Beaubien A R, Karpinski K, Ormsby E
Biopharmaceutics and Pharmacodynamics Division, Ottawa, Ontario, Canada.
Hear Res. 1995 Mar;83(1-2):62-79. doi: 10.1016/0378-5955(94)00192-s.
An extensive overview of the relationship between cochlear toxicity and amikacin blood concentrations in the guinea pig is provided which should assist in the clinical application of this class of antibiotic. A data set previously used to relate the incidence of amikacin ototoxicity to dosing rates and blood concentrations was re-examined to assess the toxicodynamics of amikacin in terms of decibels of hearing loss across dosing rate, hearing frequency and time following drug exposure. Animals in this data set had received continuously i.v. infused amikacin over an 8-fold range of dosing rates. Preliminary analysis indicated that the data were consistent with a sigmoid relationship between hearing loss (decibels) and area under the amikacin plasma concentration vs time curve cumulated over the entire course of drug administration (cAUC). The sigmoid model was therefore used as the backbone of a far more comprehensive toxicodynamic model which described all the data with a single equation. Testing with this model showed that the cAUC required to produce half-maximum hearing loss (cAUC-1/2) was related to dosing rate (P < 0.01), to hearing frequency (P < 0.00001), and to post-drug interval (P < 0.00001). Maximum hearing loss (difference between upper and lower sigmoid asymptotes) was less than total and was significantly related to frequency (P < 0.00001). No effects could be detected on the sigmoid slope. Further modelling of the significant effects detected by the comprehensive toxicodynamic model was done to determine if they could be described by simple relationships or by biologically relevant sub-models. Modelling of maximum hearing loss (postulated to represent loss of mainly outer hair cell function) indicated that this parameter was constant at about 61 decibels for 2-12 kHz and linearly decreased with log frequency for frequencies > 12 kHz. Modelling of cAUC-1/2 on frequency indicated that there was a strong inverse linear relationship to log frequency. Modelling of cAUC-1/2 on post-drug interval indicated that delayed ototoxicity continued at progressively slower rates for at least 56 days after drug administration had ceased. Modelling of cAUC-1/2 on dosing rate showed an increased requirement for drug as the dosing rate decreased. However, cAUC-1/2 changed no more than 20% across the range of dosing rates compared to the 8-fold difference in mean steady-state plasma concentrations, suggesting that plasma concentration is not a primary determinant of ototoxicity. A toxicokinetic model was developed which explained the dosing rate effect on cAUC-1/2 very successfully.(ABSTRACT TRUNCATED AT 400 WORDS)
本文全面概述了豚鼠耳蜗毒性与阿米卡星血药浓度之间的关系,这将有助于此类抗生素的临床应用。重新审视了一个先前用于将阿米卡星耳毒性发生率与给药速率和血药浓度相关联的数据集,以评估阿米卡星在给药速率、听力频率和药物暴露后的时间方面导致听力损失分贝数的毒代动力学。该数据集中的动物接受了连续静脉输注阿米卡星,给药速率范围为8倍。初步分析表明,数据与听力损失(分贝)和整个给药过程中累积的阿米卡星血浆浓度-时间曲线下面积(cAUC)之间的S形关系一致。因此,S形模型被用作一个更为全面的毒代动力学模型的基础,该模型用一个方程描述了所有数据。用该模型进行测试表明,产生半数最大听力损失所需的cAUC(cAUC-1/2)与给药速率(P<0.01)、听力频率(P<0.00001)和给药后间隔时间(P<0.00001)有关。最大听力损失(S形上下渐近线之间的差值)小于总损失,且与频率显著相关(P<0.00001)。未检测到对S形斜率的影响。对综合毒代动力学模型检测到的显著效应进行了进一步建模,以确定它们是否可以用简单关系或生物学相关的子模型来描述。对最大听力损失(假定代表主要外毛细胞功能丧失)的建模表明,该参数在2至12kHz时约为61分贝恒定,在频率>12kHz时随对数频率线性下降。对cAUC-1/2与频率的建模表明,与对数频率存在强烈的负线性关系。对cAUC-1/2与给药后间隔时间的建模表明,停药后至少56天,迟发性耳毒性以逐渐减慢的速率持续存在。对cAUC-1/2与给药速率的建模表明,随着给药速率降低,药物需求量增加。然而,与平均稳态血浆浓度的8倍差异相比,cAUC-1/2在给药速率范围内变化不超过20%,这表明血浆浓度不是耳毒性的主要决定因素。开发了一个毒代动力学模型,该模型非常成功地解释了给药速率对cAUC-1/2的影响。(摘要截短至400字)
