HGPRT and PNP: Recombinant Enzymes from Schistosoma mansoni and Their Role in Immunotherapy during Experimental Murine Schistosomiasis

Schistosomiasis is a parasitic infection caused by trematode worms (also called blood flukes) of the genus Schistosoma sp., which affects over 230 million people worldwide, causing 200,000 deaths annually. There is no vaccine or new drugs available, which represents a worrying aspect, since there is...

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Autores principales: de Lima Fragelli, Bruna Dias, Fattori, Ana Carolina Maragno, de Almeida Montija, Elisandra, de Almeida Rodolpho, Joice Margareth, de Castro, Cynthia Aparecida, de Godoy, Krissia Franco, Nogueira, Camila Tita, Rodrigues, Vanderlei, Soares, Edson Garcia, Romanello, Larissa, Torini, Juliana R., Pereira, Humberto D’Muniz, de Freitas Anibal, Fernanda
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10144537/
https://www.ncbi.nlm.nih.gov/pubmed/37111413
http://dx.doi.org/10.3390/pathogens12040527
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author de Lima Fragelli, Bruna Dias
Fattori, Ana Carolina Maragno
de Almeida Montija, Elisandra
de Almeida Rodolpho, Joice Margareth
de Castro, Cynthia Aparecida
de Godoy, Krissia Franco
Nogueira, Camila Tita
Rodrigues, Vanderlei
Soares, Edson Garcia
Romanello, Larissa
Torini, Juliana R.
Pereira, Humberto D’Muniz
de Freitas Anibal, Fernanda
author_facet de Lima Fragelli, Bruna Dias
Fattori, Ana Carolina Maragno
de Almeida Montija, Elisandra
de Almeida Rodolpho, Joice Margareth
de Castro, Cynthia Aparecida
de Godoy, Krissia Franco
Nogueira, Camila Tita
Rodrigues, Vanderlei
Soares, Edson Garcia
Romanello, Larissa
Torini, Juliana R.
Pereira, Humberto D’Muniz
de Freitas Anibal, Fernanda
author_sort de Lima Fragelli, Bruna Dias
collection PubMed
description Schistosomiasis is a parasitic infection caused by trematode worms (also called blood flukes) of the genus Schistosoma sp., which affects over 230 million people worldwide, causing 200,000 deaths annually. There is no vaccine or new drugs available, which represents a worrying aspect, since there is loss of sensitivity of the parasite to the medication recommended by the World Health Organization, Praziquantel. The present study evaluated the effects of the recombinant enzymes of S. mansoni Hypoxanthine-Guanine Phosphoribosyltransferase (HGPRT), Purine Nucleoside Phosphorylase (PNP) and the MIX of both enzymes in the immunotherapy of schistosomiasis in murine model. These enzymes are part of the purine salvage pathway, the only metabolic pathway present in the parasite for this purpose, being essential for the synthesis of DNA and RNA. Female mice of Swiss and BALB/c strains were infected with cercariae and treated, intraperitoneally, with three doses of 100 µg of enzymes. After the immunotherapy, the eggs and adult worms were counted in the feces; the number of eosinophils from the fluid in the peritoneal cavity and peripheral blood was observed; and the quantification of the cytokine IL-4 and the production of antibodies IgE was analyzed. The evaluation of the number of granulomas and collagen deposition via histological slides of the liver was performed. The results demonstrate that immunotherapy with the enzyme HGPRT seems to stimulate the production of IL-4 and promoted a significant reduction of granulomas in the liver in treated animals. The treatment with the enzyme PNP and the MIX was able to reduce the number of worms in the liver and in the mesenteric vessels of the intestine, to reduce the number of eggs in the feces and to negatively modulate the number of eosinophils. Therefore, immunotherapy with the recombinant enzymes of S. mansoni HGPRT and PNP might contribute to the control and reduction of the pathophysiological aspects of schistosomiasis, helping to decrease the morbidity associated with the infection in murine model.
