| Literature DB >> 28634183 |
Antonella Pantaleo1, Kristina R Kesely2, Maria Carmina Pau1, Ioannis Tsamesidis3, Evelin Schwarzer4, Oleksii A Skorokhod4, Huynh D Chien5, Marta Ponzi6,7, Lucia Bertuccini7,8, Philip S Low2, Francesco M Turrini4.
Abstract
Band 3 (also known as the anion exchanger, SLCA1, AE1) constitutes the major attachment site of the spectrin-based cytoskeleton to the erythrocyte's lipid bilayer and thereby contributes critically to the stability of the red cell membrane. During the intraerythrocytic stage of Plasmodium falciparum's lifecycle, band 3 becomes tyrosine phosphorylated in response to oxidative stress, leading to a decrease in its affinity for the spectrin/actin cytoskeleton and causing global membrane destabilization. Because this membrane weakening is hypothesized to facilitate parasite egress and the consequent dissemination of released merozoites throughout the bloodstream, we decided to explore which tyrosine kinase inhibitors might block the kinase-induced membrane destabilization. We demonstrate here that multiple Syk kinase inhibitors both prevent parasite-induced band 3 tyrosine phosphorylation and inhibit parasite-promoted membrane destabilization. We also show that the same Syk kinase inhibitors suppress merozoite egress near the end of the parasite's intraerythrocytic lifecycle. Because the entrapped merozoites die when prevented from escaping their host erythrocytes and because some Syk inhibitors have displayed long-term safety in human clinical trials, we suggest Syk kinase inhibitors constitute a promising class of antimalarial drugs that can suppress parasitemia by inhibiting a host target that cannot be mutated by the parasite to evolve drug resistance.Entities:
Mesh:
Substances:
Year: 2017 PMID: 28634183 PMCID: PMC8939463 DOI: 10.1182/blood-2016-11-748053
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113