SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4295079882> ?p ?o ?g. }

Showing items 1 to 100 of ±121 with 100 items per page.

W4295079882 endingPage "41" @default.
W4295079882 startingPage "41" @default.
W4295079882 abstract "Schistosomiasis is a debilitating parasitic disease caused by intravascular flatworms called schistosomes (blood flukes) that affects >200 million people worldwide. Proteomic analysis has revealed the surprising presence of classical glycolytic enzymes - typically cytosolic proteins - located on the extracellular surface of the parasite tegument (skin). Immunolocalization experiments show that phosphoglycerate mutase (PGM) is widely expressed in parasite tissues and is highly expressed in the tegument. We demonstrate that live Schistosoma mansoni parasites express enzymatically active PGM on their tegumental surface. Suppression of PGM using RNA interference (RNAi) diminishes S. mansoni PGM (SmPGM) gene expression, protein levels, and surface enzyme activity. Sequence comparisons place SmPGM in the cofactor (2,3-bisphosphoglycerate)-dependent PGM (dPGM) family. We have produced recombinant SmPGM (rSmPGM) in an enzymatically active form in Escherichia coli. The Michaelis-Menten constant (Km) of rSmPGM for its glycolytic substrate (3-phosphoglycerate) is 0.85 mM ± 0.02. rSmPGM activity is inhibited by the dPGM-specific inhibitor vanadate. Here, we show that rSmPGM not only binds to plasminogen but also promotes its conversion to an active form (plasmin) in vitro. This supports the hypothesis that host-interactive tegumental proteins (such as SmPGM), by enhancing plasmin formation, may help degrade blood clots around the worms in the vascular microenvironment and thus promote parasite survival in vivo.La phosphoglycérate mutase de Schistosoma mansoni – une ectoenzyme glycolytique avec un potentiel thrombolytique.La schistosomiase est une maladie parasitaire débilitante causée par des vers plats intravasculaires appelés schistosomes qui affecte plus de 200 millions de personnes dans le monde. L’analyse protéomique a révélé la présence surprenante d’enzymes glycolytiques classiques – typiquement des protéines cytosoliques – situées sur la surface extracellulaire du tégument du parasite. Des expériences d’immunolocalisation montrent que la phosphoglycérate mutase (PGM) est largement exprimée dans les tissus parasitaires et fortement exprimée dans le tégument. Nous démontrons que les parasites Schistosoma mansoni vivants expriment une PGM enzymatiquement active sur leur surface tégumentaire. La suppression de la PGM à l’aide de l’interférence ARN (ARNi) diminue l’expression du gène PGM de S. mansoni (SmPGM), les niveaux de protéines et l’activité enzymatique de surface. Les comparaisons de séquences placent la SmPGM dans la famille des PGM dépendantes du cofacteur (2,3-bisphosphoglycérate) (dPGM). Nous avons produit de la SmPGM recombinante (rSmPGM) sous une forme enzymatiquement active dans Escherichia coli. La constante de Michaelis-Menten (Km) de rSmPGM pour son substrat glycolytique (3-phosphoglycérate) est de 0,85 mM ± 0,02. L’activité de la rSmPGM est inhibée par le vanadate, un inhibiteur spécifique des dPGM. Ici, nous montrons que rSmPGM non seulement se lie au plasminogène mais favorise également sa conversion en une forme active (plasmine) in vitro. Cela soutient l’hypothèse selon laquelle les protéines tégumentaires interactives avec l’hôte (telles que SmPGM), en améliorant la formation de plasmine, peuvent aider à dégrader les caillots sanguins autour des vers dans le microenvironnement vasculaire et ainsi favoriser la survie du parasite in vivo." @default.
W4295079882 created "2022-09-10" @default.
W4295079882 creator A5015751956 @default.
W4295079882 creator A5057808894 @default.
W4295079882 creator A5086382938 @default.
W4295079882 date "2022-01-01" @default.
W4295079882 modified "2023-10-05" @default.
W4295079882 title "<i>Schistosoma mansoni</i> phosphoglycerate mutase: a glycolytic ectoenzyme with thrombolytic potential" @default.
W4295079882 cites W1525635642 @default.
W4295079882 cites W1527548373 @default.
W4295079882 cites W1556023848 @default.
W4295079882 cites W1857401373 @default.
W4295079882 cites W1971366710 @default.
