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中性粒细胞激活肽ENA-78的受体结合特异性及肺部基因表达

Receptor binding specificity and pulmonary gene expression of the neutrophil-activating peptide ENA-78.

作者信息

Bozic C R, Gerard N P, Gerard C

机构信息

Ina Sue Perlmutter Laboratory, Department of Pediatrics, Children's Hospital, Boston, Massachusetts, USA.

出版信息

Am J Respir Cell Mol Biol. 1996 Mar;14(3):302-8. doi: 10.1165/ajrcmb.14.3.8845182.

DOI:10.1165/ajrcmb.14.3.8845182
PMID:8845182
Abstract

Neutrophil-activating peptide ENA-78 is a novel chemotactic cytokine isolated from a human type II pulmonary epithelial cell line. It is a member of the chemokine family of proinflammatory polypeptides and exhibits structural homology to interleukin-8 (IL-8) and GROalpha. The immunohistochemical identification of ENA-78 in pulmonary alveolar leukocytes of bovine pneumonic lungs supports a role for ENA-78 in the pathogenesis of pulmonary inflammation. Although ENA-78 is able to stimulate polymorphonuclear neutrophils (PMN), neither its binding specificities nor its expression in human pulmonary disease states have been determined. 125I-labeled ENA-78 binds with high affinity to human PMN. Its actions on PMN appear to be mediated by the IL-8 type B receptor, to which it binds with a K(d) of 2.2 nM. Human IL-8, GROalpha, and murine KC compete with high affinity for 125I-ENA-78 binding to the human IL-8 type B receptor. In contrast, 125I-ENA-78 does not bind to the IL-8 type A receptor nor does it compete significantly for 125I-IL-8 binding to this same receptor. ENA-78 is a potent upregulator of Mac-1 cell surface expression. In addition, ENA-78 mRNA is detected in cystic fibrosis lung but is not detected in normal donor lung. Thus, ENA-78 mRNA levels appear to be increased in human pulmonary inflammation and its stimulatory activities on PMN appear to be a function mediated primarily by the IL-8 type B receptor.

摘要

中性粒细胞激活肽ENA - 78是一种从人II型肺上皮细胞系中分离出的新型趋化细胞因子。它是促炎多肽趋化因子家族的成员,与白细胞介素-8(IL - 8)和GROα具有结构同源性。在牛肺炎肺的肺泡白细胞中对ENA - 78进行免疫组织化学鉴定,支持ENA - 78在肺部炎症发病机制中的作用。尽管ENA - 78能够刺激多形核中性粒细胞(PMN),但其结合特异性及其在人类肺部疾病状态下的表达尚未确定。125I标记的ENA - 78与人类PMN高亲和力结合。它对PMN的作用似乎是由IL - 8 B型受体介导的,其与该受体结合的解离常数(K(d))为2.2 nM。人类IL - 8、GROα和小鼠KC与125I - ENA - 78竞争与人类IL - 8 B型受体的结合,且亲和力高。相比之下,125I - ENA - 78不与IL - 8 A型受体结合,也不显著竞争125I - IL - 8与同一受体的结合。ENA - 78是Mac - 1细胞表面表达的有效上调因子。此外,在囊性纤维化肺中检测到ENA - 78 mRNA,但在正常供体肺中未检测到。因此,ENA - 78 mRNA水平在人类肺部炎症中似乎升高,其对PMN的刺激活性似乎主要是由IL - 8 B型受体介导的功能。

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