Chemical Ligand Space of Cereblon | Zendy

Iuliia Boichenko | Zendy; Kerstin Bär | Zendy; Silvia Deiss | Zendy; Christopher Heim | Zendy; Reinhard Albrecht | Zendy; Andrei N. Lupas | Zendy; Birte Hernandez Alvarez | Zendy; M.D. Hartmann | Zendy

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Chemical Ligand Space of Cereblon

Author(s) -

Iuliia Boichenko,

Kerstin Bär,

Silvia Deiss,

Christopher Heim,

Reinhard Albrecht,

Andrei N. Lupas,

Birte Hernandez Alvarez,

M.D. Hartmann

Publication year - 2018

Publication title -

acs omega

Language(s) - Uncategorized

Resource type - Journals

ISSN - 2470-1343

DOI - 10.1021/acsomega.8b00959

Subject(s) - cereblon , ubiquitin ligase , zebrafish , ubiquitin protein ligases , chemistry , ubiquitin , ligand (biochemistry) , chemical biology , computational biology , biology , biochemistry , receptor , gene

The protein cereblon serves as a substrate receptor of a ubiquitin ligase complex that can be tuned toward different target proteins by cereblon-binding agents. This approach to targeted protein degradation is exploited in different clinical settings and has sparked the development of a growing number of thalidomide derivatives. Here, we probe the chemical space of cereblon binding beyond such derivatives and work out a simple set of chemical requirements, delineating the metaclass of cereblon effectors. We report co-crystal structures for a diverse set of compounds, including commonly used pharmaceuticals, but also find that already minimalistic cereblon-binding moieties might exert teratogenic effects in zebrafish. Our results may guide the design of a post-thalidomide generation of therapeutic cereblon effectors and provide a framework for the circumvention of unintended cereblon binding by negative design for future pharmaceuticals.

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