Araujo D M, Lapchak P A, Hefti F
Department of Neurogerontology, Andrus Gerontology Center, University of Southern California, Los Angeles.
J Neurochem. 1993 Sep;61(3):899-910. doi: 10.1111/j.1471-4159.1993.tb03601.x.
The present study compares the effects of chronic administration of basic fibroblast growth factor (bFGF) and nerve growth factor (NGF) on various hippocampal cholinergic parameters in rats with partial unilateral fimbrial transections. Lesions resulted in marked reductions of several presynaptic cholinergic parameters: choline acetyltransferase (ChAT) activity (by 50%), [3H]-acetylcholine ([3H]ACh) synthesis (by 59%), basal and veratridine (1 microM)-evoked [3H]ACh release (by 44 and 57%, respectively), and [3H]vesamicol binding site densities (by 35%). In addition, [3H]AF-DX 116/muscarinic M2 binding site densities were also modestly decreased (by 23%). In contrast, [3H]pirenzepine/muscarinic M1 and [3H]AF-DX 384/muscarinic M2/M4 binding site densities were not altered by the lesions, nor were they affected by any of the treatments. Intracerebroventricular administration of bFGF (10 ng, every other day, for 21 days) partially prevented the lesion-induced deficit in hippocampal ChAT activity, an effect that was not markedly different from that measured in the NGF-treated (1 microgram, intracerebroventricularly, every other day, for 21 days) rats. In rats treated with a combination of bFGF and NGF, ChAT activity was not different from that in rats treated with the individual factors alone. In contrast, the lesion-induced deficits in the other cholinergic parameters were not attenuated by bFGF treatment, although they were at least partially prevented by NGF administration. To determine whether higher concentrations of bFGF are necessary to affect cholinergic parameters other than hippocampal ChAT activity, rats were treated with 1 microgram (every other day, 21 days) of the growth factor. In this group of rats, detrimental effects of bFGF, manifested by an increased death rate (46%), and marked reductions in body weight of the survivors, were observed. In addition, this concentration of bFGF appeared to exacerbate the lesion-induced reduction in [3H]ACh synthesis by hippocampal slices; [3H]ACh synthesis in lesioned hippocampi represented 36 and 52% of that in contralateral unlesioned hippocampi for the bFGF-treated and control groups, respectively. In conclusion, although bFGF administration attenuates the deficit in hippocampal ChAT activity induced by partial fimbrial transections, this does not appear to translate into enhanced functional capacity of the cholinergic terminals. This is clearly in contrast to NGF, which enhances not only hippocampal ChAT activity, but also other parameters indicative of increased function in the cholinergic terminals.
本研究比较了长期给予碱性成纤维细胞生长因子(bFGF)和神经生长因子(NGF)对部分单侧穹窿横断大鼠海马多种胆碱能参数的影响。损伤导致多个突触前胆碱能参数显著降低:胆碱乙酰转移酶(ChAT)活性(降低50%)、[3H] - 乙酰胆碱([3H]ACh)合成(降低59%)、基础状态及藜芦碱(1 microM)诱发的[3H]ACh释放(分别降低44%和57%)以及[3H]vesamicol结合位点密度(降低35%)。此外,[3H]AF - DX 116/毒蕈碱M2结合位点密度也略有降低(降低23%)。相比之下,[3H]哌仑西平/毒蕈碱M1和[3H]AF - DX 384/毒蕈碱M2/M4结合位点密度未因损伤而改变,也不受任何一种处理的影响。脑室内给予bFGF(10 ng,隔日一次,共21天)部分预防了损伤诱导的海马ChAT活性缺陷,该效应与NGF处理组(1微克,脑室内给药,隔日一次,共21天)大鼠所测效应无明显差异。在同时接受bFGF和NGF联合治疗的大鼠中,ChAT活性与单独接受单一因子治疗的大鼠无差异。相比之下,bFGF治疗并未减轻损伤诱导的其他胆碱能参数缺陷,尽管NGF给药至少部分预防了这些缺陷。为了确定是否需要更高浓度的bFGF来影响除海马ChAT活性之外的胆碱能参数,对大鼠给予1微克(隔日一次,共21天)的生长因子。在这组大鼠中,观察到bFGF的有害作用,表现为死亡率增加(46%)以及存活者体重显著降低。此外,该浓度的bFGF似乎加剧了损伤诱导的海马切片[
