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内皮素受体的表达与定位:对周围神经胶质细胞参与痛觉感受的意义。

Expression and localization of endothelin receptors: implications for the involvement of peripheral glia in nociception.

作者信息

Pomonis J D, Rogers S D, Peters C M, Ghilardi J R, Mantyh P W

机构信息

Departments of Preventive Science, Neuroscience, and Psychiatry, University of Minnesota, Minneapolis, Minnesota 55455, USA.

出版信息

J Neurosci. 2001 Feb 1;21(3):999-1006. doi: 10.1523/JNEUROSCI.21-03-00999.2001.

Abstract

The endothelins (ETs) are peptides that have a diverse array of functions mediated by two receptor subtypes, the endothelin A receptor (ET(A)R) and the endothelin B receptor (ET(B)R). Pharmacological studies have suggested that in peripheral tissues, ET(A)R expression may play a role in signaling acute or neuropathic pain, whereas ET(B)R expression may be involved in the transmission of chronic inflammatory pain. To begin to define the mechanisms by which ET can drive nociceptive signaling, autoradiography and immunohistochemistry were used to examine the distribution of ET(A)R and ET(B)R in dorsal root ganglia (DRG) and peripheral nerve of the rat, rabbit, and monkey. In DRG and peripheral nerve, ET(A)R-immunoreactivity was present in a subset of small-sized peptidergic and nonpeptidergic sensory neurons and their axons and to a lesser extent in a subset of medium-sized sensory neurons. However, ET(B)R-immunoreactivity was not seen in DRG neurons or axons but rather in DRG satellite cells and nonmyelinating ensheathing Schwann cells. Thus, when ETs are released in peripheral tissues, they could act directly on ET(A)R-expressing sensory neurons and on ET(B)R-expressing DRG satellite cells or nonmyelinating Schwann cells. These data indicate that ETs can have direct, nociceptive effects on the peripheral sensory nervous system and that peripheral glia may be directly involved in signaling nociceptive events in peripheral tissues.

摘要

内皮素(ETs)是一类肽,通过两种受体亚型,即内皮素A受体(ET(A)R)和内皮素B受体(ET(B)R)介导多种功能。药理学研究表明,在周围组织中,ET(A)R的表达可能在急性或神经性疼痛信号传导中起作用,而ET(B)R的表达可能参与慢性炎症性疼痛的传递。为了开始确定ET驱动伤害性信号传导的机制,采用放射自显影和免疫组织化学方法研究了ET(A)R和ET(B)R在大鼠、兔和猴的背根神经节(DRG)和周围神经中的分布。在DRG和周围神经中,ET(A)R免疫反应性存在于一小部分小型肽能和非肽能感觉神经元及其轴突中,在中等大小感觉神经元的子集中程度较低。然而,在DRG神经元或轴突中未观察到ET(B)R免疫反应性,而是在DRG卫星细胞和无髓鞘包绕雪旺细胞中观察到。因此,当ETs在周围组织中释放时,它们可以直接作用于表达ET(A)R的感觉神经元以及表达ET(B)R的DRG卫星细胞或无髓鞘雪旺细胞。这些数据表明,ETs可对周围感觉神经系统产生直接的伤害性作用,并且周围神经胶质细胞可能直接参与周围组织中伤害性事件的信号传导。

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