Kelley Marian, DeSilva Binodh
Centocor R&D Inc, Radnor, PA, USA.
AAPS J. 2007 May 18;9(2):E156-63. doi: 10.1208/aapsj0902017.
The Third American Association of Pharmaceutical Scientists/US Food and Drug Administration (FDA) Bioanalytical Workshop, which was held May 1 and 2, 2006, in Arlington, VA, addressed bioanalytical assays that are being used for the quantification of therapeutic candidates in support of pharmacokinetic evaluations. One of the main goals of this workshop was to discuss best practices used in bioanalysis regardless of the size of the therapeutic candidates. Since the last bioanalytical workshop, technological advancements in the field and in the statistical understanding of the validation issues have generated a variety of interpretations to clarify and understand the practicality of using the current FDA guidance for assaying macromolecular therapeutics. This article addresses some of the key elements that are essential to the validation of macromolecular therapeutics using ligand binding assays. Because of the nature of ligand binding assays, attempts have been made within the scientific community to use statistical approaches to interpret the acceptance criteria that are aligned with the prestudy validation and in-study validation (sample analysis) processes. We discuss, among other topics, using the total error criterion or confidence interval approaches for acceptance of assays and using anchor calibrators to fit the nonlinear regression models.
第三届美国药物科学家协会/美国食品药品监督管理局(FDA)生物分析研讨会于2006年5月1日至2日在弗吉尼亚州阿灵顿举行,会议讨论了用于定量治疗候选物以支持药代动力学评估的生物分析方法。本次研讨会的主要目标之一是讨论生物分析中使用的最佳实践,而不考虑治疗候选物的大小。自上次生物分析研讨会以来,该领域的技术进步以及对验证问题的统计学理解产生了各种解释,以阐明和理解使用当前FDA指南检测大分子治疗药物的实用性。本文讨论了使用配体结合测定法验证大分子治疗药物的一些关键要素。由于配体结合测定法的性质,科学界已尝试使用统计方法来解释与研究前验证和研究中验证(样品分析)过程一致的验收标准。我们除了讨论其他主题外,还讨论了使用总误差标准或置信区间方法来验收测定法以及使用锚定校准物来拟合非线性回归模型。