Protective immune responses against Schistosoma mansoni infection by immunization with functionally active gut-derived cysteine peptidases alone and in combination with glyceraldehyde 3-phosphate dehydrogenase

Tallima, Hatem; Dvořák, Jan; Kareem, Sahira; Dahab, Marwa Abou El; Aziz, Nada Abdel; Dalton, John P.; Ridi, Rashika El

doi:10.1371/journal.pntd.0005443

Cited by 45 publications

(55 citation statements)

References 36 publications

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“…Our results confirm an association of SmGAPDH with the tegumental surface of the worm. This further reconciles results that previously characterized SmGAPDH as a protective vaccine target (Argiro et al, 2000b;El Ridi and Tallima, 2013;Tallima et al, 2017;Tang et al, 2019). Before these results, how such an intracellular cytosolic enzyme might be accessed by damaging immune effectors was a conundrum.…”

Section: Discussionsupporting

confidence: 85%

“…GAPDH is best known as a key enzyme in glycolysis, facilitating the conversion of glyceraldehyde-3-phosphate (GAP) in the presence of nicotinamide adenide dinucleotide (NAD) to 1,3-bisphosphoglycerate (1,3BPG) and generating NADH (Seidler, 2013). S. mansoni GAPDH (SmGAPDH) has been previously expressed in an enzymatically active recombinant form (Argiro et al, 2000a;El Ridi et al, 2001, 2004, has been characterized as a potential vaccine candidate and has been shown to be a target for antibodies in the sera of schistosomiasisresistant individuals (Argiro et al, 2000a,b;Dessein et al, 1988;Goudot-Crozel et al, 1989;Tallima et al, 2017;Tang et al, 2019).…”

Section: Introductionmentioning

confidence: 99%

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Schistosoma mansoniglyceraldehyde-3-phosphate dehydrogenase enhances formation of the blood-clot lysis protein plasmin

2020

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Schistosomes are intravascular blood flukes that cause the parasitic disease schistosomiasis. In agreement with Schistosoma mansoni (Sm) proteomic analysis, we show here that the normally intracellular glycolytic enzyme glyceraldehyde-3-phosphate dehydrogenase (GAPDH) is also found at the parasite surface; live worms from all intravascular life stages display GAPDH activity. Suppressing GAPDH gene expression using RNA interference significantly lowers this live worm surface activity. Medium in which the worms are cultured overnight displays essentially no activity, showing that the enzyme is not shed or excreted but remains associated with the worm surface. Immunolocalization experiments confirm that the enzyme is highly expressed in the parasite tegument (skin). Surface activity in schistosomula amounts to ∼8% of that displayed by equivalent parasite lysates. To address the functional role of SmGAPDH, we purified the protein following its expression in Escherichia coli strain DS113. The recombinant protein displays optimal enzymatic activity at pH 9.2, shows robust activity at the temperature of the parasite's hosts, and has a Michaelis-Menten constant for glyceraldehyde-3-phosphate (GAP) of 1.4 mM±0.24. We show that recombinant SmGAPDH binds plasminogen (PLMG) and promotes PLMG conversion to its active form (plasmin) in a dose response in the presence of tissue plasminogen activator. Since plasmin is a key mediator of thrombolysis, our results support the hypothesis that SmGAPDH, a host-interactive tegumental protein that can enhance PLMG activation, could help degrade blood clots around the worms in the vascular microenvironment and thus promote parasite survival in vivo. This article has an associated First Person interview with the first author of the paper.

