Potent and selective inhibitors for M32 metallocarboxypeptidases identified from high-throughput screening of anti-kinetoplastid chemical boxes

Salas-Sarduy, Emir; Landaburu, Lionel Urán; Carmona, Adriana K.; Cazzulo, Juán José; Agüero, Fernán; Álvarez, Vanina E.; Niemirowicz, Gabriela T.

doi:10.1371/journal.pntd.0007560

Cited by 3 publications

(2 citation statements)

References 46 publications

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“…GlaxoSmithKline HAT and CHAGAS boxes (13) were received as 10 mM stock solutions in DMSO. For primary screening, a working solution (final concentration of 2 mM) for each compound was prepared by 1/5 dilution in DMSO while 1 µL of the 10 mM stock solution was used for secondary screening of selected compounds (42). Nine compounds from Maybridge database, previously identified by virtual screening as potential inhibitors of the cysteine peptidase falcipain-2 (Clan CA) from Plasmodium falciparum (14),…”

Section: Compound Collectionsmentioning

confidence: 99%

“…After agitation, the fluorescence of AMC was acquired kinetically for each well (12 read cycles, one cycle every 300 seconds). Considering our previous experiences (25,42), the auto-fluorescent cut-off was arbitrarily set at 5x10 6 RFU to discard highly interfering compounds. All compounds were assayed in singlet (without replicates) due to the limited availability of stocks.…”

Section: Primary Screeningmentioning

confidence: 99%

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Screening and Identification of Metacaspase Inhibitors: Evaluation of Inhibition Mechanism and Trypanocidal Activity

Pérez

Bouvier

Cazzulo

et al. 2021

Antimicrob Agents Chemother

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A common strategy to identify new antiparasitic agents is the targeting of proteases due to their essential contribution to parasite growth and development. Metacaspases (MCAs) are cysteine proteases present in fungi, protozoa and plants. These enzymes, which are associated with crucial cellular events in trypanosomes, are absent in the human host, thus arising as attractive drug targets. To find new MCA inhibitors with trypanocidal activity, we adapted a continuous fluorescent enzymatic assay to a medium-throughput format and carried out screening of different compound collections, followed by the construction of dose-response curves for the most promising hits. We used MCA5 from T. brucei (TbMCA5) as a model for the identification of inhibitors from the GlaxoSmithKline HAT and CHAGAS chemical boxes. We also assessed a third collection of 9 compounds from the Maybridge database identified by virtual screening as potential inhibitors of the cysteine peptidase falcipain-2 (Clan CA) from Plasmodium falciparum. Compound HTS01959 (from the Maybridge collection) was the most potent inhibitor with IC50 of 14.39 μM; also inhibiting other MCAs from T. brucei and T. cruzi (TbMCA2=4.14 μM, TbMCA3=5.04 μM and TcMCA5=151 μM). HTS01959 behaved as a reversible, slow binding and noncompetitive inhibitor of TbMCA2, with a mechanism of action that included redox components. Importantly, HTS01959 displayed trypanocidal activity against bloodstream forms of T. brucei and trypomastigotes forms of T. cruzi, without cytotoxic effect on VERO cells. Thus, HTS01959 is a promising starting point to develop more specific and potent chemical structures to target MCAs.

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Section: Compound Collectionsmentioning

confidence: 99%

Section: Primary Screeningmentioning

confidence: 99%

Screening and Identification of Metacaspase Inhibitors: Evaluation of Inhibition Mechanism and Trypanocidal Activity

Pérez

Bouvier

Cazzulo

et al. 2021

Antimicrob Agents Chemother

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Update on relevant trypanosome peptidases: Validated targets and future challenges

Álvarez

Iribarren

Niemirowicz

et al. 2021

Biochimica et Biophysica Acta (BBA) - Proteins and Proteomics

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Towards discovery of new leishmanicidal scaffolds able to inhibitLeishmaniaGSK-3

Iturrate

Sebastián-Pérez

Nachér-Vázquez

et al. 2019

Journal of Enzyme Inhibition and Medicinal Chemistry

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Previous reports have validated the glycogen synthase kinase-3 (GSK-3) as a druggable target against the human protozoan parasite Leishmania. This prompted us to search for new leishmanicidal scaffolds as inhibitors of this enzyme from our in-house library of human GSK-3b inhibitors, as well as from the Leishbox collection of leishmanicidal compounds developed by GlaxoSmithKline. As a result, new leishmanicidal inhibitors acting on Leishmania GSK-3 at micromolar concentrations were found. These inhibitors belong to six different chemical classes (thiadiazolidindione, halomethylketone, maleimide, benzoimidazole, N-phenylpyrimidine-2-amine and oxadiazole). In addition, the binding mode of the most active compounds into Leishmania GSK-3 was approached using computational tools. On the whole, we have uncovered new chemical scaffolds with an appealing prospective in the development and use of Leishmania GSK-3 inhibitors against this infectious protozoan. GRAPHICAL ABSTRACT ARTICLE HISTORY

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Potent and selective inhibitors for M32 metallocarboxypeptidases identified from high-throughput screening of anti-kinetoplastid chemical boxes

Cited by 3 publications

References 46 publications

Screening and Identification of Metacaspase Inhibitors: Evaluation of Inhibition Mechanism and Trypanocidal Activity

Screening and Identification of Metacaspase Inhibitors: Evaluation of Inhibition Mechanism and Trypanocidal Activity

Update on relevant trypanosome peptidases: Validated targets and future challenges

Towards discovery of new leishmanicidal scaffolds able to inhibitLeishmaniaGSK-3

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