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首页> 外文期刊>Experimental Neurology >Role of cortical reorganization on the effect of 5-HT pharmacotherapy for spinal cord injury.
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Role of cortical reorganization on the effect of 5-HT pharmacotherapy for spinal cord injury.

机译:皮质重组对5-HT药物治疗脊髓损伤的作用。

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Cortical reorganization or expansion of the intact cortical regions into the deafferented cortex after complete spinal transection in neonatally spinalized rats was shown to be essential for increases in weight-supported stepping at adulthood. The novel somatotopic organization identified in these animals can be induced by exercise or spinal transplants that bridge the site of injury. However, the role of cortical reorganization in increased weight-supported (WS) stepping after pharmacotherapy is unknown. For the neonatally spinalized rat model, the 5-HT(2C) receptor agonist 1-(m-chlorophenyl)-piperazine hydrochloride (mCPP) increases the number of WS steps taken when administered to adult rats spinalized as neonates (mCPP+) though not all animals showed this effect (mCPP-). Since no differences in the behavior of the animals off-drug has been demonstrated, it is unclear why acute administration of 5-HT affects only a subset of animals. One possibility is that differences in cortical organization between mCPP+ and mCPP- may contribute to the differences in the functional effect of mCPP. To test this, we recorded from single neurons in the deafferented hindlimb sensorimotor cortex during passive sensory stimulation of the cutaneous surface of the forepaws and during active sensorimotor stimulation of the forepaws while the animals locomoted on a motorized treadmill. Our results show that neurons recorded from mCPP+ animals increased their responsiveness to both passive and active stimulation off-drug in comparison to neurons from mCPP- animals. These data suggest that differences in the cortical organization of mCPP+ compared to mCPP- animals may be at least partially responsible for the effect of a 5-HT(2C) receptor agonist on functional outcome.
机译:新生脊椎大鼠完全脊柱横断后,皮质重组或将完整皮质区域扩展为脱去皮层的皮质对于成年体重增加的步伐增加至关重要。在这些动物中鉴定出的新颖的躯体组织可以通过桥接损伤部位的运动或脊柱移植来诱导。然而,在药物治疗后皮质重组在增加体重支持(WS)的过程中的作用尚不清楚。对于新生的脊柱大鼠模型,当将5-HT(2C)受体激动剂1-(间氯苯基)-哌嗪盐酸盐(mCPP)给药给成脊柱的新生大鼠(mCPP +)时,WS步骤数增加,尽管并非全部动物显示出这种作用(mCPP-)。由于尚未证明药物外动物的行为有差异,因此尚不清楚为什么急性给予5-HT仅影响一部分动物。一种可能性是,mCPP +和mCPP-之间的皮质组织差异可能会导致mCPP功能作用的差异。为了测试这一点,我们记录了在前臂的皮肤表面被动感觉刺激和前臂的主动感觉运动刺激过程中,当动物在电动跑步机上运动时,脱去力的后肢感觉运动皮质中的单个神经元的记录。我们的结果表明,与来自mCPP-动物的神经元相比,从mCPP +动物记录的神经元增加了对被动和主动非药物刺激的反应性。这些数据表明,与mCPP-动物相比,mCPP +的皮质组织的差异可能至少部分负责了5-HT(2C)受体激动剂对功能结局的影响。

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