Synthetic compounds from an <i>in house</i> library as inhibitors of falcipain-2 from <i>Plasmodium falciparum</i>

Bertoldo, Jean B.; Chiaradia-Delatorre, Louise Domeneghini; Mascarello, Alessandra; Leal, Paulo César; Cordeiro, Mabel Mariela Rodríguez; Nunes, Ricardo José; Salas-Sarduy, Emir; Rosenthal, Philip J.; Terenzi, Hernán

doi:10.3109/14756366.2014.920839

Cited by 22 publications

(57 citation statements)

References 29 publications

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“…Several findings support the existence of allosteric modulation in the papain-like proteases [29–35]. One key example is the work of Novinec et al ., where several allosteric sites of human cathepsin K (HCatK) and the sector residues potentially mediating allosteric communication in the aforementioned protein family were identified employing the statistical coupling analysis (SCA) method (Fig 1) [36].…”

Section: Introductionmentioning

confidence: 84%

Dissecting a novel allosteric mechanism of cruzain: A computer-aided approach

et al. 2019

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Trypanosoma cruzi is the causative agent of Chagas disease, a neglected infection affecting millions of people in tropical regions. There are several chemotherapeutic agents for the treatment of this disease, but most of them are highly toxic and generate resistance. Currently, the development of allosteric inhibitors constitutes a promising research field, since it can improve the accessibility to more selective and less toxic medicines. To date, the allosteric drugs prediction is a state-of-the-art topic in rational structure-based computational design. In this work, a simulation strategy was developed for computational discovery of allosteric inhibitors, and it was applied to cruzain, a promising target and the major cysteine protease of T. cruzi. Molecular dynamics simulations, binding free energy calculations and network-based modelling of residue interactions were combined to characterize and compare molecular distinctive features of the apo form and the cruzain-allosteric inhibitor complexes. By using geometry-based criteria on trajectory snapshots, we predicted two main allosteric sites suitable for drug targeting. The results suggest dissimilar mechanisms exerted by the same allosteric site when binding different potential allosteric inhibitors. Finally, we identified the residues involved in suboptimal paths linking the identified site and the orthosteric site. The present study constitutes the first approximation to the design of cruzain allosteric inhibitors and may serve for future pharmacological intervention. Here, no major effects on active site structure were observed due to compound binding (modification of distance and angles between catalytic residues), which indicates that allosteric regulation in cruzain might be mediated via alterations of its dynamical properties similarly to allosteric inhibition of human cathepsin K (HCatK). The current findings are particularly relevant for the design of allosteric modulators of papain-like cysteine proteases.

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Section: Introductionmentioning

confidence: 84%

Dissecting a novel allosteric mechanism of cruzain: A computer-aided approach

et al. 2019

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“…Besides the chalcone hybrids mentioned above, chalcone–furan/thiophene, [ 95,96 ] chalcone–indole, [ 97 ] chalcone–pyrimidine, [ 98 ] and chalcone–sulfamide [ 99–101 ] hybrids also showed certain antiplasmodial activity, but the majority of them were not superior to the references.…”

Section: Miscellaneous Chalcone Hybridsmentioning

confidence: 99%

Chalcone hybrids and their antimalarial activity

Cheng

Yang

Huang

et al. 2020

Archiv der Pharmazie

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Malaria, one of the most striking, re‐emerging infectious diseases caused by the genus Plasmodium, places a huge burden on global healthcare systems. A major challenge in the control and eradication of malaria is the continuous emergence of increasingly widespread drug‐resistant malaria, creating an urgent need to develop novel antimalarial agents. Chalcone derivatives are ubiquitous in nature and have become indispensable units in medicinal chemistry applications due to their diverse biological profiles. Many chalcone derivatives demonstrate potential in vitro and in vivo antimalarial activity, so chalcone could be a useful template for the development of novel antimalarial agents. This review covers the recent development of chalcone hybrids as antimalarial agents. The critical aspects of the design and structure–activity relationship of these compounds are also discussed.

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“…Combined structural biology tools and mass spectrometry enabled investigators to characterize the allosteric mechanism for inhibition of new non-peptidic organic compounds against FP-2 activity. The investigators demonstrated that compound 66 is the best non-competitive inhibitor that showed allosteric binding between FP-2 catalytic site and the hemoglobin binding arm [139] . As previously reported, certain residues at the interface of FPs pro-and mature domain are essentially required for prodomain dissociation and FPs auto-processing (hot spot) [38] .…”

Section: D] Allosteric Site Inhibitorsmentioning

confidence: 99%

Expression of cysteine proteinases and cystatins in parasites and use of cysteine proteinase inhibitors in parasitic diseases. Part III: Protozoa (2): Plasmodium spp.

Abaza

2019

Parasitologists United Journal

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Synthetic compounds from an in house library as inhibitors of falcipain-2 from Plasmodium falciparum

Cited by 22 publications

References 29 publications

Dissecting a novel allosteric mechanism of cruzain: A computer-aided approach

Dissecting a novel allosteric mechanism of cruzain: A computer-aided approach

Chalcone hybrids and their antimalarial activity

Expression of cysteine proteinases and cystatins in parasites and use of cysteine proteinase inhibitors in parasitic diseases. Part III: Protozoa (2): Plasmodium spp.

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