Superfamily-wide portrait of serine hydrolase inhibition achieved by library-versus-library screening

Bachovchin, Daniel A.; Ji, Tianyang; Li, Weiwei; Simón, Gabriel; Blankman, Jacqueline L.; Adibekian, Alexander; Hoover, Heather; Niessen, Sherry; Cravatt, Benjamin F.

doi:10.1073/pnas.1011663107

Cited by 225 publications

(331 citation statements)

References 43 publications

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“…This strategy may also be useful for studying the properties of pseudokinases, for which there is no good readout of active site occupancy. The use of irreversible inhibitors for poorly studied members of large families allows rapid validation of target specificity when downstream assays are not known, as has been shown in the serine hydrolase family (46). In addition, the technology reported in this study may enable multiplex inhibitor studies, such as those requiring washing steps or the use of more than one chemical genetic inhibitor.…”

Section: Discussionmentioning

confidence: 95%

Chemical genetic strategy for targeting protein kinases based on covalent complementarity

Garske

Peters

Cortesi

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

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The conserved nature of the ATP-binding site of the >500 human kinases renders the development of specific inhibitors a challenging task. A widely used chemical genetic strategy to overcome the specificity challenge exploits a large-to-small mutation of the gatekeeper residue (a conserved hydrophobic amino acid) and the use of a bulky inhibitor to achieve specificity via shape complementarity. However, in a number of cases, introduction of a glycine or alanine gatekeeper results in diminished kinase activity and ATP affinity. A new chemical genetic approach based on covalent complementarity between an engineered gatekeeper cysteine and an electrophilic inhibitor was developed to address these challenges. This strategy was evaluated with Src, a proto-oncogenic tyrosine kinase known to lose some enzymatic activity using the shape complementarity chemical genetic strategy. We found that Src with a cysteine gatekeeper recapitulates wild type activity and can be irreversibly inhibited both in vitro and in cells. A cocrystal structure of T338C c-Src with a vinylsulfonamide-derivatized pyrazolopyrimidine inhibitor was solved to elucidate the inhibitor binding mode. A panel of electrophilic inhibitors was analyzed against 307 kinases and MOK (MAPK/MAK/MRK overlapping kinase), one of only two human kinases known to have an endogenous cysteine gatekeeper. This analysis revealed remarkably few offtargets, making these compounds the most selective chemical genetic inhibitors reported to date. Protein engineering studies demonstrated that it is possible to increase inhibitor potency through secondary-site mutations. These results suggest that chemical genetic strategies based on covalent complementarity should be widely applicable to the study of protein kinases. chemical genetics | irreversible inhibitor | SgK494

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Section: Discussionmentioning

confidence: 95%

Chemical genetic strategy for targeting protein kinases based on covalent complementarity

Garske

Peters

Cortesi

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

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“…ABHD6 is an ;30-kDa integral membrane serine hydrolase predicted to adopt an intracellular orientation (Blankman et al, 2007). Murine ABHD6 expression is abundant in brain and multiple peripheral tissues and cell types (Su et al, 2002;Bachovchin et al, 2010;Marrs et al, 2010). In the mouse brain, ABHD6 is highly expressed in cortical areas, where it preferentially localizes to postsynaptic dendrites that are often juxtaposed to presynaptic CB1 receptors (Marrs et al, 2010).…”

Section: B 2-ag Hydrolysis By Monoacylglycerol Lipasementioning

confidence: 99%

Chemical Probes of Endocannabinoid Metabolism

2013

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“…CC-ABPP did not reveal any other major off-targets for SA-57yne with the exception of a faint 70 kDa protein in soluble mouse brain at doses of 6.25− 12.5 mg kg . This enzyme likely represents the carboxylesterase ES-1, a common off-target of carbamates 22,32,50,51 that originates from contaminating blood 52 in the brain proteome samples. Considering that ES-1 signals were not noticeably depleted by SA-57yne in our competitive ABPP experiments (Figure 7b), we conclude that this inhibitor only partially inactivates ES-1 at high doses.…”

Section: Acs Chemical Neurosciencementioning

confidence: 99%

O-Hydroxyacetamide Carbamates as a Highly Potent and Selective Class of Endocannabinoid Hydrolase Inhibitors

Niphakis

Johnson

Ballard

et al. 2011

ACS Chem. Neurosci.

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The two major endocannabinoid transmitters, anandamide (AEA) and 2-arachidonoylglycerol (2-AG), are degraded by distinct enzymes in the nervous system, fatty acid amide hydrolase (FAAH) and monoacylglycerol lipase (MAGL), respectively. FAAH and MAGL inhibitors cause elevations in brain AEA and 2-AG levels, respectively, and reduce pain, anxiety, and depression in rodents without causing the full spectrum of psychotropic behavioral effects observed with direct cannabinoid receptor-1 (CB1) agonists. These findings have inspired the development of several classes of endocannabinoid hydrolase inhibitors, most of which have been optimized to show specificity for either FAAH or MAGL or, in certain cases, equipotent activity for both enzymes. Here, we investigate an unusual class of Ohydroxyacetamide carbamate inhibitors and find that individual compounds from this class can serve as selective FAAH or dual FAAH/MAGL inhibitors in vivo across a dose range (0.125−12.5 mg kg ) suitable for behavioral studies. Competitive and click chemistry activity-based protein profiling confirmed that the O-hydroxyacetamide carbamate SA-57 is remarkably selective for FAAH and MAGL in vivo, targeting only one other enzyme in brain, the additional 2-AG hydrolase ABHD6. These data designate O-hydroxyacetamide carbamates as a versatile chemotype for creating endocannabinoid hydrolase inhibitors that display excellent in vivo activity and tunable selectivity for FAAH-anandamide versus MAGL (and ABHD6)-2-AG pathways.

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Superfamily-wide portrait of serine hydrolase inhibition achieved by library-versus-library screening

Cited by 225 publications

References 43 publications

Chemical genetic strategy for targeting protein kinases based on covalent complementarity

Chemical genetic strategy for targeting protein kinases based on covalent complementarity

Chemical Probes of Endocannabinoid Metabolism

O-Hydroxyacetamide Carbamates as a Highly Potent and Selective Class of Endocannabinoid Hydrolase Inhibitors

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