Nature Search

Sec6l-mediated transfer of a membrane protein from the endoplasmic reticulum to the proteasome for destruction

Emmanuel J. H. J. Wiertz
Domenico Tortorella
Hidde L. Ploegh
Research05 Dec 1996
Nature

Volume: 384, P: 432-438
Identification of proteases that regulate erythrocyte rupture by the malaria parasite Plasmodium falciparum

Shirin Arastu-Kapur
Elizabeth L Ponder
Matthew Bogyo
Research03 Feb 2008
Nature Chemical Biology

Volume: 4, P: 203-213
A pipeline for proteome-wide analysis of electrophile selectivity

In the growing field of chemical proteomics, there is a need for general methods to map the reactivity profiles of covalent probes in complex proteomes. Now, a completely unbiased proteomic workflow has been developed that enables global characterization of the amino acid residues, chemically labelled by reactive electrophilic probes.

Jeyun Jo
Matthew Bogyo
News & Views30 Oct 2025
Nature Chemistry

Volume: 17, P: 1638-1640
Caspase-1 activity is required to bypass macrophage apoptosis upon Salmonella infection

AWP28, an activity-based probe for caspase-1, reveals that caspase-1 is required to bypass apoptosis for pyroptotic cell death during bacterial infection of macrophages.

Aaron W Puri
Petr Broz
Matthew Bogyo
Research15 Jul 2012
Nature Chemical Biology

Volume: 8, P: 745-747
Small-molecule inhibition of a depalmitoylase enhances Toxoplasma host-cell invasion

A small-molecule enhancer of Toxoplasma gondii invasion inhibits a previously uncharacterized parasite palmitoyl thioesterase, TgPPT1.

Matthew A Child
Carolyn I Hall
Matthew Bogyo
Research11 Aug 2013
Nature Chemical Biology

Volume: 9, P: 651-656
Identification of covalent inhibitors of Staphylococcus aureus serine hydrolases important for virulence and biofilm formation

Covalent inhibitors that selectively target bacterial enzymes are potential antibiotic drug candidates. Here, the authors apply high-throughput screening to identify selective covalent inhibitors that target serine hydrolases in Staphylococcus aureus

Tulsi Upadhyay
Emily C. Woods
Matthew Bogyo
ResearchOpen Access30 May 2025
Nature Communications

Volume: 16, P: 1-19
Metabolomics cuts to the chase to chase the cuts

Peptidases are enzymes that trim small protein fragments called peptides to regulate their biological functions. A new method opens the door to chasing down and identifying important cutting events mediated by peptidases involved in metabolic regulation.

Matthew Bogyo
News & Views01 Jan 2009
Nature Chemical Biology

Volume: 5, P: 5-6
Activity-based probes that target diverse cysteine protease families

Daisuke Kato
Kelly M Boatright
Matthew Bogyo
Research24 May 2005
Nature Chemical Biology

Volume: 1, P: 33-38
A proteolytic system that compensates for loss of proteasome function

Rickard Glas
Matthew Bogyo
Hidde L. Ploegh
Research09 Apr 1998
Nature

Volume: 392, P: 618-622
An in vivo multiplexed small-molecule screening platform

The combination of cellular barcoding and treatment with a library of small molecules before injecting the treated cells into mice allows the screening for compounds that inhibit metastatic seeding.

Barbara M Grüner
Christopher J Schulze
Monte M Winslow
Research12 Sept 2016
Nature Methods

Volume: 13, P: 883-889
AND-gate contrast agents for enhanced fluorescence-guided surgery

Optical contrast agents using AND-gate logic enhance the specificity and sensitivity of fluorescence-guided imaging in the resection of tumours and in the detection of metastases in mouse models of cancer.

John C. Widen
Martina Tholen
Matthew Bogyo
Research28 Sept 2020
Nature Biomedical Engineering

Volume: 5, P: 264-277
Reactive-site-centric chemoproteomics identifies a distinct class of deubiquitinase enzymes

Deubiquitinases are proteases that cleave after the C-terminus of ubiquitin to hydrolyze ubiquitin chains and cleave ubiquitin from substrates. Here the authors describe a reactive-site-centric chemoproteomics approach to studying deubiquitinase activity, and expand the repertoire of known deubiquitinases.

David S. Hewings
Johanna Heideker
Ingrid E. Wertz
ResearchOpen Access21 Mar 2018
Nature Communications

Volume: 9, P: 1-17
Chemoproteomic identification of a DPP4 homolog in Bacteroides thetaiotaomicron

Bioinformatic and chemoproteomic approaches resulted in the identification of a homolog of human dipeptidyl peptidase 4 in the gut bacterium Bacteroides thetaiotaomicron that regulates envelope integrity and community fitness.

