首页> 外文OA文献 >Receptor binding sites for substance P, but not substance K or neuromedin K, are expressed in high concentrations by arterioles, venules, and lymph nodules in surgical specimens obtained from patients with ulcerative colitis and Crohn disease.
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Receptor binding sites for substance P, but not substance K or neuromedin K, are expressed in high concentrations by arterioles, venules, and lymph nodules in surgical specimens obtained from patients with ulcerative colitis and Crohn disease.

机译:在溃疡性结肠炎和克罗恩病患者的手术标本中,小动脉,小静脉和淋巴结结以高浓度表达P物质而非K物质或神经调节素K的受体结合位点。

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摘要

Several lines of evidence indicate that tachykinin neuropeptides [substance P (SP), substance K (SK), and neuromedin K (NK)] play a role in regulating the inflammatory and immune responses. To test this hypothesis in a human inflammatory disease, quantitative receptor autoradiography was used to examine possible abnormalities in tachykinin binding sites in surgical specimens from patients with inflammatory bowel disease. Surgical specimens of colon were obtained from patients with ulcerative colitis (n = 4) and Crohn disease (n = 4). Normal tissue was obtained from uninvolved areas of extensive resections for carcinoma (n = 6). In all cases, specimens were obtained less than 5 min after removal to minimize influences associated with degradation artifacts and were processed for quantitative receptor autoradiography by using 125I-labeled Bolton-Hunter conjugates of NK, SK, and SP. In the normal colon a low concentration of SP receptor binding sites is expressed by submucosal arterioles and venules and a moderate concentration is expressed by the external circular muscle, whereas SK receptor binding sites are expressed in low concentrations by the external circular and longitudinal muscle. In contrast, specific NK binding sites were not observed in any area of the human colon. In colon tissue obtained from ulcerative colitis and Crohn disease patients, however, very high concentrations of SP receptor binding sites are expressed by arterioles and venules located in the submucosa, muscularis mucosa, external circular muscle, external longitudinal muscle, and serosa. In addition, very high concentrations of SP receptor binding sites are expressed within the germinal center of lymph nodules, whereas the concentrations of SP and SK binding sites expressed by the external muscle layers are not altered significantly. These results demonstrate that receptor binding sites for SP, but not SK or NK, are ectopically expressed in high concentrations (1000-2000 times normal) by cells involved in mediating inflammatory and immune responses. These data suggest that SP may be involved in the pathophysiology of inflammatory bowel disease and might provide some insight into the interaction between the nervous system and the regulation of inflammation and the immune response in human inflammatory disease.
机译:几项证据表明速激肽神经肽[P(SP),K物质(SK)和Neuromedin K(NK)]在调节炎症和免疫反应中起作用。为了在人类炎症性疾病中检验这一假设,使用定量受体放射自显影技术检查了炎症性肠病患者手术标本中速激肽结合位点的可能异常。从溃疡性结肠炎(n = 4)和克罗恩病(n = 4)患者获得结肠手术标本。正常组织取自未进行大范围切除的癌区域(n = 6)。在所有情况下,均应在取出后不到5分钟的时间内获取标本,以最大程度地减少与降解伪影相关的影响,并使用NK,SK和SP的125I标记的Bolton-Hunter共轭物对标本进行定量放射自显影。在正常结肠中,粘膜下小动脉和小静脉表达低浓度的SP受体结合位点,外环肌表达中等浓度,而外环肌和纵肌以低浓度表达SK受体结合位点。相反,在人结肠的任何区域都没有观察到特异性的NK结合位点。然而,在得自溃疡性结肠炎和克罗恩病患者的结肠组织中,位于粘膜下层,肌层粘膜,外环肌,外纵肌和浆膜的小动脉和小静脉表达非常高浓度的SP受体结合位点。另外,在淋巴结的生发中心内表达非常高浓度的SP受体结合位点,而由外部肌肉层表达的SP和SK结合位点的浓度没有明显改变。这些结果表明,参与介导炎症和免疫应答的细胞高浓度(正常浓度的1000-2000倍)异位表达SP而不是SK或NK的受体结合位点。这些数据表明,SP可能参与了炎症性肠病的病理生理,并且可能为神经系统与炎症调节以及人类炎症性疾病的免疫反应之间的相互作用提供一些见识。

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