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蛋白质性质和蛋白质修饰对抗癌抗体、抗体衍生物和非免疫球蛋白支架的生物分布和肿瘤摄取的影响。

Influence of protein properties and protein modification on biodistribution and tumor uptake of anticancer antibodies, antibody derivatives, and non-Ig scaffolds.

机构信息

Department of Clinical Pharmacy and Pharmacology, University Medical Center Groningen, University of Groningen, Groningen, The Netherlands.

Department of Nuclear Medicine and Molecular Imaging, University Medical Center Groningen, University of Groningen, Groningen, The Netherlands.

出版信息

Med Res Rev. 2018 Sep;38(6):1837-1873. doi: 10.1002/med.21498. Epub 2018 Apr 10.

Abstract

Newly developed protein drugs that target tumor-associated antigens are often modified in order to increase their therapeutic effect, tumor exposure, and safety profile. During the development of protein drugs, molecular imaging is increasingly used to provide additional information on their in vivo behavior. As a result, there are increasing numbers of studies that demonstrate the effect of protein modification on whole body distribution and tumor uptake of protein drugs. However, much still remains unclear about how to interpret obtained biodistribution data correctly. Consequently, there is a need for more insight in the correct way of interpreting preclinical and clinical imaging data. Summarizing the knowledge gained to date may facilitate this interpretation. This review therefore provides an overview of specific protein properties and modifications that can affect biodistribution and tumor uptake of anticancer antibodies, antibody fragments, and nonimmunoglobulin scaffolds. Protein properties that are discussed in this review are molecular size, target interaction, FcRn binding, and charge. Protein modifications that are discussed are radiolabeling, fluorescent labeling drug conjugation, glycosylation, humanization, albumin binding, and polyethylene glycolation.

摘要

新开发的靶向肿瘤相关抗原的蛋白质药物通常经过修饰以提高其治疗效果、肿瘤暴露度和安全性。在蛋白质药物开发过程中,分子成像越来越多地用于提供其体内行为的附加信息。因此,越来越多的研究表明蛋白质修饰对蛋白质药物的全身分布和肿瘤摄取的影响。然而,对于如何正确解释获得的生物分布数据,仍有许多不清楚的地方。因此,需要更多地了解正确解释临床前和临床成像数据的方法。总结迄今为止获得的知识可能有助于进行这种解释。因此,本综述概述了可能影响抗癌抗体、抗体片段和非免疫球蛋白支架的生物分布和肿瘤摄取的特定蛋白质特性和修饰。本综述中讨论的蛋白质特性包括分子大小、靶标相互作用、FcRn 结合和电荷。讨论的蛋白质修饰包括放射性标记、荧光标记、药物偶联、糖基化、人源化、白蛋白结合和聚乙二醇化。

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