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对新西兰黑鼠中与狼疮性肾炎易感基因座相关的多种自身抗体的控制。

Control of multiple autoantibodies linked with a lupus nephritis susceptibility locus in New Zealand black mice.

作者信息

Vyse T J, Rozzo S J, Drake C G, Izui S, Kotzin B L

机构信息

Department of Pediatrics, National Jewish Medical and Research Center, Denver, CO 80206, USA.

出版信息

J Immunol. 1997 Jun 1;158(11):5566-74.

PMID:9164982
Abstract

An NZB locus on distal chromosome 1 has been linked to murine lupus nephritis in backcross analyses of New Zealand mice. This locus, designated Nba2 for New Zealand Black autoimmunity 2, was found to colocalize in both (NZB x SM/J)F1 x NZW and (B6.H2z x NZB)F1 x NZB backcrosses, and was most likely situated between 92 and 97 cM from the centromere. This region of mouse chromosome 1 encodes several candidate genes, including the low affinity Fc gamma receptor genes. Both backcrosses were examined by interval mapping for quantitative trait loci linked with autoantibody and total Ig production. Nba2 was linked with elevated serum levels of multiple autoantibodies, including a variety of antinuclear Abs (anti-dsDNA, anti-chromatin and anti-histone) and autoantibodies to gp70, in both backcrosses. Nba2 was also linked (or showed a trend for linkage) with hypergammaglobulinemia and IgG1, IgG2a, and/or IgG3 levels in each backcross. In the (B6.H2z x NZB)F1 x NZB backcross, MHC was an additional genetic contribution that interacted with Nba2 in the production of autoantibodies and the development of nephritis. Together, these data provide new insight into the nature of one important genetic contribution to murine lupus and suggest that Nba2 may act as an immune response gene that influences Ag-driven B cell responses to self and possibly to exogenous Ags.

摘要

在对新西兰小鼠的回交分析中,1号染色体远端的一个新西兰黑鼠(NZB)基因座与小鼠狼疮性肾炎相关联。这个基因座被命名为Nba2(代表新西兰黑鼠自身免疫2),发现在(NZB×SM/J)F1×NZW和(B6.H2z×NZB)F1×NZB回交中都共定位,并且最有可能位于距着丝粒92至97厘摩之间。小鼠1号染色体的这个区域编码几个候选基因,包括低亲和力Fcγ受体基因。通过区间定位检查这两个回交,以寻找与自身抗体和总免疫球蛋白产生相关的数量性状基因座。在两个回交中,Nba2都与多种自身抗体的血清水平升高有关,包括多种抗核抗体(抗双链DNA、抗染色质和抗组蛋白)以及针对gp70的自身抗体。在每个回交中,Nba2还与高球蛋白血症以及IgG1、IgG2a和/或IgG3水平相关联(或显示出关联趋势)。在(B6.H2z×NZB)F1×NZB回交中,主要组织相容性复合体(MHC)是另一个遗传因素,它在自身抗体产生和肾炎发展过程中与Nba2相互作用。这些数据共同为小鼠狼疮的一个重要遗传因素的本质提供了新的见解,并表明Nba2可能作为一个免疫反应基因,影响抗原驱动的B细胞对自身以及可能对外源性抗原的反应。

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