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spelling pubmed-101445372023-04-29 HGPRT and PNP: Recombinant Enzymes from Schistosoma mansoni and Their Role in Immunotherapy during Experimental Murine Schistosomiasis de Lima Fragelli, Bruna Dias Fattori, Ana Carolina Maragno de Almeida Montija, Elisandra de Almeida Rodolpho, Joice Margareth de Castro, Cynthia Aparecida de Godoy, Krissia Franco Nogueira, Camila Tita Rodrigues, Vanderlei Soares, Edson Garcia Romanello, Larissa Torini, Juliana R. Pereira, Humberto D’Muniz de Freitas Anibal, Fernanda Pathogens Article Schistosomiasis is a parasitic infection caused by trematode worms (also called blood flukes) of the genus Schistosoma sp., which affects over 230 million people worldwide, causing 200,000 deaths annually. There is no vaccine or new drugs available, which represents a worrying aspect, since there is loss of sensitivity of the parasite to the medication recommended by the World Health Organization, Praziquantel. The present study evaluated the effects of the recombinant enzymes of S. mansoni Hypoxanthine-Guanine Phosphoribosyltransferase (HGPRT), Purine Nucleoside Phosphorylase (PNP) and the MIX of both enzymes in the immunotherapy of schistosomiasis in murine model. These enzymes are part of the purine salvage pathway, the only metabolic pathway present in the parasite for this purpose, being essential for the synthesis of DNA and RNA. Female mice of Swiss and BALB/c strains were infected with cercariae and treated, intraperitoneally, with three doses of 100 µg of enzymes. After the immunotherapy, the eggs and adult worms were counted in the feces; the number of eosinophils from the fluid in the peritoneal cavity and peripheral blood was observed; and the quantification of the cytokine IL-4 and the production of antibodies IgE was analyzed. The evaluation of the number of granulomas and collagen deposition via histological slides of the liver was performed. The results demonstrate that immunotherapy with the enzyme HGPRT seems to stimulate the production of IL-4 and promoted a significant reduction of granulomas in the liver in treated animals. The treatment with the enzyme PNP and the MIX was able to reduce the number of worms in the liver and in the mesenteric vessels of the intestine, to reduce the number of eggs in the feces and to negatively modulate the number of eosinophils. Therefore, immunotherapy with the recombinant enzymes of S. mansoni HGPRT and PNP might contribute to the control and reduction of the pathophysiological aspects of schistosomiasis, helping to decrease the morbidity associated with the infection in murine model. MDPI 2023-03-29 /pmc/articles/PMC10144537/ /pubmed/37111413 http://dx.doi.org/10.3390/pathogens12040527 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
de Lima Fragelli, Bruna Dias
Fattori, Ana Carolina Maragno
de Almeida Montija, Elisandra
de Almeida Rodolpho, Joice Margareth
de Castro, Cynthia Aparecida
de Godoy, Krissia Franco
Nogueira, Camila Tita
Rodrigues, Vanderlei
Soares, Edson Garcia
Romanello, Larissa
Torini, Juliana R.
Pereira, Humberto D’Muniz
de Freitas Anibal, Fernanda
HGPRT and PNP: Recombinant Enzymes from Schistosoma mansoni and Their Role in Immunotherapy during Experimental Murine Schistosomiasis
title HGPRT and PNP: Recombinant Enzymes from Schistosoma mansoni and Their Role in Immunotherapy during Experimental Murine Schistosomiasis
title_full HGPRT and PNP: Recombinant Enzymes from Schistosoma mansoni and Their Role in Immunotherapy during Experimental Murine Schistosomiasis
title_fullStr HGPRT and PNP: Recombinant Enzymes from Schistosoma mansoni and Their Role in Immunotherapy during Experimental Murine Schistosomiasis
title_full_unstemmed HGPRT and PNP: Recombinant Enzymes from Schistosoma mansoni and Their Role in Immunotherapy during Experimental Murine Schistosomiasis
title_short HGPRT and PNP: Recombinant Enzymes from Schistosoma mansoni and Their Role in Immunotherapy during Experimental Murine Schistosomiasis
title_sort hgprt and pnp: recombinant enzymes from schistosoma mansoni and their role in immunotherapy during experimental murine schistosomiasis
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10144537/
https://www.ncbi.nlm.nih.gov/pubmed/37111413
http://dx.doi.org/10.3390/pathogens12040527
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