Spinal AMPA receptors: Amenable players in central sensitization for chronic pain therapy?

Olga Kopach, Nana Voitenko
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Abstract

The activity-dependent trafficking of AMPA receptors (AMPAR) mediates synaptic strength and plasticity, while the perturbed trafficking of the receptors of different subunit compositions has been linked to memory impairment and to causing neuropathology. In the spinal cord, nociceptive-induced changes in AMPAR trafficking determine the central sensitization of the dorsal horn (DH): changes in AMPAR subunit composition compromise the balance between synaptic excitation and inhibition, rendering interneurons hyperexcitable to afferent inputs, and promoting Ca2+ influx into the DH neurons, thereby amplifying neuronal hyperexcitability. The DH circuits become over-excitable and carry out aberrant sensory processing; this causes an increase in pain sensation in central sensory pathways, giving rise to chronic pain syndrome. Current knowledge of the contribution of spinal AMPAR to the cellular mechanisms relating to chronic pain provides opportunities for developing target-based therapies for chronic pain intervention.

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脊髓 AMPA 受体:用于慢性疼痛治疗的中枢敏化作用?
依赖于活动的 AMPA 受体(AMPAR)贩运介导了突触强度和可塑性,而不同亚单位组成的受体的贩运紊乱与记忆损伤和神经病理学有关。在脊髓中,痛觉诱导的 AMPAR 贩卖变化决定了背角(DH)的中枢敏化:AMPAR 亚单位组成的变化损害了突触兴奋和抑制之间的平衡,使中间神经元对传入输入过度兴奋,并促进 Ca2+ 流入 DH 神经元,从而放大神经元的过度兴奋性。DH 环路变得过度兴奋,并进行异常的感觉处理;这会导致中枢感觉通路的痛觉增强,从而引发慢性疼痛综合征。目前关于脊髓 AMPAR 对慢性疼痛相关细胞机制的贡献的知识为开发基于靶点的慢性疼痛干预疗法提供了机会。
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