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肝细胞生长因子基因的局部给药可促进急性切开伤口真皮的再生。

Local administration of hepatocyte growth factor gene enhances the regeneration of dermis in acute incisional wounds.

作者信息

Ono Ichiro, Yamashita Toshiharu, Hida Tokimasa, Jin Hai-Ying, Ito Yoshinori, Hamada Hirobumi, Akasaka Yoshikiyo, Ishii Toshiharu, Jimbow Kowichi

机构信息

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

出版信息

J Surg Res. 2004 Jul;120(1):47-55. doi: 10.1016/j.jss.2003.08.242.

Abstract

Hepatocyte growth factor (HGF) has a number of biological activities, e.g., mitogenic, motogenic, antiapoptotic, antifibrous, and morphogenic. It also has angiogenic and angioprotective activities for endothelial cells. The aim of this study was to characterize the role of HGF in wound healing by administering the HGF gene locally to acute incisional skin wounds created on the backs of rats. To create wounds, the backs of Wistar rats were clipped and three 2-cm-long incisional wounds were made deep to the fascia. The wounds contained pannicrus carnosum and were created at intervals of 2 cm. After suturing, the HGF gene was then administered intradermally. Apoptotic cells in wound lesions were identified by TUNEL method as well as by immunological detection of active caspase-3. In the HGF-treated animals, we found almost complete suppression of apoptosis and well-organized wound healing. Histopathological examination revealed that the proliferation of fibroblasts was suppressed and that scar formation was less apparent in the HGF-treated animals compared to the controls. It is thought that administration of the HGF gene immediately after surgery may enhance the healing process through suppressing apoptosis, which occurred in the controls 1 week after suturing the incisional wound. In addition, locally increased HGF expression due to the introduction of the HGF gene to cells around wounds enhances dermal regeneration, possibly by promoting regeneration of dermal tissue, which results in less scarring due to its antifibrotic effect. Thus, HGF supplementation through gene therapy may be an effective strategy for treating wounds, as it increases the regeneration of the dermis to allow for "scarless wound healing."

摘要

肝细胞生长因子(HGF)具有多种生物学活性,例如促有丝分裂、促运动、抗凋亡、抗纤维化和形态发生活性。它对内皮细胞还具有血管生成和血管保护活性。本研究的目的是通过将HGF基因局部施用于大鼠背部造成的急性切开皮肤伤口,来阐明HGF在伤口愈合中的作用。为了造成伤口,将Wistar大鼠的背部毛发剪去,并在深至筋膜处制作三个2厘米长的切开伤口。伤口包含 pannicrus carnosum,且每隔2厘米制作一个。缝合后,将HGF基因进行皮内给药。通过TUNEL法以及活性半胱天冬酶 - 3的免疫检测来鉴定伤口病变中的凋亡细胞。在接受HGF治疗的动物中,我们发现凋亡几乎完全受到抑制,伤口愈合组织良好。组织病理学检查显示,与对照组相比,HGF治疗组动物中,成纤维细胞的增殖受到抑制,瘢痕形成不太明显。据认为,术后立即给予HGF基因可能通过抑制凋亡来加速愈合过程,而对照组在切开伤口缝合1周后发生了凋亡。此外,由于将HGF基因导入伤口周围细胞而导致局部HGF表达增加,可能通过促进真皮组织再生来增强真皮再生,因其抗纤维化作用而导致瘢痕形成减少。因此,通过基因治疗补充HGF可能是治疗伤口的有效策略,因为它可增加真皮再生,实现“无瘢痕伤口愈合”。

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