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膜相关孕酮结合蛋白25-Dx:脑和脊髓损伤后的表达、细胞定位及上调

The membrane-associated progesterone-binding protein 25-Dx: expression, cellular localization and up-regulation after brain and spinal cord injuries.

作者信息

Guennoun R, Meffre D, Labombarda F, Gonzalez S L, Gonzalez Deniselle M C, Stein D G, De Nicola A F, Schumacher M

机构信息

Inserm UMR788 and University Paris 11, Kremlin-Bicêtre, France.

出版信息

Brain Res Rev. 2008 Mar;57(2):493-505. doi: 10.1016/j.brainresrev.2007.05.009. Epub 2007 Jun 9.

Abstract

Progesterone has neuroprotective effects in the injured and diseased spinal cord and after traumatic brain injury (TBI). In addition to intracellular progesterone receptors (PR), membrane-binding sites of progesterone may be involved in neuroprotection. A first putative membrane receptor of progesterone, distinct from the classical intracellular PR isoforms, with a single membrane-spanning domain, has been cloned from porcine liver. Homologous proteins were cloned in rats (25-Dx), mice (PGRMC1) and humans (Hpr.6). We will refer to this progesterone-binding protein as 25-Dx. The distribution and regulation of 25-Dx in the nervous system may provide some clues to its functions. In spinal cord, 25-Dx is localized in cell membranes of dorsal horn neurons and ependymal cells lining the central canal. A role of 25-Dx in mediating the protective effects of progesterone in the spinal cord is supported by the observation that its mRNA and protein are up-regulated by progesterone in dorsal horn of the injured spinal cord. In contrast, the classical intracellular PRs were down-regulated under these conditions. In brain, 25-Dx is particularly abundant in the hypothalamic area, circumventricular organs, ependymal cells of the ventricular walls, and the meninges. Interestingly, it is co-expressed with vasopressin in neurons of the paraventricular, supraoptic and retrochiasmatic nuclei. In response to TBI, 25-Dx expression is up-regulated in neurons and induced in astrocytes. The expression of 25-Dx in structures involved in cerebrospinal fluid production and osmoregulation, and its up-regulation after brain damage, point to a potentially important role of this progesterone-binding protein in the maintenance of water homeostasis after TBI. Our observations suggest that progesterone's actions may involve different signaling mechanisms depending on the pathophysiological context, and that 25-Dx may be involved in the neuroprotective effect of progesterone in the injured brain and spinal cord.

摘要

孕酮对脊髓损伤、患病脊髓以及创伤性脑损伤(TBI)后具有神经保护作用。除细胞内孕酮受体(PR)外,孕酮的膜结合位点可能也参与神经保护作用。一种首个被认为是孕酮的膜受体,不同于经典的细胞内PR亚型,具有单个跨膜结构域,已从猪肝中克隆出来。在大鼠(25-Dx)、小鼠(PGRMC1)和人类(Hpr.6)中也克隆出了同源蛋白。我们将这种孕酮结合蛋白称为25-Dx。25-Dx在神经系统中的分布和调节可能为其功能提供一些线索。在脊髓中,25-Dx定位于背角神经元和中央管内衬室管膜细胞的细胞膜上。损伤脊髓的背角中,其mRNA和蛋白被孕酮上调,这一观察结果支持了25-Dx在介导孕酮对脊髓的保护作用中发挥作用。相比之下,在这些条件下经典的细胞内PRs被下调。在脑中,25-Dx在下丘脑区域、室周器官、脑室壁的室管膜细胞和脑膜中特别丰富。有趣的是,它在室旁核、视上核和视交叉后核的神经元中与血管加压素共表达。在TBI后,25-Dx在神经元中表达上调,并在星形胶质细胞中诱导表达。25-Dx在参与脑脊液生成和渗透压调节的结构中的表达,以及其在脑损伤后的上调,表明这种孕酮结合蛋白在TBI后维持水平衡方面可能发挥重要作用。我们的观察结果表明,孕酮的作用可能根据病理生理背景涉及不同的信号机制,并且25-Dx可能参与孕酮对损伤脑和脊髓的神经保护作用。

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