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健康受试者口服给药后,艾沙康唑的吸收情况与静脉给药相当,且不受食物或改变胃pH值药物的影响。

Isavuconazole absorption following oral administration in healthy subjects is comparable to intravenous dosing, and is not affected by food, or drugs that alter stomach pH.

作者信息

Schmitt-Hoffmann Anne, Desai Amit, Kowalski Donna, Pearlman Helene, Yamazaki Takao, Townsend Robert

出版信息

Int J Clin Pharmacol Ther. 2016 Aug;54(8):572-80. doi: 10.5414/CP202434.

DOI:10.5414/CP202434
PMID:27345284
Abstract

OBJECTIVE/METHODS: Two openlabel, single-dose, randomized crossover studies and one open-label, multiple-dose, parallel group study in healthy volunteers were conducted with the prodrug, isavuconazonium sulfate, to determine absolute bioavailability of the active triazole, isavuconazole (EudraCT 2007-004949-15; n = 14), and the effect of food (EudraCT 2007- 004940-63; n = 26), and pH (NCT02128893; n = 24) on the absorption of isavuconazole. Isavuconazonium sulfate 744 mg designed to deliver 400 mg of the active triazole isavuconazole was administered in the absolute bioavailability (oral or intravenous (IV) (2-hour infusion)) and food-effect studies (oral). In the pH-effect study, isavuconazonium sulfate 372 mg designed to deliver 200 mg of isavuconazole was administered orally three times daily (t.i.d.) for 2 days, followed by a single daily oral dose for 3 days, in the presence of steady state esomeprazole dosed orally at 40 mg/day.

RESULTS

Isavuconazole was well tolerated in each study. Bioavailability: Geometric least squares mean ratios (GLSMR; oral/IV) for isavuconazole AUC∞, and Cmax were 98% (90% confidence interval (CI): 94, 101) and 78% (90% CI: 72, 85), respectively. Food-effect: GLSMR (fed/fasted) for AUC∞ and Cmax of isavuconazole in plasma were 110% (90% CI: 102, 118) and 92% (90% CI: 86, 98), respectively. Median tmax was 5 hours with food and 3 hours under fasted conditions. pH-effect: GLSMR for isavuconazole AUCtau and Cmax were 108% (90% CI: 89, 130) and 105% (90% CI: 89, 124), respectively.

CONCLUSIONS

Orally administered isavuconazonium sulfate effectively delivers isavuconazole, as evidenced by the fact that oral isavuconazole is bioequivalent to the IV formulation. Dose adjustments are not required when switching between oral and IV formulations, regardless of food or drugs that increase gastric pH.

摘要

目的/方法:对健康志愿者进行了两项开放标签、单剂量、随机交叉研究以及一项开放标签、多剂量、平行组研究,使用前体药物硫酸艾沙康唑硫酸酯来确定活性三唑类药物艾沙康唑的绝对生物利用度(欧洲药品临床试验数据库编号2007 - 004949 - 15;n = 14),以及食物(欧洲药品临床试验数据库编号2007 - 004940 - 63;n = 26)和pH值(临床研究编号NCT02128893;n = 24)对艾沙康唑吸收的影响。在绝对生物利用度(口服或静脉注射(静脉输注2小时))和食物影响研究(口服)中,给予设计用于提供400mg活性三唑类药物艾沙康唑的744mg硫酸艾沙康唑硫酸酯。在pH值影响研究中,设计用于提供200mg艾沙康唑的372mg硫酸艾沙康唑硫酸酯,在每天口服40mg埃索美拉唑达到稳态的情况下,每日口服三次(每日三次),持续2天,随后每日单次口服剂量,持续3天。

结果

在每项研究中,艾沙康唑耐受性良好。生物利用度:艾沙康唑AUC∞和Cmax的几何最小二乘均值比(GLSMR;口服/静脉注射)分别为98%(90%置信区间(CI):94,101)和78%(90%CI:72,85)。食物影响:血浆中艾沙康唑AUC∞和Cmax的GLSMR(进食/禁食)分别为110%(90%CI:102,118)和92%(90%CI:86,98)。进食时tmax中位数为5小时,禁食条件下为3小时。pH值影响:艾沙康唑AUCtau和Cmax的GLSMR分别为108%(90%CI:89,130)和105%(90%CI:89,124)。

结论

口服硫酸艾沙康唑硫酸酯可有效递送艾沙康唑,口服艾沙康唑与静脉制剂生物等效即证明了这一点。无论食物或增加胃pH值的药物如何,在口服和静脉制剂之间切换时无需调整剂量。

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