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培养的中隔和海马神经元对乙醇及神经营养物质的反应性。

Responsiveness of cultured septal and hippocampal neurons to ethanol and neurotrophic substances.

作者信息

Heaton M B, Paiva M, Swanson D J, Walker D W

机构信息

Department of Neuroscience, University of Florida Brain Institute, Gainesville.

出版信息

J Neurosci Res. 1994 Oct 15;39(3):305-18. doi: 10.1002/jnr.490390308.

Abstract

Dissociated septal and hippocampal neurons from E18 fetal rats were cultured with varying concentrations of ethanol (0.6-2.4 g/dl) and in cultures containing ethanol plus nerve growth factor (NGF) or basic fibroblast growth factor (bFGF). These substances have been shown to provide neurotrophic support for these populations and to afford neuroprotection against certain toxic substances or conditions applied to some neuronal populations. Both the septal and hippocampal neurons responded to ethanol in a dose-dependent manner. Survival of septal neurons was generally unaffected by initial ethanol concentrations of 0.6 and 1.2 g/dl but was considerably impaired by higher concentrations (1.8 and 2.4 g/dl), while neurite outgrowth was compromised by all ethanol concentrations except the lowest one applied. The hippocampal neurons survived ethanol concentrations up to 2.4 g/dl, although process extension was decreased in concentrations of 1.2 g/dl and higher. NGF or bFGF in the culture medium (in cultures without ethanol) did not affect neuronal survival or process outgrowth in either population, probably owing to the relatively high plating densities of the cultures. NGF did tend to have a moderate ameliorative effect on the ethanol neurotoxicity in the septal cultures, however, and was slightly effective in this regard in hippocampal cultures at intermediate ethanol concentrations (1.8 g/dl). High concentrations of ethanol (2.4 g/dl) reduced the proportion of cholinergic cells in the septal preparations by approximately 50%. This neuronal loss could be reversed by inclusion of high concentrations of NGF in the culture medium (100 ng/ml) but not by a lower concentration (20 ng/ml). bFGF provided some protection against ethanol cytotoxicity with respect to both populations. The implications of these results for studies of fetal alcohol effects are discussed, as well as their relation to prior reports of trophic factor neuroprotection.

摘要

将来自E18胎鼠的分离的隔区和海马神经元与不同浓度的乙醇(0.6 - 2.4 g/dl)一起培养,并在含有乙醇加神经生长因子(NGF)或碱性成纤维细胞生长因子(bFGF)的培养物中培养。这些物质已被证明可为这些细胞群体提供神经营养支持,并对应用于某些神经元群体的某些有毒物质或条件提供神经保护作用。隔区和海马神经元均以剂量依赖性方式对乙醇作出反应。隔区神经元的存活通常不受初始乙醇浓度0.6和1.2 g/dl的影响,但在较高浓度(1.8和2.4 g/dl)时会受到显著损害,而除了所应用的最低浓度外,所有乙醇浓度都会损害神经突生长。海马神经元在高达2.4 g/dl的乙醇浓度下存活,尽管在1.2 g/dl及更高浓度下突起延伸减少。培养基中的NGF或bFGF(在无乙醇的培养物中)对这两种细胞群体的神经元存活或突起生长均无影响,这可能是由于培养物的接种密度相对较高。然而,NGF确实倾向于对隔区培养物中的乙醇神经毒性有适度的改善作用,并且在中等乙醇浓度(1.8 g/dl)下在海马培养物中在这方面有轻微效果。高浓度的乙醇(2.4 g/dl)使隔区制剂中胆碱能细胞的比例降低了约50%。这种神经元损失可通过在培养基中加入高浓度的NGF(100 ng/ml)来逆转,但不能通过较低浓度(20 ng/ml)逆转。bFGF对这两种细胞群体的乙醇细胞毒性都提供了一定的保护作用。讨论了这些结果对胎儿酒精效应研究的意义,以及它们与先前关于营养因子神经保护作用报告之间的关系。

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