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首页> 外文期刊>The Journal of Physiology >Synaptic and paracrine mechanisms at carotid body arterial chemoreceptors
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Synaptic and paracrine mechanisms at carotid body arterial chemoreceptors

机译:颈动脉体化学感受器的突触和旁分泌机制

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摘要

Mammalian carotid bodies are the main peripheral arterial chemoreceptors, strategically located at the bifurcation of the common carotid artery. When stimulated these receptors initiate compensatory respiratory and cardiovascular reflexes to maintain homeostasis. Thus, in response to low oxygen (hypoxia) or increased CO2/H+ (acid hypercapnia), chemoreceptor type I cells depolarize and release excitatory neurotransmitters, such as ATP, which stimulate postsynaptic P2X2/3 receptors on afferent nerve terminals. The afferent discharge is shaped by autocrine and paracrine mechanisms involving both excitatory and inhibitory neuromodulators such as adenosine, serotonin (5-HT), GABA and dopamine. Recent evidence suggests that paracrine activation of P2Y2 receptors on adjacent glia-like type II cells may help boost the ATP signal via the opening of pannexin-1 channels. The presence of an inhibitory efferent innervation, mediated by release of nitric oxide, provides additional control of the afferent discharge. The broad array of neuromodulators and their receptors appears to endow the carotid body with a remarkable plasticity, most apparent during natural and pathophysiological conditions associated with chronic sustained and intermittent hypoxia.
机译:哺乳动物的颈动脉体是主要的外周动脉化学感受器,策略性地位于颈总动脉的分叉处。当受到刺激时,这些受体开始代偿性呼吸和心血管反射,以维持体内平衡。因此,响应低氧(缺氧)或增加CO2 / H +(酸性高碳酸血症),I型化学感受器细胞去极化并释放兴奋性神经递质,例如ATP,它会刺激传入神经末梢的突触后P2X2 / 3受体。传入放电是由涉及兴奋性和抑制性神经调节剂(如腺苷,5-羟色胺(5-HT),GABA和多巴胺)的自分泌和旁分泌机制决定的。最近的证据表明,相邻神经胶质样II型细胞上P2Y2受体的旁分泌激活可能通过pannexin-1通道的开放来增强ATP信号。一氧化氮释放介导的抑制性传出神经支配的存在,提供了对传入放电的额外控制。各种各样的神经调节剂及其受体似乎赋予颈动脉以显着的可塑性,在与慢性持续性和间歇性缺氧有关的自然和病理生理条件下最明显。

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