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Publisher Correction: Non-functional ubiquitin C-terminal hydrolase L1 drives podocyte injury through impairing proteasomes in autoimmune glomerulonephritis

Julia Reichelt
Wiebke Sachs
Catherine Meyer-Schwesinger
Amendments and CorrectionsOpen Access28 Apr 2023
Nature Communications

Volume: 14, P: 1
Discovery of a NAPE-PLD inhibitor that modulates emotional behavior in mice

An inhibitor of NAPE-PLD involved in lipid biosynthesis lowers levels of the endocannabinoid anandamide and other N-acylethanolamines in cells and mouse brain and activates the hypothalamus–pituitary–adrenal axis and impaired fear extinction.

Elliot D. Mock
Mohammed Mustafa
Mario van der Stelt
Research11 May 2020
Nature Chemical Biology

Volume: 16, P: 667-675
A monoacylglycerol lipase inhibitor showing therapeutic efficacy in mice without central side effects or dependence

Chemotherapy-induced peripheral neuropathy (CIPN) represents a major reason for discontinuation of treatment. Here, the authors show that LEI-515, a peripherally restricted monoacylglycerol lipase inhibitor, suppresses CIPN without inducing central nervous system side effects or physical dependence.

Ming Jiang
Mirjam C. W. Huizenga
Mario van der Stelt
ResearchOpen Access05 Dec 2023
Nature Communications

Volume: 14, P: 1-19
The proteasome modulates endocytosis specifically in glomerular cells to promote kidney filtration

In the kidney, maintaining permeability of the filtration barrier is critical. Here, Sachs W. et al show that homeostasis of podocytes and glomerular endothelial cells relies on differing proteasome constitutions which orchestrate endocytic activity in addition to protein degradation.

Wiebke Sachs
Lukas Blume
Catherine Meyer-Schwesinger
ResearchOpen Access01 Mar 2024
Nature Communications

Volume: 15, P: 1-21
Non-functional ubiquitin C-terminal hydrolase L1 drives podocyte injury through impairing proteasomes in autoimmune glomerulonephritis

In membranous nephropathy autoantibodies target podocytes of the kidney filter resulting in injury. Here the authors show that the ensuing proteostatic disturbances and proteinuria relate to aberrant interactions of non-functional UCH-L1 enzyme with the proteasome, curtailing its capacity.

Julia Reichelt
Wiebke Sachs
Catherine Meyer-Schwesinger
ResearchOpen Access13 Apr 2023
Nature Communications

Volume: 14, P: 1-19
Spatiotemporal proteomics uncovers cathepsin-dependent macrophage cell death during Salmonella infection

Using the proteome-wide pSILAC-AHA labelling approach, the authors resolve the host proteome spatiotemporal dynamics during macrophage infection with Salmonella enterica Typhimurium and reveal the active role of cathepsins in cell death via the non-canonical inflammasome.

Joel Selkrig
Nan Li
Athanasios Typas
Research08 Jun 2020
Nature Microbiology

Volume: 5, P: 1119-1133
Chemical genetics strategy to profile kinase target engagement reveals role of FES in neutrophil phagocytosis

Chemical tools to monitor drug-target engagement of endogenous enzymes are essential for preclinical target validation. Here, the authors present a chemical genetics strategy to study target engagement of endogenous kinases, achieving specific labeling and inactivation of FES kinase to provide insights into FES’ role in neutrophil phagocytosis.

Tom van der Wel
Riet Hilhorst
Mario van der Stelt
ResearchOpen Access25 Jun 2020
Nature Communications

Volume: 11, P: 1-20
Activity-based probes for functional interrogation of retaining β-glucuronidases

Synthesis and application of activity-based probes based on cyclophellitol enabled the cellular profiling of β-glucuronidase activity and revealed an unexpected feature of endo-acting heparanase processing.

Liang Wu
Jianbing Jiang
Gideon J Davies
Research05 Jun 2017
Nature Chemical Biology

Volume: 13, P: 867-873
Ultrasensitive in situ visualization of active glucocerebrosidase molecules

Fluorescent high-affinity activity-based probes used to monitor the activity and presence of active glucocerebrosidase in vitro and in vivo help in understanding Gaucher disease and its treatment with pharmacological chaperones.

Martin D Witte
Wouter W Kallemeijn
Johannes M F G Aerts
Research31 Oct 2010
Nature Chemical Biology

Volume: 6, P: 907-913
Integrated transcriptomics- and structure-based drug repositioning identifies drugs with proteasome inhibitor properties

Peter Larsson
Maria Cristina De Rosa
Toshima Z. Parris
ResearchOpen Access13 Aug 2024
Scientific Reports

Volume: 14, P: 1-18
Relative quantification of proteasome activity by activity-based protein profiling and LC-MS/MS

Nan Li
Chi-Lin Kuo
Bogdan I Florea
Protocols23 May 2013
Nature Protocols

Volume: 8, P: 1155-1168
Near infrared emission properties of Er doped cubic sesquioxides in the second/third biological windows

Daniel Avram
Ion Tiseanu
Carmen Tiseanu
ResearchOpen Access21 Dec 2018
Scientific Reports

Volume: 8, P: 1-12
Mapping in vivo target interaction profiles of covalent inhibitors using chemical proteomics with label-free quantification

This protocol describes the identification of in vivo target interaction profiles of covalent enzyme inhibitors using chemical proteomics. Enzymes are enriched by activity-based probes and quantified by label-free mass spectrometry.

Eva J van Rooden
Bogdan I Florea
Mario van der Stelt
Protocols22 Mar 2018
Nature Protocols

Volume: 13, P: 752-767
Milder degenerative effects of Carfilzomib vs. Bortezomib in the Drosophila model: a link to clinical adverse events

Eleni N. Tsakiri
Evangelos Terpos
Ioannis P. Trougakos
ResearchOpen Access19 Dec 2017
Scientific Reports

Volume: 7, P: 1-12

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Publisher Correction: Non-functional ubiquitin C-terminal hydrolase L1 drives podocyte injury through impairing proteasomes in autoimmune glomerulonephritis

Discovery of a NAPE-PLD inhibitor that modulates emotional behavior in mice

A monoacylglycerol lipase inhibitor showing therapeutic efficacy in mice without central side effects or dependence

The proteasome modulates endocytosis specifically in glomerular cells to promote kidney filtration

Non-functional ubiquitin C-terminal hydrolase L1 drives podocyte injury through impairing proteasomes in autoimmune glomerulonephritis

Spatiotemporal proteomics uncovers cathepsin-dependent macrophage cell death during Salmonella infection

Chemical genetics strategy to profile kinase target engagement reveals role of FES in neutrophil phagocytosis

Activity-based probes for functional interrogation of retaining β-glucuronidases

Ultrasensitive in situ visualization of active glucocerebrosidase molecules

Integrated transcriptomics- and structure-based drug repositioning identifies drugs with proteasome inhibitor properties

Relative quantification of proteasome activity by activity-based protein profiling and LC-MS/MS

Near infrared emission properties of Er doped cubic sesquioxides in the second/third biological windows

Mapping in vivo target interaction profiles of covalent inhibitors using chemical proteomics with label-free quantification

Milder degenerative effects of Carfilzomib vs. Bortezomib in the Drosophila model: a link to clinical adverse events

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