[胆脂瘤型慢性中耳炎中骨吸收的分子调控]
[Molecular control of bone resorption in chronic otitis media with cholesteatoma].
作者信息
Kuczkowski Jerzy, Kobierska-Gulida Grazyna, Izycka-Swieszewska Ewa, Potocka Małgorzata, Mikaszewski Bogusław, Sierszeń Wojciech
机构信息
Katedra i Klinika Chorób Uszu, Nosa, Gardła i Krtani, Gdański Uniwersytet Medyczny.
出版信息
Otolaryngol Pol. 2010 Jul-Aug;64(4):219-24. doi: 10.1016/S0030-6657(10)70019-6.
UNLABELLED
Bone destruction in chronic otitis media with cholesteatoma is a common phenomenon. Expanding growth of cholesteatoma in the middle ear causes ischemia of the mucosa and bones with granulation tissue production.
THE AIM OF THIS STUDY
was to assess the expression and distribution of the key regulators of bone destruction: osteoprotegerin (OPG), Receptor Activator for Nuclear Factor kappa B Ligand (RANKL) and tumour necrosis factor alpha (TNF-alpha) in chronic otitis media with cholesteatoma and their role in the pathomechanism of bone resorption.
MATERIAL AND METHODS
We performed immunohistochemical study of the cholesteatoma tissue collected from 21 patients suffering from chronic otitis media with cholesteatoma and 16 samples of normal external auditory meatal skin. This material was analysed histopathologically and by means of immunoperoxidase immunohistochemical technique with the use of antibodies against OPG, RANKL and TNF-alpha and their quantitive evaluation.
RESULTS
In all patients with cholesteatoma, features of auditory ossicles and temporal bone destruction were demonstrated. We found that cholesteatoma and granulation tissue cells release factors of the OPG/ RANKL/RANK system and TNF-alpha. In cholestatoma a higher expression of RANKL, OPG and TNF-alpha positive was demonstrated when comparing to the skin of external auditory meatus. These factors were relatively higher expressed in the stroma rather than in the epithelium of cholesteatoma. RANKL-positive cells were demonstrated mainly in the stroma cells, whereas OPG-positive ones in the cholesteatoma epithelium. The reaction with the antibodies against OPG, RANKL and TNF-alpha was weak in the external auditory meatal skin.
CONCLUSIONS
Bone destruction in chronic otitis media with cholesteatoma is a common process dependent on osteoclast activating factors. OPG/ RANKL/RANK system and TNF-alpha play a key role in the process of osteolysis in otitis media with cholesteatoma. We found no positive correlation between bone destruction advancement and the level of examinated proteins.
未标记
胆脂瘤型慢性中耳炎中的骨质破坏是一种常见现象。中耳胆脂瘤的不断生长会导致黏膜和骨质缺血,并产生肉芽组织。
本研究的目的
是评估骨质破坏关键调节因子骨保护素(OPG)、核因子κB受体活化因子配体(RANKL)和肿瘤坏死因子α(TNF-α)在胆脂瘤型慢性中耳炎中的表达和分布,以及它们在骨质吸收发病机制中的作用。
材料与方法
我们对从21例胆脂瘤型慢性中耳炎患者收集的胆脂瘤组织以及16例正常外耳道皮肤样本进行了免疫组织化学研究。对该材料进行了组织病理学分析,并采用免疫过氧化物酶免疫组织化学技术,使用抗OPG、RANKL和TNF-α的抗体进行定量评估。
结果
在所有胆脂瘤患者中,均显示出听小骨和颞骨破坏的特征。我们发现胆脂瘤和肉芽组织细胞释放OPG/RANKL/RANK系统因子和TNF-α。与外耳道皮肤相比,胆脂瘤中RANKL、OPG和TNF-α阳性的表达更高。这些因子在胆脂瘤的基质中表达相对较高,而非上皮中。RANKL阳性细胞主要见于基质细胞,而OPG阳性细胞见于胆脂瘤上皮。外耳道皮肤与抗OPG、RANKL和TNF-α抗体的反应较弱。
结论
胆脂瘤型慢性中耳炎中的骨质破坏是一个依赖破骨细胞激活因子的常见过程。OPG/RANKL/RANK系统和TNF-α在胆脂瘤型中耳炎的骨溶解过程中起关键作用。我们发现骨质破坏进展与检测蛋白水平之间无正相关。
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