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司美格鲁肽在健康超重/肥胖受试者3个不同注射部位的皮下生物利用度

Subcutaneous Bioavailability of Taspoglutide at 3 Different Injection Sites in Healthy Overweight/Obese Subjects.

作者信息

Sturm-Pellanda Carolina, Abt Markus, Sanwald-Ducray Patricia, Schmitt Christophe

机构信息

F. Hoffmann-La Roche AG, Basel, Switzerland.

F. Hoffmann-La Roche AG, Basel, Switzerland.

出版信息

Clin Ther. 2015 Nov 1;37(11):2439-48. doi: 10.1016/j.clinthera.2015.08.022. Epub 2015 Sep 26.

Abstract

PURPOSE

Taspoglutide is a long-acting glucagon-like peptide-1 (GLP-1) receptor agonist that has >90% homology with the endogenous GLP-1 while retaining equivalent potency. Once-weekly subcutaneous injections with taspoglutide demonstrated meaningful antihyperglycemic and weight loss effects in patients with type 2 diabetes. The present study was performed to compare the relative bioavailability of taspoglutide injected subcutaneously in the abdomen, upper arm, and thigh.

METHODS

Healthy overweight/obese subjects were randomized in an open-label, 3-way crossover study. A single 20-mg dose of taspoglutide was injected subcutaneously on 3 occasions in the abdomen, upper arm, or thigh. Each injection was separated by a 12-week washout period. Blood was sampled up to 12 weeks for the pharmacokinetic evaluation of taspoglutide.

FINDINGS

Sixty subjects were randomized into the study (mean age, 45.5 years; body weight, 97.6 kg; and body mass index, 31.4 kg/m(2)). AUClast values (geometric mean) for subcutaneous injections in the abdomen, upper arm, and thigh were 44.2, 61.2, and 50.0 ng·h/mL, respectively. The geometric mean ratio (relative bioavailability) for the upper arm versus the abdomen was 1.41 (90% CI: 1.22-1.62) and for the thigh versus the abdomen was 1.13 (90% CI: 0.98-1.31). Corresponding Cmax values for subcutaneous injections in the abdomen, upper arm, and thigh were 0.268, 0.382, and 0.341 ng/mL, respectively, and the geometric mean ratio for the upper arm versus the abdomen was 1.43 (90% CI: 1.24-1.64) and for the thigh versus the abdomen was 1.27 (90% CI: 1.10-1.46). Decreases in taspoglutide exposure were observed with each subsequent period. AUClast values (geometric mean across injections sites) for periods 1, 2, and 3 were 97.2, 42.6, and 31.5 ng·h/mL, respectively. The geometric mean ratio for period 2 versus 1 was 0.44 (90% CI: 0.38-0.50) and for period 3 versus 1 was 0.32 (90% CI: 0.27-0.37). Analysis of pharmacokinetic data after first injection only (period 1) showed comparable AUClast across the 3 injection sites and lower initial Cmax after injection into the abdomen compared with the other 2 injection sites. Overall, taspoglutide was well tolerated by most subjects in all 3 injection sites, with a lower incidence of nausea and vomiting when injected in the abdomen.

IMPLICATIONS

Regardless of a pronounced period effect, relative bioavailability of taspoglutide was different across injection sites, with the lowest exposure and incidence of nausea and vomiting seen after administration in the abdomen. In the absence of comparable bioavailability, taspoglutide was recommended to be injected into the abdomen.

摘要

目的

塔司格鲁肽是一种长效胰高血糖素样肽-1(GLP-1)受体激动剂,与内源性GLP-1具有>90%的同源性,同时保留同等效力。每周一次皮下注射塔司格鲁肽在2型糖尿病患者中显示出显著的降糖和减重效果。本研究旨在比较塔司格鲁肽分别皮下注射于腹部、上臂和大腿后的相对生物利用度。

方法

健康超重/肥胖受试者被随机分配至一项开放标签的三交叉研究中。单次20 mg剂量的塔司格鲁肽分别在腹部、上臂或大腿皮下注射3次。每次注射间隔12周的洗脱期。在长达12周的时间内采集血样,用于塔司格鲁肽的药代动力学评估。

结果

60名受试者被随机纳入研究(平均年龄45.5岁;体重97.6 kg;体重指数31.4 kg/m²)。腹部、上臂和大腿皮下注射的末次观察浓度-时间曲线下面积(AUClast)值(几何均值)分别为44.2、61.2和50.0 ng·h/mL。上臂与腹部的几何平均比值(相对生物利用度)为1.41(90%置信区间:1.22 - 1.62),大腿与腹部的几何平均比值为1.13(90%置信区间:0.98 -131)。腹部、上臂和大腿皮下注射的相应达峰浓度(Cmax)值分别为0.268、0.382和0.341 ng/mL,上臂与腹部的几何平均比值为1.43(90%置信区间:1.24 - 1.64),大腿与腹部的几何平均比值为1.27(90%置信区间:1.10 - 1.46)。在随后的每个时间段均观察到塔司格鲁肽暴露量的下降。第1、2和3时间段的AUClast值(各注射部位的几何均值)分别为97.2、42.6和31.5 ng·h/mL。第2时间段与第1时间段的几何平均比值为0.44(90%置信区间:0.38 - 0.50),第3时间段与第1时间段的几何平均比值为0.32(90%置信区间:0.27 - 0.37)。仅分析首次注射后(第1时间段)的药代动力学数据显示,3个注射部位的AUClast相当,且与其他2个注射部位相比,注射至腹部后的初始Cmax较低。总体而言,所有3个注射部位的大多数受试者对塔司格鲁肽耐受性良好,在腹部注射时恶心和呕吐的发生率较低。

结论

尽管存在明显的时间段效应,但塔司格鲁肽在不同注射部位的相对生物利用度不同,在腹部给药后暴露量最低,恶心和呕吐的发生率也最低。在生物利用度无可比性的情况下,建议将塔司格鲁肽注射至腹部。

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