首页> 外文期刊>Journal of the American Society of Nephrology: JASN >Single injection of naked plasmid encoding hepatocyte growth factor prevents cell death and ameliorates acute renal failure in mice.
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Single injection of naked plasmid encoding hepatocyte growth factor prevents cell death and ameliorates acute renal failure in mice.

机译:单次注射编码肝细胞生长因子的裸质粒可防止细胞死亡并改善小鼠的急性肾衰竭。

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摘要

Hepatocyte growth factor (HGF) is a pleiotrophic factor that plays an important role in tissue repair and regeneration after injury. The expression of both HGF and its c-met receptor genes is rapidly upregulated after acute renal injury induced by folic acid. In this study, the role of exogenous HGF in preventing acute renal failure by systemic administration of naked plasmid containing human HGF cDNA driven under the cytomegalovirus promoter (pCMV-HGF) was examined in mice. Intravenous injection of pCMV-HGF plasmid produced substantial levels of human HGF protein in mouse kidneys. Simultaneous injection of HGF plasmid DNA significantly ameliorated renal dysfunctions and accelerated recovery from the acute injury induced by folic acid. Of interest, preadministration of HGF plasmid 24 h before folic acid injection dramatically protected renal epithelial cells from both apoptotic and necrotic death and preserved the structural and functional integrity of renal tubules. Expression of HGF transgene activated protein kinase B/Akt kinase and preserved prosurvival Bcl-xL protein expression in vivo. These results indicate that a single, intravenous injection of naked plasmid containing HGF gene not only promotes renal regeneration after injury but also protects tubular epithelial cells from the initial injury and cell death in the first place. These data suggest that HGF gene therapy may provide a new avenue for exploring a novel therapeutic strategy for clinical acute renal failure.
机译:肝细胞生长因子(HGF)是一种多营养因子,在损伤后的组织修复和再生中起着重要作用。叶酸诱导的急性肾损伤后,HGF及其c-met受体基因的表达均迅速上调。在这项研究中,在小鼠中检查了外源性HGF通过全身施用含巨细胞病毒启动子(pCMV-HGF)驱动的人HGF cDNA的裸质粒预防急性肾衰竭的作用。静脉内注射pCMV-HGF质粒在小鼠肾脏中产生了大量的人类HGF蛋白。同时注射HGF质粒DNA可显着改善肾功能不全,并加速从叶酸引起的急性损伤中恢复。有趣的是,在叶酸注射前24小时预先施用HGF质粒可显着保护肾脏上皮细胞免于凋亡和坏死,并保留了肾小管的结构和功能完整性。 HGF转基因的表达在体内激活了蛋白激酶B / Akt激酶并保留了生存前Bcl-xL蛋白表达。这些结果表明,单次静脉内注射含有HGF基因的裸质粒,不仅促进了损伤后的肾脏再生,而且还保护了肾小管上皮细胞免受最初的损伤和细胞死亡。这些数据表明,HGF基因治疗可能为探索临床急性肾功能衰竭的新治疗策略提供一条新途径。

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