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佐剂诱导的关节炎症可导致支配感觉神经节中的β-前速激肽原和α-CGRP基因非常快速的转录。

Adjuvant-induced joint inflammation causes very rapid transcription of beta-preprotachykinin and alpha-CGRP genes in innervating sensory ganglia.

作者信息

Bulling D G, Kelly D, Bond S, McQueen D S, Seckl J R

机构信息

Molecular Endocrinology, Molecular Medicine Centre, Western General Hospital, Edinburgh, UK.

出版信息

J Neurochem. 2001 Apr;77(2):372-82. doi: 10.1046/j.1471-4159.2001.00175.x.

DOI:10.1046/j.1471-4159.2001.00175.x
PMID:11299299
Abstract

Neuropeptides synthesized in dorsal root ganglia (DRG) have been implicated in neurogenic inflammation and nociception in experimental and clinical inflammatory arthritis. We examined the very early changes in response to adjuvant injection in a rat model of unilateral tibio-tarsal joint inflammation and subsequent monoarthritis. Within 30 min of adjuvant injection ipsilateral swelling and hyperalgesia were apparent, and marked increases in beta-preprotachykinin-A (beta-PPT-A) and alpha-calcitonin gene-related peptide (CGRP)-encoding mRNAs were observed in small-diameter L5 DRG neurones innervating the affected joint. This response was augmented by recruitment of additional small-diameter DRG neurones expressing beta-PPT-A and CGRP transcripts. The increased mRNA was paralleled by initial increases in L5 DRG content of the protein products, substance P and calcitonin gene-related peptide. Within 15 min of adjuvant injection there were increases in electrical activity in sensory nerves innervating a joint. Blockade of this activity prevented the rapid induction in beta-PPT-A and CGRP mRNA expression in DRG neurones. Increased expression of heteronuclear (intron E) beta-PPT-A RNA suggests that increases in beta-PPT-A mRNA levels were, at least in part, due to transcription. Pre-treatment with the protein synthesis inhibitor cycloheximide had no effect upon the early rise in neuropeptide mRNAS: This and the rapid time course of these changes suggest that increased sensory neural discharge and activation of a latent modulator of transcription are involved.

摘要

在实验性和临床炎症性关节炎中,背根神经节(DRG)合成的神经肽与神经源性炎症和伤害感受有关。我们在单侧胫跗关节炎症及随后的单关节炎大鼠模型中,研究了对佐剂注射的早期反应变化。佐剂注射后30分钟内,同侧出现肿胀和痛觉过敏,在支配患侧关节的小直径L5 DRG神经元中,观察到β-前速激肽原A(β-PPT-A)和α-降钙素基因相关肽(CGRP)编码mRNA显著增加。通过募集额外表达β-PPT-A和CGRP转录本的小直径DRG神经元,这种反应增强。mRNA增加的同时,L5 DRG中蛋白产物P物质和降钙素基因相关肽的含量最初也增加。佐剂注射后15分钟内,支配关节的感觉神经电活动增加。阻断这种活动可防止DRG神经元中β-PPT-A和CGRP mRNA表达的快速诱导。异核(内含子E)β-PPT-A RNA表达增加表明,β-PPT-A mRNA水平的增加至少部分是由于转录。用蛋白质合成抑制剂环己酰亚胺预处理对神经肽mRNA的早期升高没有影响:这些变化及其快速的时间进程表明,感觉神经放电增加和潜在转录调节因子的激活参与其中。

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