Towards discovery of new leishmanicidal scaffolds able to inhibit Leishmania GSK-3

de Iturrate, Paula Martínez; Sebastián-Pérez, Victor; Nácher-Vázquez, Montserrat; Tremper, Catherine S.; Smirlis, Despina; Martín, Julio; Martínez, Ana; Campillo, Nuria E.; Rivas, Luis; Gil, Carmen

doi:10.6084/m9.figshare.10732328.v1

ienz_a_1693704_sm6011.pdf (3.87 MB)

Towards discovery of new leishmanicidal scaffolds able to inhibit Leishmania GSK-3

journal contribution

posted on 2019-11-22, 08:06 authored by Paula Martínez de Iturrate, Victor Sebastián-Pérez, Montserrat Nácher-Vázquez, Catherine S. Tremper, Despina Smirlis, Julio Martín, Ana Martínez, Nuria E. Campillo, Luis Rivas, Carmen Gil

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-3β 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.