Abstract
BackgroundProtein structure plays a pivotal role in elucidating mechanisms of parasite functioning and drug resistance. Moreover, protein structure aids the determination of protein function, which can together with the structure be used to identify novel drug targets in the parasite. However, various structural features in Plasmodium falciparum proteins complicate the experimental determination of protein structures. Limited similarity to proteins in the Protein Data Bank and the shortage of solved protein structures in the malaria parasite necessitate genome-scale structural annotation of P. falciparum proteins. Additionally, the annotation of a range of structural features facilitates the identification of suitable targets for experimental and computational studies.MethodsAn integrated structural annotation system was developed and applied to P. falciparum, Plasmodium vivax and Plasmodium yoelii. The annotation included searches for sequence similarity, patterns and domains in addition to the following predictions: secondary structure, transmembrane helices, protein disorder, low complexity, coiled-coils and small molecule interactions. Subsequently, candidate proteins for further structural studies were identified based on the annotated structural features.ResultsThe annotation results are accessible through a web interface, enabling users to select groups of proteins which fulfil multiple criteria pertaining to structural and functional features [1]. Analysis of features in the P. falciparum proteome showed that protein-interacting proteins contained a higher percentage of predicted disordered residues than non-interacting proteins. Proteins interacting with 10 or more proteins have a disordered content concentrated in the range of 60–100%, while the disorder distribution for proteins having only one interacting partner, was more evenly spread.ConclusionA series of P. falciparum protein targets for experimental structure determination, comparative modelling and in silico docking studies were putatively identified. The system is available for public use, where researchers may identify proteins by querying with multiple physico-chemical, sequence similarity and interaction features.
Highlights
Protein structure plays a pivotal role in elucidating mechanisms of parasite functioning and drug resistance
Following the rise in resistance, there has been a pressing need to understand the mechanism of drug resistance and develop novel anti-malarial drugs
Protein structure has previously been used to elucidate the mechanism of resistance in Plasmodium falciparum [4,5]
Summary
Protein structure plays a pivotal role in elucidating mechanisms of parasite functioning and drug resistance. Protein structure aids the determination of protein function, which can together with the structure be used to identify novel drug targets in the parasite. Various structural features in Plasmodium falciparum proteins complicate the experimental determination of protein structures. Protein structure has previously been used to elucidate the mechanism of resistance in Plasmodium falciparum [4,5]. As resistance to existing drugs is a globally occurring phenomenon, new information regarding the structure and function of the proteins in especially the P. falciparum genome is of importance. Various features of the parasite genome and proteome complicate functional and structural characterization studies, including a high AT-content and the presence of low complexity regions and inserts [8,9]
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