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在BALB/c背景下,来自新西兰黑鼠和新西兰白鼠4号和12号染色体上的新基因座会引发狼疮样疾病。

New loci from New Zealand Black and New Zealand White mice on chromosomes 4 and 12 contribute to lupus-like disease in the context of BALB/c.

作者信息

Rigby Robert J, Rozzo Stephen J, Boyle Joseph J, Lewis Margarita, 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 1;172(7):4609-17. doi: 10.4049/jimmunol.172.7.4609.

Abstract

New Zealand Black (NZB) and New Zealand White (NZW) mice are genetically predisposed to a lupus-like autoimmune syndrome. To further define the loci linked to disease traits in NZB and NZW mice in the context of the BALB/c genetic background, linkage analyses were conducted in two crosses: (NZW x BALB/c.H2(z))F(1) x NZB and (NZB x BALB/c)F(2). Novel loci linked to autoantibody production and glomerulonephritis, present in both NZB and NZW mice, were identified on proximal chromosomes 12 and 4. The chromosome 12 locus showed the strongest linkage to anti-nuclear Ab production. Additionally, a number of other novel loci linked to lupus traits derived from both the New Zealand and non-autoimmune BALB/c genomes were identified. Furthermore, we confirm the linkage of disease to a number of previously described lupus-associated loci, demonstrating that they are relatively background independent. These data provide a number of additional candidate gene regions in murine lupus, and highlight the powerful effect the non-autoimmune background strain has in influencing the genetic loci linked to disease.

摘要

新西兰黑鼠(NZB)和新西兰白鼠(NZW)具有患狼疮样自身免疫综合征的遗传易感性。为了在BALB/c遗传背景下进一步确定与NZB和NZW小鼠疾病特征相关的基因座,在两个杂交组合中进行了连锁分析:(NZW×BALB/c.H2(z))F(1)×NZB和(NZB×BALB/c)F(2)。在近端12号和4号染色体上鉴定出了与NZB和NZW小鼠自身抗体产生及肾小球肾炎相关的新基因座。12号染色体基因座与抗核抗体产生的连锁最强。此外,还鉴定出了一些其他源自新西兰和非自身免疫性BALB/c基因组且与狼疮特征相关的新基因座。此外,我们证实了疾病与一些先前描述的狼疮相关基因座的连锁关系,表明它们相对不依赖背景。这些数据提供了小鼠狼疮中的一些额外候选基因区域,并突出了非自身免疫性背景品系在影响与疾病相关的遗传基因座方面的强大作用。

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