Title : Discovery of Modulators of Adipocyte Physiology Using Fully Functionalized Fragments - Galmozzi_2018_Methods.Mol.Biol_1787_115 |
Author(s) : Galmozzi A , Parker CG , Kok BP , Cravatt BF , Saez E |
Ref : Methods Mol Biol , 1787 :115 , 2018 |
Abstract :
Defects in adipocyte function associated with obesity drive the development of systemic insulin resistance and type 2 diabetes. Agents that correct obesity-linked adipocyte dysfunction serve as useful insulin sensitizers in humans, as is exemplified by the thiazolidinediones (TZDs). We have developed a new platform that integrates advanced chemoproteomics with phenotypic screening to identify small molecules that promote differentiation and lipid storage in adipocytes, and, in tandem, their molecular target(s). These molecules mimic the activity of TZDs in culture and thus may also serve as insulin sensitizers in vivo. Central to this platform is the use of fully functionalized fragment (FFF) probes that consist of a variable, fragment-like recognition element linked to an alkyne-diazirine group that enables the photoactivated capture of probe-bound proteins directly in living cells and subsequent copper-catalyzed azide-alkyne cycloaddition to reporter tags for enrichment and identification of these probe-bound proteins by mass spectrometry. This platform, which can be adapted to diverse screens and cell types beyond adipocytes, has the potential to uncover new biological pathways amenable to pharmacological modulation that may impact human disease. |
PubMedSearch : Galmozzi_2018_Methods.Mol.Biol_1787_115 |
PubMedID: 29736714 |
Galmozzi A, Parker CG, Kok BP, Cravatt BF, Saez E (2018)
Discovery of Modulators of Adipocyte Physiology Using Fully Functionalized Fragments
Methods Mol Biol
1787 :115
Galmozzi A, Parker CG, Kok BP, Cravatt BF, Saez E (2018)
Methods Mol Biol
1787 :115