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   Naphthoquinone Derivatives Exert Their Antitrypanosomal Activity via a Multi-Target Mechanism  
   
نویسنده pieretti s. ,haanstra j.r. ,mazet m. ,perozzo r. ,bergamini c. ,prati f. ,fato r. ,lenaz g. ,capranico g. ,brun r. ,bakker b.m. ,michels p.a.m. ,scapozza l. ,bolognesi m.l. ,cavalli a.
منبع plos neglected tropical diseases - 2013 - دوره : 7 - شماره : 1
چکیده    Background and methodology: recently,we reported on a new class of naphthoquinone derivatives showing a promising anti-trypanosomatid profile in cell-based experiments. the lead of this series (b6,2-phenoxy-1,4-naphthoquinone) showed an ed50 of 80 nm against trypanosoma brucei rhodesiense,and a selectivity index of 74 with respect to mammalian cells. a multitarget profile for this compound is easily conceivable,because quinones,as natural products,serve plants as potent defense chemicals with an intrinsic multifunctional mechanism of action. to disclose such a multitarget profile of b6,we exploited a chemical proteomics approach. principal findings: a functionalized congener of b6 was immobilized on a solid matrix and used to isolate target proteins from trypanosoma brucei lysates. mass analysis delivered two enzymes,i.e. glycosomal glycerol kinase and glycosomal glyceraldehyde-3-phosphate dehydrogenase,as potential molecular targets for b6. both enzymes were recombinantly expressed and purified,and used for chemical validation. indeed,b6 was able to inhibit both enzymes with ic50 values in the micromolar range. the multifunctional profile was further characterized in experiments using permeabilized trypanosoma brucei cells and mitochondrial cell fractions. it turned out that b6 was also able to generate oxygen radicals,a mechanism that may additionally contribute to its observed potent trypanocidal activity. conclusions and significance: overall,b6 showed a multitarget mechanism of action,which provides a molecular explanation of its promising anti-trypanosomatid activity. furthermore,the forward chemical genetics approach here applied may be viable in the molecular characterization of novel multitarget ligands. © 2013 pieretti et al.
آدرس department of pharmacy and biotechnology,university of bologna,bologna,italy,pharmaceutical biochemistry group,school of pharmaceutical sciences,university of geneva,university of lausanne,geneva,switzerland,department of biochemistry,university of bologna,bologna, Italy, department of pediatrics,centre for liver,digestive and metabolic diseases,university of groningen,university medical centre groningen,groningen,netherlands,department of molecular cell physiology,faculty of earth and life sciences,vrije universiteit amsterdam,amsterdam, Netherlands, research unit for tropical diseases,de duve institute and laboratory of biochemistry,université catholique de louvain,brussels,belgium,centre de résonance magnétique des systémes biologiques (rmsb),umr 5536 cnrs,université victor segalen bordeaux 2,bordeaux, France, pharmaceutical biochemistry group,school of pharmaceutical sciences,university of geneva,university of lausanne,geneva, Switzerland, department of biochemistry,university of bologna,bologna, Italy, department of pharmacy and biotechnology,university of bologna,bologna,italy,department of drug discovery and development,istituto italiano di tecnologia,genova, Italy, department of biochemistry,university of bologna,bologna, Italy, department of biochemistry,university of bologna,bologna, Italy, department of biochemistry,university of bologna,bologna, Italy, swiss tropical institute,basel, Switzerland, department of pediatrics,centre for liver,digestive and metabolic diseases,university of groningen,university medical centre groningen,groningen,netherlands,department of molecular cell physiology,faculty of earth and life sciences,vrije universiteit amsterdam,amsterdam, Netherlands, research unit for tropical diseases,de duve institute and laboratory of biochemistry,université catholique de louvain,brussels, Belgium, pharmaceutical biochemistry group,school of pharmaceutical sciences,university of geneva,university of lausanne,geneva, Switzerland, department of pharmacy and biotechnology,university of bologna,bologna, Italy, department of pharmacy and biotechnology,university of bologna,bologna,italy,department of drug discovery and development,istituto italiano di tecnologia,genova, Italy
 
     
   
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