| Literature DB >> 25728610 |
Kata Horváti1, Bernadett Bacsa1, Nóra Szabó2, Kinga Fodor3, Gyula Balka4, Miklós Rusvai4, Éva Kiss5, Gábor Mező1, Vince Grolmusz6, Beáta Vértessy7, Ferenc Hudecz8, Szilvia Bősze9.
Abstract
New pyridopyrimidine derivatives were defined using a novel HTS in silico docking method (FRIGATE). The target protein was a dUTPase enzyme (EC 3.6.1.23; Rv2697) which plays a key role in nucleotide biosynthesis of Mycobacterium tuberculosis (Mtb). Top hit molecules were assayed in vitro for their antimycobacterial effect on Mtb H37Rv culture. In order to enhance the cellular uptake rate, the TB820 compound was conjugated to a peptid-based carrier and a nanoparticle type delivery system (polylactide-co-glycolide, PLGA) was applied. The conjugate had relevance to in vitro antitubercular activity with low in vitro and in vivo toxicity. In a Mtb H37Rv infected guinea pig model the in vivo efficacy of orally administrated PLGA encapsulated compound was proven: animals maintained a constant weight gain and no external clinical signs of tuberculosis were observed. All tissue homogenates from lung, liver and kidney were found negative for Mtb, and diagnostic autopsy showed that no significant malformations on the tissues occurred.Entities:
Keywords: Guinea pig infection model; In silico docking; PLGA encapsulation; Peptide conjugate; Pyridopyrimidines
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Year: 2015 PMID: 25728610 DOI: 10.1016/j.tube.2015.02.026
Source DB: PubMed Journal: Tuberculosis (Edinb) ISSN: 1472-9792 Impact factor: 3.131