Laura J. Keller
Taylor H. Nguyen
Matthew Bogyo
Research22 Jun 2023
Nature Chemical Biology

Volume: 19, P: 1469-1479
Labeling of active proteases in fresh-frozen tissues by topical application of quenched activity-based probes

This protocol describes the use of fluorescently quenched activity-based probes (qABPs) that target cysteine cathepsins. This approach allows for tracking of protease activity in tissue samples, which can be used for the detection of tumor resection margins.

Nimali P Withana
Megan Garland
Matthew Bogyo
Protocols30 Dec 2015
Nature Protocols

Volume: 11, P: 184-191
Discovery of small molecules that normalize the transcriptome and enhance cysteine cathepsin activity in progranulin-deficient microglia

Maria A. Telpoukhovskaia
Kai Liu
Li Gan
ResearchOpen Access13 Aug 2020
Scientific Reports

Volume: 10, P: 1-12
Identification of highly selective covalent inhibitors by phage display

Covalent inhibitors with high selectivity are rapidly identified by phage display.

Shiyu Chen
Scott Lovell
Matthew Bogyo
Research16 Nov 2020
Nature Biotechnology

Volume: 39, P: 490-498
Identification of a S. aureus virulence factor by activity-based protein profiling (ABPP)

ABP profiling identifies uncharacterized S. aureus serine hydrolases, including the surface-localized FphB, which processes lipid ester substrates and is required for infection in vivo. An FphB inhibitor reduces in vivo bacterial load.

Christian S. Lentz
Jessica R. Sheldon
Matthew Bogyo
Research16 May 2018
Nature Chemical Biology

Volume: 14, P: 609-617
Ferri-liposomes as an MRI-visible drug-delivery system for targeting tumours and their microenvironment

Magnetic nanoparticles encapsulated inside liposomes can deliver drug cargo, target tumours and their microenvironment, and simultaneously act as magnetic resonance contrast agents.

Georgy Mikhaylov
Ursa Mikac
Olga Vasiljeva
Research07 Aug 2011
Nature Nanotechnology

Volume: 6, P: 594-602
Uncovering an overlooked consequence of phosphorylation: change in cysteine reactivity

Global profiling of changes in the reactivity of cysteine residues in response to phosphorylation during mitosis identifies cysteine residues as potential regulatory and drug binding sites on proteins.

Markus Lakemeyer
Matthew Bogyo
News & Views28 Feb 2022
Nature Methods

Volume: 19, P: 281-283
A ‘Swiss army knife’ probe for metastatic cancers

A nanosensor probe that combines a tumour-targeting peptide, a diagnostic reporter and an imaging contrast agent enables early diagnosis, precision imaging, disease stratification and downstream therapeutic response monitoring of metastatic cancer.

Matthew Bogyo
News & Views24 Sept 2021
Nature Materials

Volume: 20, P: 1312-1314
Metalloproteases see the light

Small-molecule probes that chemically tag targets by virtue of their enzymatic activities offer a means to focus system-wide experiments and provide functional information for entire families of proteins. Recent advances in the design and application of light-activated probes that target metalloproteases have created the opportunity to study this medically important family of enzymes in unprecedented detail.

Matthew Bogyo
News & Views01 May 2006
Nature Chemical Biology

Volume: 2, P: 229-230
Mechanistic and structural insights into the proteolytic activation of Vibrio cholerae MARTX toxin

Aimee Shen
Patrick J Lupardus
Matthew Bogyo
Research24 May 2009
Nature Chemical Biology

Volume: 5, P: 469-478
Noninvasive optical imaging of cysteine protease activity using fluorescently quenched activity-based probes

Galia Blum
Georges von Degenfeld
Matthew Bogyo
Research09 Sept 2007
Nature Chemical Biology

Volume: 3, P: 668-677
Defining an allosteric circuit in the cysteine protease domain of Clostridium difficile toxins

Knowledge of the molecular mechanisms of activation of Clostridium difficile toxins will significantly enhance the ability to design specific anti-virulence therapies. Using activity-based chemical probes in combination with other techniques, this study reveals mechanistic insights into how inositol hexakisphosphate binding at the active site of the cysteine protease domain shifts the conformational equilibrium towards an active conformer.

Aimee Shen
Patrick J Lupardus
Matthew Bogyo
Research13 Feb 2011
Nature Structural & Molecular Biology

Volume: 18, P: 364-371
A protease draws first blood

Foreign proteins in a cell are chopped up and presented to the immune system by molecules of the major histocompatibility complex. What enzymes are responsible for making these cuts? The enzyme that delivers the initial blow specifically to the tetanus toxin has now been identified as asparaginyl endopeptidase.

Matthew Bogyo
Hidde L. Ploegh
News & Views17 Dec 1998
Nature

Volume: 396, P: 625-627
Toxoplasma depends on lysosomal consumption of autophagosomes for persistent infection

Disruption of a cysteine protease that localizes to the vacuolar compartment of Toxoplasma gondii shows that autophagy is required for the intracellular survival of the parasite during chronic infection.

