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特发性间质性肺炎中再生上皮的表型

Phenotype of regenerative epithelium in idiopathic interstitial pneumonias.

作者信息

Hinata Nae, Takemura Tamiko, Ikushima Soichiro, Yanagawa Takashi, Ando Tsunehiro, Okada Junko, Oritsu Masaru, Koike Morio

机构信息

Department of Human Pathology, School of Medicine Tokyo Medical and Dental University, Japan.

出版信息

J Med Dent Sci. 2003 Sep;50(3):213-24.

PMID:15074359
Abstract

The epithelial alteration in interstitial pneumonias is one of the repair processes at the sites of disease activity. Regenerative epithelial cells may participate in remodeling of the lung. To determine the phenotype of regenerative epithelial cells in usual interstitial pneumonia (UIP) and nonspecific interstitial pneumonia (NSIP), the expression of Clara cell 10KD protein (CC10), cytokeratin (CK) 14 and 17, surfactant apoprotein (SP)-A, KL-6/MUC1, transforming growth factor (TGF) beta2 were examined in 25 patients with UIP, 9 patients with NSIP and normal lung tissues from 10 patients with lung cancer. In honeycomb lesions of UIP, non-ciliated columnar cells mainly expressed CC10, cuboidal cells expressed CC10, CK17, CK14 and SP-A in descending order. Fibroblastic foci are covered by CK17, CK14, CC10, and a few SP-A positive flattened or cuboidal cells. Regenerative epithelium in NSIP mainly comprised cuboidal cells expressing SP-A, CC10 and CK17. KL-6 was more remarkably expressed in cuboidal and non-ciliated columnar cells both in UIP and NSIP. Expression of TGFbeta2 was observed in cuboidal and flattened epithelium. In severe fibrotic areas, CC10 expressing cells were more prominent, while SP-A positive cells were more prominent in less fibrotic areas. Regenerative epithelial cells in remodeling area in UIP may be derived from bronchiolar basal cells and Clara cells, while most of those in NSIP may be derived from type II pneumocytes. The different origin of regenerative epithelium may reflect the severity and extent of the injury and the degree of consequent fibrosis in UIP and NSIP.

摘要

间质性肺炎中的上皮改变是疾病活动部位的修复过程之一。再生上皮细胞可能参与肺的重塑。为了确定寻常型间质性肺炎(UIP)和非特异性间质性肺炎(NSIP)中再生上皮细胞的表型,检测了25例UIP患者、9例NSIP患者以及10例肺癌患者正常肺组织中克拉拉细胞10KD蛋白(CC10)、细胞角蛋白(CK)14和17、表面活性物质载脂蛋白(SP)-A、KL-6/MUC1、转化生长因子(TGF)β2的表达。在UIP的蜂窝状病变中,无纤毛柱状细胞主要表达CC10,立方细胞依次表达CC10、CK17、CK14和SP-A。成纤维细胞灶被CK17、CK14、CC10以及一些SP-A阳性的扁平或立方细胞覆盖。NSIP中的再生上皮主要由表达SP-A、CC10和CK17的立方细胞组成。KL-6在UIP和NSIP的立方细胞和无纤毛柱状细胞中表达更显著。TGFβ2在立方和平扁上皮中表达。在严重纤维化区域,表达CC10的细胞更突出,而在纤维化较轻区域,SP-A阳性细胞更突出。UIP重塑区域的再生上皮细胞可能来源于细支气管基底细胞和克拉拉细胞,而NSIP中的大多数再生上皮细胞可能来源于II型肺泡上皮细胞。再生上皮的不同来源可能反映了UIP和NSIP中损伤的严重程度和范围以及随之而来的纤维化程度。

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