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克罗恩病患儿中血管活性肠肽能和一氧化氮能神经元的不同反应

Differential responses of VIPergic and nitrergic neurons in paediatric patients with Crohn's disease.

作者信息

Boyer Lee, Sidpra Dolar, Jevon Gareth, Buchan Alison M, Jacobson Kevan

机构信息

Child and Family Research Institute, University of British Columbia, Vancouver, British Columbia, Canada.

出版信息

Auton Neurosci. 2007 Jul 31;134(1-2):106-14. doi: 10.1016/j.autneu.2007.03.001. Epub 2007 Apr 26.

Abstract

Inflammatory bowel disease is a recurrent intestinal inflammatory disorder that in adults has been associated with changes in enteric nervous system neuropeptide expression. The aim of the present study was to determine whether similar changes were observed in paediatric Crohn's disease. The distribution of vasoactive intestinal peptide (VIP) and neuronal nitric oxide synthase (nNOS) was determined in colonic tissues from children with ileo-colonic (n=4) and colonic (n=3) Crohn's disease. The submucosal plexus of inflamed regions showed significant increase in density of VIP immunoreactive neurons (margin, 48% vs. inflamed tissue, 82% of HuC/D positive neurons). The density of submucosal plexus nNOS immunoreactive neurons was too low to be reliably quantified. Using the pan-neuronal marker HuC/D, no significant difference in numbers of HuC/D positive submucosal neurons was evident except where neurons were normalized to length of tissue (margins, 3.6+/-0.7 vs. inflamed tissue, 4.0+/-0.6 neurons/ganglia, p=0.33; margins, 2.7+/-0.4 vs. inflamed tissue, 5.7+/-1.2, neurons/mm, p=0.03). In the myenteric plexus, there was a significant increase in the percent of NOS neurons (38% vs. 82% of HuC/D positive neurons) while there was no significant difference in percent of VIP neurons (4% vs. 8%). No difference in number of HuC/D positive myenteric neurons among margin and inflamed tissues was observed (margin, 12.2+/-3.0 vs. inflamed tissue, 12.5+/-5.1 neurons/ganglia, p=0.50; margins 9.1+/-2.1 vs. inflamed tissue, 13.7+/-2.3 neurons/mm, p=0.11). These data demonstrate that inflammation is associated with a differential expression of VIP and nNOS neuronal subpopulations within the two major enteric plexi, likely due to phenotypic switch. Such changes might contribute to the pathogenesis of IBD and ongoing symptoms even in quiescent disease.

摘要

炎症性肠病是一种复发性肠道炎症性疾病,在成人中,它与肠神经系统神经肽表达的变化有关。本研究的目的是确定在儿童克罗恩病中是否观察到类似变化。对回结肠型(n = 4)和结肠型(n = 3)克罗恩病患儿的结肠组织中血管活性肠肽(VIP)和神经元型一氧化氮合酶(nNOS)的分布进行了测定。炎症区域的黏膜下神经丛中,VIP免疫反应性神经元的密度显著增加(边缘区域,HuC/D阳性神经元的48% 对比发炎组织的82%)。黏膜下神经丛nNOS免疫反应性神经元的密度过低,无法可靠地进行量化。使用泛神经元标记物HuC/D,除了将神经元数量按组织长度进行标准化外,黏膜下HuC/D阳性神经元数量没有明显差异(边缘区域,3.6±0.7对比发炎组织,4.0±0.6个神经元/神经节,p = 0.33;边缘区域,2.7±0.4对比发炎组织, 5.7±1.2个神经元/mm,p = 0.03)。在肌间神经丛中,NOS神经元的百分比显著增加(HuC/D阳性神经元的38%对比82%),而VIP神经元的百分比没有显著差异(4%对比8%)。边缘区域和发炎组织之间HuC/D阳性肌间神经元数量没有差异(边缘区域,12.2±3.0对比发炎组织,12.5±5.1个神经元/神经节,p = 0.50;边缘区域9.1±2.1对比发炎组织,13.7±2.3个神经元/mm,p = 0.11)。这些数据表明,炎症与两个主要肠神经丛内VIP和nNOS神经元亚群的差异表达有关,可能是由于表型转换。这种变化可能导致炎症性肠病的发病机制以及即使在疾病静止期仍持续存在的症状。

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