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比较非诺贝特和非诺贝特酸在人体内的胃肠道吸收和生物利用度。

Comparison of the gastrointestinal absorption and bioavailability of fenofibrate and fenofibric acid in humans.

机构信息

100 Abbott Park Road, Dept R4PK, Bldg AP13A-3, Abbott Park, IL 60064-6104, USA.

出版信息

J Clin Pharmacol. 2010 Aug;50(8):914-21. doi: 10.1177/0091270009354995. Epub 2010 Feb 9.

Abstract

This study compared the gastrointestinal (GI) absorption characteristics and absolute bioavailability of fenofibric acid and fenofibrate (which is converted to fenofibric acid in vivo) in healthy volunteers. Treatments were delivered to the proximal small bowel, distal small bowel, and colon using a site-specific delivery system (Enterion capsule) and to the stomach by oral administration of equimolar doses. Serial blood samples were collected for 120 hours postdose and assayed for plasma fenofibric acid concentrations. The absolute bioavailability of each treatment was determined relative to 50 mg of fenofibric acid administered intravenously. Plasma exposure to fenofibric acid following fenofibric acid administration was approximately 1.5 times higher than that following fenofibrate administration for delivery to the proximal and distal small bowel and following oral administration, and it was approximately 5 times higher following colon delivery. The absolute bioavailability in the stomach, proximal small bowel, distal small bowel, and colon was approximately 81%, 88%, 84%, and 78%, respectively, for fenofibric acid and 69%, 73%, 66%, and 22%, respectively, for fenofibrate (P < .0001 and P = .033 for fenofibric acid vs fenofibrate in the colon and distal small bowel, respectively). In conclusion, fenofibric acid is well absorbed throughout the GI tract and has greater bioavailability than fenofibrate in all GI regions.

摘要

这项研究比较了在健康志愿者中,非诺贝特酸和非诺贝特(在体内转化为非诺贝特酸)的胃肠道(GI)吸收特征和绝对生物利用度。使用特定部位递送系统(Enterion 胶囊)将治疗药物递送至近端小肠、远端小肠和结肠,并通过口服给予等摩尔剂量递送至胃部。在给药后 120 小时内采集连续的血样,并测定血浆中非诺贝特酸的浓度。每种治疗药物的绝对生物利用度相对于静脉给予 50mg 的非诺贝特酸来确定。非诺贝特酸给药后,与非诺贝特酸给药相比,非诺贝特酸给药后在近端和远端小肠以及口服后,血浆中非诺贝特酸的暴露量约高 1.5 倍,在结肠给药后约高 5 倍。非诺贝特酸在胃、近端小肠、远端小肠和结肠中的绝对生物利用度分别约为 81%、88%、84%和 78%,而非诺贝特酸分别约为 69%、73%、66%和 22%(P<0.0001 和 P=0.033,非诺贝特酸在结肠和远端小肠中与非诺贝特相比)。总之,非诺贝特酸在整个胃肠道中被很好地吸收,并且在所有胃肠道区域的生物利用度都大于非诺贝特。

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