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成年大鼠外周神经、视顶盖和肌肉移植物中视网膜轴突的再生

Retinal axon regeneration in peripheral nerve, tectal, and muscle grafts in adult rats.

作者信息

Tan M M, Harvey A R

机构信息

Department of Anatomy and Human Biology, The University of Western Australia, Nedlands, Perth, Western Australia 6907, Australia.

出版信息

J Comp Neurol. 1999 Oct 4;412(4):617-32. doi: 10.1002/(sici)1096-9861(19991004)412:4<617::aid-cne4>3.0.co;2-j.

Abstract

This study examined whether prior regenerative growth through peripheral nerve (PN) bridging grafts influenced the specificity with which lesioned adult rat retinal ganglion cell (RGC) axons grew into co-grafts of developing target tissue (fetal superior colliculus). Growth into nontarget (muscle) tissue was also examined. Autologous PN was grafted onto the transected optic nerve. After 14 days, the distal ends of the PNs were placed next to, or inserted into, embryonic tectal tissue or into autologous muscle grafts placed in frontal cortex cavities. Host retinal projections were examined 3-8 months later using anterograde and retrograde tracing techniques. In rats in which there was good apposition between PN and tectal tissue, small numbers of RGC axons were observed growing into the tectal grafts (maximum distance of 180 microm). No evidence of specific innervation of appropriate target regions within tectal grafts was detected, even though such regions (identified by acetylcholinesterase histochemistry) were often located close to the PN grafts. In rats with PN/muscle co-grafts, the extent of retinal axon outgrowth was greater (up to 465 microm from the PN tip) and labelled profiles that resembled motor endplates were seen contacting muscle fibres. Previous studies have shown that spontaneously regenerating RGC axons consistently and selectively innervate appropriate target areas in fetal tectal tissue grafted directly into optic tract lesion cavities. Together, the data suggest that exposure to a PN environment may have reduced the extent of adult retinal axon growth into fetal tectal transplants and affected the way regenerating axons responded to specific developmental cues expressed by target cells in the co-grafted tissue.

摘要

本研究探讨了先前通过周围神经(PN)桥接移植的再生生长是否会影响成年大鼠损伤的视网膜神经节细胞(RGC)轴突向发育中的靶组织(胎儿上丘)共移植体生长的特异性。还研究了其向非靶组织(肌肉)的生长情况。将自体PN移植到横断的视神经上。14天后,将PN的远端置于胚胎顶盖组织旁或插入其中,或插入置于额叶皮质腔的自体肌肉移植体中。3至8个月后,使用顺行和逆行追踪技术检查宿主视网膜投射。在PN与顶盖组织良好对合的大鼠中,观察到少量RGC轴突生长到顶盖移植体中(最大距离为180微米)。尽管顶盖移植体内的适当靶区域(通过乙酰胆碱酯酶组织化学鉴定)通常位于PN移植体附近,但未检测到对这些区域进行特异性神经支配的证据。在有PN/肌肉共移植的大鼠中,视网膜轴突生长的范围更大(距PN尖端可达465微米),并且可见类似运动终板的标记轮廓与肌纤维接触。先前的研究表明,自发再生的RGC轴突始终如一地、选择性地支配直接移植到视束损伤腔内的胎儿顶盖组织中的适当靶区域。总之,这些数据表明,暴露于PN环境可能会减少成年视网膜轴突向胎儿顶盖移植体的生长范围,并影响再生轴突对共移植组织中靶细胞表达的特定发育线索的反应方式。

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