Novel broad-spectrum activity-based probes to profile malarial cysteine proteases

Tan, Michele S. Y.; Davison, Dara; Sánchez, Mateo I.; Anderson, Bethany M.; Howell, Stephen H.; Snijders, Ambrosius P.; Edgington-Mitchell, Laura E.; Deu, Edgar

doi:10.1371/journal.pone.0227341

Cited by 10 publications

(9 citation statements)

References 39 publications

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“… 6 − 9 This chemotype supported the successful development of activity-based probes, modified for organelle-specific delivery to lysosomal cysteine proteases and applied as PET-imaging agents for tumor-associated cathepsin activity. 10 − 12 These reports have highlighted that azadipeptide nitriles can enrich the portfolio of inhibitors of cysteine proteases suitable as activity-based probes 13 , 14 and potential therapeutics against parasitic and protozoal infections. 15 − 18 Similar to the well-established dipeptide nitriles, azadipeptide nitriles are thought to undergo a covalent, reversible interaction with the target proteases by forming a stabilized isothiosemicarbazide adduct ( Figure 1 ).…”

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confidence: 99%

“…Azapeptides, peptides in which the CαH of at least one amino acid has been replaced with nitrogen, have emerged as particularly important peptidomimetic structures (Figure ). Compared to their parent carbapeptide analogs, bioactive azapeptides can possess improved potency and target selectivity as well as superior pharmacokinetics. − Azadipeptide nitriles were introduced as a class of efficient inhibitors of human cysteine cathepsins. − This chemotype supported the successful development of activity-based probes, modified for organelle-specific delivery to lysosomal cysteine proteases and applied as PET-imaging agents for tumor-associated cathepsin activity. − These reports have highlighted that azadipeptide nitriles can enrich the portfolio of inhibitors of cysteine proteases suitable as activity-based probes , and potential therapeutics against parasitic and protozoal infections. − Similar to the well-established dipeptide nitriles, azadipeptide nitriles are thought to undergo a covalent, reversible interaction with the target proteases by forming a stabilized isothiosemicarbazide adduct (Figure ). − …”

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confidence: 99%

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Azanitrile Inhibitors of the SmCB1 Protease Target Are Lethal to Schistosoma mansoni: Structural and Mechanistic Insights into Chemotype Reactivity

et al. 2020

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Azapeptide nitriles are postulated to reversibly covalently react with the active-site cysteine residue of cysteine proteases and form isothiosemicarbazide adducts. We investigated the interaction of azadipeptide nitriles with the cathepsin B1 drug target (SmCB1) from Schistosoma mansoni, a pathogen that causes the global neglected disease schistosomiasis. Azadipeptide nitriles were superior inhibitors of SmCB1 over their parent carba analogs. We determined the crystal structure of SmCB1 in complex with an azadipeptide nitrile and analyzed the reaction mechanism using quantum chemical calculations. The data demonstrate that azadipeptide nitriles, in contrast to their carba counterparts, undergo a change from E-to Z-configuration upon binding, which gives rise to a highly favorable energy profile of noncovalent and covalent complex formation. Finally, azadipeptide nitriles were considerably more lethal than their carba analogs against the schistosome pathogen in culture, supporting the further development of this chemotype as a treatment for schistosomiasis.

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confidence: 99%

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confidence: 99%

Azanitrile Inhibitors of the SmCB1 Protease Target Are Lethal to Schistosoma mansoni: Structural and Mechanistic Insights into Chemotype Reactivity

et al. 2020

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“…However, FY01 has a more selective labeling profile. [23] Tan et al [24] recently reported a new series of broadspectrum vinyl sulfone ABPs that efficiently labeled both subfamilies in lysates and intact cells. An alkyne handle was included, and different fluorophores were appended by click chemistry.…”

Section: Cysteine Proteasesmentioning

confidence: 99%

“…Tan et al [24] . recently reported a new series of broad‐spectrum vinyl sulfone ABPs that efficiently labeled both subfamilies in lysates and intact cells.…”

Section: Dissecting the Roles Of Specific Enzymes And Proteins In P F...mentioning

confidence: 99%

The Impact of Activity‐Based Protein Profiling in Malaria Drug Discovery

Carvalho

Bernardes

2022

ChemMedChem

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Activity‐based protein profiling (ABPP) is an approach used at the interface of chemical biology and proteomics that uses small molecular probes to provide dynamic fingerprints of enzymatic activity in complex proteomes. Malaria is a disease caused by Plasmodium parasites with a significant death burden and for which new therapies are actively being sought. Here, we compile the main achievements from ABPP studies in malaria and highlight the probes used and the different downstream platforms for data analysis. ABPP has excelled at studying Plasmodium cysteine proteases and serine hydrolase families, the targeting of the proteasome and metabolic pathways, and in the deconvolution of targets and mechanisms of known antimalarials. Despite the major impact in the field, many antimalarials and enzymatic families in Plasmodium remain to be studied, which suggests ABPP will be an evergreen technique in the field.

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“…Subsequent studies have largely expanded the scope of activity‐based probes to target Plasmodium serine hydrolases, [38] metallo‐aminopeptidases [39] and the proteasome [40–43] . The expansion of ABPP probes to a larger number of diverse proteins could provide a platform to screen different enzymes as candidate targets of antimalarial inhibitors [44] …”

Section: Activity‐based Protein Profilingmentioning

confidence: 99%

Chemoproteomics for Plasmodium Parasite Drug Target Discovery

Mansfield

Fitzgerald

et al. 2021

ChemBioChem

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Emerging Plasmodium parasite drug resistance is threatening progress towards malaria control and elimination. While recent efforts in cell‐based, high‐throughput drug screening have produced first‐in‐class drugs with promising activities against different Plasmodium life cycle stages, most of these antimalarial agents have elusive mechanisms of action. Though challenging to address, target identification can provide valuable information to facilitate lead optimization and preclinical drug prioritization. Recently, proteome‐wide methods for direct assessment of drug‐protein interactions have emerged as powerful tools in a number of systems, including Plasmodium. In this review, we will discuss current chemoproteomic strategies that have been adapted to antimalarial drug target discovery, including affinity‐ and activity‐based protein profiling and the energetics‐based techniques thermal proteome profiling and stability of proteins from rates of oxidation. The successful application of chemoproteomics to the Plasmodium blood stage highlights the potential of these methods to link inhibitors to their molecular targets in more elusive Plasmodium life stages and intracellular pathogens in the future.

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Novel broad-spectrum activity-based probes to profile malarial cysteine proteases

Cited by 10 publications

References 39 publications

Azanitrile Inhibitors of the SmCB1 Protease Target Are Lethal to Schistosoma mansoni: Structural and Mechanistic Insights into Chemotype Reactivity

Azanitrile Inhibitors of the SmCB1 Protease Target Are Lethal to Schistosoma mansoni: Structural and Mechanistic Insights into Chemotype Reactivity

The Impact of Activity‐Based Protein Profiling in Malaria Drug Discovery

Chemoproteomics for Plasmodium Parasite Drug Target Discovery

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