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一种编码含有人类钙蛋白酶抑制蛋白两个抑制结构域的多肽的cDNA克隆的检测与表达及其被类风湿性关节炎血清的识别

Detection and expression of a cDNA clone that encodes a polypeptide containing two inhibitory domains of human calpastatin and its recognition by rheumatoid arthritis sera.

作者信息

Després N, Talbot G, Plouffe B, Boire G, Ménard H A

机构信息

Rheumatic Diseases Unit, Faculty of Medicine, Université de Sherbrooke, Québec, Canada.

出版信息

J Clin Invest. 1995 Apr;95(4):1891-6. doi: 10.1172/JCI117870.

DOI:10.1172/JCI117870
PMID:7706496
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC295733/
Abstract

RA is the most frequent and most destructive inflammatory arthropathy. Rheumatoid factors, in spite of their lack of disease specificity, are important serological markers for RA and appear important in its immunopathogenesis as well. In search of more disease-specific autoimmune systems, we have screened a human placenta lambda gt11 cDNA expression library using selected sera from patients with classical erosive RA. We have identified one clone (RA-1) that is recognized by three of five screening sera. The 950-bp insert shows a complete nucleotide sequence homology to the cDNA encoding the two COOH-terminal domains of calpastatin. The deduced open reading frame of the RA-1 cDNA predicts a 284-amino acid protein, with a calculated mol wt of 35.9 kD. Calpastatin is the natural inhibitor of calpains, which are members of the cysteine proteinases recently implicated in joint destruction in rheumatic diseases. The two domains encoded by the RA-1 clone each contain the structural features associated with the inhibitory activity of human calpastatin. By Western blotting, 45.5% or 21/44 RA sera specifically recognized both the fusion and the cleaved recombinant protein. This is in contrast to 4.7% (2/43) in nonrheumatoid sera and 0/10 in normal sera. Anticalpastatin autoantibodies could represent a disease-associated marker in chronic erosive arthritis of the rheumatoid type and could hypothetically play a dual pathogenic role, directly via an immune interference and indirectly through an immune complex mechanism.

摘要

类风湿关节炎(RA)是最常见且最具破坏性的炎性关节病。类风湿因子尽管缺乏疾病特异性,但仍是RA重要的血清学标志物,且在其免疫发病机制中似乎也很重要。为了寻找更具疾病特异性的自身免疫系统,我们使用经典侵蚀性RA患者的选定血清筛选了人胎盘λgt11 cDNA表达文库。我们鉴定出一个克隆(RA-1),它能被五份筛选血清中的三份识别。950bp的插入片段与编码钙蛋白酶抑制蛋白两个COOH末端结构域的cDNA具有完全的核苷酸序列同源性。RA-1 cDNA推导的开放阅读框预测有一个284个氨基酸的蛋白质,计算分子量为35.9kD。钙蛋白酶抑制蛋白是钙蛋白酶的天然抑制剂,钙蛋白酶是最近被认为与风湿性疾病关节破坏有关的半胱氨酸蛋白酶家族成员。RA-1克隆编码的两个结构域各自包含与人类钙蛋白酶抑制蛋白抑制活性相关的结构特征。通过蛋白质印迹法,45.5%(21/44)的RA血清能特异性识别融合型和裂解型重组蛋白。相比之下,非类风湿血清中为4.7%(2/43),正常血清中为0/10。抗钙蛋白酶抑制蛋白自身抗体可能是类风湿型慢性侵蚀性关节炎中与疾病相关的标志物,并可能通过免疫干扰直接以及通过免疫复合物机制间接发挥双重致病作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e54b/295733/6c0f86e1eb0e/jcinvest00025-0477-b.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e54b/295733/89d1d42371de/jcinvest00025-0477-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e54b/295733/6c0f86e1eb0e/jcinvest00025-0477-b.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e54b/295733/89d1d42371de/jcinvest00025-0477-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e54b/295733/6c0f86e1eb0e/jcinvest00025-0477-b.jpg

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本文引用的文献

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