Expression, Characterization, and Cellular Localization of Knowpains, Papain-Like Cysteine Proteases of the Plasmodium knowlesi Malaria Parasite

Prasad, Rajesh Kumar; Atul, Atul; Soni, Awakash; Puri, Sunil K.; Sijwali, Puran Singh

doi:10.1371/journal.pone.0051619

Cited by 22 publications

(10 citation statements)

References 55 publications

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“…In T. parva they are thought to facilitate lymphocyte invasion [ 16 ]. Papain family cysteine proteases have been considered as potential vaccine targets in the related apicomplexan Plasmodium falciparum [ 17 ], and the previously described T. parva antigen Tp8, in chromosome 2 (TpMuguga_02g00140), is a papain family cysteine protease. The polymorphic papain cysteine protease identified here (TpMuguga_03g00280) is located in chromosome 3, and its antigenic potential warrants further investigation.…”

Section: Resultsmentioning

confidence: 99%

The genomes of three stocks comprising the most widely utilized live sporozoite Theileria parva vaccine exhibit very different degrees and patterns of sequence divergence

et al. 2015

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BackgroundThere are no commercially available vaccines against human protozoan parasitic diseases, despite the success of vaccination-induced long-term protection against infectious diseases. East Coast fever, caused by the protist Theileria parva, kills one million cattle each year in sub-Saharan Africa, and contributes significantly to hunger and poverty in the region. A highly effective, live, multi-isolate vaccine against T. parva exists, but its component isolates have not been characterized. Here we sequence and compare the three component T. parva stocks within this vaccine, the Muguga Cocktail, namely Muguga, Kiambu5 and Serengeti-transformed, aiming to identify genomic features that contribute to vaccine efficacy.ResultsWe find that Serengeti-transformed, originally isolated from the wildlife carrier, the African Cape buffalo, is remarkably and unexpectedly similar to the Muguga isolate. The 420 detectable non-synonymous SNPs were distributed among only 53 genes, primarily subtelomeric antigens and antigenic families. The Kiambu5 isolate is considerably more divergent, with close to 40,000 SNPs relative to Muguga, including >8,500 non-synonymous mutations distributed among >1,700 (42.5 %) of the predicted genes. These genetic markers of the component stocks can be used to characterize the composition of new batches of the Muguga Cocktail.ConclusionsDifferences among these three isolates, while extensive, represent only a small proportion of the genetic variation in the entire species. Given the efficacy of the Muguga Cocktail in inducing long-lasting protection against infections in the field, our results suggest that whole-organism vaccines against parasitic diseases can be highly efficacious despite considerable genome-wide differences relative to the isolates against which they protect.Electronic supplementary materialThe online version of this article (doi:10.1186/s12864-015-1910-9) contains supplementary material, which is available to authorized users.

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Section: Resultsmentioning

confidence: 99%

The genomes of three stocks comprising the most widely utilized live sporozoite Theileria parva vaccine exhibit very different degrees and patterns of sequence divergence

et al. 2015

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“…DTT was found to enhance enzyme activities of knowpains (Prasad et al 2012), Falcipain-2 (Sarduy et al 2012, DerF1 and DerP1 (Takai et al 2002) in a dose-dependent manner. Different pH buffers also showed significant effects on cathepsin F-like cysteine protease (Joo et al 2007), knowpains (Prasad et al 2012), Tr-cp 14 (Asp et al 2004) and Falcipain-2 (Sarduy et al 2012) activities; the maximum activities often obtained in acidic pH. The concentration of cysteine protease used in enzyme activity assays is between 0.1 and 10 nM (Bromme et al 2004).…”

Section: Cysteine Proteases Activation and Enzyme Activity Examinationmentioning

confidence: 96%

“…The buffer, DTT and EDTA concentrations vary between protocols, and their effect on the enzyme activities was in controversy. Some researchs deemed that these factors don't have a significant effect on the enzyme activities (Bromme et al 2004;Joo et al 2007;Prasad et al 2012). However, some other literatures showed different perspectives.…”

Section: Cysteine Proteases Activation and Enzyme Activity Examinationmentioning

confidence: 99%

Approaches for the generation of active papain-like cysteine proteases from inclusion bodies of Escherichia coli

Ling

Zhang

Lin

et al. 2015

World J Microbiol Biotechnol

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Papain-like cysteine proteases are widely expressed, fulfill specific functions in extracellular matrix turnover, antigen presentation and processing events, and may represent viable drug targets for major diseases. In depth and rigorous studies of the potential for these proteins to be targets for drug development require sufficient amounts of protease protein that can be used for both experimental and therapeutic purposes. Escherichia coli was widely used to express papain-like cysteine proteases, but most of those proteases are produced in insoluble inclusion bodies that need solubilizing, refolding, purifying and activating. Refolding is the most critical step in the process of generating active cysteine proteases and the current approaches to refolding include dialysis, dilution and chromatography. Purification is mainly achieved by various column chromatography. Finally, the attained refolded proteases are examined regarding their protease structures and activities.

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“…Also, KP-4 was observed to have essential role in erythrocyte cytoskeleton breakdown facilitating merozoite egress. Accordingly, the investigators suggested using in vitro culture of P. knowlesi for searching a VP specific inhibitor in the absence of an efficient in vitro culture system for P. vivax [58] .…”

Section: Homologs and Orthologsmentioning

confidence: 99%

Expression of cysteine proteinases and cystatins in parasites and use of cysteine proteinase inhibitors in parasitic diseases. Part III: Protozoa (2): Plasmodium spp.

Abaza

2019

Parasitologists United Journal

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Expression, Characterization, and Cellular Localization of Knowpains, Papain-Like Cysteine Proteases of the Plasmodium knowlesi Malaria Parasite

Cited by 22 publications

References 55 publications

The genomes of three stocks comprising the most widely utilized live sporozoite Theileria parva vaccine exhibit very different degrees and patterns of sequence divergence

The genomes of three stocks comprising the most widely utilized live sporozoite Theileria parva vaccine exhibit very different degrees and patterns of sequence divergence

Approaches for the generation of active papain-like cysteine proteases from inclusion bodies of Escherichia coli

Expression of cysteine proteinases and cystatins in parasites and use of cysteine proteinase inhibitors in parasitic diseases. Part III: Protozoa (2): Plasmodium spp.

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