化学
生物结合
前药
酪氨酸
抗体
组合化学
生物化学
免疫学
生物
作者
Jason Tao,Heemal H. Dhanjee,Michael W. Gribble,Veronika Kottisch,Jacob Rodriguez,Joseph S. Brown,Holly Schmidt,Juhi Juneja,Fabienne Denhez,Peter S. Lee,Daša Lipovšek,Stanley R. Krystek,Yihong Zhang,Patrick Bousquet,Yong Zhang,Bradley L. Pentelute,Stephen L. Buchwald
摘要
The utility of antibody therapeutics is hampered by potential cross-reactivity with healthy tissue. Over the past decade, significant advances have been made in the design of activatable antibodies, which increase, or create altogether, the therapeutic window of a parent antibody. Of these, antibody prodrugs (pro-antibodies) are masked antibodies that have advanced the most for therapeutic use. They are designed to reveal the active, parent antibody only when encountering proteases upregulated in the microenvironment of the targeted disease tissue, thereby minimizing off-target activity. However, current pro-antibody designs are relegated to fusion proteins that append masking groups restricted to the use of only canonical amino acids, offering excellent control of the site of introduction, but with no authority over where the masking group is installed other than the
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