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[人泡沫病毒在转基因小鼠中的神经毒性]

[Neurotoxicity of human foamy virus in transgenic mice].

作者信息

Aguzzi A

机构信息

Institut für Neuropathologie, Departement Pathologie, Zürich, Schweiz.

出版信息

Verh Dtsch Ges Pathol. 1994;78:180-8.

PMID:7533983
Abstract

Human foamy virus (HFV) is a human retrovirus originally isolated from patients with various neoplastic and degenerative diseases. Similarly to other human retroviruses, HFV encodes the three structural retroviral genes, gag, pol and env, and an additional region containing three open reading frames, bel-1 to bel-3. Bel-1 activates transcription of the long terminal repeat of HFV and also of HIV. Until today it has not been possible to identify HFV as the causative agent of any disease. In order to identify a possible pathogenic potential of HFV, we have introduced parts of the HFV genome into the germ line of mice. Our studies with transgenic mice have shown that HFV transgenes encompassing the bel region are transiently transcribed between midgestation and birth at moderate levels in various tissues. Expression is then suppressed, but resumes after a latency of several weeks in a restricted range of tissues and accumulate extensively in single cells. This is associated with a progressive degenerative disease of the central nervous system and of striated muscle. These findings provide the first evidence of a disease induced by HFV and suggest that HFV might also act as a human pathogen in neurological diseases. Moreover, the transgenic mouse model will be useful for studying the molecular basis of HFV-induced neurotoxicity, the role of individual disease-associated HFV genes, and the regulation of retroviral latency.

摘要

人类泡沫病毒(HFV)是一种人类逆转录病毒,最初从患有各种肿瘤和退行性疾病的患者中分离出来。与其他人类逆转录病毒类似,HFV编码三种逆转录病毒结构基因,即gag、pol和env,以及一个包含三个开放阅读框(bel-1至bel-3)的额外区域。Bel-1可激活HFV以及HIV长末端重复序列的转录。直到如今,仍无法将HFV确定为任何疾病的病原体。为了确定HFV可能的致病潜力,我们已将部分HFV基因组导入小鼠种系。我们对转基因小鼠的研究表明,包含bel区域的HFV转基因在妊娠中期至出生期间在各种组织中以中等水平短暂转录。随后表达受到抑制,但在数周的潜伏期后,在有限范围的组织中恢复表达,并在单个细胞中大量积累。这与中枢神经系统和横纹肌的进行性退行性疾病有关。这些发现提供了HFV诱发疾病的首个证据,并表明HFV在神经疾病中也可能作为人类病原体起作用。此外,转基因小鼠模型将有助于研究HFV诱导神经毒性的分子基础、单个疾病相关HFV基因的作用以及逆转录病毒潜伏期的调控。

相似文献

1
[Neurotoxicity of human foamy virus in transgenic mice].[人泡沫病毒在转基因小鼠中的神经毒性]
Verh Dtsch Ges Pathol. 1994;78:180-8.
2
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3
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The R region found in the human foamy virus long terminal repeat is critical for both Gag and Pol protein expression.在人类泡沫病毒长末端重复序列中发现的R区域对Gag和Pol蛋白的表达都至关重要。
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