肠易激综合征的药物治疗——从概念到销售。

Michael A Kamm
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摘要

功能性胃肠疾病的特点是与心理因素相关的中枢和外周生理变化。由于缺乏对症状性质及其生理和心理相关因素的充分描述,阻碍了药物的成功开发。目前缺乏慢性应激的动物模型。现在治疗非危及生命的疾病需要高度的药物安全性。一旦接近市场,患者压力团体、医疗保健提供者和保险公司、政府和互联网都可以影响药物的成功。5 -羟色胺修饰药物一直是最近开发的主要焦点,结果好坏参半。由于担心QT期延长和心律失常,西沙必利已被下架。5-HT3拮抗剂的开发基于一个有问题的假设,即它们可以改变患者的内脏感觉。阿洛司琼与缺血性结肠炎和高发生率便秘有关。5-HT4激动剂的主要作用是诱导肠蠕动,并可能改变肠道分泌和感觉功能。替加塞罗德和普鲁卡必利在便秘和相关症状患者中显示出希望。5-HT1激动剂可能在治疗功能性消化不良中发挥作用,部分是通过改善受损的胃对膳食的适应。抗抑郁药在临床上通常对这些疾病有益,但也会影响血清素的代谢。过去的成功,如洛哌丁胺或生长抑素类似物奥曲肽,涉及靶向影响运动功能或分泌的终末器官受体。改变感觉功能更具挑战性。未来对新化合物的研究需要牢记这些最近的教训。
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Pharmacological treatment of irritable bowel syndrome--from concept to sales.

Functional gastrointestinal disorders are characterised by central and peripheral physiological changes, associated with psychological factors. Successful drug development has been hindered by lack of adequate characterisation of the nature of symptoms and their physiological and psychological correlates. Animal models of chronic stress are lacking. High levels of drug safety are now demanded for treating non-life threatening conditions. Once close to market, patient pressure groups, health care providers and insurers, government, and the internet can all influence a drug's success. Serotonin-modifying drugs have been the main recent focus of development, with mixed results. Cisapride has been withdrawn because of concerns related to QT prolongation and cardiac arrhythmias. The 5-HT3 antagonists have been developed on the questionable assumption that they modify visceral sensation in patients. Problems have arisen with alosetron being associated with ischaemic colitis and a high incidence of constipation. The 5-HT4 agonists have their major effect on inducing peristalsis, and may modify gut secretion and sensory function. Tegaserod and prucalopride show promise in patients with constipation and related symptoms. 5-HT1 agonists may play a role in treating functional dyspepsia, partly by improving impaired gastric accommodation to a meal. Antidepressants, often found to be clinically beneficial in these disorders, also affect serotonin metabolism. Past successes, such as loperamide or the somatostatin analogue octreotide, involved targeting end organ receptors influencing motor function or secretion. Modifying sensory function is much more challenging. Future research with novel compounds need to keep these recent lessons in mind.

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