首页> 外文期刊>Neuroendocrinology: International Journal for Basic and Clinical Studies on Neuroendocrine Relationships >The neurotrophins NT3 and BDNF induce selective specification of neuropeptide coexpression and neuronal connectivity in arcuate and periventricular hypothalamic neurons in vitro.
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The neurotrophins NT3 and BDNF induce selective specification of neuropeptide coexpression and neuronal connectivity in arcuate and periventricular hypothalamic neurons in vitro.

机译:神经营养蛋白NT3和BDNF在体外诱导弓形和脑室下丘脑神经元中神经肽共表达和神经元连接的选择性规范。

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Little is known on the influence of epigenetic factors in the developing hypothalamus, a region particularly involved in neuroendocrine regulation and rich in neuropeptides. The present study evaluated the effects of neurotrophins and neuronal activity on neuronal differentiation in hypothalamic cultures sampled from either arcuate or anterior periventricular regions of 17-day-old Sprague-Dawley fetuses. Expression of neuropeptides, tyrosine hydroxylase, neurotrophins and neurotrophin receptors was tested on young (6 days in vitro, DIV) and more mature (14 DIV) cultured neurons by multiple reverse transcription polymerase chain reaction on single cells. In parallel, spontaneous postsynaptic currents were recorded as an index of neuronal connectivity. Neurotrophin-3 (NT3) was expressed in a much larger population of neurons than brain-derived neurotrophic factor (BDNF) at both culture times. At 6 DIV, synaptic currents were scarce and expression of the neurotrophin receptors trkB and trkC was found in a small proportion of neurons only. These parameters increased markedly between 6 and 14 DIV, and also upon addition of neurotrophins. The most striking consequence of arcuate neuron maturation in vitro between 6 and 14 DIV was a marked phenotypic specification affecting somatostatin, neuropeptide Y and pro-opiomelanocortin, the three major neuropeptides expressed in the cultures. NT3, but not BDNF, was able to reproduce maturation-related phenotypic specification in 6 DIV arcuate cultures. Maturation-dependent phenotypic specification was less marked in periventricular cultures; in that case BDNF, not NT3 had a slight effect on phenotype specification. It is concluded that NT3 plays a selective role in phenotypic specification of neuropeptides in the arcuate region, whereas other maturation parameters (neurotrophin receptor expression and/or synaptogenesis) can be potentiated by either neurotrophin in both structures.
机译:关于表观遗传因素对发育中的下丘脑的影响知之甚少,下丘脑是一个特别参与神经内分泌调节且富含神经肽的区域。本研究评估了从17天大的Sprague-Dawley胎儿的弓形或前室周围区域采集的下丘脑培养物中神经营养蛋白和神经元活性对神经元分化的影响。通过在单个细胞上进行多次逆转录聚合酶链反应,在年轻(体外培养6天,DIV)和更成熟(14 DIV)培养的神经元上测试了神经肽,酪氨酸羟化酶,神经营养蛋白和神经营养蛋白受体的表达。同时,自发的突触后电流被记录为神经元连通性的指标。在两个培养时间中,Neurotrophin-3(NT3)在比脑源性神经营养因子(BDNF)大得多的神经元中表达。在6 DIV时,突触电流稀少,仅在一小部分神经元中发现了神经营养蛋白受体trkB和trkC的表达。这些参数在6到14 DIV之间以及加入神经营养蛋白后显着增加。在6至14 DIV之间体外弓形神经元成熟的最显着结果是明显的表型指标,影响生长抑素,神经肽Y和前opiomelanocortin,这是培养物中表达的三种主要神经肽。 NT3,但不是BDNF,能够在6 DIV弓形培养物中复制与成熟相关的表型。在脑室周围培养中,与成熟有关的表型指标较少。在这种情况下,BDNF而非NT3对表型指标有轻微影响。结论是,NT3在弧形区域中神经肽的表型规范中起选择性作用,而在两个结构中,任一神经营养蛋白均可增强其他成熟参数(神经营养蛋白受体表达和/或突触形成)。

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