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胃食管反流病的药理学靶点

Pharmacological targets in gastro-oesophageal reflux disease.

作者信息

Piche Thierry, Galmiche Jean Paul

机构信息

Hepatogastroenterology, CHU Nice, France.

出版信息

Basic Clin Pharmacol Toxicol. 2005 Dec;97(6):333-41. doi: 10.1111/j.1742-7843.2005.pto_273.x.

DOI:10.1111/j.1742-7843.2005.pto_273.x
PMID:16364047
Abstract

Although proton pump inhibitors have become the mainstay of treatment in gastro-oesophageal reflux disease (GORD), there are still unmet needs in the management of this very common disorder. For example, all current proton pump inhibitors have a relatively slow onset of action and their activity is limited mainly to the post-prandial period with far less effective inhibition of nocturnal acid secretion. In order to achieve more potent, rapid and sustained acid inhibition several compounds are currently under development, such as new proton pump inhibitors with a prolonged plasma half-life, potassium competitive ATPase blockers (PCABs), histamine H3 agonists, and gastrin antagonists. Acid suppression does not, however, cure the disease and relapses are frequently observed after discontinuation of proton pump inhibitor therapy. Among the different abnormalities involved in the pathophysiology of this multifactorial disease, transient lower oesophageal sphincter relaxations represent the major mechanism responsible for episodes of reflux. Baclofen, the prototype GABA(B) receptor agonist, is one of the most potent inhibitors of transient lower oesophageal sphincter relaxations identified. To date the transfer of these relaxation-controlling pharmacological agents into clinical practice has however been hampered by the occurrence of unacceptable side effects. Beside "anti-relaxation therapy", the potential of novel prokinetics such as motilin agonists has been explored, especially since the motilin receptor has been cloned. Thus far the broad therapeutic value of prokinetics in GORD does, however, seem very limited in terms of efficacy with respect to oesophageal motility and acid exposure. Lastly, further research is necessary to better understand the complex mechanisms involved in oesophageal sensitivity and mucosal defence.

摘要

尽管质子泵抑制剂已成为胃食管反流病(GORD)治疗的主要手段,但在这种非常常见的疾病管理方面仍存在未满足的需求。例如,目前所有的质子泵抑制剂起效相对较慢,其活性主要限于餐后时段,对夜间胃酸分泌的抑制效果远不如人意。为了实现更强效、快速且持续的胃酸抑制,目前有几种化合物正在研发中,如具有延长血浆半衰期的新型质子泵抑制剂、钾竞争性ATP酶阻滞剂(PCABs)、组胺H3激动剂和胃泌素拮抗剂。然而,胃酸抑制并不能治愈该疾病,停用质子泵抑制剂治疗后经常会出现复发。在这种多因素疾病的病理生理学所涉及的不同异常情况中,一过性下食管括约肌松弛是反流发作的主要机制。巴氯芬作为GABA(B)受体激动剂的原型,是已确定的最有效的一过性下食管括约肌松弛抑制剂之一。然而,迄今为止,这些控制松弛的药物制剂向临床实践的转化受到不可接受的副作用的阻碍。除了“抗松弛疗法”,人们还探索了新型促动力药如胃动素激动剂的潜力,特别是自从胃动素受体被克隆以来。然而,就食管动力和胃酸暴露的疗效而言,促动力药在GORD中的广泛治疗价值似乎非常有限。最后,有必要进行进一步研究,以更好地理解食管敏感性和黏膜防御所涉及的复杂机制。

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