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供体年龄和脑源性神经营养因子对新生大鼠黑质纹状体共培养物中多巴胺能神经元存活及轴突生长的影响。

Effects of donor age and brain-derived neurotrophic factor on the survival of dopaminergic neurons and axonal growth in postnatal rat nigrostriatal cocultures.

作者信息

Ostergaard K, Jones S A, Hyman C, Zimmer J

机构信息

Department of Anatomy and Cell Biology, University of Odense, Denmark.

出版信息

Exp Neurol. 1996 Dec;142(2):340-50. doi: 10.1006/exnr.1996.0203.

Abstract

Early postnatal rat brain tissue can be grown for several weeks as organotypic slice cultures by the roller-tube method. We have here used this method to study the effects of donor age and brain-derived neurotrophic factor (BDNF) on the survival and growth of tyrosine hydroxylase immunoreactive (TH-i), dopaminergic (DA) neurons during the postnatal period when their nerve fibers normally innervate the striatal target. Tissue slices of ventral mesencephalon (VM) and striatum were prepared from newborn and 7-day-old rats and cocultured for 3--3 1/2 weeks with different combinations of the two donor ages. After immunocytochemical staining the number of TH-i, ventral mesencephalic neurons were counted, and the growth of TH-i fibers into the striatal part of the cocultures was evaluated. Co-cultures, with both VM and striatal slices prepared from newborn rats, contained a significantly higher number of TH-i neurons and displayed a significantly increased innervation of the striatal slices compared with other combinations of donor ages. Addition of BDNF resulted in both an increased survival of TH-i neurons and an increased growth of TH-i fibers into the cocultured striatal slices. Significant neurotrophic effect of BDNF did, however, require young donor age of both VM and striatal slices. It is suggested that BDNF induces more cells, possibly progenitor cells, to express TH immunoreactivity. Alternatively BDNF may suppress apoptotic cell death documented by others to occur in the postnatal rat substantia nigra pars compacta. Irrespective of the mechanisms, survival of more TH-i neurons was related to an increased innervation of the striatal slices by TH-i nerve fibers. The observed effects of BDNF on both survival and fiber growth of TH-i neurons indicate a potential role of BDNF for treatment of Parkinson's disease or grafts of immature DA neurons transplanted to patients with Parkinson's disease. A significant trophic effect of BDNF did, however, seem to depend on young developmental age of both striatum and VM. Parallel treatment with striatal neurotrophic factors may therefore be a necessary prerequisite to a trophic effect of BDNF under clinical conditions.

摘要

通过滚管法,出生后早期的大鼠脑组织可以作为器官型切片培养物生长数周。我们在此使用该方法研究供体年龄和脑源性神经营养因子(BDNF)对酪氨酸羟化酶免疫反应性(TH-i)多巴胺能(DA)神经元在出生后时期的存活和生长的影响,此时期其神经纤维通常支配纹状体靶区。从新生大鼠和7日龄大鼠制备腹侧中脑(VM)和纹状体的组织切片,并将来自两种供体年龄的不同组合的切片共同培养3 - 3.5周。免疫细胞化学染色后,计数TH-i腹侧中脑神经元的数量,并评估TH-i纤维向共同培养物的纹状体部分的生长情况。与其他供体年龄组合相比,由新生大鼠制备的VM和纹状体切片的共同培养物中,TH-i神经元数量显著更多,并且纹状体切片的神经支配显著增加。添加BDNF导致TH-i神经元的存活率增加以及TH-i纤维向共同培养的纹状体切片中的生长增加。然而,BDNF的显著神经营养作用确实需要VM和纹状体切片均来自年轻的供体。提示BDNF诱导更多细胞,可能是祖细胞,表达TH免疫反应性。或者,BDNF可能抑制其他人记录到的在出生后大鼠黑质致密部发生的凋亡性细胞死亡。无论机制如何,更多TH-i神经元的存活与TH-i神经纤维对纹状体切片的神经支配增加有关。观察到的BDNF对TH-i神经元的存活和纤维生长的影响表明BDNF在治疗帕金森病或移植到帕金森病患者的未成熟DA神经元移植物方面具有潜在作用。然而,BDNF的显著营养作用似乎取决于纹状体和VM两者的年轻发育年龄。因此,在临床条件下,与纹状体神经营养因子的联合治疗可能是BDNF产生营养作用的必要前提。

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