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孕酮对脊髓神经退行性变的保护作用基础。

Basis of progesterone protection in spinal cord neurodegeneration.

作者信息

Gonzalez Deniselle Maria Claudia, Lopez Costa Juan José, Gonzalez Susana L, Labombarda Florencia, Garay Laura, Guennoun Rachida, Schumacher Michael, De Nicola Alejandro F

机构信息

Laboratory of Neuroendocrine Biochemistry, Department of Human Biochemistry, Faculty of Medicine, Instituto de Biologia y Medicina Experimental, University of Buenos Aires, Obligado 2490, 1428 Buenos Aires, Argentina.

出版信息

J Steroid Biochem Mol Biol. 2002 Dec;83(1-5):199-209. doi: 10.1016/s0960-0760(02)00262-5.

Abstract

Progesterone neuroprotection has been reported in experimental brain, peripheral nerve and spinal cord injury. To investigate for a similar role in neurodegeneration, we studied progesterone effects in the Wobbler mouse, a mutant presenting severe motoneuron degeneration and astrogliosis of the spinal cord. Implant of a single progesterone pellet (20 mg) during 15 days produced substantial changes in Wobbler mice spinal cord. Morphologically, motoneurons of untreated Wobbler mice showed severe vacuolation of intracellular organelles including mitochondria. In contrast, neuropathology was less pronounced in Wobbler mice receiving progesterone, together with a reduction of vacuolated cells and preservation of mitochondrial ultrastructure. Determination of mRNAs for the alpha 3 and beta 1 subunits of neuronal Na, K-ATPase, showed that mRNA levels in untreated mice were significantly reduced, whereas progesterone therapy re-established the expression of both subunits. Additionally, progesterone treatment of Wobbler mice attenuated the aberrant expression of the growth-associated protein (GAP-43) mRNA which otherwise occurred in motoneurons of untreated animals. The hormone, however, was without effect on astrocytosis of Wobbler mice, determined by glial fibrillary acidic protein (GFAP)-immunostaining. Lastly, progesterone treatment of Wobbler mice enhanced grip strength and prolonged survival at the end of the 15-day observation period. Recovery of morphology and molecular motoneuron parameters of Wobbler mice receiving progesterone, suggest a new and important role for this hormone in the prevention of spinal cord neurodegenerative disorders.

摘要

已有报道称孕酮在实验性脑损伤、周围神经损伤和脊髓损伤中具有神经保护作用。为了研究其在神经退行性变中的类似作用,我们对Wobbler小鼠进行了研究,该小鼠是一种表现出严重运动神经元变性和脊髓星形胶质细胞增生的突变体。在15天内植入单个孕酮丸剂(20毫克)对Wobbler小鼠的脊髓产生了显著变化。在形态学上,未治疗的Wobbler小鼠的运动神经元显示出包括线粒体在内的细胞内细胞器严重空泡化。相比之下,接受孕酮治疗的Wobbler小鼠的神经病理学表现不那么明显,空泡化细胞减少,线粒体超微结构得以保留。对神经元钠钾ATP酶α3和β1亚基的mRNA测定表明,未治疗小鼠的mRNA水平显著降低,而孕酮治疗可重新建立这两个亚基的表达。此外,对Wobbler小鼠进行孕酮治疗可减弱生长相关蛋白(GAP-43)mRNA的异常表达,而在未治疗动物的运动神经元中会出现这种异常表达。然而,通过胶质纤维酸性蛋白(GFAP)免疫染色测定,该激素对Wobbler小鼠的星形胶质细胞增生没有影响。最后,在15天观察期结束时,对Wobbler小鼠进行孕酮治疗可增强握力并延长生存期。接受孕酮治疗的Wobbler小鼠的形态和运动神经元分子参数的恢复,表明该激素在预防脊髓神经退行性疾病中具有新的重要作用。

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