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Publication : Assignment of endogenous substrates to enzymes by global metabolite profiling.

First Author  Saghatelian A Year  2004
Journal  Biochemistry Volume  43
Issue  45 Pages  14332-9
PubMed ID  15533037 Mgi Jnum  J:94013
Mgi Id  MGI:3510518 Doi  10.1021/bi0480335
Citation  Saghatelian A, et al. (2004) Assignment of endogenous substrates to enzymes by global metabolite profiling. Biochemistry 43(45):14332-9
abstractText  Enzymes regulate biological processes through the conversion of specific substrates to products. Therefore, of fundamental interest for every enzyme is the elucidation of its natural substrates. Here, we describe a general strategy for identifying endogenous substrates of enzymes by untargeted liquid chromatography-mass spectrometry (LC-MS) analysis of tissue metabolomes from wild-type and enzyme-inactivated organisms. We use this method to discover several brain lipids regulated by the mammalian enzyme fatty acid amide hydrolase (FAAH) in vivo, including known signaling molecules (e.g., the endogenous cannabinoid anandamide) and a novel family of nervous system-enriched natural products, the taurine-conjugated fatty acids. Remarkably, the relative hydrolytic activity that FAAH exhibited for lipid metabolites in vitro was not predictive of the identity of specific FAAH substrates in vivo. Thus, global metabolite profiling establishes unanticipated connections between the proteome and metabolome that enable assignment of an enzyme's unique biochemical functions in vivo.
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