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雷贝拉唑诱导胃酸缺乏的健康志愿者使用盐酸甜菜碱进行胃再酸化。

Gastric reacidification with betaine HCl in healthy volunteers with rabeprazole-induced hypochlorhydria.

作者信息

Yago Marc R, Frymoyer Adam R, Smelick Gillian S, Frassetto Lynda A, Budha Nageshwar R, Dresser Mark J, Ware Joseph A, Benet Leslie Z

机构信息

Department of Bioengineering and Therapeutic Sciences, University of California, San Francisco , 533 Parnassus Avenue, San Francisco, California 94143-0912, United States.

出版信息

Mol Pharm. 2013 Nov 4;10(11):4032-7. doi: 10.1021/mp4003738. Epub 2013 Sep 10.

Abstract

Previous studies have demonstrated that increased gastric pH from the use of acid-reducing agents, such as proton-pump inhibitors or H2-receptor antagonists, can significantly impact the absorption of weakly basic drugs that exhibit pH-dependent solubility. Clinically practical strategies to mitigate this interaction have not been developed. This pilot study evaluated the extent and time course of gastric reacidification after a solid oral dosage form of anhydrous betaine HCl in healthy volunteers with pharmacologically induced hypochlorhydria. Six healthy volunteers with baseline normochlorhydria (fasting gastric pH < 4) were enrolled in this single period study. Hypochlorhydria was induced via 20 mg oral rabeprazole twice daily for four days. On the fifth day, an additional 20 mg dose of oral rabeprazole was given and gastric pH was monitored continuously using the Heidelberg pH capsule. After gastric pH > 4 was confirmed for 15 min, 1500 mg of betaine HCl was given orally with 90 mL of water and gastric pH was continuously monitored for 2 h. Betaine HCl significantly lowered gastric pH by 4.5 (± 0.5) units from 5.2 (± 0.5) to 0.6 (± 0.2) (P < 0.001) during the 30 min interval after administration. The onset of effect of betaine HCl was rapid, with a mean time to pH < 3 of 6.3 (± 4.3) min. The reacidification period was temporary with a gastric pH < 3 and < 4 lasting 73 (± 33) and 77 (± 30) min, respectively. Betaine HCl was well tolerated by all subjects. In healthy volunteers with pharmacologically induced hypochlorhydria, betaine HCl was effective at temporarily lowering gastric pH. The rapid onset and relatively short duration of gastric pH reduction gives betaine HCl the potential to aid the absorption of orally administered weakly basic drugs that exhibit pH-dependent solubility when administered under hypochlorhydric conditions.

摘要

先前的研究表明,使用质子泵抑制剂或H2受体拮抗剂等抑酸剂导致胃内pH值升高,会显著影响具有pH依赖性溶解度的弱碱性药物的吸收。目前尚未制定出临床上切实可行的减轻这种相互作用的策略。这项初步研究评估了在患有药物性胃酸过少的健康志愿者中,口服无水盐酸甜菜碱固体剂型后胃再酸化的程度和时间进程。六名基线胃酸正常(空腹胃pH值<4)的健康志愿者参与了这项单周期研究。通过每天口服20毫克雷贝拉唑,持续四天诱导胃酸过少。在第五天,额外给予20毫克口服雷贝拉唑,并使用海德堡pH胶囊连续监测胃pH值。在确认胃pH值>4持续15分钟后,口服1500毫克盐酸甜菜碱并同时饮用90毫升水,然后连续监测胃pH值2小时。给药后30分钟内,盐酸甜菜碱使胃pH值从5.2(±0.5)显著降低4.5(±0.5)个单位至0.6(±0.2)(P<0.001)。盐酸甜菜碱起效迅速,pH值<3的平均时间为6.3(±4.3)分钟。再酸化期是暂时的,胃pH值<3和<4分别持续73(±33)和77(±30)分钟。所有受试者对盐酸甜菜碱耐受性良好。在患有药物性胃酸过少的健康志愿者中,盐酸甜菜碱能有效暂时降低胃pH值。胃pH值降低的快速起效和相对较短的持续时间使盐酸甜菜碱有潜力在胃酸过少条件下给药时,辅助口服具有pH依赖性溶解度的弱碱性药物的吸收。

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