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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Basal forebrain neurons modulate the synthesis and expression of neuropeptides in the rat suprachiasmatic nucleus.
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Basal forebrain neurons modulate the synthesis and expression of neuropeptides in the rat suprachiasmatic nucleus.

机译:基底前脑神经元调节大鼠视交叉上核中神经肽的合成和表达。

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We tested the hypothesis that efferents from the nucleus basalis magnocellularis (NBM) play a direct role in the regulation of neuropeptide synthesis and expression by neurons of the rat suprachiasmatic nucleus (SCN). Adult male rats in which the NBM was destroyed with quinolinic acid, either unilaterally or bilaterally, were compared with rats injected with physiological saline and with control rats. The estimators used to assess the effects of cholinergic deafferentation on the neuroanatomy and neurochemistry of the SCN were the total number of SCN neurons, the total number and somatic size of SCN neurons producing vasopressin (VP) and vasoactive intestinal polypeptide (VIP), and the respective mRNA levels. Bilateral destruction of the NBM did not produce cell death in the SCN, but caused a marked reduction in the number and somatic size of SCN neurons expressing VP and VIP, and in the mRNA levels of these peptides. The decrease in the number of VP- and VIP-producing neurons provoked by unilateral lesions was less striking than that resulting from bilateral lesions. It was, however, statistically significant in the ipsilateral hemisphere, but not in the contralateral hemisphere. The results show that the reduction of cholinergic inputs to the SCN impairs the synthesis, and thereby decreases the expression of neuropeptides by SCN neurons, and that the extent of the decline correlates with the amount of cholinergic afferents destroyed. This supports the notion that acetylcholine plays an important, and direct role in the regulation of the metabolic activity of SCN neurons.
机译:我们测试的假设,即从基底大细胞核(NBM)传出的神经元在大鼠视交叉上核(SCN)的神经元合成和表达的调节中起直接作用。将成年雄性大鼠的单侧或双侧用喹啉酸破坏了NBM,并与注射生理盐水的大鼠和对照组进行了比较。用于评估胆碱能脱除咖啡因对SCN的神经解剖学和神经化学的影响的估算器包括SCN神经元总数,产生加压素(VP)和血管活性肠多肽(VIP)的SCN神经元总数和体细胞大小,以及各自的mRNA水平。 NBM的双边破坏不会在SCN中产生细胞死亡,但会导致表达VP和VIP的SCN神经元的数量和体细胞大小以及这些肽的mRNA水平显着降低。由单侧病变引起的产生VP和VIP的神经元数量的减少不如由双侧病变引起的明显。然而,在同侧半球中有统计学意义,但在对侧半球中无统计学意义。结果表明,SCN的胆碱能输入的减少损害了合成,从而降低了SCN神经元神经肽的表达,并且下降的程度与被破坏的胆碱能传入量有关。这支持了乙酰胆碱在SCN神经元代谢活性的调节中起着重要而直接的作用的观点。

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