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神经元抑制素对垂体的作用与其同属肽生长抑素不同。

Neuronostatin exerts actions on pituitary that are unique from its sibling peptide somatostatin.

机构信息

Maimonides Institute of Biomedical Research of Cordoba (IMIBIC), Cordoba, Spain.

Department of Cell Biology, Physiology and Immunology, University of Córdoba, Cordoba, Spain.

出版信息

J Endocrinol. 2018 Jun;237(3):217-227. doi: 10.1530/JOE-18-0135. Epub 2018 Apr 3.

Abstract

Neuronostatin, a somatostatin gene-encoded peptide, exerts important physiological and metabolic actions in diverse tissues. However, the direct biological effects of neuronostatin on pituitary function of humans and primates are still unknown. This study used baboon () primary pituitary cell cultures, a species that closely models human physiology, to demonstrate that neuronostatin inhibits basal, but not ghrelin-/GnRH-stimulated, growth hormone (GH) and luteinizing hormone (LH) secretion in a dose- and time-dependent fashion, without affecting the secretion of other pituitary hormones (prolactin, ACTH, FSH, thyroid-stimulating hormone (TSH)) or changing mRNA levels. Actions of neuronostatin differs from somatostatin which in this study reduced GH/PRL/ACTH/LH/TSH secretion and GH/PRL/POMC/LH gene expression. Remarkably, we found that inhibitory actions of neuronostatin are likely mediated through: (1) the orphan receptor GPCR107 (found to be highly expressed in pituitary compared to somatostatin-receptors), (2) common (i.e. adenylyl cyclase/protein kinase A/MAPK/extra-/intracellular Ca mobilization, but not phospholipase C/protein kinase C/mTOR) and distinct (i.e. PI3K) signaling pathways than somatostatin and; (3) dissimilar molecular mechanisms than somatostatin (i.e. upregulation of GPCR107 and downregulation of GHS-R/Kiss1-R expression by neuronostatin and, upregulation of sst1-5 expression by somatostatin). Altogether, the results of this study provide the first evidence that there is a functional neuronostatin signaling circuit, unique from somatostatin, which may work in concert with somatostatin to fine-tune hormone release from somatostropes and gonadotropes.

摘要

神经元抑制素是一种由生长抑素基因编码的肽,在多种组织中发挥着重要的生理和代谢作用。然而,神经元抑制素对人类和灵长类动物垂体功能的直接生物学影响尚不清楚。本研究使用狒狒()原代垂体细胞培养物,这种物种与人类生理学密切相关,证明神经元抑制素以剂量和时间依赖的方式抑制基础但不抑制促胃液素/ GnRH 刺激的生长激素(GH)和黄体生成素(LH)分泌,而不影响其他垂体激素(催乳素、ACTH、FSH、促甲状腺激素(TSH))的分泌或改变 mRNA 水平。神经元抑制素的作用不同于生长抑素,生长抑素在本研究中降低了 GH/PRL/ACTH/LH/TSH 的分泌和 GH/PRL/POMC/LH 基因表达。值得注意的是,我们发现神经元抑制素的抑制作用可能是通过以下途径介导的:(1)孤儿 GPCR107 受体(与生长抑素受体相比,在垂体中高度表达),(2)共同(即腺苷酸环化酶/蛋白激酶 A/MAPK/细胞外/细胞内钙动员,但不包括磷脂酶 C/蛋白激酶 C/mTOR)和独特(即 PI3K)信号通路,而不是生长抑素;(3)不同于生长抑素的分子机制(即神经元抑制素上调 GPCR107 和下调 GHS-R/Kiss1-R 表达,而生长抑素上调 sst1-5 表达)。总之,本研究的结果首次提供了证据,证明存在一种功能性的神经元抑制素信号通路,与生长抑素不同,它可能与生长抑素协同作用,精细调节生长激素和促性腺激素的释放。

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