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Section: Discussionsupporting

confidence: 85%

Section: Introductionmentioning

confidence: 99%

Schistosoma mansoniglyceraldehyde-3-phosphate dehydrogenase enhances formation of the blood-clot lysis protein plasmin

2020

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“…Moreover, Sm CB1 is a promising vaccine candidate because its administration elicits protection against S . mansoni challenge infection in mice and hamsters [ 30 , 31 ]. A direct link with HDACs has never been reported.…”

Section: Resultsmentioning

confidence: 99%

Analysis of the interactome of Schistosoma mansoni histone deacetylase 8

et al. 2017

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BackgroundHistone deacetylase 8 from Schistosoma mansoni (SmHDAC8) is essential to parasite growth and development within the mammalian host and is under investigation as a target for the development of selective inhibitors as novel schistosomicidal drugs. Although some protein substrates and protein partners of human HDAC8 have been characterized, notably indicating a role in the function of the cohesin complex, nothing is known of the partners and biological function of SmHDAC8.Methodology/Principal findingsWe therefore employed two strategies to characterize the SmHDAC8 interactome. We first used SmHDAC8 as a bait protein in yeast two-hybrid (Y2H) screening of an S. mansoni cDNA library. This allowed the identification of 49 different sequences encoding proteins. We next performed co-immunoprecipitation (Co-IP) experiments on parasite extracts with an anti-SmHDAC8 antibody. Mass spectrometry (MS) analysis allowed the identification of 160 different proteins.Conclusions/SignificanceSmHDAC8 partners are involved in about 40 different processes, included expected functions such as the cohesin complex, cytoskeleton organization, transcriptional and translational regulation, metabolism, DNA repair, the cell cycle, protein dephosphorylation, proteolysis, protein transport, but also some proteasome and ribosome components were detected. Our results show that SmHDAC8 is a versatile deacetylase, potentially involved in both cytosolic and nuclear processes.

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“…Several studies have reported remarkable cases of resistance to PZQ which include the development of heritable trait that maintained drug resistance to PZQ in more than six generations (Devaney, 2006;Doenhoff, Cioli & Utzinger, 2008;Fallon et al, 1996;Masamba et al, 2016;William et al, 2001). Only 13% of targeted population received praziquantel treatment, with the drug not capable of preventing reinfection, requires repeated treatment and its characterised by reduction in efficiency among population with heavy infection (Tallima et al, 2017). With the endemicity of schistosomiasis still on the increase across many countries, with increased cases of Schistosoma resistance to the most used and reliable drug PZQ.…”

Section: Discussionmentioning

confidence: 99%

An immunoinformatics approach for the design of a multi-epitope subunit vaccine for urogenital schistosomiasis

Onile

Fadahunsi

Adekunle

et al. 2020

PeerJ

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Discovery of T and B memory cells capable of eliciting long-term immunity against schistosomiasisis is important for people in endemic areas. Changes in schistosomes environment due to developmental cycle, induces up-regulation of Heat Shock Proteins (HSPs) which assist the parasite in coping with the hostile conditions associated with its life cycle. This study therefore focused on exploring the role of HSPs in urogenital schistosomiasis to develop new multi-epitope subunit vaccine against the disease using immunoinformatic approaches. The designed subunit vaccine was subjected to in silico antigenicity, immunogenicity, allergenicity and physicochemical parameters analysis. A 3D structure of the vaccine construct was predicted, followed by disulphide engineering for stability, codon adaptation and in silico cloning for proper expression and molecular protein–protein docking of vaccine construct in the vector against toll-like receptor 4 receptor, respectively. Consequently, a 493 amino acid multi-epitope vaccine construct of antigenicity probability of 0.91 was designed. This was predicted to be stable, non-allergenic in nature and safe for human use.

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Protective immune responses against Schistosoma mansoni infection by immunization with functionally active gut-derived cysteine peptidases alone and in combination with glyceraldehyde 3-phosphate dehydrogenase

Cited by 45 publications

References 36 publications

Schistosoma mansoniglyceraldehyde-3-phosphate dehydrogenase enhances formation of the blood-clot lysis protein plasmin

Schistosoma mansoniglyceraldehyde-3-phosphate dehydrogenase enhances formation of the blood-clot lysis protein plasmin

Analysis of the interactome of Schistosoma mansoni histone deacetylase 8

An immunoinformatics approach for the design of a multi-epitope subunit vaccine for urogenital schistosomiasis

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