使用反应面统计设计来检测生物反应调节剂如IL-2的效果。

Biotechnology therapeutics Pub Date : 1994-01-01
G L DeNardo, K R Lamborn, S J DeNardo, L A Kroger
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引用次数: 0

摘要

近年来,许多生物反应调节剂被发现或生产出来,但其作用尚不完全清楚。这些药物的作用是复杂的,因为它们不仅依赖于给药剂量,甚至依赖于给药和观察效果之间的时间间隔,而且还因为可以调用的级联相互作用。传统的实验设计是测试特定的组合,寻找统计意义,并且涉及进行一系列研究,每次改变一个参数,可能需要大量的动物或患者来回答可能的效果问题,并且由于没有选择正确的参数水平组合,因此很有可能完全错过效果。响应面设计旨在同时进行多参数评估,因此不太可能错过效果。然而,如果采用固定样本设计,所需的受试者数量仍然可能相当大。基于响应面模型的序列设计已经在其他领域得到了应用,但现在才开始在生物学和医学领域得到应用。我们已经探索了使用这些设计来评估白细胞介素-2 (IL-2)在裸鼠中增加随后给予抗体的肿瘤摄取的潜在有用性。我们发现这些方法使我们能够有效地确定IL-2剂量的最佳组合以及IL-2与抗体给药之间的时间间隔。IL-2增强了肿瘤对抗体的摄取,这在数量上是可观的,足以刺激患者的研究,我们将使用类似的顺序方法进行试验设计。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Use of response surface statistical designs to detect effects of biologic response modifiers such as IL-2.

Recently many biologic response modifiers have been discovered or produced, but their effects are incompletely understood. The effects of these agents are complicated by their dependence not merely upon the administered dose, nor even the interval of time between administration and observation of effect, but also because of the cascade of interactions that can be invoked. Conventional experimental designs that test a specific combination looking for statistical significance, and that involve doing a series of studies varying one parameter at a time, are likely to require large numbers of animals or patients to answer the question of possible effect, and have a high likelihood of missing the effect altogether because of not selecting the correct combination of parameter levels. Response surface designs are intended for simultaneous multiparameter evaluation and so are less likely to miss an effect. However, if fixed sample designs are employed, the number of subjects required may still be quite large. Sequential designs based on response surface models have been used in other fields but are only now being applied in the fields of biology and medicine. We have explored the use of these designs to evaluate the potential usefulness of interleukin-2 (IL-2) to increase tumor uptake of subsequently administered antibody in nude mice. We found that these methods enabled us to efficiently determine optimal combinations of dose of IL-2 and interval of time between IL-2 and antibody administration for enhancement. Enhancement of tumor uptake of the antibody by IL-2 was substantial in amount and sufficient to stimulate studies in patients where we will use similar sequential methodology for trial design.

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