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源自人内皮细胞的白细胞介素1增强T淋巴细胞迁移的黏附及趋化步骤。

Interleukin 1 derived from human endothelial cells enhances the binding and chemotactic step of T lymphocyte emigration.

作者信息

Miossec P, Cavender D, Ziff M

机构信息

Department of Internal Medicine (Inflammation Research Unit), University of Texas Health Science Center, Dallas 75235.

出版信息

Clin Exp Immunol. 1988 Aug;73(2):250-4.

Abstract

Recent evidence indicates that interleukin 1 (IL-1) from different sources has varying molecular weights, amino acid and gene sequences and biological properties. In previous experiments, it has been shown that monocyte derived IL-1 was chemotactic for lymphocytes and stimulated their binding to endothelial cells (EC). These phenomena are important in the emigration of lymphocytes in inflammatory states. In the present investigation, EC were stimulated with LPS and from the supernatants the IL-1 activity was isolated. After AcA 54 gel filtration, the active 17 kD fraction was further purified by chromatofocusing, yielding active fractions with pI of 7.0 and 5.0. All of these fractions showed T lymphocyte chemotactic activity, stimulated the binding of T cells to EC and the proliferation of fibroblasts. It is concluded, therefore, that EC-derived IL-1 has similar biological activity to that of monocyte-derived IL-1 and that it can exert a true autocrine effect at the blood-tissue endothelial interface.

摘要

近期证据表明,来自不同来源的白细胞介素1(IL-1)具有不同的分子量、氨基酸和基因序列以及生物学特性。在先前的实验中,已表明单核细胞衍生的IL-1对淋巴细胞具有趋化作用,并刺激它们与内皮细胞(EC)结合。这些现象在炎症状态下淋巴细胞的迁移中很重要。在本研究中,用脂多糖刺激EC,并从其培养上清液中分离出IL-1活性。经AcA 54凝胶过滤后,通过色谱聚焦进一步纯化活性17 kD组分,得到pI为7.0和5.0的活性组分。所有这些组分均显示出T淋巴细胞趋化活性,刺激T细胞与EC结合以及成纤维细胞增殖。因此得出结论,EC衍生的IL-1具有与单核细胞衍生的IL-1相似的生物学活性,并且它可以在血液-组织内皮界面发挥真正的自分泌作用。

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