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Antibody Conjugation of a Chimeric BET Degrader Enables in vivo Activity
Authors:Dr Thomas H Pillow  Pragya Adhikari  Dr Robert A Blake  Dr Jinhua Chen  Geoffrey Del Rosario  Gauri Deshmukh  Dr Isabel Figueroa  Dr Karen E Gascoigne  Dr Amrita V Kamath  Susan Kaufman  Tracy Kleinheinz  Dr Katherine R Kozak  Brandon Latifi  Douglas D Leipold  Dr Chun Sing Li  Ruina Li  Dr Melinda M Mulvihill  Aimee O'Donohue  Dr Rebecca K Rowntree  Dr Jack D Sadowsky  Dr John Wai  Xinxin Wang  Dr Cong Wu  Zijin Xu  Hui Yao  Shang-Fan Yu  Dr Donglu Zhang  Dr Richard Zang  Dr Hongyan Zhang  Hao Zhou  Dr Xiaoyu Zhu  Dr Peter S Dragovich
Affiliation:1. Genentech Inc., 1 DNA Way, South San Francisco, CA 94080 USA;2. Wuxi Apptec, 288 Fute Zhong Road Waigaoqiao Free Trade Zone, Shanghai, 200131 China
Abstract:The ability to selectively degrade proteins with bifunctional small molecules has the potential to fundamentally alter therapy in a variety of diseases. However, the relatively large size of these chimeric molecules often results in challenging physico-chemical properties (e. g., low aqueous solubility) and poor pharmacokinetics which may complicate their in vivo applications. We recently discovered an exquisitely potent chimeric BET degrader (GNE-987) which exhibited picomolar cell potencies but also demonstrated low in vivo exposures. In an effort to improve the pharmacokinetic properties of this molecule, we discovered the first degrader-antibody conjugate by attaching GNE-987 to an anti-CLL1 antibody via a novel linker. A single IV dose of the conjugate afforded sustained in vivo exposures that resulted in antigen-specific tumor regressions. Enhancement of a chimeric protein degrader with poor in vivo properties through antibody conjugation thereby expands the utility of directed protein degradation as both a biological tool and a therapeutic possibility.
Keywords:antibodies  antibody-drug conjugate  BRD4  chimeric protein degrader  drug delivery
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