Rapid and direct control of target protein levels with VHL-recruiting dTAG molecules

Behnam Nabet,Fleur M. Ferguson,Bo Kyung A. Seong,Miljan Kuljanin,Alan L. Leggett,Mikaela L. Mohardt,Amanda L. Robichaud,Amy Saur Conway,Dennis L. Buckley,Joseph D. Mancias,James E. Bradner,Kimberly Stegmaier,Nathanael S. Gray

Rapid and direct control of target protein levels with VHL-recruiting dTAG molecules

2020

Behnam Nabet
Fleur M. Ferguson
Bo Kyung A. Seong
Miljan Kuljanin
Alan L. Leggett
Mikaela L. Mohardt
Amanda L. Robichaud
Amy Saur Conway
Dennis L. Buckley
Joseph D. Mancias
James E. Bradner
Kimberly Stegmaier
Nathanael S. Gray

Chemical biology strategies for directly perturbing protein homeostasis including the degradation tag (dTAG) system provide temporal advantages over genetic approaches and improved selectivity over small molecule inhibitors. We describe dTAGV-1, an exclusively selective VHL-recruiting dTAG molecule, to rapidly degrade FKBP12F36V-tagged proteins. dTAGV-1 overcomes a limitation of previously reported CRBN-recruiting dTAG molecules to degrade recalcitrant oncogenes, supports combination degrader studies and facilitates investigations of protein function in cells and mice.

Keywords:

direct control
Genetics
Small molecule
Chemical biology
Cell biology
Protein Homeostasis
Target protein
protein function
Molecule
Biology

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