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2
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Single-ascending-dose pharmacokinetics and safety of the novel broad-spectrum antifungal triazole BAL4815 after intravenous infusions (50, 100, and 200 milligrams) and oral administrations (100, 200, and 400 milligrams) of its prodrug, BAL8557, in healthy volunteers.新型广谱抗真菌三唑类药物BAL4815的前体药物BAL8557在健康志愿者中静脉输注(50、100和200毫克)及口服给药(100、200和400毫克)后的单剂量递增药代动力学及安全性研究。
Antimicrob Agents Chemother. 2006 Jan;50(1):279-85. doi: 10.1128/AAC.50.1.279-285.2006.
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Recent developments in the management of invasive fungal infections in patients with hematological malignancies.血液系统恶性肿瘤患者侵袭性真菌感染管理的最新进展
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Urinary 6beta-hydroxycortisol: a validated test for evaluating drug induction or drug inhibition mediated through CYP3A in humans and in animals.尿6β-羟基皮质醇:一种用于评估人类和动物中通过CYP3A介导的药物诱导或药物抑制作用的有效检测方法。
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新型抗真菌三唑类药物BAL4815在健康志愿者静脉输注其前体药物BAL8557及口服给药后的多剂量药代动力学和安全性。

Multiple-dose pharmacokinetics and safety of the new antifungal triazole BAL4815 after intravenous infusion and oral administration of its prodrug, BAL8557, in healthy volunteers.

作者信息

Schmitt-Hoffmann Anne, Roos Brigitte, Maares Jürgen, Heep Markus, Spickerman Jochen, Weidekamm Erhard, Brown Tom, Roehrle Michael

机构信息

Basilea Pharmaceutica, Ltd., P.O. Box 3255, 4002 Basel, Switzerland.

出版信息

Antimicrob Agents Chemother. 2006 Jan;50(1):286-93. doi: 10.1128/AAC.50.1.286-293.2006.

DOI:10.1128/AAC.50.1.286-293.2006
PMID:16377699
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1346776/
Abstract

BAL8557 is the water-soluble prodrug of BAL4815, a new broad-spectrum antifungal. Healthy male subjects were randomly assigned to four treatment cohorts to receive multiple oral doses or multiple 1-h constant-rate intravenous infusions of BAL8557. Loading doses of BAL8557 were equivalent to 100 mg (followed by once-daily maintenance doses of 50 mg) or 200 mg (followed by once-daily maintenance doses of 100 mg) of BAL4815. In each cohort, six subjects received active drug and two subjects received the placebo. Study duration was 21 days (oral) and 14 days (intravenous). All adverse events reported were mild or moderate, except one severe rhinitis event which was not related to trial medication. After both routes of administration, maximum drug concentration observed in plasma (C(max)) and area under the concentration-time curve (AUC) values of BAL4815 increased proportionally to the administered dose. AUC values reflected a fourfold to fivefold accumulation of active drug in plasma during once-daily dosing, which is in line with the long elimination half-life of BAL4815 determined after the last administration (mean, 84.5 to 117 h). At steady state, the volume of distribution was large and amounted to 308 to 542 liters. Systemic clearance reached only 2.4 to 4.1 liter/h. At the levels obtained in the present study, C(max) values of 2.56 and 2.55 microg/ml after oral and intravenous administrations, respectively, there was no indication of CYP3A4 induction or inhibition (as revealed by the urinary 6-beta-hydroxycortisol/cortisol test). Based on AUC values after oral and intravenous administration, an excellent oral bioavailability can be predicted for BAL4815. Once-daily oral dosing of 50- or 100-mg equivalents of BAL8557 were recently demonstrated to be efficacious in a phase 2 study conducted with patients with esophageal candidiasis. These doses (preceded by adequate loading dose[s]) will be further explored in the treatment of systemic mycoses.

摘要

BAL8557是新型广谱抗真菌药BAL4815的水溶性前体药物。健康男性受试者被随机分配到四个治疗组,接受多次口服剂量或多次1小时恒速静脉输注BAL8557。BAL8557的负荷剂量相当于100mg(随后每日一次维持剂量为50mg)或200mg(随后每日一次维持剂量为100mg)的BAL4815。在每个治疗组中,六名受试者接受活性药物,两名受试者接受安慰剂。研究持续时间为21天(口服)和14天(静脉注射)。报告的所有不良事件均为轻度或中度,除了一起严重鼻炎事件,该事件与试验用药无关。两种给药途径后,血浆中观察到的BAL4815的最大药物浓度(C(max))和浓度-时间曲线下面积(AUC)值与给药剂量成比例增加。AUC值反映了每日一次给药期间活性药物在血浆中的四倍至五倍蓄积,这与末次给药后测定的BAL4815的长消除半衰期(平均84.5至117小时)一致。在稳态时,分布容积很大达308至542升。全身清除率仅达到2.4至4.1升/小时。在本研究获得的水平下,口服和静脉给药后C(max)值分别为2.56和2.55μg/ml,没有CYP3A4诱导或抑制的迹象(如尿6-β-羟基皮质醇/皮质醇试验所示)。基于口服和静脉给药后的AUC值,可以预测BAL4815具有优异的口服生物利用度。最近在一项针对食管念珠菌病患者进行的2期研究中证明,每日一次口服50mg或100mg当量的BAL8557是有效的。这些剂量(在适当的负荷剂量之前)将在系统性真菌病的治疗中进一步探索。