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人泡沫病毒蛋白在神经元中积累,并在转基因小鼠大脑中诱导形成多核巨细胞。

Human foamy virus proteins accumulate in neurons and induce multinucleated giant cells in the brain of transgenic mice.

作者信息

Aguzzi A, Wagner E F, Netzer K O, Bothe K, Anhauser I, Rethwilm A

机构信息

Institute of Molecular Pathology, Vienna, Austria.

出版信息

Am J Pathol. 1993 Apr;142(4):1061-71.

Abstract

Human foamy virus (HFV) is a retrovirus encoding structural genes and, like human immunodeficiency virus and human T cell leukemia virus I, several ancillary reading frames collectively termed the be1 genes. We have previously shown that HFV transgenic mice develop an encephalopathy with neuronal loss in hippocampus and cerebral cortex. We have now raised and characterized rabbit antisera to various recombinant portions of gag, pol, env, and bel-1, the viral trans-activator. Immunoreactivity for gag and bel-1 was observed in nuclei and processes of hippocampal and cortical neurons before the onset of morphological lesions and correlated with the appearance of HFV mRNA. Astrocyte-derived multinucleated giant cells containing HFV proteins were present in the brain of transgenic mice coexpressing full-length HFV genes but not in mice expressing truncated gag and env, suggesting that these genes contain a fusogenic domain. Expression of full-length structural genes decreased the life expectancy of transgenic mice, implying an adjuvant role for these proteins in HFV-induced brain damage.

摘要

人泡沫病毒(HFV)是一种逆转录病毒,编码结构基因,并且与人类免疫缺陷病毒和人类T细胞白血病病毒I一样,有几个辅助阅读框统称为be1基因。我们之前已经表明,HFV转基因小鼠会出现脑病,海马体和大脑皮层中的神经元会丢失。我们现在制备了针对gag、pol、env和病毒反式激活因子bel-1的各种重组部分的兔抗血清,并对其进行了表征。在形态学病变出现之前,在海马体和皮层神经元的细胞核及突起中观察到了对gag和bel-1的免疫反应性,这与HFV mRNA的出现相关。在共表达全长HFV基因的转基因小鼠大脑中存在含有HFV蛋白的星形胶质细胞来源的多核巨细胞,但在表达截短的gag和env的小鼠大脑中则不存在,这表明这些基因含有一个融合结构域。全长结构基因的表达降低了转基因小鼠的预期寿命,这意味着这些蛋白在HFV诱导的脑损伤中起辅助作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a69d/1886887/c4916a398c35/amjpathol00076-0103-a.jpg

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