Green J T, Evans B K, Rhodes J, Thomas G A, Ranshaw C, Feyerabend C, Russell M A
Department of Gastroenterology, University Hospital of Wales, Cardiff, UK.
Br J Clin Pharmacol. 1999 Oct;48(4):485-93. doi: 10.1046/j.1365-2125.1999.00057.x.
Ulcerative colitis is predominantly a disease of nonsmokers and transdermal nicotine has therapeutic value in active disease; however side-effects are troublesome. The aim of this study was to develop an oral formulation of nicotine which would be slowly released in the colon over 6 h, and to examine its pharmacokinetic profile in 12 healthy volunteers, with measurements of serum nicotine and cotinine, its principal metabolite.
Nicotine was combined with a polyacrylic carbomer, Carbopol 974P which was incorporated into 13 different vehicles and their release profiles examined in vitro. The polyglycolized glyceride, Gelucire 50/13, was chosen for subsequent kinetic studies because it consistently produced a suitable release pattern which was linear. Capsules containing 3 mg nicotine, combined with carbomer in Gelucire 50/13, were coated with an acrylic resin Eudragit L; this ensured the capsule would remain intact until the ileum. On 2 separate days, 6 and 15 mg nicotine, contained in 2 and 5 capsules, respectively, were administered to 12 subjects, all nonsmokers, mean age 28 years. Serial blood measurements were taken for 36 h, serum nicotine and cotinine concentrations were measured by gas liquid chromatography.
There was considerable intersubject variability in the nicotine and cotinine values. Plasma nicotine levels began to rise about 4 h after ingestion of the capsules, corresponding with the oro-caecal transit time. Cmax nicotine values were 2.2 and 5 ng ml-1, obtained 7 h after the ingestion of 6 and 15 mg, respectively, of the formulation. The corresponding Cmax values for cotinine were 37 and 94.4 ng ml-1, occurring after 9-10 h. The mean for elimination half-lives in the 24 studies, including the 6 and 15 mg doses, for nicotine were 4.3+/-2.7 h and for cotinine 16.8+/-7.5 h. With 6 mg nicotine-carbomer, only 1 of 12 volunteers had possible side-effects, but with the 15 mg dose 11 out of the 12 reported adverse effects which were systemic or gastrointestinal in nature-their timing corresponded with peak serum concentrations of nicotine.
An oral formulation of nicotine has been developed; in the ileum and colon, this becomes available for slow linear release over 6 h and delivers high concentrations of nicotine for topical effect on the colon. 6 mg Nicotine was well tolerated, whilst 15 mg gave both systemic and gastrointestinal side-effects. High concentrations of topical nicotine in the colon are achieved with relatively low systemic bioavailablity-reflected by the Cmax and AUC values for nicotine. This, or comparable formulations, may be of therapeutic value in ulcerative colitis.
溃疡性结肠炎主要是一种非吸烟者易患的疾病,经皮尼古丁对活动性疾病具有治疗价值;然而,其副作用令人困扰。本研究的目的是开发一种尼古丁口服制剂,使其在结肠中能在6小时内缓慢释放,并在12名健康志愿者中检测其药代动力学特征,测量血清尼古丁及其主要代谢物可替宁的水平。
将尼古丁与聚丙烯酸卡波姆(卡波姆974P)混合,该卡波姆被纳入13种不同的载体中,并在体外检测其释放曲线。选择聚乙二醇化甘油酯(Gelucire 50/13)用于后续的动力学研究,因为它始终能产生合适的、呈线性的释放模式。含有3毫克尼古丁并与卡波姆在Gelucire 50/13中混合的胶囊,用丙烯酸树脂Eudragit L包衣;这确保胶囊在到达回肠之前保持完整。在2个不同的日子里,分别向12名受试者(均为非吸烟者,平均年龄28岁)给予2粒和5粒胶囊中所含的6毫克和15毫克尼古丁。连续采血36小时,通过气液色谱法测量血清尼古丁和可替宁浓度。
受试者之间尼古丁和可替宁的值存在相当大的差异。血浆尼古丁水平在摄入胶囊后约4小时开始上升,这与口腔至盲肠的转运时间相对应。摄入6毫克和15毫克制剂后7小时,尼古丁的Cmax值分别为2.2和5纳克/毫升。可替宁的相应Cmax值分别为37和94.4纳克/毫升,在9至10小时后出现。在包括6毫克和15毫克剂量的24项研究中,尼古丁消除半衰期的平均值为4.3±2.7小时,可替宁为16.8±7.5小时。服用6毫克尼古丁-卡波姆时,12名志愿者中只有1人可能出现副作用,但服用15毫克剂量时,12人中有11人报告了全身性或胃肠道的不良反应,其发生时间与尼古丁血清浓度峰值相对应。
已开发出一种尼古丁口服制剂;在回肠和结肠中,该制剂可在6小时内缓慢线性释放,并能提供高浓度的尼古丁以对结肠产生局部作用。6毫克尼古丁耐受性良好,而15毫克则会产生全身性和胃肠道副作用。通过相对较低的全身生物利用度可在结肠中实现高浓度的局部尼古丁,这由尼古丁的Cmax和AUC值反映出来。这种制剂或类似制剂可能对溃疡性结肠炎具有治疗价值。