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新生大鼠心脏、肾脏和肺中大分子合成的β-肾上腺素能调控:与交感神经元发育的关系。

Beta adrenergic control of macromolecule synthesis in neonatal rat heart, kidney and lung: relationship to sympathetic neuronal development.

作者信息

Slotkin T A, Whitmore W L, Orband-Miller L, Queen K L, Haim K

机构信息

Department of Pharmacology, Duke University Medical Center, Durham, North Carolina.

出版信息

J Pharmacol Exp Ther. 1987 Oct;243(1):101-9.

PMID:2444697
Abstract

The sympathetic nervous system has been hypothesized to coordinate the timing of cellular development in peripheral tissues. In the current study, we evaluated the relationships among the ontogeny of sympathetic projections to peripheral organs, the patterns of macromolecule synthesis in those organs and the reactivity of synthetic processes to beta adrenergic stimulation by isoproterenol. The major developmental rise in norepinephrine concentration and turnover, as well as in numbers of beta receptors, occurred during the second to fourth postnatal weeks in renal and lung sympathetic pathways and slightly earlier in the cardiac-sympathetic axis. The developmental decline in DNA synthesis in heart, kidney and lung coincided with the maturation of sympathetic projections. Direct stimulation of beta receptors by the in vivo administration of isoproterenol caused acute reductions in DNA synthesis in an age-dependent manner. In the heart, isoproterenol was first able to suppress DNA synthesis at 5 days of age and a maximal effect was seen at 9 days; this early phase was characterized by a rapid time constant of coupling of beta receptors to the DNA effect (maximal effect at 6 h after isoproterenol). Reactivity was lessened by 12 days of age and thereafter displayed a longer time constant (maximal effect at 12-24 h). Reactivity of DNA synthesis to isoproterenol challenge was slightly different in kidney and lung (detectable by 2 days of age), but bore similar developmental characteristics to the pattern in the heart (peak of reactivity at 9 days and a decline in reactivity and lengthening of the time constant after 16 days).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

交感神经系统被假设为协调外周组织中细胞发育的时间。在当前研究中,我们评估了交感神经向外周器官投射的个体发生、这些器官中大分子合成模式以及合成过程对异丙肾上腺素β-肾上腺素能刺激的反应性之间的关系。去甲肾上腺素浓度和周转率以及β受体数量的主要发育性升高发生在出生后第二至第四周的肾和肺交感神经通路中,而在心脏交感神经轴中略早。心脏、肾脏和肺中DNA合成的发育性下降与交感神经投射的成熟相吻合。通过体内给予异丙肾上腺素直接刺激β受体,以年龄依赖性方式导致DNA合成急性减少。在心脏中,异丙肾上腺素在5日龄时首次能够抑制DNA合成,9日龄时出现最大效应;这个早期阶段的特征是β受体与DNA效应偶联的时间常数很快(异丙肾上腺素后6小时达到最大效应)。12日龄时反应性降低,此后表现出更长的时间常数(12 - 24小时达到最大效应)。肾脏和肺中DNA合成对异丙肾上腺素刺激的反应性略有不同(2日龄时可检测到),但与心脏中的模式具有相似的发育特征(9日龄时反应性达到峰值,16天后反应性下降且时间常数延长)。(摘要截断于250字)

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