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大鼠脑中雌激素、孕激素和睾酮的膜受体:幻想还是现实。

Membrane receptors for estrogen, progesterone, and testosterone in the rat brain: fantasy or reality.

作者信息

Ramirez V D, Zheng J, Siddique K M

机构信息

Department of Molecular and Integrative Physiology, University of Illinois, Urbana 61801, USA.

出版信息

Cell Mol Neurobiol. 1996 Apr;16(2):175-98. doi: 10.1007/BF02088175.

Abstract
  1. There are numerous circumstantial evidence supporting the concept that steroid hormones control cellular function by means other than the nuclear receptor steroid binding mechanism. It is the intent of this report to present evidence indicating that steroids bind to specific sites in neuronal membranes. 2. Some of the criteria to define steroid membrane receptors using steroid-BSA conjugates that can be radioiodinated to desired specific activity have been fulfilled for each of the three sex steroids using crude synaptosomal membrane preparations (P2 fractions) from the CNS of female and male rats. Ligand binding for each of the three steroids indicate high-affinity and high-capacity sites with distinct brain selectivity and stereospecificity. For example, 17 beta-E-6-[125I]BSA binds hypothalamic P2 fractions (HYP-P2) with an estimated Kd of about 3 +/- 0.7 nM (X +/- SE; n = 3), whereas the cerebellum P2 (CB-P2) fractions bind the ligand with a Kd of 34 +/- 7 nM and, a Bmax of 3 and 42 pmol/mg protein, respectively. Estrogen and testosterone binding fit best a one-single site, while progesterone binding sites can be best represented by a two-binding site, one high-affinity (Kd = 1-2 nM) and one low affinity (Kd = 62 nM), in CB-P2 fractions from intact adult female rat brain. Kinetics studies for T-3-[125I]BSA indicate that the estimated Kd of 30 +/- 2 nM for the olfactory bulb P2 fractions (OB-P2) from male rats is in good agreement with Kd values computed from Scatchard-derived data using the LIGAND algorithm. 3. 17 beta-E-6-[125I]BSA binding sites are stereospecific and appears to be present as early as 5 days of age in both the OB- and the CB-P2 fractions without changes during development. In contrast, P-6-[125I]BSA binding sites are practically absent during days 5 and 12 and appear by day 22. 4. Finally, membrane receptor molecules for estrogen and progesterone have been isolated and purified by affinity chromatography and characterized by PAGE and Western blot. Microsequencing of one of the membrane estrogen binding proteins indicates that the high-affinity site corresponds to the OSCP subunit of the proton ATP synthase. 5. It remains to be determined if P and T also bind to this complex enzyme or if they bind to other subunits of the family of proton ATPases. Overall the data indicate that steroid hormones conjugated to BSA are important tools to study the "reality of membrane steroid receptors."
摘要
  1. 有大量间接证据支持这样一种观点,即甾体激素通过核受体甾体结合机制以外的方式控制细胞功能。本报告旨在提供证据表明甾体与神经元膜中的特定位点结合。2. 使用可放射性碘化至所需比活度的甾体 - 牛血清白蛋白(BSA)偶联物来定义甾体膜受体的一些标准,已通过使用来自雌性和雄性大鼠中枢神经系统的粗制突触体膜制剂(P2 组分)对三种性甾体中的每一种得以实现。三种甾体各自的配体结合表明存在具有明显脑选择性和立体特异性的高亲和力和高容量位点。例如,17β - E - 6 - [125I]BSA 与下丘脑 P2 组分(HYP - P2)结合,估计解离常数(Kd)约为 3 ± 0.7 nM(X ± 标准误;n = 3),而小脑 P2(CB - P2)组分结合该配体的 Kd 为 34 ± 7 nM,最大结合量(Bmax)分别为 3 和 42 pmol/mg 蛋白。雌激素和睾酮的结合最符合单一结合位点模型,而在成年雌性大鼠完整脑的 CB - P2 组分中,孕酮结合位点最好由两个结合位点表示,一个高亲和力(Kd = 1 - 2 nM)和一个低亲和力(Kd = 62 nM)。对 T - 3 - [125I]BSA 的动力学研究表明,雄性大鼠嗅球 P2 组分(OB - P2)的估计 Kd 为 30 ± 2 nM,与使用 LIGAND 算法从 Scatchard 推导数据计算出的 Kd 值高度一致。3. 17β - E - 6 - [125I]BSA 结合位点具有立体特异性,并且在嗅球和小脑的 P2 组分中早在出生后 5 天就已出现,在发育过程中没有变化。相比之下,P - 6 - [125I]BSA 结合位点在第 5 天和第 12 天几乎不存在,在第 22 天出现。4. 最后,已通过亲和色谱法分离和纯化了雌激素和孕酮的膜受体分子,并通过聚丙烯酰胺凝胶电泳(PAGE)和蛋白质免疫印迹法(Western blot)进行了表征。对其中一种膜雌激素结合蛋白的微量测序表明,高亲和力位点对应于质子 ATP 合酶的寡霉素敏感性赋予蛋白(OSCP)亚基。5. 尚有待确定孕酮(P)和睾酮(T)是否也与这种复合酶结合,或者它们是否与质子 ATP 酶家族的其他亚基结合。总体而言,数据表明与 BSA 偶联的甾体激素是研究“膜甾体受体真实性”的重要工具。

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