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GENE TRANSFER USING NONVIRAL DELIVERY SYSTEMS.

机译:使用非病毒传递系统进行基因转移。

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In peritoneal dialysis, loss of peritoneal function is a major factor in treatment failure. The alterations in peritoneal function are related to structural changes in the peritoneal membrane, including peritoneal sclerosis with increased extracellular matrix. Although peritoneal sclerosis is considered reversible to some extent through peritoneal rest, which improves peritoneal function and facilitates morphological changes, there has been no therapeutic intervention and no drug against the development and progression of peritoneal sclerosis. Using recent biotechnological advances in genetic engineering, a strategy based on genetic modification of the peritoneal membrane could be a potential therapeutic maneuver against peritoneal sclerosis and peritoneal membrane failure. Before this gene therapy may be applied clinically, a safe and effective gene delivery system as well as the selection of a gene therapy method must be established. There are presently two kinds of gene transfer vectors: viral and nonviral. Viral vectors are used mainly as a gene delivery system in the field of continuous ambulatory peritoneal dialysis research; however, they have several problems such as immunogenicity and toxicity. On the other hand, nonviral vectors have several advantages over viral vectors. We review here gene transfer using nonviral vector systems in the peritoneum: electroporation, liposomes, and cationized gelatin microspheres. In the field of peritoneal dialysis, gene therapy research using nonviral vectors is presently limited. Improvement in delivery methods together with an intelligent design of targeted genes has brought about large degrees of enhancement in the efficiency, specificity, and temporal control of nonviral vectors.
机译:在腹膜透析中,腹膜功能丧失是治疗失败的主要因素。腹膜功能的改变与腹膜的结构变化有关,包括具有增加的细胞外基质的腹膜硬化。尽管腹膜硬化被认为​​可通过腹膜休息在某种程度上可逆,从而改善腹膜功能并促进形态学改变,但尚无治疗干预措施,也没有针对腹膜硬化发展和进程的药物。利用基因工程领域的最新生物技术进展,基于腹膜遗传修饰的策略可能是针对腹膜硬化和腹膜衰竭的潜在治疗手段。在该基因治疗可以临床应用之前,必须建立安全有效的基因递送系统以及选择基因治疗方法。目前有两种基因转移载体:病毒和非病毒。在连续非卧床腹膜透析研究领域中,病毒载体主要用作基因传递系统。但是,它们具有一些问题,例如免疫原性和毒性。另一方面,非病毒载体比病毒载体具有多个优点。我们在这里回顾了在腹膜中使用非病毒载体系统进行的基因转移:电穿孔,脂质体和阳离子化明胶微球。在腹膜透析领域,使用非病毒载体的基因治疗研究目前受到限制。递送方法的改进以及靶向基因的智能设计已经带来了非病毒载体效率,特异性和时间控制的极大提高。

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