Structural analysis of malaria-parasite lysyl-tRNA synthetase provides a platform for drug development

Khan, Sameena; Garg, Ankur; Camacho, Noelia; Rooyen, Jason M. van; Pole, Anil Kumar; Belrhali, Hassan; Pouplana, Lluı́s Ribas de; Sharma, Vinay; Sharma, Amit

doi:10.1107/s0907444913001923

Cited by 58 publications

(93 citation statements)

References 34 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…To fulfill the requirements of protein synthesis, malaria parasite protein translation enzymes and their reaction substrates and products need to be distributed between apicoplasts, mitochondria, and cytoplasm (7,8,13,14,22). In P. falciparum, dual localization of single-copy aaRSs has been observed in the cases of Ala-RS, Gly-RS, Thr-RS, and Cys-RS (7,8,13,14,23).…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Inhibition of Protein Synthesis and Malaria Parasite Development by Drug Targeting of Methionyl-tRNA Synthetases

Hussain

Yogavel

Sharma

2015

Antimicrob Agents Chemother

Self Cite

View full text Add to dashboard Cite

Aminoacyl-tRNA synthetases (aaRSs) are housekeeping enzymes that couple cognate tRNAs with amino acids to transmit genomic information for protein translation. The Plasmodium falciparum nuclear genome encodes two P. falciparum methionyl-tRNA synthetases (PfMRS), termed PfMRS cyt and PfMRS api . Phylogenetic analyses revealed that the two proteins are of primitive origin and are related to heterokonts (PfMRS cyt ) or proteobacteria/primitive bacteria (PfMRS api ). We show that PfMRS cyt localizes in parasite cytoplasm, while PfMRS api localizes to apicoplasts in asexual stages of malaria parasites. Two known bacterial MRS inhibitors, REP3123 and REP8839, hampered Plasmodium growth very effectively in the early and late stages of parasite development. Small-molecule drug-like libraries were screened against modeled PfMRS structures, and several "hit" compounds showed significant effects on parasite growth. We then tested the effects of the hit compounds on protein translation by labeling nascent proteins with 35 S-labeled cysteine and methionine. Three of the tested compounds reduced protein synthesis and also blocked parasite growth progression from the ring stage to the trophozoite stage. Drug docking studies suggested distinct modes of binding for the three compounds, compared with the enzyme product methionyl adenylate. Therefore, this study provides new targets (PfMRSs) and hit compounds that can be explored for development as antimalarial drugs. P lasmodium falciparum is the most virulent form of Plasmodium and a causative agent of malaria. The World Health Organization (WHO) estimates that there are ϳ0.62 million deaths due to malaria per year (1). The P. falciparum genome is AT-rich (81%) and codes for ϳ5,300 proteins, with unusual distributions of several residues (2). Almost 60% of encoded proteins appear to be unique to the parasite, reflecting great evolutionary distance between the parasite and the genomes of known eukaryotes (3). The malaria parasite (and the related apicomplexan Toxoplasma gondii) has three translationally active compartments, i.e., cytoplasm, apicoplasts, and mitochondria (4-8). All malaria parasite proteins involved in the protein synthesis machinery are encoded by the nuclear genome. Either these proteins are transported to target organelles or their modified/activated substrates are transported across the organelles to perform required functions (4-9). The primary enzymes responsible for translating genetic code into polypeptide chains are aminoacyl-tRNA synthetases (aaRSs). The canonical function of aaRSs is to ligate a specific amino acid to its cognate tRNA, which is then employed in protein synthesis. The aaRSs are an ancient class of essential enzymes, and their catalytic domains are conserved in all kingdoms (bacteria, archaebacteria, and eukaryotes). On the basis of catalytic domain architecture, aaRSs are classified into two categories, with each class containing ϳ10 aaRSs (10). Although aaRSs perform the basic function of charging tRNA molecules for protein synthesis, a...

show abstract

Section: Discussionmentioning

confidence: 99%

“…Malaria parasite aaRSs are currently being explored as new targets for drug development (22,23). Within aaRSs, MRSs can serve as valuable drug targets because of their sequence and domain heterogeneity.…”

mentioning

confidence: 99%

Inhibition of Protein Synthesis and Malaria Parasite Development by Drug Targeting of Methionyl-tRNA Synthetases

