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Altered CNS response to injury in the MRL/MpJ mouse.

机译:MRL / MpJ小鼠中CNS对损伤的反应改变。

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摘要

The MRL/MpJ mouse has a greatly enhanced healing response and an absence of scarring compared with other mouse strains. Following lesions to the CNS mammals show a scarring response known as reactive gliosis, and this CNS scar tissue blocks regeneration of cut axons. We have therefore compared reactive gliosis in the MRL/MpJ mouse and the Swiss Webster mouse, which exhibits normal scarring in the periphery. The lesion model was a stab lesion to the cortex, in which reactive gliosis has previously been quantified. Axon regeneration was examined following a cut lesion to the dopaminergic projection from the substantia nigra to the striatum used in previous regeneration experiments. In the MRL/MpJ following the lesion compared with Swiss Webster mice there was greater cell loss around the lesion followed by greater and more widespread and more prolonged cellular proliferation. Early after the lesion there was a greater loss of glial fibrillary acidic protein (GFAP)-positive astrocytes around the injury site in the MRL/MpJ, and an enhancement and prolongation of the microglial inflammatory response. This was accompanied by greater and more widespread blood-brain barrier leakage following injury. RNA levels for the matrix metalloproteinases (MMP)-2 and MMP-9 as well as for the thrombin receptors PAR-1 and PAR-4 were also greater at the MRL/MpJ injury site. All of these differences were transient and by 14 days post-injury there were no differences observed between MRL/MpJ and control mice. No axonal regeneration was observed following axotomy to the nigrostriatal pathway of the MRL/MpJ or the Swiss Webster mice at any time point.
机译:与其他小鼠品系相比,MRL / MpJ小鼠的愈合反应大大增强,并且没有疤痕。对CNS哺乳动物的损伤之后显示出疤痕反应,称为反应性神经胶质增生,这种CNS疤痕组织阻碍了切割轴突的再生。因此,我们比较了MRL / MpJ小鼠和Swiss Webster小鼠的反应性神经胶质增生,后者在外周表现出正常的瘢痕形成。病变模型是皮层的刺伤,先前已对其中的反应性神经胶质增生进行了量化。在从先前的再生实验中使用的黑质到纹状体的多巴胺能投影切开病变后,检查轴突再生。与Swiss Webster小鼠相比,病变后的MRL / MpJ中,病变周围的细胞损失更大,随后细胞增殖更大,分布更广,时间更长。病变后早期,MRL / MpJ损伤部位周围神经胶质纤维酸性蛋白(GFAP)阳性星形胶质细胞的损失更大,小胶质细胞炎症反应的增强和延长。这伴随着受伤后血脑屏障的泄漏越来越广泛。在MRL / MpJ损伤部位,基质金属蛋白酶(MMP)-2和MMP-9以及凝血酶受体PAR-1和PAR-4的RNA水平也更高。所有这些差异都是短暂的,并且在损伤后14天时,MRL / MpJ与对照小鼠之间没有观察到差异。在任何时间点对MRL / MpJ或Swiss Webster小鼠的黑质纹状体途径进行轴切后,均未观察到轴突再生。

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