血小板衍生因子调节吞噬细胞功能并与白细胞介素1协同作用的表征。

Lymphokine research Pub Date : 1989-01-01
E Brandt, M Ernst, H Loppnow, H D Flad
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引用次数: 0

摘要

在实验中,针对天然人白细胞介素2单克隆抗体的产生,获得了一种不同特异性的抗体,识别用于免疫的抗原制剂中的多肽污染物。这种抗原被证明是人类血小板中的一种释放蛋白。免疫纯化抗原的氨基酸序列分析显示其为β -血栓球蛋白抗原。根据抗原来源(新鲜裂解的血小板,含有细胞培养上清的血小板)不同形式的多肽,不同程度的n端截断,被发现。不同肽组成的β -血栓球蛋白抗原制剂也具有不同的调节人类单核细胞和粒细胞自发以及fc受体依赖的化学发光的能力。与以前的报道相反,单独使用β - tg抗原(CTAP III)没有发现人真皮成纤维细胞的有丝分裂活性,而只有与人白细胞介素1和肝素联合使用时才发现,这三种分子协同作用。这些发现表明- tg抗原可能在连接血液凝固系统和免疫系统方面发挥功能作用。
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Characterization of a platelet derived factor modulating phagocyte functions and cooperating with interleukin 1.

During experiments aiming at the generation of monoclonal antibodies against native human interleukin 2 an antibody of different specificity was obtained, recognizing a polypeptide contaminant within the antigen preparation used for immunization. This antigen was shown to represent a release protein from human blood platelets. Amino acid sequence analysis of the immunopurified antigen revealed its identity as beta-thromboglobulin antigen. Depending on the source of antigen (freshly lysed platelets, platelet containing cell culture supernatants) various forms of the polypeptide, differing in the degree of N-terminal truncation, were found. Beta-thromboglobulin antigen preparations differing in peptide composition also had different capacities for modulating spontaneous as well as Fc-receptor dependent chemiluminescence of human monocytes and granulocytes. In contrast to former reports, no mitogenic activity for human dermal fibroblasts was found with beta-TG antigen (CTAP III) alone, but only in combination with human interleukin 1 and heparin, the three molecules acting synergistically. These findings indicate that beta-TG antigen could play a functional role in linking the blood clotting system to the immune system.

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