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. 2020 Jan 7;15(1):17-25.
doi: 10.1002/cmdc.201900497. Epub 2019 Nov 14.

Antibody Conjugation of a Chimeric BET Degrader Enables in vivo Activity

Thomas H Pillow  1 Pragya Adhikari  1 Robert A Blake  1 Jinhua Chen  2 Geoffrey Del Rosario  1 Gauri Deshmukh  1 Isabel Figueroa  1 Karen E Gascoigne  1 Amrita V Kamath  1 Susan Kaufman  1 Tracy Kleinheinz  1 Katherine R Kozak  1 Brandon Latifi  1 Douglas D Leipold  1 Chun Sing Li  2 Ruina Li  1 Melinda M Mulvihill  1 Aimee O'Donohue  1 Rebecca K Rowntree  1 Jack D Sadowsky  1 John Wai  2 Xinxin Wang  2 Cong Wu  1 Zijin Xu  2 Hui Yao  2 Shang-Fan Yu  1 Donglu Zhang  1 Richard Zang  1 Hongyan Zhang  2 Hao Zhou  2 Xiaoyu Zhu  2 Peter S Dragovich  1
Affiliations

Antibody Conjugation of a Chimeric BET Degrader Enables in vivo Activity

Thomas H Pillow et al. ChemMedChem. .

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: BRD4; antibodies; antibody-drug conjugate; chimeric protein degrader; drug delivery.

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