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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Spinal cord dynorphin precursor intermediates decline during late gestation.
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Spinal cord dynorphin precursor intermediates decline during late gestation.

机译:妊娠晚期脊髓强啡肽前体中间体下降。

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This laboratory has previously reported that the maternal opioid analgesia associated with pregnancy and parturition is mediated, at least in part, by a maternal spinal cord dynorphin/kappa opioid system. This analgesia is accompanied by an increase in dynorphin peptides (1-17 and 1-8) in the lumbar spinal cord. Levels of trypsin-generated arginine6-leucine-enkephalin (Leu-Enk-Arg)-immunoreactive determinants were also determined and used to reflect the content of dynorphin precursor intermediates. In spinal tissue, the amount of dynorphin A (1-17) contained in the form of precursor is, at a minimum, 10-fold higher than the content of mature dynorphin A (1-17) or dynorphin (1-8). During gestational day 22, the content of dynorphin precursor is reduced significantly (approximately 50%). The decline in the magnitude of dynorphin precursor intermediates in the spinal cord of pregnant rats vastly exceeds the magnitude of increase in the content of dynorphin peptides (1-17 and 1-8). This difference can bestbe explained by postulating a corresponding increase in the rate of release of spinal cord dynorphin (1-17). It is suggested that enhanced processing of dynorphin precursor intermediates represents the initial biochemical level of adaptation of spinal dynorphin neurons to increased demands of pregnancy.
机译:该实验室先前已经报道,与妊娠和分娩相关的母亲阿片类镇痛作用至少部分由母亲脊髓强啡肽/κ阿片类药物系统介导。这种镇痛作用伴随着腰脊髓强啡肽的增加(1-17和1-8)。还确定了胰蛋白酶产生的精氨酸6-亮氨酸-脑啡肽(Leu-Enk-Arg)-免疫反应决定簇的水平,并用于反映强啡肽前体中间体的含量。在脊髓组织中,前体形式的强啡肽A(1-17)的含量至少比成熟强啡肽A(1-17)或强啡肽(1-8)的含量高10倍。在妊娠第22天,强啡肽前体的含量显着降低(约50%)。孕鼠脊髓中强啡肽前体中间体的含量下降幅度大大超过了强啡肽含量(1-17和1-8)的上升幅度。可以通过假设脊髓强啡肽释放速率的相应增加来最好地解释这种差异(1-17)。提示强啡肽前体中间体的增强处理代表了脊髓强啡肽神经元适应妊娠需求增加的初始生化水平。

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