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大鼠肾上腺中外周型苯二氮䓬受体的发育表达及类固醇生成的出现。

Developmental expression of the peripheral-type benzodiazepine receptor and the advent of steroidogenesis in rat adrenal glands.

作者信息

Zilz A, Li H, Castello R, Papadopoulos V, Widmaier E P

机构信息

Department of Biology, Boston University, Massachusetts 02215, USA.

出版信息

Endocrinology. 1999 Feb;140(2):859-64. doi: 10.1210/endo.140.2.6475.

Abstract

Although the precise mechanism whereby cholesterol is transported across the outer mitochondrial membrane is uncertain, a multimeric receptor complex termed the peripheral-type benzodiazepine receptor (PBR) appears essential for this process. We therefore predicted that adrenal cells at different developmental stages would express PBR coincidentally with the advent of steroidogenesis. Adrenals of neonatal rats demonstrate greatly reduced sensitivity to ACTH that gradually increases after the first 2 weeks of life. Thus, neonates have lower circulating corticosterone levels following exposure to stress. We examined mitochondrial PBR ligand binding activity, immunoreactive (ir) PBR content, and adrenal sensitivity to ACTH in vivo and in vitro. Ontogeny of both mitochondrial PBR ligand binding capacity and irPBR directly paralleled that of ACTH-inducible steroidogenesis in isolated rat adrenal cells and in rats injected with ACTH. In addition, neonatal PBR had approximately 2-fold higher affinity for PK11195, a synthetic ligand that binds with high affinity to PBR. No correlation was observed during neonatal life between ir-steroidogenic acute regulatory (StAR) protein content and steroidogenesis. These results are consistent with the hypothesis that PBR is an absolute prerequisite for adrenocortical steroidogenesis, and suggest that the stress hyporesponsive period of neonatal rats may result from decreased PBR expression. In addition, the higher affinity of neonatal PBR and the relatively high basal expression of StAR protein in neonatal adrenals may partly explain the high constitutive steroidogenesis characteristic of neonatal rat adrenal cells.

摘要

尽管胆固醇穿过线粒体外膜的确切机制尚不确定,但一种被称为外周型苯二氮䓬受体(PBR)的多聚体受体复合物似乎是这一过程所必需的。因此,我们预测处于不同发育阶段的肾上腺细胞会随着类固醇生成的出现而同时表达PBR。新生大鼠的肾上腺对促肾上腺皮质激素(ACTH)的敏感性大大降低,在出生后的前两周后逐渐增加。因此,新生儿在受到应激后循环皮质酮水平较低。我们在体内和体外检测了线粒体PBR配体结合活性、免疫反应性(ir)PBR含量以及肾上腺对ACTH的敏感性。线粒体PBR配体结合能力和irPBR的个体发生与分离的大鼠肾上腺细胞以及注射ACTH的大鼠中ACTH诱导的类固醇生成直接平行。此外,新生PBR对PK11195(一种与PBR具有高亲和力结合的合成配体)的亲和力约高2倍。在新生期,ir-类固醇生成急性调节(StAR)蛋白含量与类固醇生成之间未观察到相关性。这些结果与PBR是肾上腺皮质类固醇生成的绝对先决条件这一假设一致,并表明新生大鼠的应激低反应期可能是由于PBR表达降低所致。此外,新生PBR的较高亲和力以及新生肾上腺中StAR蛋白相对较高的基础表达可能部分解释了新生大鼠肾上腺细胞的高组成型类固醇生成特征。

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