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当前的ADC连接子化学

Current ADC Linker Chemistry.

作者信息

Jain Nareshkumar, Smith Sean W, Ghone Sanjeevani, Tomczuk Bruce

机构信息

The Chemistry Research Solution, LLC, 360 George Patterson Blvd., Suite 101E, Bristol, Pennsylvania, 19007, USA.

出版信息

Pharm Res. 2015 Nov;32(11):3526-40. doi: 10.1007/s11095-015-1657-7. Epub 2015 Mar 11.

Abstract

The list of ADCs in the clinic continues to grow, bolstered by the success of first two marketed ADCs: ADCETRIS® and Kadcyla®. Currently, there are 40 ADCs in various phases of clinical development. However, only 34 of these have published their structures. Of the 34 disclosed structures, 24 of them use a linkage to the thiol of cysteines on the monoclonal antibody. The remaining 10 candidates utilize chemistry to surface lysines of the antibody. Due to the inherent heterogeneity of conjugation to the multiple lysines or cysteines found in mAbs, significant research efforts are now being directed toward the production of discrete, homogeneous ADC products, via site-specific conjugation. These site-specific conjugations may involve genetic engineering of the mAb to introduce discrete, available cysteines or non-natural amino acids with an orthogonally-reactive functional group handle such as an aldehyde, ketone, azido, or alkynyl tag. These site-specific approaches not only increase the homogeneity of ADCs but also enable novel bio-orthogonal chemistries that utilize reactive moieties other than thiol or amine. This broadens the diversity of linkers that can be utilized which will lead to better linker design in future generations of ADCs.

摘要

在首批两款上市的ADC药物(ADCETRIS®和Kadcyla®)取得成功的推动下,临床中的ADC药物名单持续增加。目前,有40种ADC药物处于临床开发的不同阶段。然而,其中只有34种公布了其结构。在这34种已披露的结构中,有24种使用与单克隆抗体上半胱氨酸的巯基相连的连接子。其余10种候选药物利用化学方法连接到抗体的表面赖氨酸上。由于与单克隆抗体中发现的多个赖氨酸或半胱氨酸缀合存在固有的异质性,目前大量研究工作正致力于通过位点特异性缀合来生产离散的、均一的ADC产品。这些位点特异性缀合可能涉及对单克隆抗体进行基因工程改造,以引入离散的、可用的半胱氨酸或带有醛、酮、叠氮基或炔基标签等正交反应性功能基团的非天然氨基酸。这些位点特异性方法不仅提高了ADC的均一性,还能实现利用除巯基或胺以外的反应性部分的新型生物正交化学。这拓宽了可利用的连接子的多样性,将有助于在下一代ADC药物中设计出更好的连接子。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/64d2/4596905/e04108c1dc0d/11095_2015_1657_Fig1_HTML.jpg

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