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在大鼠实验性伤口中,三肽 - 铜复合物甘氨酰 - L - 组氨酰 - L - 赖氨酸 - Cu2+对结缔组织积累的体内刺激作用。

In vivo stimulation of connective tissue accumulation by the tripeptide-copper complex glycyl-L-histidyl-L-lysine-Cu2+ in rat experimental wounds.

作者信息

Maquart F X, Bellon G, Chaqour B, Wegrowski J, Patt L M, Trachy R E, Monboisse J C, Chastang F, Birembaut P, Gillery P

机构信息

Laboratory of Biochemistry, CNRS ERS F0017, Faculté de Médecine, Reims, France.

出版信息

J Clin Invest. 1993 Nov;92(5):2368-76. doi: 10.1172/JCI116842.

Abstract

The tripeptide-copper complex glycyl-L-histidyl-L-lysine-Cu2+ (GHK-Cu) was first described as a growth factor for differentiated cells. Recent in vitro data showed that it possesses several properties of a potential activator of wound repair. We investigated the effects of GHK-Cu in vivo, using the wound chamber model described previously (Schilling, J.A., W. Joel, and M.T. Shurley, 1959. Surgery [St. Louis]. 46:702-710). Stainless steel wire mesh cylinders were implanted subcutaneously on the back of rats. The animals were divided into groups that received sequential injections into the wound chamber of either saline (control group) or various concentrations of GHK-Cu. At the end of the experiments, rats were killed, wound chambers were collected, and their content was analyzed for dry weight, total proteins, collagen, DNA, elastin, glycosaminoglycans, and specific mRNAs for collagens and TGF beta. In the GHK-Cu-injected wound chambers, a concentration-dependent increase of dry weight, DNA, total protein, collagen, and glycosaminoglycan contents was found. The stimulation of collagen synthesis was twice that of noncollagen proteins. Type I and type III collagen mRNAs were increased but not TGF beta mRNAs. An increase of the relative amount of dermatan sulfate was also found. A control tripeptide, L-glutamyl-L-histidyl-L-proline, had no significant effect. These results demonstrate that GHK-Cu is able to increase extracellular matrix accumulation in wounds in vivo.

摘要

三肽 - 铜复合物甘氨酰 - L - 组氨酰 - L - 赖氨酸 - Cu2 +(GHK - Cu)最初被描述为分化细胞的生长因子。最近的体外数据表明,它具有伤口修复潜在激活剂的多种特性。我们使用先前描述的伤口腔室模型(Schilling,J.A.,W. Joel,和M.T. Shurley,1959年。《外科学》[圣路易斯]。46:702 - 710)研究了GHK - Cu在体内的作用。将不锈钢丝网圆柱体皮下植入大鼠背部。动物被分为几组,分别向伤口腔室中依次注射生理盐水(对照组)或不同浓度的GHK - Cu。在实验结束时,处死大鼠,收集伤口腔室,并分析其内容物的干重、总蛋白、胶原蛋白、DNA、弹性蛋白、糖胺聚糖以及胶原蛋白和转化生长因子β(TGFβ)的特异性mRNA。在注射了GHK - Cu的伤口腔室中,发现干重、DNA、总蛋白、胶原蛋白和糖胺聚糖含量呈浓度依赖性增加。胶原蛋白合成的刺激作用是非胶原蛋白的两倍。I型和III型胶原蛋白mRNA增加,但TGFβ mRNA未增加。还发现硫酸皮肤素的相对量增加。对照三肽L - 谷氨酰 - L - 组氨酰 - L - 脯氨酸没有显著影响。这些结果表明,GHK - Cu能够在体内增加伤口中细胞外基质的积累。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/26bb/288419/30b72a0db0be/jcinvest00043-0292-a.jpg

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