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中隔切片中乙酰胆碱的释放是否源于携带p75(神经营养因子受体)受体的内在胆碱能神经元?一项对大鼠使用192 IgG-皂草素损伤的研究。

Does the release of acetylcholine in septal slices originate from intrinsic cholinergic neurons bearing p75(NTR) receptors? A study using 192 IgG-saporin lesions in rats.

作者信息

Birthelmer A, Lazaris A, Riegert C, Marques Pereira P, Koenig J, Jeltsch H, Jackisch R, Cassel J-C

机构信息

Institut für Experimentelle und Klinische Pharmakologie und Toxikologie der Universität Freiburg, Neuropharmakologisches Labor, Hansastrasse 9A, D-79104 Freiburg, Germany.

出版信息

Neuroscience. 2003;122(4):1059-71. doi: 10.1016/j.neuroscience.2003.09.001.

Abstract

In previous studies electrically-evoked release of acetylcholine in septal slices was demonstrated. The present experiment aimed at verifying if this release involved intrinsic neurons bearing p75(NTR) receptors. Long-Evans rats sustained injections of 192 IgG-saporin into the medial septum/diagonal band of Broca (0.8 microg). Sham-operated rats served as controls. Two to 3.5 weeks later, the electrically-evoked release of acetylcholine ([(3)H]ACh) was measured in slices from the lateral septum (LS), medial septum (MS) and diagonal band of Broca (DBB). Choline acetyltransferase (ChAT) and acetylcholinesterase (AChE) activity, and monoamine concentrations were measured in the septum, cortex and hippocampus. The lesion extent was also assessed by ChAT immunostaining in a separate series of rats. In the septum, the number of ChAT-positive neurons was depleted dramatically (>90% at the level of the injection site). In the hippocampus, the lesions reduced ChAT and AChE activity by 91% and 84%, respectively. In the cortex, this reduction was weaker (-55% and -47%). In the septal region, the reduction was either weak or not significant. The evoked release of acetylcholine in septal slices was not reduced, except in the slices from the LS (-64%). The effects of physostigmine and atropine confirmed the presence of autoreceptors. Our data exclude that a major part of the acetylcholine released by MS and DBB slices derived from intrinsic neurons bearing p75(NTR) receptors. In the LS, part of the released acetylcholine might be from projections of such neurons located in the LS, MS and/or DBB. These data also suggest that the MS and the DBB may be the target of extrinsic cholinergic innervation that does not bear p75(NTR) receptors.

摘要

在先前的研究中已证实,在隔区切片中可通过电刺激诱发乙酰胆碱释放。本实验旨在验证这种释放是否涉及表达p75(NTR)受体的内在神经元。将192 IgG-皂草素持续注射到Long-Evans大鼠的内侧隔区/布罗卡斜角带(0.8微克)。假手术大鼠作为对照。2至3.5周后,测量外侧隔区(LS)、内侧隔区(MS)和布罗卡斜角带(DBB)切片中电刺激诱发的乙酰胆碱([³H]ACh)释放。测量隔区、皮质和海马中的胆碱乙酰转移酶(ChAT)和乙酰胆碱酯酶(AChE)活性以及单胺浓度。在另一组大鼠中,还通过ChAT免疫染色评估损伤程度。在隔区,ChAT阳性神经元数量大幅减少(注射部位水平减少>90%)。在海马中,损伤分别使ChAT和AChE活性降低91%和84%。在皮质中,这种降低较弱(-55%和-47%)。在隔区区域,降低要么较弱,要么不显著。隔区切片中乙酰胆碱的诱发释放未减少,除了LS切片(-64%)。毒扁豆碱和阿托品的作用证实了自身受体的存在。我们的数据排除了MS和DBB切片释放的乙酰胆碱主要来源于表达p75(NTR)受体的内在神经元的可能性。在LS中,部分释放的乙酰胆碱可能来自位于LS、MS和/或DBB中的此类神经元的投射。这些数据还表明,MS和DBB可能是不表达p75(NTR)受体的外在胆碱能神经支配的靶点。

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