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TGF-α/HA 复合物通过 ErbB1 受体促进鼓膜角质细胞的迁移和增殖。

TGF-α/HA complex promotes tympanic membrane keratinocyte migration and proliferation via ErbB1 receptor.

机构信息

Ear Sciences Centre, School of Surgery, The University of Western Australia, Nedlands, WA, Australia.

出版信息

Exp Cell Res. 2013 Apr 1;319(6):790-9. doi: 10.1016/j.yexcr.2013.01.015. Epub 2013 Feb 4.

DOI:10.1016/j.yexcr.2013.01.015
PMID:23384599
Abstract

Tympanic membrane perforations are common and represent a management challenge to clinicians. Current treatments for chronic perforations involve a graft surgery and require general anaesthesia, including associated costs and morbidities. Bioactive molecules (e.g. growth factors, cytokines) play an important role in promoting TM wound healing following perforation and the use of growth factors as a topical treatment for tympanic membrane perforations has been suggested as an alternative to surgery. However, the choice of bioactive molecules best suited to promote wound healing has yet to be identified. We investigated the effects of hyaluronic acid, vitronectin, TGF-α, IL-24 and their combinations on migration, proliferation and adhesion of cultured human tympanic membrane-derived keratinocytes (hTM), in addition to their possible mechanisms of action. We found that TGF-α, TGF-α/HA and TGF-α/IL-24 promoted wound healing by significantly increasing both migration and proliferation. TGF-α and/or HA treated cells showed comparable cell-cell adhesion whilst maintaining an epithelial cell phenotype. With the use of receptor binding inhibitors for ErbB1 (AG1478) and CD44 (BRIC235), we revealed that the activation of ErbB1 is required for TGF-α/HA-mediated migration and proliferation. These results suggest factors that may be incorporated into a tissue-engineered membrane or directly as topical treatment for tympanic membrane perforations and hence reduce the need for a surgery.

摘要

鼓膜穿孔较为常见,是临床医生面临的一个治疗挑战。目前治疗慢性穿孔的方法包括移植物手术,需要全身麻醉,包括相关的费用和并发症。生物活性分子(例如生长因子、细胞因子)在促进穿孔后的鼓膜伤口愈合方面发挥着重要作用,将生长因子作为鼓膜穿孔的局部治疗已被提议作为手术的替代方法。然而,促进伤口愈合的最佳生物活性分子的选择尚未确定。我们研究了透明质酸、纤连蛋白、TGF-α、IL-24 及其组合对培养的人鼓膜来源角质细胞(hTM)迁移、增殖和黏附的影响,以及它们可能的作用机制。我们发现 TGF-α、TGF-α/HA 和 TGF-α/IL-24 通过显著增加迁移和增殖来促进伤口愈合。TGF-α 和/或 HA 处理的细胞表现出相似的细胞间黏附,同时保持上皮细胞表型。使用 ErbB1(AG1478)和 CD44(BRIC235)受体结合抑制剂,我们揭示了 ErbB1 的激活对于 TGF-α/HA 介导的迁移和增殖是必需的。这些结果表明,这些因子可能被纳入组织工程膜或直接作为鼓膜穿孔的局部治疗,从而减少手术的需求。

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