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Dual intra- and extracellular release of monomethyl auristatin E from a neutrophil elastase-sensitive antibody-drug conjugate

连接器 化学 结合 内化 抗体-药物偶联物 细胞外 体内 单克隆抗体 药物输送 体外 作用机理 生物化学 药理学 抗体 细胞 免疫学 生物 数学分析 生物技术 操作系统 数学 计算机科学 有机化学
作者
Imène Ait Mohamed Amar,Steve Huvelle,Emmanuel Douez,Stéphanie Letast,Sylvain Henrion,Marie‐Claude Viaud‐Massuard,Nicolas Aubrey,Émilie Allard-Vannier,Nicolas Joubert,Caroline Denevault‐Sabourin
出处
期刊:European journal of medicinal chemistry [Elsevier BV]
卷期号:229: 114063-114063 被引量:15
标识
DOI:10.1016/j.ejmech.2021.114063
摘要

Antibody-drug conjugates (ADCs) are targeted therapies, mainly used in oncology, consisting in a three-component molecular architecture combining a highly potent drug conjugated via a linker onto a monoclonal antibody (mAb), designed for the selective delivery of the drug to the tumor site. The linker is a key component, defining the ADC stability and mechanism of action, and particularly the drug release strategy. In this study, we have developed and synthesized a cleavable linker, which possesses an Asn-Pro-Val (NPV) sequence sensitive to the human neutrophil elastase (HNE), overexpressed in the tumor microenvironment. This linker permitted the site-specific conjugation of the cell-permeable drug, monomethyl auristatin E (MMAE), onto trastuzumab, using a disulfide re-bridging technology. The resulting ADC was then evaluated in vitro. This conjugate demonstrated retained antigen (Ag) binding affinity and exhibited high subnanomolar potency against Ag-positive tumor cells after internalization, suggesting an intracellular mechanism of linker cleavage. While no internalization and cytotoxic activity of this ADC was observed on Ag-negative cells in classical conditions, the supplementation of exogenous HNE permitted to restore a nanomolar activity on these cells, suggesting an extracellular mechanism of drug release in these conditions. This in vitro proof of concept tends to prove that the NPV sequence could allow a dual intra- and extracellular mechanism of drug release. This work represents a first step in the design of original ADCs with a new dual intra- and extracellular drug delivery system and opens the way to further experimentations to evaluate their full potential in vivo.
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