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A single administration of adenoviral-mediated HGF cDNA permits survival of mice from acute hepatic failure.

机译:腺病毒介导的HGF cDNA的单次给药可使小鼠从急性肝衰竭中存活下来。

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摘要

Heptatocyte growth factor (HGF) having a variety of biological activity was suggested as a protective agent against acute toxic hepatic injury or a potentially therapeutic agent. For the efficient in vivo application of this factor, we employed adenoviral-mediated HGF gene delivery system. In this study, we constructed E1-deleted recombinant adenovirus carrying cDNA of human HGF (Ad.hHGF) and elucidated that HGF was efficiently expressed in the liver of C57/BL mice. A mouse model of acute hepatic failure was induced by high dose (1000mg/kg) of thioacetamide (TA) administration. Mice infected with Ad.hHGF showed a dramatic resistance to TA-induced acute hepatic injury. Serum ALT was increased transiently and then the level was normalized in Ad.hHGF-infected mice with TA administration. Furthermore, the survival rate was remarkably enhanced in the mice infected with Ad.hHGF. In the histological examination, massive hepatic necrosis induced by TA was almost completely protected by HGF produced by Ad.hHGF.Our results indicate that a single dose of HGF-encoding adenoviral vector maintained liver function and prevented the progression of liver necrosis in a mouse model of acute hepatic failure.
机译:具有多种生物学活性的七细胞生长因子(HGF)被建议作为针对急性毒性肝损伤的保护剂或潜在的治疗剂。为了在体内有效地应用该因子,我们采用了腺病毒介导的HGF基因递送系统。在这项研究中,我们构建了带有人类HGF(Ad.hHGF)cDNA的E1缺失重组腺病毒,并阐明了HGF在C57 / BL小鼠肝脏中有效表达。高剂量(1000mg / kg)的硫代乙酰胺(TA)给药可诱发小鼠急性肝衰竭模型。感染Ad.hHGF的小鼠对TA诱导的急性肝损伤表现出显着的抵抗力。血清ALT短暂升高,然后在接受TA的Ad.hHGF感染小鼠中将其水平正常化。此外,用Ad.hHGF感染的小鼠的存活率显着提高。在组织学检查中,TA.hHGF产生的HGF几乎完全保护了TA诱导的大面积肝坏死。我们的结果表明,在小鼠模型中单剂量的编码HGF的腺病毒载体可以维持肝功能并阻止肝坏死的进展急性肝衰竭。

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