W4295079882 cites W1972812075 @default.
W4295079882 cites W1973633999 @default.
W4295079882 cites W1974177779 @default.
W4295079882 cites W1975086865 @default.
W4295079882 cites W1983094284 @default.
W4295079882 cites W1988834288 @default.
W4295079882 cites W1992685096 @default.
W4295079882 cites W2001993518 @default.
W4295079882 cites W2017264401 @default.
W4295079882 cites W2022602601 @default.
W4295079882 cites W2028944012 @default.
W4295079882 cites W2051942624 @default.
W4295079882 cites W2064899900 @default.
W4295079882 cites W2073544824 @default.
W4295079882 cites W2084358662 @default.
W4295079882 cites W2091790046 @default.
W4295079882 cites W2097780360 @default.
W4295079882 cites W2099365295 @default.
W4295079882 cites W2107277218 @default.
W4295079882 cites W2114509436 @default.
W4295079882 cites W2121014456 @default.
W4295079882 cites W2122518986 @default.
W4295079882 cites W2126924068 @default.
W4295079882 cites W2132753699 @default.
W4295079882 cites W2152141463 @default.
W4295079882 cites W2192080449 @default.
W4295079882 cites W2200082027 @default.
W4295079882 cites W2204809370 @default.
W4295079882 cites W2222045825 @default.
W4295079882 cites W2410393981 @default.
W4295079882 cites W2512336527 @default.
W4295079882 cites W2743496055 @default.
W4295079882 cites W2779300148 @default.
W4295079882 cites W2806262432 @default.
W4295079882 cites W2889156744 @default.
W4295079882 cites W2982336998 @default.
W4295079882 cites W3007654429 @default.
W4295079882 cites W3014373623 @default.
W4295079882 cites W3084367718 @default.
W4295079882 cites W3087859267 @default.
W4295079882 cites W3094779895 @default.
W4295079882 cites W3194483137 @default.
W4295079882 cites W3206593628 @default.
W4295079882 cites W3214389223 @default.
W4295079882 cites W4211093028 @default.
W4295079882 cites W4211120517 @default.
W4295079882 cites W4211128418 @default.
W4295079882 cites W4243129459 @default.
W4295079882 doi "https://doi.org/10.1051/parasite/2022042" @default.
W4295079882 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/36083036" @default.
W4295079882 hasPublicationYear "2022" @default.
W4295079882 type Work @default.
W4295079882 citedByCount "1" @default.
W4295079882 crossrefType "journal-article" @default.
W4295079882 hasAuthorship W4295079882A5015751956 @default.
W4295079882 hasAuthorship W4295079882A5057808894 @default.
W4295079882 hasAuthorship W4295079882A5086382938 @default.
W4295079882 hasBestOaLocation W42950798821 @default.
W4295079882 hasConcept C146998594 @default.
W4295079882 hasConcept C153911025 @default.
W4295079882 hasConcept C155911427 @default.
W4295079882 hasConcept C159047783 @default.
W4295079882 hasConcept C165901193 @default.
W4295079882 hasConcept C181199279 @default.
W4295079882 hasConcept C20251656 @default.
W4295079882 hasConcept C203014093 @default.
W4295079882 hasConcept C2776225656 @default.
W4295079882 hasConcept C2776863245 @default.
W4295079882 hasConcept C2781071845 @default.
W4295079882 hasConcept C55493867 @default.
W4295079882 hasConcept C86803240 @default.
W4295079882 hasConcept C91754966 @default.
W4295079882 hasConceptScore W4295079882C146998594 @default.
W4295079882 hasConceptScore W4295079882C153911025 @default.
W4295079882 hasConceptScore W4295079882C155911427 @default.
W4295079882 hasConceptScore W4295079882C159047783 @default.
W4295079882 hasConceptScore W4295079882C165901193 @default.
W4295079882 hasConceptScore W4295079882C181199279 @default.
W4295079882 hasConceptScore W4295079882C20251656 @default.
W4295079882 hasConceptScore W4295079882C203014093 @default.
W4295079882 hasConceptScore W4295079882C2776225656 @default.
W4295079882 hasConceptScore W4295079882C2776863245 @default.
W4295079882 hasConceptScore W4295079882C2781071845 @default.
W4295079882 hasConceptScore W4295079882C55493867 @default.
W4295079882 hasConceptScore W4295079882C86803240 @default.