Structure-Based Design of Inhibitors Selective for Human Proteasome β2c or β2i Subunits

Xin, Bo‐Tao; Huber, E.M.; Bruin, Gerjan de; Heinemeyer, Wolfgang; Maurits, Elmer; Espinal, Christofer; Du, Yimeng; Janssens, Marissa; Weyburne, Emily S.; Kisselev, Alexei F.; Florea, Bogdan I.; Driessen, Christoph; Marel, Gijsbert A. van der; Groll, M.; Overkleeft, Herman S.

doi:10.1021/acs.jmedchem.8b01884

Cited by 24 publications

(27 citation statements)

References 45 publications

(82 reference statements)

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“…The synthesis of norbornene‐ABPs 11 , 13 , and 14 are also based on click ligation of norbornene‐alkyne 15 to their corresponding azide precursors (Figure ). The synthesis of 16 has been reported and the preparation of compounds 17 and 18 are described in the Supporting Information.…”

Section: Resultsmentioning

confidence: 99%

“…In the first instance, we assessed their subunit‐selectivity and activity by competitive ABPP making use of the activity‐based proteasome profiling assay and the structures of these probes are shown in Figure B . The activity, selectivity and cell permeability of azides 1 , 2 , 3 , and 5 in such assays had already been described. The results on the behavior of norbornenes 8 – 14 in competitive ABPP, in particular their activity, selectivity, and cell permeability are summarized in Figure and Tables and .…”

Section: Resultsmentioning

confidence: 99%

“…In total, the research described herein has expanded the proteasome ABP toolset to include five new in vitro ABPs, of which four can also be applied to monitor proteasome activity profiles in living cells. Further studies are required to complete a toolset for labeling each immunoproteasome and constitutive proteasome activity individually, this to complement our three‐probe multiplexing ABPP that is currently in use by us and others.…”

Section: Discussionmentioning

confidence: 99%

“…In case the inhibitors are covalent and irreversible, they can be modified to contain reporter entities for activity‐based proteasome profiling purposes. Recently, we disclosed a set of inhibitors selective for one of each of the six catalytic subunits of human constitutive proteasomes and immunoproteasomes (Figure ),– whereas activity‐based proteasome probes have also been reported by other research groups –. With this set of subunit‐selective inhibitors 1 – 7 (Figure A), each human proteasome activity can be inhibited at will.…”

Section: Introductionmentioning

confidence: 95%

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Two‐Step Bioorthogonal Activity‐Based Protein Profiling of Individual Human Proteasome Catalytic Sites

et al. 2019

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Bioorthogonal chemistry allows the selective modification of biomolecules in complex biological samples. One application of this methodology is in two‐step activity‐based protein profiling (ABPP), a methodology that is particularly attractive where direct ABPP using fluorescent or biotinylated probes is ineffective. Herein we describe a set of norbornene‐modified, mechanism‐based proteasome inhibitors aimed to be selective for each of the six catalytic sites of human constitutive proteasomes and immunoproteasomes. The probes developed for β1i, β2i, β5c, and β5i proved to be useful two‐step ABPs that effectively label their developed proteasome subunits in both Raji cell extracts and living Raji cells through inverse‐electron‐demand Diels–Alder (iEDDA) ligation. The compound developed for β1c proved incapable of penetrating the cell membrane, but effectively labels β1c in vitro. The compound developed for β2c proved not selective, but its azide‐containing analogue LU‐002c proved effective in labeling of β2c via azide–alkyne click ligation chemistry both in vitro and in situ. In total, our results contribute to the growing list of proteasome activity tools to include five subunit‐selective activity‐based proteasome probes, four of which report on proteasome activities in living cells.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 95%

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Two‐Step Bioorthogonal Activity‐Based Protein Profiling of Individual Human Proteasome Catalytic Sites

et al. 2019

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“…As presented in Figure 1, the differences projected by several biphenyl rotational values are relatively modest, suggesting steric mimicry between these two groups, though the effective functional mimicry is very much dependent upon the actual biochemical settings [67]. In this context, the bioisosteric relationships between CF3 and i-Pr can be used for 2-amino-4,4,4-trifluorobutanoic acid 1 [68][69][70][71][72][73][74][75][76] substitution for leucine 2 in the de novo design of biologically active peptides and peptidomimetics [77][78][79][80][81][82][83]. As part of our ongoing research program focused on the application of fluorinated tailor-made AAs in pharmaceutical discovery, we needed a convenient access to large quantities of Fmoc-2amino-4,4,4-trifluorobutanoic acid 1 in both enantiomeric forms.…”

Section: Introductionmentioning

confidence: 99%

Preparative Method for Asymmetric Synthesis of (S)-2-Amino-4,4,4-trifluorobutanoic Acid

et al. 2019

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Enantiomerically pure derivatives of 2-amino-4,4,4-trifluorobutanoic acid are in great demand as bioisostere of leucine moiety in the drug design. Here, we disclose a method specifically developed for large-scale (>150 g) preparation of the target (S)-N-Fmoc-2-amino-4,4,4-trifluorobutanoic acid. The method employs a recyclable chiral auxiliary to form the corresponding Ni(II) complex with glycine Schiff base, which is alkylated with CF3–CH2–I under basic conditions. The resultant alkylated Ni(II) complex is disassembled to reclaim the chiral auxiliary and 2-amino-4,4,4-trifluorobutanoic acid, which is in situ converted to the N-Fmoc derivative. The whole procedure was reproduced several times for consecutive preparation of over 300 g of the target (S)-N-Fmoc-2-amino-4,4,4-trifluorobutanoic acid.

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Deconstructive Carboxylation of Activated Alkenes with Carbon Dioxide

Yuan,

Yang,

Zhang

et al. 2023

Angewandte Chemie

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Carboxylation with carbon dioxide (CO2) represents one notable methodology to produce carboxylic acids. In contrast to carbon–heteroatom bonds, carbon–carbon bond cleavage for carboxylation with CO2 is far more challenging due to their inherent and less favorable orbital directionality for interacting with transition metals. Here we report a photocatalytic protocol for the deconstructive carboxylation of alkenes with CO2 to generate carboxylic acids in the absence of transition metals. It is emphasized that our protocol provides carboxylic acids with obviously unchanged carbon numbers when terminal alkenes were used. To show the power of this strategy, a variety of pharmaceutically relevant applications including the modular synthesis of propionate nonsteroidal anti‐inflammatory drugs and the late‐stage carboxylation of bioactive molecule derivatives are demonstrated.

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Structure-Based Design of Inhibitors Selective for Human Proteasome β2c or β2i Subunits

Cited by 24 publications

References 45 publications

Two‐Step Bioorthogonal Activity‐Based Protein Profiling of Individual Human Proteasome Catalytic Sites

Two‐Step Bioorthogonal Activity‐Based Protein Profiling of Individual Human Proteasome Catalytic Sites

Preparative Method for Asymmetric Synthesis of (S)-2-Amino-4,4,4-trifluorobutanoic Acid

Deconstructive Carboxylation of Activated Alkenes with Carbon Dioxide

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