Hussain

Yogavel

Sharma

2015

Antimicrob Agents Chemother

Self Cite

View full text Add to dashboard Cite

show abstract

“…One early study reported aaRS activity in P. berghei cell-free extracts (89), and genome sequencing later revealed the entire complement of aaRSs in Plasmodium (10,68,88). But to date, cytoplasmic and apicoplast P. falciparum aspartyl-tRNA synthetase (28,29), lysyltRNA synthetase (30,31), and tryptophanyl-tRNA synthetase (32,33) are the only other malarial aaRSs besides PfGluRS to be functionally or structurally characterized.…”

Section: Discussionmentioning

confidence: 99%

“…Mupirocin, for example, is a topical antibiotic already in clinical use, and other aaRS inhibitors such as the boronated antifungal compound AN2690 (27) are being developed. Aminoacylation in malaria parasites had been little studied despite its critical role in parasite biology and potential as a drug target, but studies describing the apicoplast (28) and cytoplasmic aspartyl-tRNA synthetases (29), lysyl-tRNA synthetases (30,31), and tryptophanyl-tRNA synthetases (32,33) were recently published.…”

mentioning

confidence: 99%

A Nondiscriminating Glutamyl-tRNA Synthetase in the Plasmodium Apicoplast

Mailu

Ramasamay

Mudeppa

et al. 2013

Journal of Biological Chemistry

View full text Add to dashboard Cite

Background: Plasmodium apicoplast protein synthesis is essential, but few apicoplast tRNA synthetases have been characterized. Results: Apicoplast glutamyl-tRNA synthetase aminoacylates tRNA Glu and tRNA Gln , is sensitive to a bacterial inhibitor, and is essential in blood stages. Conclusion: Formation of apicoplast Gln-tRNAGln is via indirect aminoacylation. Significance: We demonstrate that the apicoplast glutamyl-tRNA synthetase is a potential drug target.

show abstract

“…Ap4A hydrolase in the parasite hints at a special role for this molecule in parasite physiology. [9,10] Sulfonamides represent an important class of medically important compound, which is present in a number of biologically active molecules. In addition, sulfonamide derivatives are extensively used as antitumor, [11,12] antiviral, [13] antimalarial, [14,15] anti-inflammatory, [16] anticancer, [17] anti-carbonic anhydrase, [18] antidiabetic agents, [19] and in Alzheimer's diseases.…”

Section: Introductionmentioning

confidence: 99%

Untitled

2017

AJP

View full text Add to dashboard Cite

Aims: Malaria remains a worldwide health problem. Resistance to antimalarial drugs by the Plasmodium falciparum malaria parasite is posing a serious impediment in malaria control program. Hence continuous efforts on the development of new antimalarial are required. Being an important enzyme in parasite physiology diadenosine tetraphosphate (Ap4A) hydrolase may prove a good target for antimalarial drugs. The aim of this study was to explore the inhibitory potential of some sulfonamide derivatives against malaria parasite Ap4A hydrolase. Materials and Methods: The molecular three-dimensional structural data of malaria parasite Ap4A hydrolase were obtained from protein databank (PDB ID: 5CFI) and used as a drug target. The molecular docking approach was employed to find out the in silico inhibitory potential of the sulfonamide derivatives against Ap4A hydrolase and their relative stabilities were studied. Results and Discussion: All sulfonamide derivatives showed good binding affinity against the target protein. The binding free energy of compound 4-amino-N-(quinoxalin-2yl) benzenesulfonamide S6 (−8.43 Kcal/mole) showed it to be the most optimal sulfonamide derivative as inhibitor for Ap4A hydrolase enzyme. Conclusions: Evaluation of binding affinities using free energy simulations allowed establishing that sulfonamides having quinoxaline moiety is the highest quality compound of the series. The findings attained through this study on the molecular interaction mode of sulfonamide derivatives, and Ap4A hydrolase enzyme can be considered for further in vitro and in vivo validation for designing new potential antimalarial drugs.

show abstract

Structural analysis of malaria-parasite lysyl-tRNA synthetase provides a platform for drug development

Cited by 58 publications

References 34 publications

Inhibition of Protein Synthesis and Malaria Parasite Development by Drug Targeting of Methionyl-tRNA Synthetases

Inhibition of Protein Synthesis and Malaria Parasite Development by Drug Targeting of Methionyl-tRNA Synthetases

A Nondiscriminating Glutamyl-tRNA Synthetase in the Plasmodium Apicoplast

Untitled

Contact Info

Product

Resources

About