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移植到大鼠臂部损伤腔中的胎儿顶盖或皮质组织:对宿主视网膜轴突再生的影响。

Fetal tectal or cortical tissue transplanted into brachial lesion cavities in rats: influence on the regrowth of host retinal axons.

作者信息

Harvey A R, Gan S K, Pauken J M

机构信息

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

出版信息

J Comp Neurol. 1987 Sep 1;263(1):126-36. doi: 10.1002/cne.902630111.

Abstract

Fetal neural tissue was transplanted into suction lesions of the left brachium and pretectal region in young rats. Tectal tissue was grafted into 6-18-day-old rats and cortical tissue was transplanted into 17-20-day-old animals. The aim was to determine whether grafts could potentiate the regrowth of damaged retinal axons and, as a consequence, stimulate the axons to reenter their host target, the superior colliculus (SC). Fifteen to 581 days after transplantation, host retinal projections were traced by injecting the right eye with horseradish peroxidase (HRP). Parallel series of frozen brain sections were stained for HRP histochemistry, acetylcholinesterase, Nissl, or neurofibrils. At all ages studied, grafts survived and grew within the wound cavity; survival was better in the older animals. Most cortical grafts and a small number of tectal grafts filled the wound cavity and formed complete tissue bridges across the lesion. The majority of tectal grafts were attached to one or the other side of the lesion and were connected to the opposite lesion face by glial and connective tissue membranes that formed over the lesion site. In many animals that received tectal transplants, host retinal axons were traced growing into the grafts. Regenerating axons innervated specific, localized areas within the grafts, and it appeared that the axons retained the ability to recognize their appropriate target cells within the graft neuropil. Comparable ingrowth into cortical grafts was not observed. Optic axons were occasionally seen reentering the superficial layers of the host SC; however, compared to fetal tectal grafts, the density of host SC innervation was sparse. The implications of these data are discussed with regard to the possible use of fetal neural tissue grafts as reconstructive tissue bridges in the mammalian central nervous system.

摘要

将胎儿神经组织移植到幼鼠左侧臂丛和顶盖前区的抽吸性损伤部位。将顶盖组织移植到6 - 18日龄的大鼠体内,将皮质组织移植到17 - 20日龄的动物体内。目的是确定移植组织是否能增强受损视网膜轴突的再生,并因此刺激轴突重新进入其宿主靶区——上丘(SC)。移植后15至581天,通过向右眼注射辣根过氧化物酶(HRP)来追踪宿主视网膜投射。对平行系列的冰冻脑切片进行HRP组织化学、乙酰胆碱酯酶、尼氏染色或神经原纤维染色。在所有研究的年龄组中,移植组织在伤口腔内存活并生长;年长动物的存活率更高。大多数皮质移植组织和少数顶盖移植组织填满了伤口腔,并在损伤部位形成了完整的组织桥。大多数顶盖移植组织附着在损伤的一侧或另一侧,并通过在损伤部位形成的神经胶质和结缔组织膜与相对的损伤面相连。在许多接受顶盖移植的动物中,追踪到宿主视网膜轴突长入移植组织。再生轴突支配移植组织内特定的、局部的区域,并且轴突似乎保留了在移植神经毡内识别其合适靶细胞的能力。未观察到轴突长入皮质移植组织的类似情况。偶尔可见视神经轴突重新进入宿主上丘的表层;然而,与胎儿顶盖移植组织相比,宿主上丘的神经支配密度稀疏。结合胎儿神经组织移植作为哺乳动物中枢神经系统重建组织桥的可能用途,对这些数据的意义进行了讨论。

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