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首页> 外文期刊>NMR in biomedicine >Quantitative manganese tract tracing: dose-dependent and activity-independent terminal labelling in the mouse visual system
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Quantitative manganese tract tracing: dose-dependent and activity-independent terminal labelling in the mouse visual system

机译:定量锰线描迹:鼠标视觉系统中的剂量依赖性和活性依赖性终端标记

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摘要

At concentrations sufficient for visualisation using MRI, manganese (Mn) is believed to behave as a calcium analogue. This Study examines different concentrations of Mn for enhanced MR tract tracing. The premise of activity-dependent axonal transport was also examined by partial or complete blockade of retinal ganglion cell activity. Quantitative T-1, maps and semi-quantitative normalised signal intensities in the superior colliculi facilitated assessment of applied intraocular concentrations and activity dependence, respectively. Varying the concentration of applied Mn revealed a non-monotonic profile, with optimal, unfavourable and undesirable effects noted: 25 mM proved optimal, showing a maximal decrease in T-1, whereas 400 mM was associated with no terminal-field enhancement. The estimated vitreal concentration for optimal transport of Mn (2 mM) is substantially lower than that used in previous Studies of the mouse. Both the partial blockade of inputs to 50% of retinal ganglion cells by a mGluR6 glutamate agonist and the complete blockade of all retinal ganglion cell activity with tetrodotoxin failed to decrease the relative enhancement in the superior colliculus. The failure to prevent axonal transport of Mn by blocking activity (and therefore theoretically the intracellular influx) appeared to be paradoxical. The optimal vitreal concentration of Mn has previously been shown to facilitate massive intracellular uptake of Mn, competitively blocking calcium, and 1 mM Mn blocks neurotransmission pre-synaptically. These results Suggest that. at concentrations required for optimal Mn-enhanced MRI tract tracing in the Visual system of the mouse, the uptake and transport of Mn may be dominated by passive mechanisms, which may also block neurotransmission. Copyright (C) 2008 John Wiley & Sons, Ltd.
机译:在足以使用MRI可视化的浓度下,锰(Mn)被认为具有钙类似物的作用。这项研究检查了不同浓度的Mn,以增强MR道追踪。还通过部分或完全阻断视网膜神经节细胞活性来检查依赖于活性的轴突运输的前提。上丘中的定量T-1,图谱和半定量归一化信号强度分别有助于评估眼内浓度和活动依赖性。改变所施加的Mn浓度显示出非单调曲线,并注意到最佳,不利和不良影响:25 mM被证明是最佳的,显示出T-1的最大降低,而400 mM与终端场增强无关。用于最佳运输锰的估计玻璃体浓度(2 mM)大大低于先前对小鼠的研究。 mGluR6谷氨酸激动剂部分阻断50%的视网膜神经节细胞的输入,而河豚毒素完全阻断所有视网膜神经节细胞的活性,均不能降低上丘的相对增强。通过阻止活性来阻止Mn轴突运输的失败(因此从理论上讲是细胞内的涌入)似乎是自相矛盾的。先前已证明最佳的玻璃体内Mn浓度可促进细胞内大量摄取Mn,竞争性阻断钙,而1 mM Mn则先突触地阻断神经传递。这些结果表明。在小鼠视觉系统中最佳锰增强MRI描迹所需的浓度下,锰的吸收和运输可能受被动机制支配,这也可能阻止神经传递。版权所有(C)2008 John Wiley&Sons,Ltd.

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