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Differential expression of ryanodine receptor isoforms after spinal cord injury

机译:脊髓损伤后ryanodine受体同种型的差异表达

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Highlights ? RyR2 and RyR3 are upregulated in dorsal root ganglion neurons acutely after SCI. ? RyR2 and RyR3 are upregulated in the lesion site after SCI. ? RyR1 remained unchanged acutely following SCI. ? RyR2 and RyR3 spatially overlap with dystrophic axons after SCI. Abstract Ryanodine receptors (RyRs) are highly conductive intracellular Ca 2+ release channels and are widely expressed in many tissues, including the central nervous system. RyRs have been implicated in intracellular Ca 2+ overload which can drive secondary damage following traumatic injury to the spinal cord (SCI), but the spatiotemporal expression of the three isoforms of RyRs (RyR1-3) after SCI remains unknown. Here, we analyzed the gene and protein expression of RyR isoforms in the murine lumbar dorsal root ganglion (DRG) and the spinal cord lesion site at 1, 2 and 7 d after a mild contusion SCI. Quantitative RT PCR analysis revealed that RyR3 was significantly increased in lumbar DRGs and at the lesion site at 1 and 2 d post contusion compared to sham (laminectomy only) controls. Additionally, RyR2 expression was increased at 1 d post injury within the lesion site. RyR2 and -3 protein expression was localized to lumbar DRG neurons and their spinal projections within the lesion site acutely after SCI. In contrast, RyR1 expression within the DRG and lesion site remained unaltered following trauma. Our study shows that SCI initiates acute differential expression of RyR isoforms in DRG and spinal cord.
机译:强调 ?在SCI之后急性地在背根神经节神经元中上调Ryr2和Ryr3。还是在SCI后,RYR2和RYR3在病变部位上调。还是ryr1追随SCI后急剧保持不变。还是Ryr2和Ryr3在SCI后与营养不良轴突重叠。摘要雷马丁籽受体(RYR)是高导电的细胞内Ca 2+释放通道,并且在许多组织中广泛表达,包括中枢神经系统。 RYR已经涉及细胞内Ca 2+过载,其可以在脊髓(SCI)上创伤后损伤后的二次损伤,但SCI后的三种同种型的时尚表达仍然未知。在这里,我们分析了在轻度挫伤Sci的1,2和7d中鼠腰背根神经节(DRG)和脊髓病变位点中Ryr Isoform的基因和蛋白表达。定量RT PCR分析显示,与假(仅限椎板切除术)对照相比,Ryr3在腰部DRG和病变部位下显着增加,并且在1和2d末端挫伤。另外,在病变位点内的1 d后损伤下,Ryr2表达增加。 Ryr2和-3蛋白表达在SCI后急性地定位于腰部DRG神经元及其在病变部位内的脊柱突起。相反,DRG和病变位点内的RYR1表达在创伤后残留不变。我们的研究表明,SCI在DRG和脊髓中引发Ryr Isoforms的急性差异表达。

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