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一种用于成年哺乳动物脑内体内基因转移的强大非病毒载体:聚乙烯亚胺。

A powerful nonviral vector for in vivo gene transfer into the adult mammalian brain: polyethylenimine.

作者信息

Abdallah B, Hassan A, Benoist C, Goula D, Behr J P, Demeneix B A

机构信息

Laboratoire de Physiologie Générale et Comparée, U.R.A. 90 CNRS, Muséum National d'Histoire Naturelle, Paris, France.

出版信息

Hum Gene Ther. 1996 Oct 20;7(16):1947-54. doi: 10.1089/hum.1996.7.16-1947.

Abstract

Nonviral gene transfer into the central nervous system (CNS) offers the prospect of providing safe therapies for neurological disorders and manipulating gene expression for studying neuronal function. However, results reported so far have been disappointing. We show that the cationic polymer polyethylenimine (PEI) provides unprecedentedly high levels of transgene expression in the mature mouse brain. Three different preparations of PEI (25-, 50-, and 800-kD) were compared for their transfection efficiencies in the brains of adult mice. The highest levels of transfection were obtained with the 25-kD polymer. With this preparation, DNA/PEI complexes bearing mean ionic charge ratios closest to neutrality gave the best results. Under such conditions, and using a cytomegalovirus (CMV)-luciferase construction, we obtained up to 0.4 10(6) RLU/microgram DNA (equivalent to 0.4 ng of luciferase), which is close to the values obtained using PEI to transfect neuronal cultures and the more easily transfected newborn mouse brain (10(6) RLU/microgram DNA). Widespread expression (over 6 mm3) of marker (luciferase) or functional genes (bcl2) was obtained in neurons and glia after injection into the cerebral cortex, hippocampus, and hypothalamus. Transgene expression was found more than 3 months post-injection in cortical neurons. No morbidity was observed with any of the preparations used. Thus, PEI, a low-toxicity vector, appears to have potential for fundamental research and genetic therapy of the brain.

摘要

非病毒基因导入中枢神经系统(CNS)为神经疾病提供安全治疗以及为研究神经元功能而操纵基因表达带来了希望。然而,目前报道的结果并不理想。我们发现阳离子聚合物聚乙烯亚胺(PEI)能在成熟小鼠脑中实现前所未有的高水平转基因表达。比较了三种不同制备的PEI(25kD、50kD和800kD)在成年小鼠脑内的转染效率。25kD聚合物的转染水平最高。用这种制剂,平均离子电荷比最接近中性的DNA/PEI复合物效果最佳。在这种条件下,使用巨细胞病毒(CMV)-荧光素酶构建体,我们获得了高达0.4×10⁶RLU/μg DNA(相当于0.4 ng荧光素酶),这接近使用PEI转染神经元培养物以及更容易转染的新生小鼠脑所获得的值(10⁶RLU/μg DNA)。将标记基因(荧光素酶)或功能基因(bcl2)注入大脑皮层、海马体和下丘脑后,在神经元和神经胶质细胞中获得了广泛表达(超过6 mm³)。在注射后3个多月仍能在皮层神经元中发现转基因表达。使用的任何制剂均未观察到发病情况。因此,低毒性载体PEI似乎在脑的基础研究和基因治疗方面具有潜力。

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