辣椒素作为新的口服胃保护和治疗药物单独或与非甾体抗炎药合用在健康人群和患者中。

Gyula Mózsik
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引用次数: 39

摘要

背景:辣椒素是一种作用于辣椒素敏感传入神经的特殊化合物。目的:利用辣椒素研究人体胃肠道生理、病理、临床药理学的不同事件,以及在健康人群和不同胃肠道疾病患者中增强胃肠道黏膜防御的可能治疗途径,以及辣椒素与非甾体抗炎药(NSAIDs)在健康人群和患者中的应用。材料与方法:对198名健康受试者和178名不同胃肠道疾病(胃炎、糜烂、溃疡、息肉、癌症、炎症性肠病、结直肠息肉、癌症)患者以及69名慢性(幽门螺杆菌阳性和阴性)胃炎患者(根除治疗前后)进行观察。研究了辣椒素单独应用、乙醇单独应用和辣椒素联合应用时,吲哚美辛诱导的胃黏膜微出血的胃分泌反应及其化学组成、胃排空、糖负荷试验、胃粘膜电位差(GTPD)。对胃肠道,特别是慢性胃炎患者(有无幽门螺杆菌感染、经典根除治疗前后)进行辣椒素受体(TRVP1)、降钙素基因相关肽(CGRP)、P物质(SP)的免疫组化检测。应用经典分子药理学方法研究了抑制胃底酸分泌的药物。结果:辣椒素降低胃底输出量,增强胃分泌反应的“非壁”(缓冲)成分,促进胃排空和胰高血糖素的释放。辣椒素对吲哚美辛和乙醇诱导的胃粘膜损伤有预防作用;同时辣椒素本身也增强了GTPD。辣椒素对吲哚美辛所致胃粘膜微出血有预防作用。慢性胃炎患者胃黏膜TRVP1和CGRP表达升高(与是否存在幽门螺杆菌感染无关),根除治疗成功。人体第一期试验(乙酰水杨酸(ASA)、双氯芬酸和萘普生与辣椒素类药物一起应用(剂量刺激辣椒素敏感的传入迷走神经)显示ASA和双氯芬酸的药代动力学参数以及ASA和双氯芬酸诱导的血小板聚集没有变化。结论:辣椒素是一种新的口服胃保护剂,适用于健康人、不同化学物质和幽门螺杆菌引起的粘膜损伤患者以及许多其他需要使用非甾体抗炎药治疗的疾病。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Capsaicin as new orally applicable gastroprotective and therapeutic drug alone or in combination with nonsteroidal anti-inflammatory drugs in healthy human subjects and in patients.

Background: Capsaicin is a specific compound acting on capsaicin-sensitive afferent nerves.

Aim: Capsaicin was used to study the different events of human gastrointestinal physiology, pathology, and clinical pharmacology, and possible therapeutic approaches to enhance gastrointestinal mucosal defense in healthy human subjects and in patients with various different gastrointestinal disorders as well as its use with nonsteroidal anti-inflammatory drugs (NSAIDs) in healthy subjects and in patients.

Materials and methods: The observations were carried out in 198 healthy human subjects and in 178 patients with different gastrointestinal (GI) diseases (gastritis, erosions, ulcer, polyps, cancer, inflammatory bowel diseases, colorectal polyps, cancers), and in 69 patients with chronic (Helicobacter pylori positive and negative) gastritis (before and after eradication treatment). The gastric secretory responses and their chemical composition, gastric emptying, sugar loading test, gastric transmucosal potential difference (GTPD) with application of capsaicin alone, after ethanol alone and with capsaicin, indomethacin-induced gastric mucosal microbleeding without and with capsaicin were studied. The immunohistochemical examinations of the capsaicin receptor (TRVP1), calcitonin gene- related peptide (CGRP), and substance P (SP) were carried out in gastrointestinal tract, and especially in patients with chronic gastritis (with and without Helicobacter infection, before and after classical eradication treatment). Classical molecular pharmacological methods were applied to study the drugs inhibiting the gastric basal acid output.

Results: Capsaicin decreased the gastric basal output, enhanced the "non-parietal" (buffering) component of gastric secretory responses, and gastric emptying, and the release of glucagon. Capsaicin prevented the indomethacin- and ethanol-induced gastric mucosal damage; meanwhile capsaicin itself enhanced (GTPD). Capsaicin prevented the indomethacin-induced gastric mucosal microbleeding. The expression of TRVP1 and CGRP increased in the gastric mucosa of patients with chronic gastritis (independently of the presence of Helicobacter pylori infection), and the successfully carried out eradication treatment. The human first phase examinations (the application of acetylsalicylic acid (ASA), diclqfenac, and naproxen together with capcaicinoids) (given in doses that stimulate capsaicin-sensitive afferent vagal nerves) showed no change in the pharmacokinetic parameters of ASA and diclofenac and the ASA and diclofenac-induced platelet aggregation.

Conclusions: Capsaicin represents a new orally applicable gastroprotective agent in healthy human subjects and in patients with different chemical and Helicobacter pylori-induced mucosal damage and in many other diseases requiring treatment with NSAIDs.

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