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首页> 外文期刊>The Journal of Experomental Medicine >Human HLA-DR beta gene hypervariable region homology in the biobreeding BB rat: selection of the diabetic-resistant subline as a rheumatoid arthritis research tool to characterize the immunopathologic response to human type II collagen.
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Human HLA-DR beta gene hypervariable region homology in the biobreeding BB rat: selection of the diabetic-resistant subline as a rheumatoid arthritis research tool to characterize the immunopathologic response to human type II collagen.

机译:生物繁殖BB大鼠中的人类HLA-DR beta基因高变区同源性:选择抗糖尿病亚类作为类风湿关节炎研究工具,以表征对人类II型胶原蛋白的免疫病理反应。

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Collagen arthritis (CA), an autoimmune model of rheumatoid arthritis (RA), has been studied in various animals. However, it has not been studied in an animal with a genetic background relevant to RA. We selected rats from a diabetic-resistant (DR) subline of the diabetic BB rat because they have an autoimmune disease-prone background, but not the immunodeficiencies of the diabetic BB rat, and the third hypervariable region (HVRIII) of the BB RT1.D beta gene appeared to encode a nucleotide sequence of the human HLA DR beta gene, which has been reported to be associated with susceptibility to RA. We synthesized oligonucleotide primers flanking the RT1.D beta HVRIII, cloned polymerase chain reaction-amplified DNA into M13mp18, and confirmed the presence of the susceptibility sequence (SS) (RRRAA) by the dideoxy sequencing method in a colony of DR BB/Wor-UTM rats. When immunized with human type II collagen (CII) in incomplete Freunds adjuvant (IFA), arthritis developed rapidly by day 10 with 100% incidence. Light and electron microscopy revealed an unusually severe and aggressive, bidirectional pattern of cartilage resorption by synovial and subchondral mononuclear and multinucleated inflammatory cells. These findings coincided with a predominant humoral response to the cyanogen bromide (CB) 11 fragment of the human CII molecule by the pathogenic IgG2a isotype. This study provides further support to the role of CA as a relevant RA model, the specific roles of the CB11 fragment as a major site of arthritogenic epitopes, and of antibody mechanisms in the pathogenesis of CA. Furthermore, the identification of an RA SS in an immune response gene of the DR BB rat presents a novel opportunity to determine with an animal model the role of other antigens as well as this SS in RA.
机译:胶原蛋白关节炎(CA)是类风湿关节炎(RA)的一种自身免疫模型,已在多种动物中进行了研究。但是,尚未在具有与RA相关的遗传背景的动物中进行研究。我们从糖尿病BB大鼠的糖尿病抵抗性(DR)亚系中选择了大鼠,因为它们具有容易发生自身免疫性疾病的背景,但没有糖尿病BB大鼠的免疫缺陷以及BB RT1的第三个高变区(HVRIII)。 D beta基因似乎编码人HLA DR beta基因的核苷酸序列,据报道与RA的易感性有关。我们合成了位于RT1.D beta HVRIII两侧的寡核苷酸引物,将聚合酶链反应扩增的DNA克隆到M13mp18中,并通过双脱氧测序法在DR BB / Wor-菌落中证实了敏感性序列(SS)(RRRAA)的存在。 UTM大鼠。当在不完全的弗氏佐剂(IFA)中用人II型胶原(CII)免疫时,关节炎在第10天迅速发展,发病率为100%。光镜和电子显微镜显示,滑膜和软骨下单核和多核炎性细胞的软骨吸收异常严重且具有侵略性,是双向的。这些发现与致病性IgG2a同种型对人CII分子的溴化氰(CB)11片段的主要体液反应相吻合。这项研究进一步支持了CA作为相关RA模型的作用,CB11片段作为引起关节炎的抗原决定簇的主要位点的特定作用以及抗体在CA发病机理中的作用。此外,在DR BB大鼠的免疫应答基因中鉴定RA SS提供了一个新的机会,可以用动物模型确定其他抗原以及该SS在RA中的作用。

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