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获得性中耳胆脂瘤中Id1的鉴定。

Identification of Id1 in acquired middle ear cholesteatoma.

作者信息

Zhang Quan-An, Hamajima Yuki, Zhang Qing, Lin Jizhen

机构信息

Department of Otolaryngology, Xi'an Jiao University, Xi'an, People's Republic of China.

出版信息

Arch Otolaryngol Head Neck Surg. 2008 Mar;134(3):306-10. doi: 10.1001/archotol.134.3.306.

Abstract

OBJECTIVES

To determine (1) the relationship between chronic inflammatory changes in the ossicular chain area (OCA) and the formation of cholesteatoma and (2) the correlates between aberrant gene expression and abnormal proliferation of cholesteatoma.

METHODS

Two hundred sixty-four ears with chronic otitis media that had undergone ear surgery were included in this study for statistical analysis of the relationship between abnormalities in the OCA and cholesteatoma. Fourteen middle ear cholesteatoma specimens were collected for immunohistochemical analysis of candidate molecules involved in the abnormal proliferation of keratinocytes. A cell model was used for verification of candidate molecule involvement.

RESULTS

The formation of cholesteatoma was accompanied by chronic inflammatory changes in the OCA, including granulated tissue, adhesion, and stagnating effusion. The inhibitor of the DNA-binding (Id1) gene, which is involved in controlling cell cycle progression, was abundantly expressed in cholesteatoma epithelium. In vitro studies indicate that Id1 regulated the expression of nuclear factor kappaB, cyclin D1, proliferating cell nuclear antigen, and cell cycle progression of keratinocytes,

CONCLUSIONS

Chronic inflammation in the OCA is closely related to the formation of cholesteatoma. The Id1/nuclear factor kappaB/cyclin D1/proliferating cell nuclear antigen signaling pathway is involved in the abnormal proliferation of keratinocytes in acquired cholesteatoma.

摘要

目的

确定(1)听骨链区域(OCA)的慢性炎症变化与胆脂瘤形成之间的关系,以及(2)异常基因表达与胆脂瘤异常增殖之间的相关性。

方法

本研究纳入264例接受耳部手术的慢性中耳炎患者,对OCA异常与胆脂瘤之间的关系进行统计分析。收集14例中耳胆脂瘤标本,对参与角质形成细胞异常增殖的候选分子进行免疫组化分析。使用细胞模型验证候选分子的参与情况。

结果

胆脂瘤的形成伴随着OCA的慢性炎症变化,包括肉芽组织、粘连和积液停滞。参与控制细胞周期进程的DNA结合抑制因子(Id1)基因在胆脂瘤上皮中大量表达。体外研究表明,Id1调节核因子κB、细胞周期蛋白D1、增殖细胞核抗原的表达以及角质形成细胞的细胞周期进程。

结论

OCA中的慢性炎症与胆脂瘤的形成密切相关。Id1/核因子κB/细胞周期蛋白D1/增殖细胞核抗原信号通路参与后天性胆脂瘤中角质形成细胞的异常增殖。

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