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多关节炎中脊髓I层锥体神经元中神经激肽1受体的从头表达。

De novo expression of the neurokinin 1 receptor in spinal lamina I pyramidal neurons in polyarthritis.

作者信息

Almarestani L, Waters S M, Krause J E, Bennett G J, Ribeiro-da-Silva A

机构信息

Department of Pharmacology & Therapeutics, McGill University, Montreal, Quebec, Canada.

出版信息

J Comp Neurol. 2009 May 20;514(3):284-95. doi: 10.1002/cne.22024.

DOI:10.1002/cne.22024
PMID:19296480
Abstract

Spinal lamina I (LI) neurons play a major role in the transmission and integration of pain-related information that is relayed to higher centers. Alterations in the excitability of these neurons influence chronic pain development, and expression of the neurokinin 1 receptor (NK-1r) is thought to play a major role in such changes. Novel expression of NK-1r may underlie hyperexcitability in new populations of LI neurons. LI projection neurons can be classified morphologically into fusiform, pyramidal, and multipolar cells, differing in their functional properties, with the pyramidal type being nonnociceptive. In agreement with this, we have shown that spinoparabrachial pyramidal neurons seldom express NK-1r, in contrast with the other two cell types. In this study we investigated in the rat the long-term changes in NK-1r expression by spinoparabrachial LI neurons following the unilateral injection in the hindpaw plantar surface of complete Freund's adjuvant (CFA). Cholera toxin subunit B (CTb) was injected unilaterally into the parabrachial nucleus. Our results revealed that, ipsilaterally, pyramidal neurons were seldom immunoreactive for NK-1r both in saline-injected and in CFA-injected rats, up to 10 days post-CFA. However, a considerable number of pyramidal cells were immunoreactive for NK-1r at 15, 21, and 30 days post-CFA. Our data raise the possibility -- which needs to be confirmed by electrophysiology -- that most LI projection neurons of the pyramidal type are likely nonnociceptive in naive animals but might become nociceptive following the development of arthritis.

摘要

脊髓I层(LI)神经元在疼痛相关信息的传递和整合中起主要作用,这些信息会传递至更高的中枢。这些神经元兴奋性的改变会影响慢性疼痛的发展,并且神经激肽1受体(NK-1r)的表达被认为在这种变化中起主要作用。NK-1r的新表达可能是LI神经元新群体中兴奋性过高的基础。LI投射神经元在形态上可分为梭形、锥形和多极细胞,它们的功能特性不同,其中锥形细胞类型无伤害感受性。与此一致的是,我们已经表明,与其他两种细胞类型相比,脊髓臂旁锥体神经元很少表达NK-1r。在本研究中,我们在大鼠身上研究了在其右后足底注射完全弗氏佐剂(CFA)后,脊髓臂旁LI神经元NK-1r表达的长期变化。霍乱毒素B亚单位(CTb)单侧注射到臂旁核中。我们的结果显示,在同侧,无论是注射生理盐水的大鼠还是注射CFA的大鼠,直到CFA注射后10天,锥体神经元很少对NK-1r呈免疫反应性。然而,在CFA注射后15、21和30天,相当数量的锥体细胞对NK-1r呈免疫反应性。我们的数据提出了一种可能性——这需要通过电生理学来证实——即大多数锥形类型的LI投射神经元在未成熟动物中可能无伤害感受性,但在关节炎发展后可能会变成伤害感受性。

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