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弹性蛋白酶在人肺气肿肺组织中的免疫定位

Immunolocalization of elastase in human emphysematous lungs.

作者信息

Damiano V V, Tsang A, Kucich U, Abrams W R, Rosenbloom J, Kimbel P, Fallahnejad M, Weinbaum G

出版信息

J Clin Invest. 1986 Aug;78(2):482-93. doi: 10.1172/JCI112600.

Abstract

The current working hypothesis concerning the pathogenesis of human pulmonary emphysema proposes that neutrophils migrate through the alveolar interstitium and degranulate, releasing proteolytic enzymes into the interstitium. These enzymes, in particular elastase, can bind to and degrade interstitial elastin. This report describes an immunohistochemical, ultrastructural technique that utilizes polyclonal antibodies to localize neutrophil elastase in human lungs. Using both the immunoperoxidase and the immunogold methods on thin, embedded sections of surgically resected human emphysematous lung tissue, elastase was localized in neutrophils in the lung interstitium and extracellularly in association with interstitial elastic fibers in human lungs that showed local emphysema of varying severity. Quantitative morphometric data were obtained from the lungs of eight patients undergoing lobectomy for removal of pulmonary carcinomas. Patients had preoperative forced expiratory volume (FEV1)% levels ranging from 55 to 77. There was a correlation between a quantitative measure of the local distribution of neutrophil elastase in contact with alveolar interstitial elastin and the local presence of emphysematous change as determined by mean linear intercept of the various histologic sections. These data support the validity of the "protease-protease inhibitor balance hypothesis" as an explanation of the pathogenesis of human pulmonary emphysema.

摘要

目前关于人类肺气肿发病机制的工作假说提出,中性粒细胞穿过肺泡间质并脱颗粒,将蛋白水解酶释放到间质中。这些酶,尤其是弹性蛋白酶,能够结合并降解间质弹性蛋白。本报告描述了一种免疫组织化学超微结构技术,该技术利用多克隆抗体在人肺中定位中性粒细胞弹性蛋白酶。通过对手术切除的人肺气肿肺组织的薄切片进行免疫过氧化物酶法和免疫金法检测,发现弹性蛋白酶定位于肺间质中的中性粒细胞内,并且在细胞外与显示不同严重程度局部肺气肿的人肺间质弹性纤维相关联。从八名因肺癌接受肺叶切除术的患者的肺中获取了定量形态学数据。患者术前用力呼气量(FEV1)%水平在55至77之间。通过各种组织学切片的平均线性截距确定,与肺泡间质弹性蛋白接触的中性粒细胞弹性蛋白酶局部分布的定量测量值与局部肺气肿的存在之间存在相关性。这些数据支持了“蛋白酶-蛋白酶抑制剂平衡假说”作为人类肺气肿发病机制解释的有效性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f63c/423585/625fb072a663/jcinvest00107-0164-a.jpg

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