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在具有延长寿命的传代hTERT转染人鼻上皮细胞中紧密连接蛋白的诱导。

Induction of claudins in passaged hTERT-transfected human nasal epithelial cells with an extended life span.

作者信息

Kurose Makoto, Kojima Takashi, Koizumi Jun-Ichi, Kamekura Ryuta, Ninomiya Takafumi, Murata Masaki, Ichimiya Shingo, Osanai Makoto, Chiba Hideki, Himi Tetsuo, Sawada Norimasa

机构信息

Department of Otolaryngology, Sapporo Medical University School of Medicine, Sapporo, Japan.

出版信息

Cell Tissue Res. 2007 Oct;330(1):63-74. doi: 10.1007/s00441-007-0453-z. Epub 2007 Aug 14.

Abstract

The epithelial barrier of the upper respiratory tract, such as that of the nasal mucosa, plays a crucial role in host defense. The epithelial barrier is regulated in large part by the apical-most intercellular junctions, referred to as tight junctions. However, the mechanisms regulating of tight junction barrier in human nasal epithelial cells remain unclear because the proliferation and storage of epithelial cells in primary cultures are limited. In the present study, we introduced the catalytic component of telomerase, the hTERT gene, into primary cultured human nasal epithelial cells and examined the properties of the transfectants, including their expression of tight junctions, compared with primary cultures. The ectopic expression of hTERT in the epithelial cells resulted in adequate growth potential and a longer lifespan of the cells. The properties of the passaged hTERT-transfected cells including tight junctions were similar to those of the cells in primary cultures. The barrier function in the transfectants after treatment with 10% FBS was significantly enhanced with increases of integral tight junction proteins claudin-1 and -4. When the transfectants were treated with TGF-beta, which is assosciated with nasal polyposis and chronic rhinosinusitis, upregulation of only claudin-4 was observed, without a change of barrier function. In human nasal epithelial cells, the claudins may be important for barrier function and a novel target for a drug-delivery system. Our results indicate that hTERT-transfected human nasal epithelial cells with an extended lifespan can be used as an indispensable and stable model for studying the regulation of claudins in human nasal epithelium.

摘要

上呼吸道的上皮屏障,如鼻黏膜的上皮屏障,在宿主防御中起着关键作用。上皮屏障在很大程度上由最顶端的细胞间连接(即紧密连接)调节。然而,由于原代培养中上皮细胞的增殖和储存有限,人类鼻上皮细胞中紧密连接屏障的调节机制仍不清楚。在本研究中,我们将端粒酶的催化成分hTERT基因导入原代培养的人类鼻上皮细胞,并与原代培养物比较,检测转染细胞的特性,包括它们紧密连接的表达情况。上皮细胞中hTERT的异位表达导致细胞具有足够的生长潜力和更长的寿命。传代的hTERT转染细胞包括紧密连接的特性与原代培养细胞相似。用10%胎牛血清处理后,转染细胞中的屏障功能随着紧密连接整合蛋白claudin-1和-4的增加而显著增强。当转染细胞用与鼻息肉病和慢性鼻窦炎相关的转化生长因子-β处理时,仅观察到claudin-4上调,而屏障功能无变化。在人类鼻上皮细胞中,claudin蛋白可能对屏障功能很重要,并且是药物递送系统的一个新靶点。我们的结果表明,具有延长寿命的hTERT转染人类鼻上皮细胞可作为研究人类鼻上皮中claudin蛋白调节的不可或缺且稳定的模型。

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