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五种治疗性蛋白质清除率和分布容积数据的种间缩放

Interspecies scaling of clearance and volume of distribution data for five therapeutic proteins.

作者信息

Mordenti J, Chen S A, Moore J A, Ferraiolo B L, Green J D

机构信息

Department of Pharmacokinetics, Genentech, Inc., South San Francisco, California 94080.

出版信息

Pharm Res. 1991 Nov;8(11):1351-9. doi: 10.1023/a:1015836720294.

Abstract

The clearance and volume of distribution of five human proteins (recombinant CD4, CD4 immunoglobulin G, growth hormone, tissue-plasminogen activator, and relaxin) in humans and laboratory animals were analyzed as a function of body weight using allometric scaling techniques. These proteins cover a 16-fold range of molecular weight (6 to 98 kD), are produced by recombinant or synthetic methods, and may be cleared by different mechanisms. The analyses revealed that the clearance and volume data for each protein were satisfactorily described by an allometric equation (Y = a Wb). The allometric exponent (b) for clearance (ml/min) ranged from 0.65 to 0.84, the allometric exponent for the initial volume of distribution (ml) ranged from 0.83 to 1.05, and the allometric exponent for the volume of distribution at steady state (ml) ranged from 0.84 to 1.02. Exponent values from 0.6 to 0.8 for clearance and 0.8 to 1.0 for volumes are frequently cited for small molecules and are expected based on empirical interspecies relationships. When the preclinical data were analyzed separately, the preclinical allometric relationships were usually predictive of the human results. These findings indicate that the clearance and volume of distribution of select biomacromolecules follow well-defined, size-related physiologic relationships, and preclinical pharmacokinetic studies provide reasonable estimates of human disposition. Employing this methodology during the early phases of drug development may provide a more rational basis for dose selection in the clinical environment.

摘要

采用异速生长比例技术,分析了五种人类蛋白质(重组CD4、CD4免疫球蛋白G、生长激素、组织纤溶酶原激活剂和松弛素)在人类和实验动物体内的清除率和分布容积与体重的关系。这些蛋白质分子量范围为16倍(6至98 kD),通过重组或合成方法生产,且可能通过不同机制清除。分析表明,每种蛋白质的清除率和容积数据都能通过异速生长方程(Y = aWb)得到满意描述。清除率(ml/分钟)的异速生长指数(b)范围为0.65至0.84,初始分布容积(ml)的异速生长指数范围为0.83至1.05,稳态分布容积(ml)的异速生长指数范围为0.84至1.02。小分子的清除率指数值通常在0.6至0.8之间,容积指数值在0.8至1.0之间,这是基于经验性种间关系得出的预期值。当单独分析临床前数据时,临床前的异速生长关系通常能预测人体结果。这些发现表明,特定生物大分子的清除率和分布容积遵循明确的、与大小相关的生理关系,临床前药代动力学研究能为人体处置提供合理估计。在药物开发早期阶段采用这种方法,可为临床环境中的剂量选择提供更合理的依据。

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