Discovery of bivalent small molecule degraders of cyclin-dependent kinase 7 (CDK7)

Wenzhi Ji; Guangyan Du; Jie Jiang; Wenchao Lu; Caitlin E. Mills; Linjie Yuan; Fen Jiang; Zhixiang He; Gary A. Bradshaw; Mirra Chung; Zixuan Jiang; Woong Sub Byun; Stephen M. Hinshaw; Tinghu Zhang; Nathanael S. Gray

doi:10.1016/j.ejmech.2024.116613

Discovery of bivalent small molecule degraders of cyclin-dependent kinase 7 (CDK7)

Wenzhi Ji
, Guangyan Du
, Jie Jiang
, Wenchao Lu
, Caitlin E. Mills
, Linjie Yuan
, Fen Jiang
, Zhixiang He
, Gary A. Bradshaw
, Mirra Chung
, Zixuan Jiang
, Woong Sub Byun
, Stephen M. Hinshaw
, Tinghu Zhang
, Nathanael S. Gray

Department of Pharmacy

Research output: Contribution to journal › Article › peer-review

3 Scopus citations

Abstract

Cyclin-dependent kinase 7, along with cyclin H and MAT1, forms the CDK-activating complex (CAK), which directs cell cycle progression via T-loop phosphorylation of cell cycle CDKs. Pharmacological inhibition of CDK7 leads to selective anti-cancer effects in cellular and in vivo models, motivating several ongoing clinical investigations of this target. Current CDK7 inhibitors are either reversible or covalent inhibitors of its catalytic activity. We hypothesized that small molecule targeted protein degradation (TPD) might result in differentiated pharmacology due to the loss of scaffolding functions. Here, we report the design and characterization of a potent CDK7 degrader that is comprised of an ATP-competitive CDK7 binder linked to a CRL2^VHL recruiter. JWZ-5-13 effectively degrades CDK7 in multiple cancer cells and leads to a potent inhibition of cell proliferation. Additionally, compound JWZ-5-13 displayed bioavailability in a pharmacokinetic study conducted in mice. Therefore, JWZ-5-13 is a useful chemical probe to investigate the pharmacological consequences of CDK7 degradation.

Original language	English
Article number	116613
Journal	European Journal of Medicinal Chemistry
Volume	276
DOIs	https://doi.org/10.1016/j.ejmech.2024.116613
State	Published - 5 Oct 2024

Keywords

CDK7
PROTAC
Protein degrader
Selective

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.ejmech.2024.116613

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title = "Discovery of bivalent small molecule degraders of cyclin-dependent kinase 7 (CDK7)",

abstract = "Cyclin-dependent kinase 7, along with cyclin H and MAT1, forms the CDK-activating complex (CAK), which directs cell cycle progression via T-loop phosphorylation of cell cycle CDKs. Pharmacological inhibition of CDK7 leads to selective anti-cancer effects in cellular and in vivo models, motivating several ongoing clinical investigations of this target. Current CDK7 inhibitors are either reversible or covalent inhibitors of its catalytic activity. We hypothesized that small molecule targeted protein degradation (TPD) might result in differentiated pharmacology due to the loss of scaffolding functions. Here, we report the design and characterization of a potent CDK7 degrader that is comprised of an ATP-competitive CDK7 binder linked to a CRL2VHL recruiter. JWZ-5-13 effectively degrades CDK7 in multiple cancer cells and leads to a potent inhibition of cell proliferation. Additionally, compound JWZ-5-13 displayed bioavailability in a pharmacokinetic study conducted in mice. Therefore, JWZ-5-13 is a useful chemical probe to investigate the pharmacological consequences of CDK7 degradation.",

keywords = "CDK7, PROTAC, Protein degrader, Selective",

author = "Wenzhi Ji and Guangyan Du and Jie Jiang and Wenchao Lu and Mills, \{Caitlin E.\} and Linjie Yuan and Fen Jiang and Zhixiang He and Bradshaw, \{Gary A.\} and Mirra Chung and Zixuan Jiang and Byun, \{Woong Sub\} and Hinshaw, \{Stephen M.\} and Tinghu Zhang and Gray, \{Nathanael S.\}",

note = "Publisher Copyright: {\textcopyright} 2024 Elsevier Masson SAS",

year = "2024",

month = oct,

day = "5",

doi = "10.1016/j.ejmech.2024.116613",

language = "English",

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journal = "European Journal of Medicinal Chemistry",

