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脑源性神经营养因子(BDNF)可防止穹窿横断后内侧隔区胆碱能神经元的退变。

Brain-derived neurotrophic factor (BDNF) prevents the degeneration of medial septal cholinergic neurons following fimbria transection.

作者信息

Morse J K, Wiegand S J, Anderson K, You Y, Cai N, Carnahan J, Miller J, DiStefano P S, Altar C A, Lindsay R M

机构信息

Regeneron Pharmaceuticals Inc., Tarrytown, New York 10591-6707.

出版信息

J Neurosci. 1993 Oct;13(10):4146-56. doi: 10.1523/JNEUROSCI.13-10-04146.1993.

Abstract

Brain-derived neurotrophic factor (BDNF), a member of the neurotrophin family, supports the survival of developing basal forebrain cholinergic neurons in vitro and is retrogradely transported by cholinergic neurons of the medial septum and diagonal band following intrahippocampal injections in vivo. To substantiate a potential role for BDNF in the maintenance of forebrain cholinergic neurons in the adult brain, we assessed the ability of BDNF to sustain the phenotype of medial septal cholinergic neurons following a unilateral transection of the fimbria. BDNF, NGF, or vehicle solutions were infused continuously in adult female rats either into the lateral ventricle (intracerebroventricularly) or directly into the septum for 2 weeks beginning at the time of the transection. In vehicle-infused animals, only 28% of the ChAT-immunoreactive neurons remained on the side ipsilateral to the lesion compared to the contralateral intact side. When infused intracerebroventricularly, both BDNF and NGF reduced the extent of the phenotypic loss, in that 44% and 68%, respectively, of the ChAT-immunopositive neurons remained on the lesioned side. Intraseptal infusion proved even more effective, in that following BDNF and NGF treatment 60% and 86%, respectively, of the normal complement of ChAT-immunopositive neurons were apparent on the side ipsilateral to the lesion. Similar results were obtained when an antibody to the low-affinity NGF receptor was used to identify the cholinergic neurons. To determine if the apparent greater efficacy of NGF compared to BDNF might be related to differences in delivery, we examined the patterns of distribution of radiolabeled BDNF and NGF injected into the lateral ventricle. 125I-BDNF showed only very little diffusion from the ventricles into the adjacent neural tissue and negligible retrograde labeling of the neurons within the basal forebrain. 125I-NGF, however, diffused readily into the brain, resulting in widespread retrograde labeling of basal forebrain neurons. A similarly limited distribution pattern was observed where BDNF was detected immunohistochemically in animals infused intracerebroventricularly (12 micrograms/d) for 2 weeks. In contrast, when delivered intraseptally, the same dose of BDNF exhibited a widespread diffusion within the surrounding neuropil and retrograde labeling of neurons in the medial septum and the vertical limb of the diagonal band. Thus, when delivered effectively, BDNF has a substantial capacity to rescue axotomized cholinergic neurons.

摘要

脑源性神经营养因子(BDNF)是神经营养因子家族的一员,在体外可支持发育中的基底前脑胆碱能神经元的存活,并且在体内海马注射后,可被内侧隔核和斜角带的胆碱能神经元逆行转运。为了证实BDNF在成体大脑中维持前脑胆碱能神经元方面的潜在作用,我们评估了BDNF在海马伞单侧横断后维持内侧隔核胆碱能神经元表型的能力。从横断时开始,将BDNF、神经生长因子(NGF)或赋形剂溶液连续2周注入成年雌性大鼠的侧脑室(脑室内)或直接注入隔核。在注入赋形剂的动物中,与对侧完整侧相比,损伤同侧仅28%的胆碱乙酰转移酶(ChAT)免疫反应性神经元存活。当脑室内注入时,BDNF和NGF均减少了表型丧失的程度,损伤侧分别有44%和68%的ChAT免疫阳性神经元存活。隔核内注入更为有效,在BDNF和NGF处理后,损伤同侧分别有60%和86%的正常ChAT免疫阳性神经元数量。当使用低亲和力NGF受体抗体鉴定胆碱能神经元时,也得到了类似的结果。为了确定与BDNF相比,NGF明显更高的效力是否可能与递送差异有关,我们检查了注入侧脑室的放射性标记BDNF和NGF的分布模式。125I-BDNF仅从脑室向邻近神经组织有极少的扩散,并且在前脑基底内的神经元逆行标记可忽略不计。然而,125I-NGF很容易扩散到脑内,导致前脑基底神经元广泛的逆行标记。在脑室内注入(12微克/天)2周的动物中,通过免疫组织化学检测到的BDNF也观察到类似的有限分布模式。相反,当隔核内递送时,相同剂量的BDNF在周围神经毡内广泛扩散,并在内侧隔核和斜角带垂直支的神经元中逆行标记。因此,当有效递送时,BDNF具有挽救轴突切断的胆碱能神经元的巨大能力。

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