Discovery of Potent Degraders of the Dengue Virus Envelope Protein

Author:

Li Zhengnian1,Liu Han‐Yuan2,He Zhixiang34,Chakravarty Antara2,Golden Ryan P.1,Jiang Zixuan1,You Inchul1,Yue Hong,Donovan Katherine A.4,Du Guangyan34,Che Jianwei3,Tse Jason1,Che Isaac1,Lu Wenchao1,Fischer Eric S.34,Zhang Tinghu1,Gray Nathanael S.1ORCID,Yang Priscilla L.2

Affiliation:

1. Department of Chemical and Systems Biology Chem‐H and Stanford Cancer Institute Stanford Medicine Stanford University 290 Jane Stanford Way Stanford CA 94305 USA

2. Department of Microbiology and Immunology Stanford University School of Medicine 279 Campus Drive Palo Alto CA 94305 USA

3. Department of Cancer Biology Dana‐Farber Cancer Institute 450 Brookline Avenue Boston 02215 USA

4. Department of Biological Chemistry and Molecular Pharmacology Harvard Medical School 240 Longwood Avenue Boston 02115 USA

Abstract

AbstractTargeted protein degradation has been widely adopted as a new approach to eliminate both established and previously recalcitrant therapeutic targets. Here, it is reported that the development of small molecule degraders of the envelope (E) protein of dengue virus. Two classes of bivalent E‐degraders are developed by linking two previously reported E‐binding small molecules, GNF‐2, and CVM‐2‐12‐2, to a glutarimide‐based recruiter of the CRL4CRBN ligase to effect proteosome‐mediated degradation of the E protein. ZXH‐2‐107 (based on GNF‐2) is an E‐degrader with ABL inhibitory activity while ZXH‐8‐004 (based on CVM‐2‐12‐2) is a selective and potent E‐degrader. These two compounds provide proof of concept that difficult‐to‐drug targets such as a viral envelope protein can be effectively eliminated using a bivalent degrader and provide starting points for the future development of a new class of direct‐acting antiviral drugs.

Funder

Mark Foundation For Cancer Research

Publisher

Wiley

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