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一个新的基因座在与BALB/c杂交时,调控新西兰小鼠的逆转录病毒糖蛋白70和抗糖蛋白70抗体的产生。

A novel locus regulates both retroviral glycoprotein 70 and anti-glycoprotein 70 antibody production in New Zealand mice when crossed with BALB/c.

作者信息

Rigby Robert J, Rozzo Stephen J, Gill Herpreet, Fernandez-Hart Timothy, Morley Bernard J, Izui Shozo, Kotzin Brian L, Vyse Timothy J

机构信息

Rheumatology Section, Imperial College Faculty of Medicine, Hammersmith Campus, London, United Kingdom.

出版信息

J Immunol. 2004 Apr 15;172(8):5078-85. doi: 10.4049/jimmunol.172.8.5078.

Abstract

Lupus-prone New Zealand Black and New Zealand White mice produce high serum levels of the endogenous retroviral envelope protein gp70 and develop an Ab response to this autoantigen as part of their autoimmune disease. Linkage analysis of two crosses involving New Zealand and BALB/c mice mapped these traits to a group of overlapping loci, including a novel locus on proximal chromosome 12. This locus was linked with serum gp70 and the autoimmune response against it. The linkage of serum gp70 levels to a previously described locus on distal chromosome 4 was also confirmed. Sequence analysis of a candidate gene on distal chromosome 4, Fv1, provided support that this gene may be associated with the control of serum gp70 levels in both New Zealand Black and New Zealand White mice. Linkage data and statistical analysis confirmed a close correlation between gp70 Ag and anti-gp70 Ab levels, and together gave support to the concept that a threshold level of gp70 is required for the production of anti-gp70 Abs. Serum levels of anti-gp70 Abs were closely correlated with the presence of renal disease, more so than anti-dsDNA Abs. Understanding the genetic basis of this complex autoantigen-autoantibody system will provide insight into the pathogenesis of lupus in mice, which may have implications for human disease.

摘要

易患狼疮的新西兰黑鼠和新西兰白鼠血清中内源性逆转录病毒包膜蛋白gp70水平较高,并作为自身免疫性疾病的一部分,对这种自身抗原产生抗体反应。对涉及新西兰小鼠和BALB/c小鼠的两个杂交组合进行连锁分析,将这些性状定位到一组重叠基因座,包括近端12号染色体上的一个新基因座。该基因座与血清gp70及其自身免疫反应相关。血清gp70水平与远端4号染色体上一个先前描述的基因座的连锁关系也得到了证实。对远端4号染色体上的一个候选基因Fv1进行序列分析,结果表明该基因可能与新西兰黑鼠和新西兰白鼠血清gp70水平的控制有关。连锁数据和统计分析证实了gp70抗原与抗gp70抗体水平之间存在密切相关性,共同支持了产生抗gp70抗体需要一定阈值水平的gp70这一概念。抗gp70抗体的血清水平与肾脏疾病的存在密切相关,比抗双链DNA抗体的相关性更强。了解这种复杂的自身抗原-自身抗体系统的遗传基础,将有助于深入了解小鼠狼疮的发病机制,这可能对人类疾病具有启示意义。

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