首页> 外文期刊>Clinical therapeutics >Effects of cilomilast, a selective phosphodiesterase 4 inhibitor, on esophageal motility and pH, and orocecal and colonic transit: two single-center, randomized, double-blind, placebo-controlled, two-part crossover studies in healthy volunteers.
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Effects of cilomilast, a selective phosphodiesterase 4 inhibitor, on esophageal motility and pH, and orocecal and colonic transit: two single-center, randomized, double-blind, placebo-controlled, two-part crossover studies in healthy volunteers.

机译:选择性磷酸二酯酶4抑制剂cilomilast对食道运动性和pH值以及口腔和结肠转运的影响:在健康志愿者中进行的两项单中心,随机,双盲,安慰剂对照,两部分交叉研究。

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BACKGROUND: Phase IIb studies have reported that cilomilast, a selective phosphodiesterase 4 inhibitor being developed for the treatment of chronic obstructive pulmonary disease, is associated with gastrointestinal (GI) adverse effects (AEs) in a small proportion (approximately 5%) of individuals. OBJECTIVES: The aims of these 2 studies were to investigate the effects of cilomilast 15 mg BID on: (1) lower esophageal sphincter pressure (LESP) and esophageal body motility and pH (study 1); and (2) orocecal and whole-gut transit times (OCTT and WGTT, respectively) (study 2) in healthy volunteers. METHODS: These 2 randomized, double-blind, placebo-controlled, 2-part crossover studies were conducted at the Neurogastroenterology Unit, Wythenshawe Hospital, Manchester, United Kingdom (study 1) and GlaxoSmithKline, Harlow, United Kingdom (study 2). In study 1, subjects were randomly assigned to receive either cilomilast (15 mg BID) or matched placebo (control) for 7 days (13 doses; subjects were not given the evening dose on day 7), and in study 2, cilomilast (15 mg BID) or matched placebo (control) for 9 days (18 doses) in each of 2 treatment periods. After study drug administration, combined esophageal motility and pH were recorded for 2 hours before and 4 hours after the administration of a standardized meal (2400 kJ [573 kcal]). Sequences of 6 consecutive 5-mL water swallows (separated by 20 seconds) were carried out 60 and 90 minutes (fasting) and 150, 180, 210, 240, 300, and 360 minutes (fed) after study drug administration. OCTT was determined from the increase in breath hydrogen after the meal. WGTT was determined from the time taken to excrete at least 16 of 20 ingested radiopaque markers, ingested as 2 capsules, each containing 10 radiopaque markers, with 240 mL of water. AEs were elicited at specified times throughout each session using nonleading questions, spontaneously reported AEs, and diary cards. RESULTS: Study 1 enrolled 20 subjects (11 men, 9 women; age range, 20-52 years). Study 2 enrolled 16 subjects (10 men, 6 women; age range, 19-48 years). No clinically significant differences in the amplitude (mean difference in postprandial-preprandial AUC0-t/t, 6.09 mm Hg; 95% CI, -10.66 to 22.84), duration (difference, -0.08 second; 95% CI, -0.54 to 0.37), or velocity of propagation (difference, 0.90 cm/s; 95% CI, -0.66 to 2.46) of esophageal contractions, LESP (difference, -0.39 mm Hg; 95% CI, -5.23 to 4.45), or preprandial or postprandial percentage time pH<4 (median differences: preprandial, 0.47% [95% CI, -0.45 to 1.27]; postprandial, -0.005% [95% CI, -1.30 to 6.27]) were found with cilomilast compared with placebo. No significant differences in OCTT (difference, -0.37 hour; 95% CI, -1.59 to 0.84) or WGTT (difference, -2.96 hours; 95% CI, -20.76 to 14.84) were found with cilomilast compared with controls. In both studies, the most frequently reported AEs with cilomilast use were nausea (8/18 in study 1 and 3/16 in study 2) and headache (8/18 in study 1 and 6/16 in study 2); however, these were generally of mild to moderate intensity. Overall, GI AEs did not correlate with changes in GI motility. CONCLUSION: The results of these 2 studies suggest that cilomilast was not associated with significant changes in esophageal motility and pH or GI transit in these healthy volunteers.
机译:背景:IIb期研究报告称,正在开发用于治疗慢性阻塞性肺疾病的选择性磷酸二酯酶4抑制剂cilomilast与胃肠道(GI)不良反应(AE)相关的比例很小(约占5%)。目的:这两项研究的目的是研究西洛司司特15 mg BID对以下方面的影响:(1)降低食道括约肌压力(LESP)和食道机体运动性和pH(研究1); (2)健康志愿者的经口和全肠运输时间(分别为OCTT和WGTT)(研究2)。方法:这两项随机,双盲,安慰剂对照,两部分交叉研究是在英国曼彻斯特Wythenshawe医院的神经胃肠病科(研究1)和英国哈洛的葛兰素史克公司(研究2)进行的。在研究1中,受试者被随机分配接受cilomilast(15 mg BID)或匹配的安慰剂(对照组),共7天(13剂;受试者在第7天未接受夜间剂量),而在研究2中,cilomilast(15 2个疗程中的每一个疗程,共9天(18剂)。服用研究药物后,在服用标准餐(2400 kJ [573 kcal])之前和之后的2小时内记录食管运动和pH值。在研究药物给药后60和90分钟(禁食)和150、180、210、240、300和360分钟(进食)进行6次连续5 mL水吞咽(间隔20秒)的序列。 OCTT由进餐后呼吸氢的增加确定。 WGTT是从将20份不透射线的标记物中至少16份排泄的时间确定的,这些标记物以2粒胶囊的形式摄入,每个胶囊含10个不透射线的标记物,并用水240毫升水排泄。在每个会话的特定时间,使用无先导性问题,自发报告的AE和日记卡引发AE。结果:研究1招募了20名受试者(11名男性,9名女性;年龄范围为20-52岁)。研究2招募了16名受试者(10名男性,6名女性;年龄范围为19-48岁)。振幅,持续时间(差异,-0.08秒; -95%CI,-0.54至0.37)的振幅(餐前-餐前AUC0-t / t的均值差异,6.09 mm Hg; 95%CI,-10.66至22.84)无临床显着差异)或食道收缩的传播速度(差异,0.90 cm / s; 95%CI,-0.66至2.46),LESP(差异,-0.39 mm Hg; 95%CI,-5.23至4.45),或餐前或餐后与安慰剂相比,西洛司特发现pH值小于4的时间百分比(中位数差异:餐前0.47%[95%CI,-0.45至1.27];餐后-0.005%[95%CI,-1.30至6.27])。 cilomilast与对照组相比,在OCTT(差异-0.37小时; 95%CI,-1.59至0.84)或WGTT(差异-2.96小时; 95%CI,-20.76至14.84)方面无显着差异。在两项研究中,最常报告的使用cilomilast的AEs是恶心的(在研究1中为8/18,在研究2中为3/16)和头痛(在研究1中为8/18,在研究2中为6/16)。但是,这些强度通常为轻度到中度。总体而言,胃肠道不良事件与胃肠道动力的变化无关。结论:这两项研究的结果表明,在这些健康志愿者中,cilomilast与食管运动性和pH或GI转运的显着变化无关。

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