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定量表征抗体药物偶联物的体外旁观者效应。

Quantitative characterization of in vitro bystander effect of antibody-drug conjugates.

机构信息

Department of Pharmaceutical Sciences, School of Pharmacy and Pharmaceutical Sciences, The State University of New York at Buffalo, 455 Kapoor Hall, Buffalo, NY, 14214-8033, USA.

出版信息

J Pharmacokinet Pharmacodyn. 2016 Dec;43(6):567-582. doi: 10.1007/s10928-016-9495-8. Epub 2016 Sep 26.

Abstract

Antibody-drug conjugates (ADCs) are designed to target antigen expressing (Ag+) cells in a tumor. Once processed by the Ag+ cells, ADCs can release cytotoxic drug molecules that can diffuse out of Ag+ cells into the neighboring antigen-negative (Ag-) cells to induce their cytotoxicity. This additional efficacy of ADCs on Ag- cells in the presence of Ag+ cells is known as the 'bystander effect'. Although the importance of this phenomena is widely acknowledged for effective killing of a heterogeneous tumor, the rate and extent of the bystander killing in a heterogeneous system is not quantitatively understood yet. Thus, the objectives of this manuscript were to: (1) synthesize and characterize a tool ADC Trastuzumab-vc-MMAE that is capable of exhibiting bystander effect, (2) quantify the time course of the bystander effect for the tool ADC using in vitro co-culture systems created using mixture of various HER2-expressing cell lines, and (3) develop a pharmacodynamic (PD) model that is capable of characterizing the bystander effect of ADCs. Co-culture studies conducted using GFP labelled MCF7 cells as Ag- cells and N87, BT474, and SKBR3 as Ag+ cells revealed that the bystander effect of ADC increases with increasing fraction of Ag+ cells in a co-culture system, and with increased expression level of target on Ag+ cells. A notable lag time after ADC incubation was also observed prior to significant bystander killing of Ag- cells. Based on our results we hypothesize that there may be other determinants apart from the antigen expression level that can also influence the ability of Ag+ cells to demonstrate the bystander effect in a co-culture system. The co-culture analysis also suggested that the bystander effect of the ADC can dissipate over the period of time as the population of Ag+ cells declines. A novel PD model was developed to mathematically characterize the bystander effect of ADCs by combining two different cell distribution models to represent the population of Ag+ and Ag- cells in a co-culture system. This PD model can be integrated with the systems PK model for ADCs in the future to generate a quantitative framework that is capable of supporting the discovery and development of novel ADCs with optimal bystander killing capabilities.

摘要

抗体药物偶联物 (ADC) 旨在靶向肿瘤中表达抗原 (Ag+) 的细胞。一旦被 Ag+细胞处理,ADC 可以释放细胞毒性药物分子,这些分子可以从 Ag+细胞扩散到邻近的抗原阴性 (Ag-) 细胞中,从而诱导其细胞毒性。这种 ADC 在 Ag+细胞存在的情况下对 Ag-细胞的额外疗效被称为“旁观者效应”。尽管这种现象对于有效杀伤异质性肿瘤的重要性已得到广泛认可,但对于异质性系统中旁观者杀伤的速度和程度尚未得到定量理解。因此,本手稿的目的是:(1) 合成并表征一种能够表现出旁观者效应的工具 ADC 曲妥珠单抗-vc-MMAE,(2) 使用混合各种 HER2 表达细胞系创建的体外共培养系统定量研究工具 ADC 的旁观者效应的时间过程,(3) 开发一种能够表征 ADC 旁观者效应的药效动力学 (PD) 模型。使用 GFP 标记的 MCF7 细胞作为 Ag-细胞和 N87、BT474 和 SKBR3 作为 Ag+细胞进行的共培养研究表明,随着共培养系统中 Ag+细胞比例的增加以及 Ag+细胞上靶标的表达水平增加,ADC 的旁观者效应也随之增加。在 Ag-细胞发生明显旁观者杀伤之前,还观察到 ADC 孵育后明显的滞后时间。根据我们的结果,我们假设除了抗原表达水平之外,可能还有其他决定因素也会影响 Ag+细胞在共培养系统中表现出旁观者效应的能力。共培养分析还表明,随着 Ag+细胞数量的减少,ADC 的旁观者效应可能会在一段时间内消散。开发了一种新的 PD 模型,通过结合两种不同的细胞分布模型来描述共培养系统中 Ag+和 Ag-细胞的群体,从而对 ADC 的旁观者效应进行数学表征。该 PD 模型可以与 ADC 的系统 PK 模型结合使用,以生成一种能够支持具有最佳旁观者杀伤能力的新型 ADC 的发现和开发的定量框架。

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Quantitative characterization of in vitro bystander effect of antibody-drug conjugates.定量表征抗体药物偶联物的体外旁观者效应。
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