Manlio Di Cristina
Zhicheng Dou
Vern B. Carruthers
Research19 Jun 2017
Nature Microbiology

Volume: 2, P: 1-7
Dynamic imaging of protease activity with fluorescently quenched activity-based probes

Galia Blum
Stefanie R Mullins
Matthew Bogyo
Research14 Aug 2005
Nature Chemical Biology

Volume: 1, P: 203-209
Noninvasive optical imaging of apoptosis by caspase-targeted activity-based probes

Caspases are intracellular proteases and key initiators and effectors of apoptosis. Here the authors describe fluorescently labeled activity-based probes that allow the noninvasive in vivo monitoring of the kinetics of caspase activity. Approaches to optimize the probes to enhance their specificity and increase uptake into apoptotic cells are outlined, and their use in tracking the early stages of apoptosis in two mouse models (dexamethasone and the monoclonal antibody Apomab) is demonstrated.

Laura E Edgington
Alicia B Berger
Matthew Bogyo
Research13 Jul 2009
Nature Medicine

Volume: 15, P: 967-973
Structure- and function-based design of Plasmodium-selective proteasome inhibitors

Structural and functional characterizations show that the specificity of the Plasmodium falciparum proteasome is sufficiently unique from that of the human proteasome to allow selective targeting with inhibitors.

Hao Li
Anthony J. O’Donoghue
Matthew Bogyo
Research10 Feb 2016
Nature

Volume: 530, P: 233-236
New approaches for dissecting protease functions to improve probe development and drug discovery

Edgar Deu
Martijn Verdoes
Matthew Bogyo
Reviews05 Jan 2012
Nature Structural & Molecular Biology

Volume: 19, P: 9-16
Non-invasive Imaging of Idiopathic Pulmonary Fibrosis Using Cathepsin Protease Probes

Nimali P. Withana
Xiaowei Ma
Matthew Bogyo
ResearchOpen Access22 Jan 2016
Scientific Reports

Volume: 6, P: 1-10
Commonly used caspase inhibitors designed based on substrate specificity profiles lack selectivity

Alicia B Berger
Kelly B Sexton
Matthew Bogyo
Correspondence21 Nov 2006
Cell Research

Volume: 16, P: 961-963

Search

Sec6l-mediated transfer of a membrane protein from the endoplasmic reticulum to the proteasome for destruction

Identification of proteases that regulate erythrocyte rupture by the malaria parasite Plasmodium falciparum

A pipeline for proteome-wide analysis of electrophile selectivity

Caspase-1 activity is required to bypass macrophage apoptosis upon Salmonella infection

Small-molecule inhibition of a depalmitoylase enhances Toxoplasma host-cell invasion

Identification of covalent inhibitors of Staphylococcus aureus serine hydrolases important for virulence and biofilm formation

Metabolomics cuts to the chase to chase the cuts

Activity-based probes that target diverse cysteine protease families

A proteolytic system that compensates for loss of proteasome function

An in vivo multiplexed small-molecule screening platform

AND-gate contrast agents for enhanced fluorescence-guided surgery

Reactive-site-centric chemoproteomics identifies a distinct class of deubiquitinase enzymes

Chemoproteomic identification of a DPP4 homolog in Bacteroides thetaiotaomicron

Labeling of active proteases in fresh-frozen tissues by topical application of quenched activity-based probes

Discovery of small molecules that normalize the transcriptome and enhance cysteine cathepsin activity in progranulin-deficient microglia

Identification of highly selective covalent inhibitors by phage display

Identification of a S. aureus virulence factor by activity-based protein profiling (ABPP)

Ferri-liposomes as an MRI-visible drug-delivery system for targeting tumours and their microenvironment

Uncovering an overlooked consequence of phosphorylation: change in cysteine reactivity

A ‘Swiss army knife’ probe for metastatic cancers

Metalloproteases see the light

Mechanistic and structural insights into the proteolytic activation of Vibrio cholerae MARTX toxin

Noninvasive optical imaging of cysteine protease activity using fluorescently quenched activity-based probes

Defining an allosteric circuit in the cysteine protease domain of Clostridium difficile toxins

A protease draws first blood

Toxoplasma depends on lysosomal consumption of autophagosomes for persistent infection

Dynamic imaging of protease activity with fluorescently quenched activity-based probes

Noninvasive optical imaging of apoptosis by caspase-targeted activity-based probes

Structure- and function-based design of Plasmodium-selective proteasome inhibitors

New approaches for dissecting protease functions to improve probe development and drug discovery

Non-invasive Imaging of Idiopathic Pulmonary Fibrosis Using Cathepsin Protease Probes

Commonly used caspase inhibitors designed based on substrate specificity profiles lack selectivity

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