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Constitutive overexpression of periostin delays wound healing in mouse skin

机译:本构的超表达periostin延迟伤口愈合在小鼠皮肤

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Abstract Periostin is a matricellular protein involved in development, maintenance, and regulation of tissues and organs via by binding to cell surface integrin receptors. Pathologically, periostin plays an important role in the process of wound healing: as a deficiency of the Postn gene delays wound closure and periostin is consistently up‐regulated in response to injury and skin diseases. However, the functional role of elevated periostin in the process of wound healing has not been tested. In this study, we generated Postn ‐transgenic mice under the control of the CAG promoter/enhancer to investigate the effects of constitutive overexpression of full length periostin during its pathophysiological roles. Transgenic mice showed significant overexpression of periostin in skin, lung, and heart, but no morphological changes were observed. However, when these transgenic mice were injured, periostin overexpression delayed the closure of excisional wounds. Expression of IL‐1β and TNFα, pro‐inflammatory cytokines important for wound healing, was significantly decreased in the transgenic mice, prior to delayed healing. Infiltration of neutrophils and macrophages, the main sources of IL‐1β and TNFα, was also down‐regulated in the transgenic wound sites. From these data, we conclude that enforced expression of periostin delays wound closure due to reduced infiltration of neutrophils and macrophages followed by down‐regulation of IL‐1β and TNFα expression. This suggests that regulated spatiotemporal expression of periostin is important for efficient wound healing and that constitutive periostin overexpression interrupts the normal process of wound closure.
机译:文摘Periostin是matricellular蛋白质参与开发、维护监管的组织和器官通过绑定细胞表面整合素受体。病理上,periostin扮演重要的角色在伤口愈合的过程中:作为一个缺陷Postn基因的关闭和延迟伤口periostin是一致的监管应对损伤和皮肤疾病。高架periostin的功能作用伤口愈合的过程还未经过测试。这项研究中,我们生成的Postn转基因小鼠CAG的控制下启动子/增强剂调查本构的影响超表达的完整periostin期间其病理生理作用。显示显著的periostin过度皮肤、肺和心脏,但没有形态观察变化。转基因老鼠受伤,periostin过度延迟关闭全部切除伤口。箴炎性细胞因子重要的伤口治疗,显著减少转基因小鼠,之前延迟愈合。中性粒细胞和巨噬细胞的浸润主要来源的IL 1β和肿瘤坏死因子α,也量监管转基因伤口网站。从这些数据,我们得出结论,执行表达periostin延迟伤口关闭减少中性粒细胞的浸润和巨噬细胞后,向下调节IL 1β和肿瘤坏死因子α的表达。时空表达periostin重要的有效的伤口愈合本构periostin过度中断正常的伤口闭合的过程。

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