Tunable Probes with Direct Fluorescence Signals for the Constitutive and Immunoproteasome

Christian Dubiella; Haissi Cui; Michael Groll

doi:10.1002/anie.201605753

Tunable Probes with Direct Fluorescence Signals for the Constitutive and Immunoproteasome

Christian Dubiella, Haissi Cui, Michael Groll

Chair of Biochemistry

Technical University of Munich

Research output: Contribution to journal › Article › peer-review

9 Scopus citations

Abstract

Electrophiles are commonly used for the inhibition of proteases. Notably, inhibitors of the proteasome, a central determinant of cellular survival and a target of several FDA-approved drugs, are mainly characterized by the reactivity of their electrophilic head groups. We aimed to tune the inhibitory strength of peptidic sulfonate esters by varying the leaving groups. Indeed, proteasome inhibition correlated well with the pK_aof the leaving group. The use of fluorophores as leaving groups enabled us to design probes that release a stoichiometric fluorescence signal upon reaction, thereby directly linking proteasome inactivation to the readout. This principle could be applicable to other sulfonyl fluoride based inhibitors and allows the design of sensitive probes for enzymatic studies.

Original language	English
Pages (from-to)	13330-13334
Number of pages	5
Journal	Angewandte Chemie International Edition in English
Volume	55
Issue number	42
DOIs	https://doi.org/10.1002/anie.201605753
State	Published - 10 Oct 2016

Keywords

fluorescent probes
inhibitors
probe design
proteasome
structure–activity relationships

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abstract = "Electrophiles are commonly used for the inhibition of proteases. Notably, inhibitors of the proteasome, a central determinant of cellular survival and a target of several FDA-approved drugs, are mainly characterized by the reactivity of their electrophilic head groups. We aimed to tune the inhibitory strength of peptidic sulfonate esters by varying the leaving groups. Indeed, proteasome inhibition correlated well with the pKaof the leaving group. The use of fluorophores as leaving groups enabled us to design probes that release a stoichiometric fluorescence signal upon reaction, thereby directly linking proteasome inactivation to the readout. This principle could be applicable to other sulfonyl fluoride based inhibitors and allows the design of sensitive probes for enzymatic studies.",

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AU - Cui, Haissi

AU - Groll, Michael

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AB - Electrophiles are commonly used for the inhibition of proteases. Notably, inhibitors of the proteasome, a central determinant of cellular survival and a target of several FDA-approved drugs, are mainly characterized by the reactivity of their electrophilic head groups. We aimed to tune the inhibitory strength of peptidic sulfonate esters by varying the leaving groups. Indeed, proteasome inhibition correlated well with the pKaof the leaving group. The use of fluorophores as leaving groups enabled us to design probes that release a stoichiometric fluorescence signal upon reaction, thereby directly linking proteasome inactivation to the readout. This principle could be applicable to other sulfonyl fluoride based inhibitors and allows the design of sensitive probes for enzymatic studies.

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KW - probe design

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KW - structure–activity relationships

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Tunable Probes with Direct Fluorescence Signals for the Constitutive and Immunoproteasome

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Keywords

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