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由突变基因lpr诱导的异常。纯合和杂合lpr的SJL/J小鼠的疾病模式和鼠白血病病毒的表达。

Abnormalities induced by the mutant gene, lpr. Patterns of disease and expression of murine leukemia viruses in SJL/J mice homozygous and heterozygous for lpr.

作者信息

Morse H C, Roths J B, Davidson W F, Langdon W Y, Fredrickson T N, Hartley J W

出版信息

J Exp Med. 1985 Mar 1;161(3):602-16. doi: 10.1084/jem.161.3.602.

Abstract

SJL/J mice heterozygous or homozygous for the lpr mutation were compared with SJL/J-+/+ mice for longevity, histopathology, antigenic characteristics of lymphocytes and expression of murine leukemia viruses (MuLV). In comparison to +/+ mice, lpr homozygotes had a markedly shortened life span, died with infiltrative pulmonary disease, but little or no renal disease, and expressed high levels of infectious ecotropic MuLV in lymphoid tissues. SJL-lpr/+ mice had a life span intermediate between SJL-+/+ and -lpr/lpr mice, died with lymphomas that histologically resembled the neoplasms of +/+ mice, and sometimes expressed high levels of ecotropic MuLV. The lymphomas of lpr/+ could be transplanted to +/+ recipients in 78% of cases, and continuous in vitro lines were established from some of them. Similar effects on virus expression or lymphoma development were not observed in other strains homozygous or heterozygous for the lpr mutation. These results indicate that the diseases expressed by mice homozygous for the lpr mutation are highly strain-dependent, and that this gene can have an effect in the heterozygous state in SJL mice.

摘要

将 lpr 突变杂合或纯合的 SJL/J 小鼠与 SJL/J-+/+ 小鼠在寿命、组织病理学、淋巴细胞抗原特性及鼠白血病病毒(MuLV)表达方面进行比较。与 +/+ 小鼠相比,lpr 纯合子寿命显著缩短,死于浸润性肺部疾病,但肾脏疾病很少或没有,且在淋巴组织中表达高水平的感染性亲嗜性 MuLV。SJL-lpr/+ 小鼠寿命介于 SJL-+/+ 和 -lpr/lpr 小鼠之间,死于组织学上类似于 +/+ 小鼠肿瘤的淋巴瘤,且有时表达高水平的亲嗜性 MuLV。lpr/+ 的淋巴瘤在 78% 的病例中可移植到 +/+ 受体,并且从其中一些建立了连续的体外细胞系。在 lpr 突变纯合或杂合的其他品系中未观察到对病毒表达或淋巴瘤发展的类似影响。这些结果表明,lpr 突变纯合小鼠所表现出的疾病高度依赖于品系,并且该基因在 SJL 小鼠的杂合状态下可产生影响。

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