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执业医师使用H2受体拮抗剂和质子泵抑制剂的药理学及药效学要点

Pharmacological and pharmacodynamic essentials of H(2)-receptor antagonists and proton pump inhibitors for the practising physician.

作者信息

Huang J Q, Hunt R H

机构信息

Division of Gastroenterology, Department of Medicine, McMaster University Medical Center, Hamilton, Ontario, Canada.

出版信息

Best Pract Res Clin Gastroenterol. 2001 Jun;15(3):355-70. doi: 10.1053/bega.2001.0184.


DOI:10.1053/bega.2001.0184
PMID:11403532
Abstract

The suppression of gastric acid secretion with anti-secretory agents has been the mainstay of medical treatment for patients with acid-related disorders. Although the majority of Helicobacter pylori -related peptic ulcers can be healed with antibiotics, ulcer healing and symptom control can be significantly improved when antibiotics are given with anti-secretory agents, especially with a proton pump inhibitor. There is a dynamic relationship between the suppression of intragastric acidity and the healing of peptic ulcer and erosive oesophagitis and control of acid-related symptoms. The suppression of gastric acid secretion achieved with H(2)-receptor antagonists has, however, proved to be suboptimal for effectively controlling acid-related disorders, especially for healing erosive oesophagitis and for the relief of reflux symptoms. H(2)-receptor antagonists are also not effective in inhibiting meal-stimulated acid secretion, which is required for managing patients with erosive oesophagitis. Furthermore, the rapid development of tolerance to H(2)-receptor antagonists and the rebound acid hypersecretion after the withdrawal of an H(2)-receptor antagonist further limit their clinical use. Although low-dose H(2)-receptor antagonists are currently available as over-the-counter medications for self-controlling acid-related symptoms, their pharmacology and pharmacodynamics have not been well studied, especially in the self-medicating population. Proton pump inhibitors have been proved to be very effective for suppressing intragastric acidity to all known stimuli, although variations exist in the rapidity of onset of action and the potency of acid inhibition after oral administration at the approved therapeutic doses, which may have important clinical implications for the treatment of gastro-oesophageal reflux disease and perhaps for eradicating H. pylori infection when a proton pump inhibitor is given with antibiotics. Once-daily dosing in the morning is more effective than dosing in the evening for all proton pump inhibitors with respect to the suppression of intragastric acidity and daytime gastric acid secretion in particular, which may result from a better bio-availability being achieved with the morning dose. When higher doses are needed, these drugs must be given twice daily to achieve the optimal suppression of 24 hour intragastric acidity. Preliminary results have shown that esomeprazole, the optical isomer of omeprazole, given at 40 mg, is significantly more effective than omeprazole 40 mg, lansoprazole 30 mg or pantoprazole 40 mg for suppressing gastric acid secretion. However, more studies in different patient populations are needed to compare esomeprazole with the existing proton pump inhibitors with regard to their efficacy, cost-effectiveness and long-term safety for the management of acid-related disorders.

摘要

使用抗分泌药物抑制胃酸分泌一直是治疗酸相关性疾病患者的主要药物治疗方法。虽然大多数幽门螺杆菌相关性消化性溃疡可用抗生素治愈,但当抗生素与抗分泌药物,尤其是质子泵抑制剂联用时,溃疡愈合和症状控制可得到显著改善。胃内酸度的抑制与消化性溃疡和糜烂性食管炎的愈合以及酸相关性症状的控制之间存在动态关系。然而,事实证明,H2受体拮抗剂实现的胃酸分泌抑制对于有效控制酸相关性疾病而言并不理想,尤其是对于糜烂性食管炎的愈合和反流症状的缓解。H2受体拮抗剂在抑制进餐刺激的胃酸分泌方面也无效,而这对于治疗糜烂性食管炎患者是必需的。此外,对H2受体拮抗剂的耐受性迅速发展以及停用H2受体拮抗剂后的胃酸分泌反跳性高分泌进一步限制了它们的临床应用。虽然低剂量H2受体拮抗剂目前作为非处方药物可用于自我控制酸相关性症状,但其药理学和药效学尚未得到充分研究,尤其是在自我用药人群中。质子泵抑制剂已被证明对于抑制胃内对所有已知刺激物的酸度非常有效,尽管在批准的治疗剂量下口服给药后起效速度和抑酸效力存在差异,这可能对胃食管反流病的治疗以及质子泵抑制剂与抗生素联用时根除幽门螺杆菌感染具有重要的临床意义。就胃内酸度的抑制,尤其是白天胃酸分泌的抑制而言,所有质子泵抑制剂早晨每日一次给药比晚上给药更有效,这可能是因为早晨给药能实现更好的生物利用度。当需要更高剂量时,这些药物必须每日给药两次以实现对24小时胃内酸度的最佳抑制。初步结果表明,奥美拉唑的光学异构体埃索美拉唑40毫克在抑制胃酸分泌方面显著比奥美拉唑40毫克、兰索拉唑30毫克或泮托拉唑40毫克更有效。然而,需要在不同患者群体中进行更多研究,以比较埃索美拉唑与现有质子泵抑制剂在治疗酸相关性疾病方面的疗效、成本效益和长期安全性。

相似文献

[1]
Pharmacological and pharmacodynamic essentials of H(2)-receptor antagonists and proton pump inhibitors for the practising physician.

Best Pract Res Clin Gastroenterol. 2001-6

[2]
Review article: the pharmacodynamics and pharmacokinetics of proton pump inhibitors--overview and clinical implications.

Aliment Pharmacol Ther. 2004-11

[3]
Acid suppression therapy: where do we go from here?

Dig Dis. 2006

[4]
Histamine receptor antagonists, proton pump inhibitors and their combination in the treatment of gastro-oesophageal reflux disease.

Best Pract Res Clin Gastroenterol. 2001-6

[5]
pH, healing rate, and symptom relief in patients with GERD.

Yale J Biol Med. 1999

[6]
Duodenal ulcer and gastroesophageal reflux disease today: long-term therapy--a sideways glance.

Yale J Biol Med. 1996

[7]
Progress with proton pump inhibitors in acid peptic disease: treatment of duodenal and gastric ulcer.

Clin Ther. 1993

[8]
Proton pump inhibitors and acid-related diseases.

Pharmacotherapy. 1997

[9]
[Are proton pump inhibitors superior to H2 receptor antagonists within the scope of H. pylori eradication therapy? Meta analysis of current parallel group comparisons].

Z Gastroenterol. 1996-5

[10]
Current status of acid pump antagonists (reversible PPIs).

Yale J Biol Med. 1996

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