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首页> 外文期刊>Current gene therapy >Cytoglobin: a novel potential gene medicine for fibrosis and cancer therapy.
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Cytoglobin: a novel potential gene medicine for fibrosis and cancer therapy.

机译:细胞球蛋白:一种用于纤维化和癌症治疗的新型潜在基因药物。

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摘要

Attempts have been made by conventional gene therapy to suppress hepatic fibrogenesis, but potential oncogenic activity may prevent its clinical use. Recently, a novel major approach has been developed for resolution of liver fibrosis and cirrhosis: inactivation of hepatic stellate cells (HSC) using the endogenous expressing gene, which could mediate the homeostatic adaptation of liver. Cytoglobin (Cygb), originally identified in cultured rat HSC, is in a new class of heme containing proteins known as the hexacoordinate globin superfamily. These proteins exhibit peroxidase activity against hydrogen peroxides and lipid hydroperoxides. Considerable attention has been focused on the potential benefits of use of Cygb in fibrosis therapy, as up-regulation of Cygb expression could reduce oxidant stress, suppress HSC differentiation to a myofibroblast-like phenotype and eventually prevent the progress of liver fibrosis. Cygb has also been found to be a candidate tumor suppressor gene that might provide a new option for cancer gene therapy. In this review we systematically analyze the potential of Cygb as a prospective gene medicine for curing fibrosis, cancer, and other diseases such as diabetes. The molecular structure, regulation and subcellular location of Cygb are reviewed as well.
机译:常规基因疗法已经尝试抑制肝纤维化,但是潜在的致癌活性可能阻止其临床应用。最近,已开发出一种用于解决肝纤维化和肝硬化的新的主要方法:使用内源性表达基因使肝星状细胞(HSC)失活,这可以介导肝脏的体内稳态。细胞球蛋白(Cygb)最初是在培养的大鼠HSC中鉴定的,属于一类新的血红素,含有称为六配位球蛋白超家族的蛋白质。这些蛋白质对过氧化氢和脂质氢过氧化物表现出过氧化物酶活性。 Cygb在纤维化治疗中的潜在益处已引起人们的极大关注,因为Cygb表达的上调可减少氧化应激,抑制HSC分化为成肌纤维细胞样表型,并最终阻止肝纤维化的进展。还发现Cygb是候选的抑癌基因,可能为癌症基因治疗提供新的选择。在这篇综述中,我们系统地分析了Cygb作为治疗纤维化,癌症和其他疾病(例如糖尿病)的前瞻性基因药物的潜力。还综述了Cygb的分子结构,调控和亚细胞定位。

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