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TY - JOUR

T1 - Discovery of bivalent small molecule degraders of cyclin-dependent kinase 7 (CDK7)

AU - Ji, Wenzhi

AU - Du, Guangyan

AU - Jiang, Jie

AU - Lu, Wenchao

AU - Mills, Caitlin E.

AU - Yuan, Linjie

AU - Jiang, Fen

AU - He, Zhixiang

AU - Bradshaw, Gary A.

AU - Chung, Mirra

AU - Jiang, Zixuan

AU - Byun, Woong Sub

AU - Hinshaw, Stephen M.

AU - Zhang, Tinghu

AU - Gray, Nathanael S.

PY - 2024/10/5

Y1 - 2024/10/5

N2 - Cyclin-dependent kinase 7, along with cyclin H and MAT1, forms the CDK-activating complex (CAK), which directs cell cycle progression via T-loop phosphorylation of cell cycle CDKs. Pharmacological inhibition of CDK7 leads to selective anti-cancer effects in cellular and in vivo models, motivating several ongoing clinical investigations of this target. Current CDK7 inhibitors are either reversible or covalent inhibitors of its catalytic activity. We hypothesized that small molecule targeted protein degradation (TPD) might result in differentiated pharmacology due to the loss of scaffolding functions. Here, we report the design and characterization of a potent CDK7 degrader that is comprised of an ATP-competitive CDK7 binder linked to a CRL2VHL recruiter. JWZ-5-13 effectively degrades CDK7 in multiple cancer cells and leads to a potent inhibition of cell proliferation. Additionally, compound JWZ-5-13 displayed bioavailability in a pharmacokinetic study conducted in mice. Therefore, JWZ-5-13 is a useful chemical probe to investigate the pharmacological consequences of CDK7 degradation.

AB - Cyclin-dependent kinase 7, along with cyclin H and MAT1, forms the CDK-activating complex (CAK), which directs cell cycle progression via T-loop phosphorylation of cell cycle CDKs. Pharmacological inhibition of CDK7 leads to selective anti-cancer effects in cellular and in vivo models, motivating several ongoing clinical investigations of this target. Current CDK7 inhibitors are either reversible or covalent inhibitors of its catalytic activity. We hypothesized that small molecule targeted protein degradation (TPD) might result in differentiated pharmacology due to the loss of scaffolding functions. Here, we report the design and characterization of a potent CDK7 degrader that is comprised of an ATP-competitive CDK7 binder linked to a CRL2VHL recruiter. JWZ-5-13 effectively degrades CDK7 in multiple cancer cells and leads to a potent inhibition of cell proliferation. Additionally, compound JWZ-5-13 displayed bioavailability in a pharmacokinetic study conducted in mice. Therefore, JWZ-5-13 is a useful chemical probe to investigate the pharmacological consequences of CDK7 degradation.

KW - CDK7

KW - PROTAC

KW - Protein degrader

KW - Selective

UR - https://www.scopus.com/pages/publications/85198273912

U2 - 10.1016/j.ejmech.2024.116613

DO - 10.1016/j.ejmech.2024.116613

M3 - Article

C2 - 39004018

AN - SCOPUS:85198273912

SN - 0223-5234

VL - 276

JO - European Journal of Medicinal Chemistry

JF - European Journal of Medicinal Chemistry

M1 - 116613

ER -

Discovery of bivalent small molecule degraders of cyclin-dependent kinase 7 (CDK7)

Abstract

Keywords

UN SDGs

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