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类风湿关节炎中的Ia特异性抗淋巴细胞抗体。

Ia specific antilymphocyte antibodies in rheumatoid arthritis.

作者信息

Searles R P, Okudaira K, Savage S M, Goodwin J S

出版信息

Arthritis Rheum. 1983 Apr;26(4):486-93. doi: 10.1002/art.1780260406.

Abstract

Antilymphocyte antibodies (ALA) in rheumatoid arthritis (RA) have increased reactivity with phytohemagglutinin (PHA) activated lymphoblasts which are known to have increased expression of Ia antigen. The present experiments suggest that part of this reactivity represents an Ia specificity of ALA. Fifteen of 18 RA sera tested were able to inhibit the binding of monoclonal anti-Ia antibodies as measured by a rosette method. RA sera did not inhibit the binding of other monoclonal antibodies: anti-OKT3, anti-OKT4, and anti-OKT8. The ability of RA sera to inhibit the binding of anti-Ia antibody was eliminated after absorption of the RA sera with an Ia positive human cell line (B35M) but not by an Ia negative line (MOLT4). Blocking of anti-Ia binding was greater in the IgG fraction of the RA sera but also occurred in the IgM fraction. Experiments including ultracentrifugation, pepsin digestion of RA sera, and preincubation of lymphoblasts with aggregated IgG demonstrated that Fc binding by RA sera was not a factor. Both monoclonal anti-Ia and anti-Ia heteroantiserum also had increased reactivity with lymphoblast target cells. Pepsin digested Fab fragments of the anti-Ia heteroantiserum were able to block the activity of cytotoxic RA serum. However, ALA cytotoxic to lymphoblasts did not correlate with anti-Ia by rosette method. Ia-specific ALA by rosette method was associated with donor variability but did not appear to be HLA-DR restricted. Ia-specific ALA did correlate with disease activity. These data suggest that anti-Ia activity is present in RA sera and may play an immunoregulatory role in this disease.

摘要

类风湿关节炎(RA)中的抗淋巴细胞抗体(ALA)与植物血凝素(PHA)激活的淋巴母细胞的反应性增强,已知这些淋巴母细胞Ia抗原的表达增加。目前的实验表明,这种反应性的一部分代表了ALA的Ia特异性。通过玫瑰花结法检测,18份RA血清中有15份能够抑制单克隆抗Ia抗体的结合。RA血清不抑制其他单克隆抗体的结合:抗OKT3、抗OKT4和抗OKT8。用Ia阳性人细胞系(B35M)吸收RA血清后,其抑制抗Ia抗体结合的能力消失,但用Ia阴性细胞系(MOLT4)吸收则不会。RA血清IgG部分对抗Ia结合的阻断作用更强,但IgM部分也有阻断作用。包括超速离心、用胃蛋白酶消化RA血清以及用聚集的IgG预孵育淋巴母细胞在内的实验表明,RA血清与Fc的结合不是一个影响因素。单克隆抗Ia抗体和抗Ia异种抗血清与淋巴母细胞靶细胞的反应性也增强。胃蛋白酶消化的抗Ia异种抗血清的Fab片段能够阻断细胞毒性RA血清的活性。然而,对淋巴母细胞具有细胞毒性的ALA与通过玫瑰花结法检测的抗Ia抗体不相关。通过玫瑰花结法检测的Ia特异性ALA与供体变异性有关,但似乎不受HLA-DR限制。Ia特异性ALA确实与疾病活动相关。这些数据表明,RA血清中存在抗Ia活性,可能在该疾病中发挥免疫调节作用。

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