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由腺病毒载体递送的神经营养因子-3可诱导成年大鼠损伤的背根轴突向脊髓内再生。

NT-3 delivered by an adenoviral vector induces injured dorsal root axons to regenerate into the spinal cord of adult rats.

作者信息

Zhang Y, Dijkhuizen P A, Anderson P N, Lieberman A R, Verhaagen J

机构信息

Department of Anatomy and Developmental Biology, University College London, England.

出版信息

J Neurosci Res. 1998 Nov 15;54(4):554-62. doi: 10.1002/(SICI)1097-4547(19981115)54:4<554::AID-JNR12>3.0.CO;2-M.

Abstract

Sensory axons interrupted in the dorsal roots of adult mammals are normally unable to regenerate into the spinal cord. We have investigated whether the introduction of a neurotrophin gene into the spinal cord might offer an approach to otherwise intractable spinal root injuries. The dorsal roots of the 4th, 5th, and 6th lumbar spinal nerves of adult rats were severed and reanastomosed. Fourteen to nineteen days later, adenoviral vectors containing either the LacZ or NT-3 genes were injected into the ventral horn of the lumbar spinal cord, resulting in strong expression of the transgenes in glial cells and motor neurons between 4 and 40 days after injection. When dorsal root axons were transganglionically labelled with HRP conjugated to cholera toxin subunit B, 16 to 37 days after dorsal root injury, large numbers of labelled axons could be seen to have regenerated into the cord, but only in those animals injected with vector carrying the NT-3 gene. The regenerated axons were found at the injection site, mainly in the grey matter, and had penetrated as deep as lamina V. Gene therapy with adenoviral vectors encoding a neurotrophin has therefore been shown to be capable of enhancing and directing the regeneration of a subpopulation of dorsal root axons (probably myelinated A fibres), into and through the CNS environment.

摘要

成年哺乳动物背根中被切断的感觉轴突通常无法再生进入脊髓。我们研究了将神经营养因子基因导入脊髓是否可能为原本难以治疗的脊髓神经根损伤提供一种方法。成年大鼠第4、5和6腰脊髓神经的背根被切断并重新吻合。14至19天后,将含有LacZ或NT-3基因的腺病毒载体注入腰脊髓腹角,导致转基因在注射后4至40天内在神经胶质细胞和运动神经元中强烈表达。当在背根损伤后16至37天用与霍乱毒素B亚基偶联的HRP对背根轴突进行跨神经节标记时,可以看到大量标记的轴突再生进入脊髓,但仅在那些注射了携带NT-3基因载体的动物中。再生轴突在注射部位被发现,主要在灰质中,并且已经深入到V层。因此,用编码神经营养因子的腺病毒载体进行基因治疗已被证明能够增强并引导一部分背根轴突(可能是有髓鞘的A纤维)再生进入并穿过中枢神经系统环境。

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