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神经退行性疾病中TRPM - 2的表达及TUNEL染色:对摇摆小鼠和视网膜变性小鼠的研究

TRPM-2 expression and tunel staining in neurodegenerative diseases: studies in wobbler and rd mice.

作者信息

Popper P, Farber D B, Micevych P E, Minoofar K, Bronstein J M

机构信息

Department of Neurobiology, University of California, Los Angeles, California, 90095, USA.

出版信息

Exp Neurol. 1997 Feb;143(2):246-54. doi: 10.1006/exnr.1996.6364.

DOI:10.1006/exnr.1996.6364
PMID:9056387
Abstract

Neuronal apoptosis has been described during development but little is known about whether apoptosis plays a role in neurodegenerative disease. Neurodegenerative cell death can be difficult to study because it is often a slow process and it is limited to only a few cells among many nondying cells. We used molecular methods to study cell death in the spinal cords of wobbler mice, a model of motoneuron disease, and compared it to retinas of rd mice, a model of retinitis pigmentosa, where it is known that photoreceptors die by apoptosis. Increased levels of mRNA of testosterone-repressed prostate message 2 (TRPM-2) were found in motoneurons of wobbler mice and the retinas of rd mice. In motoneurons, TRPM-2 mRNA colocalized with increased expression of the message for growth-associated protein (GAP-43). In rd retinas, TRPM-2 mRNA was localized to ganglion cells of the inner retina known to survive the disease. These suggest that TRPM-2 expression is associated with cell membrane remodeling in surviving cells associated with synaptic reorganization or change in afferent input. In situ labeling of fragmented DNA (TUNEL staining) identified dying photoreceptors in the rd mouse. In the wobbler spinal cords dying motoneurons were not labeled. These data suggest that the process of neurodegenerative motoneuron cell death in wobbler mice is different from the apoptotic process of rd photoreceptors.

摘要

神经元凋亡在发育过程中已有描述,但关于凋亡是否在神经退行性疾病中起作用却知之甚少。神经退行性细胞死亡可能难以研究,因为它通常是一个缓慢的过程,并且仅限于众多未死亡细胞中的少数细胞。我们使用分子方法研究运动神经元疾病模型——摇椅小鼠脊髓中的细胞死亡,并将其与视网膜色素变性模型——rd小鼠的视网膜进行比较,已知rd小鼠的光感受器通过凋亡死亡。在摇椅小鼠的运动神经元和rd小鼠的视网膜中发现睾酮抑制的前列腺信息2(TRPM - 2)的mRNA水平升高。在运动神经元中,TRPM - 2 mRNA与生长相关蛋白(GAP - 43)信息的表达增加共定位。在rd视网膜中,TRPM - 2 mRNA定位于已知在疾病中存活的内视网膜神经节细胞。这些表明TRPM - 2表达与与突触重组或传入输入变化相关的存活细胞中的细胞膜重塑有关。片段化DNA的原位标记(TUNEL染色)确定了rd小鼠中正在死亡的光感受器。在摇椅小鼠的脊髓中,正在死亡的运动神经元未被标记。这些数据表明,摇椅小鼠中神经退行性运动神经元细胞死亡过程与rd光感受器的凋亡过程不同。

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TRPM-2 expression and tunel staining in neurodegenerative diseases: studies in wobbler and rd mice.神经退行性疾病中TRPM - 2的表达及TUNEL染色:对摇摆小鼠和视网膜变性小鼠的研究
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