉样变性的概念。

Scrapie: concept of a virus-induced amyloidosis of the brain.

作者信息

Braig H R, Diringer H

出版信息

EMBO J. 1985 Sep;4(9):2309-12. doi: 10.1002/j.1460-2075.1985.tb03931.x.

Abstract

After an intraperitoneal infection disease-specific incorporation of [3H]leucine into protein and [3H]uridine into RNA in the brain precede clinical scrapie in hamsters. Onset of both incorporations are the earliest measurable events in the disease. Infectivity and subsequent clinical symptoms appear only after this biochemical activity has ceased. The disease-specific [3H]protein co-purifies with scrapie-associated fibrils (SAF) and infectivity during differential centrifugation and buffer extraction. SDS-PAGE shows that the [3H]protein is not SAF protein but a protein with an apparently higher mol. wt. The [3H]RNA is metabolically stable and separates from SAF and the main portion of infectivity in the last step of the purification. The appearance of SAF-protein is a late event and correlates with severe clinical symptoms. SAF seems to be derived from a brain protein turning over slowly. Our data are consistent with early pre-clinical virus replication. In this case treatment aimed at suppressing virus replication in the clinical phase of the human Creutzfeldt-Jakob disease is unlikely to produce any beneficial effect.

摘要

腹腔感染后,仓鼠脑中[3H]亮氨酸特异性掺入蛋白质以及[3H]尿苷掺入RNA的过程先于临床瘙痒病出现。这两种掺入的开始是该疾病中最早可测量的事件。只有在这种生化活性停止后,传染性和随后的临床症状才会出现。在差速离心和缓冲液提取过程中,疾病特异性的[3H]蛋白质与瘙痒病相关纤维(SAF)和传染性共同纯化。SDS-PAGE显示,[3H]蛋白质不是SAF蛋白质,而是一种分子量明显更高的蛋白质。[3H]RNA在代谢上是稳定的,并且在纯化的最后一步与SAF和大部分传染性分离。SAF蛋白质的出现是一个晚期事件,与严重的临床症状相关。SAF似乎源自一种周转缓慢的脑蛋白。我们的数据与临床前早期病毒复制一致。在这种情况下,旨在抑制人类克雅氏病临床阶段病毒复制的治疗不太可能产生任何有益效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f3d/554502/9d27c8152f5d/emboj00274-0159-a.jpg

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