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类固醇激素对大脑的作用:基因组何时发挥作用?

Steroid hormone actions on the brain: when is the genome involved?

作者信息

McEwen B S

机构信息

Laboratory of Neuroendocrinology, Rockefeller University, New York, New York 10021, USA.

出版信息

Horm Behav. 1994 Dec;28(4):396-405. doi: 10.1006/hbeh.1994.1036.

Abstract

It has become customary to distinguish between so-called "genomic" actions of steroid hormones involving intracellular receptors and "non-genomic" effects of steroids that involve putative cell surface receptors. Whereas there is no doubt that this distinction has considerable validity, it does not go far enough in addressing the variety of mechanisms that steroid hormones use to produce their effects on cells. This is because cell surface receptors may signal changes in gene expression, while genomic actions sometimes affect neuronal excitability, often doing so quite rapidly. Moreover, steroid hormones and neurotransmitters may operate together to produce effects, and sometimes these effects involve collaborations between groups of neurons. As illustrations, evidence is reviewed in this article that a number of steroid actions in the hippocampus involves the co-participation of excitatory amino acids. These interactions are evident for the regulation of synaptogenesis by estradiol in the CA1 pyramidal neurons of hippocampus and for the induction of dendritic atrophy of CA3 neurons by repeated stress as well as by glucocorticoid injections. In addition, neurogenesis in the adult and developing dentate gyrus is "contained" by adrenal steroids as well as by excitatory amino acids. In each of these three examples, NMDA receptors are involved. These results not only point to a high degree of interdependency between certain neurotransmitters and the actions of steroid hormones but also emphasize the degree to which structural plasticity is an important aspect of steroid hormone action in the adult as well as developing nervous system.

摘要

区分涉及细胞内受体的类固醇激素的所谓“基因组”作用和涉及假定细胞表面受体的类固醇的“非基因组”作用已成为惯例。虽然毫无疑问这种区分具有相当的合理性,但在解决类固醇激素用于对细胞产生作用的各种机制方面,它做得还不够。这是因为细胞表面受体可能会发出基因表达变化的信号,而基因组作用有时会影响神经元兴奋性,而且往往起效很快。此外,类固醇激素和神经递质可能共同作用产生效应,有时这些效应涉及神经元群体之间的协作。作为例证,本文回顾了证据,表明海马体中的许多类固醇作用涉及兴奋性氨基酸的共同参与。这些相互作用在海马体CA1锥体神经元中雌二醇对突触发生的调节以及重复应激和糖皮质激素注射对CA3神经元树突萎缩的诱导中很明显。此外,成年和发育中的齿状回中的神经发生受到肾上腺类固醇以及兴奋性氨基酸的“抑制”。在这三个例子中的每一个中,NMDA受体都参与其中。这些结果不仅表明某些神经递质与类固醇激素作用之间存在高度的相互依赖性,而且强调了结构可塑性在成年和发育中的神经系统中作为类固醇激素作用的一个重要方面的程度。

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