<rdf:RDF xmlns:rdf="http://www.openarchives.org/OAI/2.0/rdf/" xmlns:ow="http://www.ontoweb.org/ontology/1#" xmlns:dc="http://purl.org/dc/elements/1.1/" xmlns:ds="http://dspace.org/ds/elements/1.1/" xmlns:xsi="http://www.w3.org/2001/XMLSchema-instance" xmlns:doc="http://www.lyncode.com/xoai" xsi:schemaLocation="http://www.openarchives.org/OAI/2.0/rdf/ http://www.openarchives.org/OAI/2.0/rdf.xsd">
   <ow:Publication rdf:about="oai:digibug.ugr.es:10481/80513">
      <dc:title>Identification of compounds with activity against Trypanosoma cruzi within a collection of synthetic nucleoside analogs</dc:title>
      <dc:creator>Barnadas Carceller, Berta</dc:creator>
      <dc:creator>Córdoba Gómez, Laura</dc:creator>
      <dc:creator>Díaz Mochón, Juan José</dc:creator>
      <dc:creator>Molina Pineda Infantas, Ignacio Jesús</dc:creator>
      <dc:creator>Pineda De Las Infant Y Villatoro, María José</dc:creator>
      <dc:subject>Chagas disease</dc:subject>
      <dc:subject>Trypanosoma cruzi</dc:subject>
      <dc:subject>Purine derivatives</dc:subject>
      <dc:subject>Antiparasitic assays</dc:subject>
      <dc:subject>Cytotoxicity assays</dc:subject>
      <dc:subject>Drug discovery cascade</dc:subject>
      <dc:description>Introduction: Chagas disease is caused by the protozoan parasite&#xd;
Trypanosoma cruzi, and it is the most important neglected tropical disease in&#xd;
the Americas. Two drugs are available to treat the infection, but their efficacy in&#xd;
the chronic stage of the disease, when most cases are diagnosed, is reduced.&#xd;
Their tolerability is also hindered by common adverse effects, making the&#xd;
development of safer and efficacious alternatives a pressing need. T. cruzi is&#xd;
unable to synthesize purines de novo, relying on a purine salvage pathway to&#xd;
acquire these from its host, making it an attractive target for the development&#xd;
of new drugs.&#xd;
Methods: We evaluated the anti-parasitic activity of 23 purine analogs with&#xd;
different substitutions in the complementary chains of their purine rings. We&#xd;
sequentially screened the compounds' capacity to inhibit parasite growth, their&#xd;
toxicity in Vero and HepG2 cells, and their specific capacity to inhibit the&#xd;
development of amastigotes. We then used in-silico docking to identify their&#xd;
likely targets. Results: Eight compounds showed specific anti-parasitic activity, with IC50&#xd;
values ranging from 2.42 to 8.16 mM. Adenine phosphoribosyl transferase, and&#xd;
hypoxanthine-guanine phosphoribosyl transferase, are their most likely targets.&#xd;
Discussion: Our results illustrate the potential role of the purine salvage pathway&#xd;
as a target route for the development of alternative treatments against T. cruzi&#xd;
infection, highlithing the apparent importance of specific substitutions, like the&#xd;
presence of benzene groups in the C8 position of the purine ring, consistently&#xd;
associated with a high and specific anti-parasitic activity.</dc:description>
      <dc:date>2023-03-10T09:35:30Z</dc:date>
      <dc:date>2023-03-10T09:35:30Z</dc:date>
      <dc:date>2023-01-13</dc:date>
      <dc:type>journal article</dc:type>
      <dc:identifier>Barnadas-Carceller B... [et al.] (2023) Identification of compounds with activity against Trypanosoma cruzi within a collection of synthetic nucleoside analogs. Front. Cell. Infect. Microbiol. 12:1067461. doi: [10.3389/fcimb.2022.1067461]</dc:identifier>
      <dc:identifier>https://hdl.handle.net/10481/80513</dc:identifier>
      <dc:identifier>10.3389/fcimb.2022.1067461</dc:identifier>
      <dc:language>eng</dc:language>
      <dc:rights>http://creativecommons.org/licenses/by/4.0/</dc:rights>
      <dc:rights>open access</dc:rights>
      <dc:rights>Atribución 4.0 Internacional</dc:rights>
      <dc:publisher>Frontiers</dc:publisher>
   </ow:Publication>
</rdf:RDF>