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Author Report for: Dominguez E

Title: Integrated phenotypic and activity-based profiling links Ces3 to obesity and diabetes
Dominguez E, Galmozzi A, Chang JW, Hsu KL, Pawlak J, Li W, Godio C, Thomas J, Partida D and Saez E <6 more author(s)> Dominguez E, Galmozzi A, Chang JW, Hsu KL, Pawlak J, Li W, Godio C, Thomas J, Partida D, Niessen S, O'Brien PE, Russell AP, Watt MJ, Nomura DK, Cravatt BF, Saez E (- 6)
Ref: Nat Chemical Biology, 10:113, 2014 : PubMed
Abstract


ESTHER: Dominguez_2014_Nat.Chem.Biol_10_113
PubMedSearch: Dominguez 2014 Nat.Chem.Biol 10 113
PubMedID: 24362705
Gene_locus related to this paper: human-CES3, mouse-Ces1d
Inhibitor(s) related to this paper: WWL229, WWL113

Abstract

Phenotypic screening is making a comeback in drug discovery as the maturation of chemical proteomics methods has facilitated target identification for bioactive small molecules. A limitation of these approaches is that time-consuming genetic methods or other means are often required to determine the biologically relevant target (or targets) from among multiple protein-compound interactions that are typically detected. Here, we have combined phenotypic screening of a directed small-molecule library with competitive activity-based protein profiling to map and functionally characterize the targets of screening hits. Using this approach, we identify carboxylesterase 3 (Ces3, also known as Ces1d) as a primary molecular target of bioactive compounds that promote lipid storage in adipocytes. We further show that Ces3 activity is markedly elevated during adipocyte differentiation. Treatment of two mouse models of obesity-diabetes with a Ces3 inhibitor ameliorates multiple features of metabolic syndrome, illustrating the power of the described strategy to accelerate the identification and pharmacologic validation of new therapeutic targets.



        

Title: Application of activity-based protein profiling to study enzyme function in adipocytes
Galmozzi A, Dominguez E, Cravatt BF, Saez E
Ref: Methods Enzymol, 538:151, 2014 : PubMed
Abstract


ESTHER: Galmozzi_2014_Methods.Enzymol_538_151
PubMedSearch: Galmozzi 2014 Methods.Enzymol 538 151
PubMedID: 24529438

Abstract

Activity-based protein profiling (ABPP) is a chemical proteomics approach that utilizes small-molecule probes to determine the functional state of enzymes directly in native systems. ABPP probes selectively label active enzymes, but not their inactive forms, facilitating the characterization of changes in enzyme activity that occur without alterations in protein levels. ABPP can be a tool superior to conventional gene expression and proteomic profiling methods to discover new enzymes active in adipocytes and to detect differences in the activity of characterized enzymes that may be associated with disorders of adipose tissue function. ABPP probes have been developed that react selectively with most members of specific enzyme classes. Here, using as an example the serine hydrolase family that includes many enzymes with critical roles in adipocyte physiology, we describe methods to apply ABPP analysis to the study of adipocyte enzymatic pathways.