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克拉拉细胞和II型肺细胞系分泌黏液蛋白酶抑制剂和弹性蛋白。

Secretion of mucus proteinase inhibitor and elafin by Clara cell and type II pneumocyte cell lines.

作者信息

Sallenave J M, Silva A, Marsden M E, Ryle A P

机构信息

Department of Biochemistry, Edinburgh University Medical School, United Kingdom.

出版信息

Am J Respir Cell Mol Biol. 1993 Feb;8(2):126-33. doi: 10.1165/ajrcmb/8.2.126.

DOI:10.1165/ajrcmb/8.2.126
PMID:8427705
Abstract

The regulation of proteinases secreted by neutrophils is very important for the prevention of tissue injury. We recently described the isolation of elafin from bronchial secretions, a new elastase-specific inhibitor that is also found in the skin of patients with psoriasis. In this study, we investigated the secretion of elafin and mucus proteinase inhibitor (MPI), another inhibitor showing sequence similarity with elafin, in two lung carcinoma cell lines, NCI-H322 and A549, which have features of Clara cells and type II alveolar cells, respectively. The results presented show that the two inhibitors are produced when the cells are cultured either in serum-free or in serum-containing media. MPI was detected immunologically as a unique molecule of M(r) 14 kD, in accordance with previous studies. Conversely, one or two elafin-immunoreactive species were detected depending on the cell line: a 12- to 14-kD species was observed in the A549 cell line, regardless of the culture conditions, whereas in the NCI-H322 cell line we detected a 6-kD species in serum-containing (10% fetal calf serum) conditions and a 12- to 14-kD species in serum-free conditions. The 12- to 14-kD molecule probably represents an active precursor of elafin. Whether the cleavage of the 12- to 14-kD precursor giving rise to the elafin molecule is of any physiologic significance is not known. In showing for the first time that MPI and elafin (and its precursor) are secreted by the A549 cell line, this report implicates the type II alveolar cell in the defense of the peripheral lung against the neutrophil elastase secreted during inflammation.

摘要

中性粒细胞分泌的蛋白酶的调节对于预防组织损伤非常重要。我们最近描述了从支气管分泌物中分离出elafin,这是一种新的弹性蛋白酶特异性抑制剂,在银屑病患者的皮肤中也有发现。在本研究中,我们调查了两种肺癌细胞系NCI-H322和A549中elafin和黏液蛋白酶抑制剂(MPI)的分泌情况,这两种细胞系分别具有克拉拉细胞和II型肺泡细胞的特征。结果表明,当细胞在无血清或含血清培养基中培养时,这两种抑制剂都会产生。根据先前的研究,MPI通过免疫检测为一种独特的14 kD分子。相反,根据细胞系的不同,检测到一到两种elafin免疫反应性物质:在A549细胞系中,无论培养条件如何,都观察到一种12至14 kD的物质,而在NCI-H322细胞系中,在含血清(10%胎牛血清)条件下检测到一种6 kD的物质,在无血清条件下检测到一种12至14 kD的物质。12至14 kD的分子可能代表elafin的活性前体。导致elafin分子产生的12至14 kD前体的切割是否具有任何生理意义尚不清楚。本报告首次表明MPI和elafin(及其前体)由A549细胞系分泌,这意味着II型肺泡细胞在保护外周肺免受炎症期间分泌的中性粒细胞弹性蛋白酶的侵害中发挥作用。

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