Naturally-occurring anti-thymocyte autoantibody which identifies a restricted CD4+CD8+CD3-/lo/int thymocyte subpopulation exhibits extensive polyspecificity.

Thymus Pub Date : 1996-01-01
J R Underwood, A McCall, X F Csar
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Abstract

In this study, naturally-occurring, monoclonal IgM kappa anti-thymocyte autoantibodies from the neonatal inbred Balb/c mouse-derived hybridoma NMT-1 (NMT-1 mAb), previously reported to identify a restricted CD4+CD8+CD3/lo/int thymocyte subpopulation, have been shown to exhibit extensive polyspecificity. Using immunofluorescence, immunoblotting and antibody titration and competition ELISAs, NMT-1 mAbs exhibited polyspecific binding to 12 apparently structurally unrelated self and non-self antigens. The autoreactive component of the polyspecificity profile of NMT-1 mAbs encompassed reactivity to developmentally-related 14.5 and 18.3 kDa Thy-1 glycoforms expressed on a CD4+CD8+CD3-/lo/int thymocyte subpopulation. The autoreactivity profile of NMT-1 mAbs also included recognition of the heavy and light chains of mouse IgG1 and mouse cytokeratins within thymic medullary epithelium and basal epithelial cells of stratified squamous epithelium of mouse tongue, oesophagus, stomach, skin and vagina. Examination of the polyspecificity profile of NMT-1 mAbs was also undertaken using a panel of 23 antigens including heterologous proteins, phospholipids, haptens and bacterial antigens by antibody titration and competition ELISAs. Antibody titration ELISAs demonstrated that NMT-1 mAbs bound nine antigens including bovine carbonic anhydrase, ovalbumin, cardiolipin, phosphatidylserine, the haptens, DNP and FITC and the bacterial antigens including Escherichia coli beta-galactosidase and the toxoids from Corynebacterium tetani and Clostridium diphtheria. Competition ELISAs, based on the inhibition of NMT-1 mAb binding to antigens adsorbed to ELISA plate surfaces by inhibitor antigens in solution, demonstrated that NMT-1 mAb interactions were not dependent on multivalent binding. In these assays, NMT-1 mAbs recognized unmodified (native) epitopes on the solution phase forms of the protein antigens, including E. coli beta-galactosidase and toxoids from Corynebacterium tetani and Clostridium diphtheria, providing further evidence for the hypothesis that the binding of multiple, apparently unrelated, antigens by NMT-1 mAbs occurs via unique polyspecific antigen combining sites.

自然产生的抗胸腺细胞自身抗体可识别受限制的CD4+CD8+CD3-/lo/int胸腺细胞亚群,具有广泛的多特异性。
在这项研究中,来自新生儿自交系Balb/c小鼠源性杂交瘤NMT-1 (NMT-1 mAb)的天然单克隆IgM κ pa抗胸腺细胞自身抗体已被证明具有广泛的多特异性,该单克隆抗体先前被报道用于鉴定受限制的CD4+CD8+CD3/lo/int胸腺细胞亚群。通过免疫荧光、免疫印迹、抗体滴定和竞争elisa, NMT-1单克隆抗体显示出与12种明显结构无关的自身和非自身抗原的多特异性结合。NMT-1单克隆抗体多特异性的自身反应性成分包括对CD4+CD8+CD3-/lo/int胸腺细胞亚群上表达的发育相关的14.5和18.3 kDa Thy-1糖型的反应性。NMT-1单克隆抗体的自身反应性还包括识别胸腺髓上皮和小鼠舌、食管、胃、皮肤和阴道分层鳞状上皮基底上皮细胞内的小鼠IgG1和小鼠细胞角蛋白的重链和轻链。采用23种抗原,包括异种蛋白、磷脂、半抗原和细菌抗原,通过抗体滴定和竞争elisa检测NMT-1单克隆抗体的多特异性。抗体滴定elisa结果表明,NMT-1单抗能结合牛碳酸酐酶、卵清蛋白、心磷脂、磷脂酰丝氨酸、半抗原、DNP和FITC等9种抗原,并能结合大肠杆菌β -半乳糖苷酶、破伤风杆状杆菌和白喉梭菌类毒素等细菌抗原。竞争ELISA基于NMT-1 mAb与溶液中抑制剂抗原吸附在ELISA板表面的抗原的抑制作用,证明NMT-1 mAb的相互作用不依赖于多价结合。在这些实验中,NMT-1单抗识别了蛋白抗原溶液形态上未修饰的(天然的)表位,包括大肠杆菌β -半乳糖苷酶和来自破伤风杆状杆菌和白喉梭菌的类毒素,这进一步证明了NMT-1单抗通过独特的多特异性抗原结合位点结合多种明显不相关的抗原的假设。
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