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Forecasting cephalosporin and monobactam antibiotic half-lives in humans from data collected in laboratory animals.

机译:根据实验室动物收集的数据预测人头孢菌素和单bactam抗生素的半衰期。

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摘要

The postdistribution half-lives of 10 cephalosporin and 2 monobactam antibiotics in humans were predicted from data obtained in other mammals. This forecasting was accomplished with the allometric equation t1/2 = aWb, where a is the y intercept and b is the slope obtained from the log-log plot of antibiotic half-life (t1/2) versus body weight (W). Dimensionless similarity criteria were used to produce a biological clock for ceftizoxime elimination. The creation of the biological clock, which measured physiologic time (heartbeats) rather than chronologic time (minutes), demonstrated that ceftizoxime half-life was identical in five mammals. This methodology will contribute to infectious disease research through a greater understanding of pharmacokinetic scaling in mammals.
机译:根据在其他哺乳动物中获得的数据,可以预测10种头孢菌素和2种单bactam抗生素在人体内的分布后半衰期。该预测是通过异速方程t1 / 2 = aWb完成的,其中a是y截距,b是从抗生素半衰期(t1 / 2)对体重(W)的对数对数图获得的斜率。使用无量纲相似性标准来产生用于消除头孢唑肟的生物钟。生物钟的创建,可以测量生理时间(心跳),而不是计时时间(分钟),这表明头孢唑肟的半衰期在五只哺乳动物中是相同的。这种方法学将通过对哺乳动物药代动力学缩放的更深入了解而有助于传染病研究。

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