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首页> 外文期刊>Gene therapy >Systemic administration of naked DNA with targeting specificity to mammalian kidneys.
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Systemic administration of naked DNA with targeting specificity to mammalian kidneys.

机译:裸DNA的全身给药,对哺乳动物肾脏具有靶向特异性。

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摘要

A major challenge for gene therapy is to be able to deliver efficiently the gene of interest to specific cell types. Here we describe a safe and simple effective naked DNA gene delivery method, via inferior vena cava (IVC) injection, to the recipient's kidneys. It was further demonstrated that gene expression was concentrated in the proximal tubular epithelial cells of the cortico-medullary region of the kidney. Confocal microscopy analyses demonstrated the presence of the exogenous DNA in the renal cell membrane 10 min postgene delivery. However, it was only by 30 min that the presence of the exogenous DNA could be detected in the cell cytoplasm and in the nuclei of the renal cells. Stable expression of the beta-galactosidase gene could be detected for up to 35 days and no toxicity or any adverse pathological effect associated with the delivery method could be observed. Importantly, this IVC gene delivery method could promote the targeting of genes to carcinoma established in the kidney of SCID mice. These results provide the first evidence to support that stable gene expression could be achieved in the renal cells of kidney and the established carcinoma in the kidneys following in vivo gene delivery with naked DNA and could therefore provide the potential to design protocols for the gene therapy of the kidney diseases.
机译:基因治疗的主要挑战是能够有效地将感兴趣的基因传递给特定的细胞类型。在这里,我们描述了通过下腔静脉(IVC)注射到接受者肾脏的一种安全,简单有效的裸DNA基因传递方法。进一步证明基因表达集中在肾脏的皮质-髓质区域的近端肾小管上皮细胞中。共聚焦显微镜分析表明,在基因递送后10分钟,肾细胞膜中存在外源DNA。但是,只有到30分钟时,才能在细胞质和肾细胞核中检测到外源DNA的存在。 β-半乳糖苷酶基因可稳定表达长达35天,并且未观察到毒性或与递送方法相关的任何不良病理作用。重要的是,这种IVC基因递送方法可以促进将基因靶向SCID小鼠肾脏中建立的癌。这些结果提供了第一个证据,证明了在裸露的DNA体内基因递送后,可以在肾脏的肾细胞和已建立的肾脏癌中实现稳定的基因表达,因此可以为设计针对该基因的基因疗法提供潜力。肾脏疾病。

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