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一个高度扩增的小鼠基因与人类干扰素应答性Sp100基因同源,该基因编码一种与核点相关的自身抗原。

A highly amplified mouse gene is homologous to the human interferon-responsive Sp100 gene encoding an autoantigen associated with nuclear dots.

作者信息

Grötzinger T, Jensen K, Guldner H H, Sternsdorf T, Szostecki C, Schwab M, Savelyeva L, Reich B, Will H

机构信息

Heinrich-Pette-Institut für Experimentelle Virologie und Immunologie an der Universität Hamburg, Germany.

出版信息

Mol Cell Biol. 1996 Mar;16(3):1150-6. doi: 10.1128/MCB.16.3.1150.

Abstract

In human cells, three proteins are currently known to colocalize in di screte nuclear domains (designated nuclear dots): Sp100, a transcription-activating protein autoantigenic primarily in patients with primary biliary cirrhosis; PML, a tumor suppressor protein involved in development of acute promyelocytic leukemia; and NDP52, a protein of unknown function. Here we report sequence similarities between the Sp100 protein and a putative protein encoded by a highly amplified mouse gene which is visible as an inherited homogeneously staining region (HSR) on chromosome 1 of some mouse populations. By in situ hybridization, the Sp100 gene was mapped to locus 2q37, the syntenic region of the HSR on mouse chromosome 1. Unlike the highly amplified mouse gene, Sp100 was found to be a single-copy gene and showed no restriction fragment length polymorphisms. Sequence similarities in the promoter regions and similar exon-intron organizations of the two genes were revealed. As for Sp100, steady-state levels of the mRNAs of the HSR-encoded genes could be greatly increased by interferon (IFN) treatment. As in human cells, IFN treatment led to an enlargement in both size and number of nuclear dots in mouse cells as visualized by immunofluorescence staining with autoimmune sera from patients with primary biliary cirrhosis. These data indicate that a gene located in the inherited HSR of mice, designated mSp100, is homologous to the human Sp100 gene, has a similar gene organization, and responds similarly to IFN treatment.

摘要

在人类细胞中,目前已知三种蛋白质共定位于离散的核结构域(称为核点):Sp100,一种主要在原发性胆汁性肝硬化患者中具有自身抗原性的转录激活蛋白;PML,一种参与急性早幼粒细胞白血病发生的肿瘤抑制蛋白;以及NDP52,一种功能未知的蛋白质。在此我们报告Sp100蛋白与一个由高度扩增的小鼠基因编码的推定蛋白之间的序列相似性,该基因在一些小鼠群体的1号染色体上作为一个遗传性均匀染色区(HSR)可见。通过原位杂交,Sp100基因被定位到2q37位点,即小鼠1号染色体上HSR的同线区域。与高度扩增的小鼠基因不同,Sp100被发现是一个单拷贝基因,且未显示出限制性片段长度多态性。揭示了两个基因启动子区域的序列相似性以及相似的外显子-内含子组织。对于Sp100而言,HSR编码基因的mRNA稳态水平可通过干扰素(IFN)处理而大幅增加。与在人类细胞中一样,IFN处理导致小鼠细胞中核点的大小和数量均增加,这通过用原发性胆汁性肝硬化患者的自身免疫血清进行免疫荧光染色得以观察到。这些数据表明,位于小鼠遗传性HSR中的一个基因,命名为mSp100,与人类Sp100基因同源,具有相似的基因组织,并且对IFN处理的反应相似。

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