Study of a new adenosine receptor A2A agonist, ATL313, on Clostridium difficile toxin A-induced enteritis in ileal pouch isolated of mice

Detalhes bibliográficos
Autor(a) principal: Ingrid Chaves Cavalcante
Data de Publicação: 2005
Tipo de documento: Dissertação
Idioma: por
Título da fonte: Biblioteca Digital de Teses e Dissertações da UFC
Texto Completo: http://www.teses.ufc.br/tde_busca/arquivo.php?codArquivo=84
Resumo: C. difficile toxin A (TxA) plays an important pathogenic role in antibiotic-induced diarrhea and pseudomembranous colitis, a condition characterized by intense mucosal inflammation and secretion. Agonist activity at A2A adenosine receptors (A2A ARs) attenuates inflammation and damage in many tissues. This study evaluated the effect of a new selective A2A AR agonist (4-{3-[6-amino-9-(5-cyclopropylcarbamoyl-3,4-dihydroxytetrahydrofuran-2-yl)-9H-purin-2-yl]prop-2-ynyl}piperidine-1-carboxylic acid methyl ester; ATL313) on TxA-induced enteritis in murine ileal loops. ATL313 (0.05-5 nM) and/or the A2A AR antagonist (ZM241385; 5 nM) or PBS were injected inside ileal loops immediately prior to challenge with TxA (1-10 mg/loop) or PBS. Intestinal fluid volume/length and weight/length ratios were calculated 3 h later. Ileal tissue samples were collected for measurement of myeloperoxidase (MPO) content, evaluation of ADA activity, for histopathology and apoptotic immunohistochemistry (ApopTagÃ) and for assessment of TNF-&#945; levels by ELISA. TxA (1-10 Âg/loop) significantly (p<0.05) increased volume/length and weight/length, reaching maximum values at 5Âg/loop dosage. ATL313 (5 nM) treatment significantly (p<0.05) reduced TxA-induced volume/length and weight/length, as well as prevented mucosal disruption and TxA-induced apoptosis. These protective effects were reversed by ZM241385 (5 nM), the A2A AR antagonist. ATL313 (5 nM) also reduced neutrophil infiltration, as measured by MPO content; reduced the toxin A-induced increase in ADA activity. Prior to the challenge with TxA, a systemic injection of fucoidin, but not PBS, also reduced tissue destruction and toxin A-induced increase in ADA activity. In conclusion, the A2A AR agonist ATL313 has a great antiinflammatory effect in TxA-induced mice enteritis, significantly reducing tissue destruction and ADA activity. In addition, our data suggested that TxA-induced increase in ADA activity and tissue damage in murine ileal loops are related to the neutrophil infiltration induced by this toxin.
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spelling info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/masterThesisStudy of a new adenosine receptor A2A agonist, ATL313, on Clostridium difficile toxin A-induced enteritis in ileal pouch isolated of miceEstudo do efeito de um novo agonista do receptor a2a de adenosina, atl313, sobre a enterite induzida pela toxina a do clostridium difficile em alÃa ileal isolada de camundongos2005-04-29Gerly Anne de Castro Brito24198846391http://lattes.cnpq.br/8991062042568398ArmÃnio Aguiar dos Santos21268789372http://lattes.cnpq.br/6367176618425888 Marcus Raimundo Vale07574169420http://buscatextual.cnpq.br/buscatextual/visualizacv.jsp?id=K4783813Z067871747304Ingrid Chaves CavalcanteUniversidade Federal do CearÃPrograma de PÃs-GraduaÃÃo em FarmacologiaUFCBRClostridium difficile Toxina A InflamaÃÃo Enterite Adenosina NeutrÃfiloClostridium difficile Toxin Type A Inflammation Enteritis Adenosine Neutrophil ActivationFARMACOLOGIAC. difficile toxin A (TxA) plays an important pathogenic role in antibiotic-induced diarrhea and pseudomembranous colitis, a condition characterized by intense mucosal inflammation and secretion. Agonist activity at A2A adenosine receptors (A2A ARs) attenuates inflammation and damage in many tissues. This study evaluated the effect of a new selective A2A AR agonist (4-{3-[6-amino-9-(5-cyclopropylcarbamoyl-3,4-dihydroxytetrahydrofuran-2-yl)-9H-purin-2-yl]prop-2-ynyl}piperidine-1-carboxylic acid methyl ester; ATL313) on TxA-induced enteritis in murine ileal loops. ATL313 (0.05-5 nM) and/or the A2A AR antagonist (ZM241385; 5 nM) or PBS were injected inside ileal loops immediately prior to challenge with TxA (1-10 mg/loop) or PBS. Intestinal fluid volume/length and weight/length ratios were calculated 3 h later. Ileal tissue samples were collected for measurement of myeloperoxidase (MPO) content, evaluation of ADA activity, for histopathology and apoptotic immunohistochemistry (ApopTagÃ) and for assessment of TNF-&#945; levels by ELISA. TxA (1-10 Âg/loop) significantly (p<0.05) increased volume/length and weight/length, reaching maximum values at 5Âg/loop dosage. ATL313 (5 nM) treatment significantly (p<0.05) reduced TxA-induced volume/length and weight/length, as well as prevented mucosal disruption and TxA-induced apoptosis. These protective effects were reversed by ZM241385 (5 nM), the A2A AR antagonist. ATL313 (5 nM) also reduced neutrophil infiltration, as measured by MPO content; reduced the toxin A-induced increase in ADA activity. Prior to the challenge with TxA, a systemic injection of fucoidin, but not PBS, also reduced tissue destruction and toxin A-induced increase in ADA activity. In conclusion, the A2A AR agonist ATL313 has a great antiinflammatory effect in TxA-induced mice enteritis, significantly reducing tissue destruction and ADA activity. In addition, our data suggested that TxA-induced increase in ADA activity and tissue damage in murine ileal loops are related to the neutrophil infiltration induced by this toxin. A toxina A do Clostridium difficile (TxA) desempenha um importante papel na patogÃnese da diarrÃia induzida por antibiÃticos e na colite pseudomembranosa, uma condiÃÃo caracterizada por intensa secreÃÃo e inflamaÃÃo da mucosa. A estimulaÃÃo de receptores A2A da adenosina reduz a inflamaÃÃo e o dano tecidual. Neste estudo, avaliou-se o efeito de um novo agonista seletivo para receptores A2A da adenosina (metil Ãster do Ãcido 4-{3-[6-amino-9-(5-ciclopropilcarbamoil-3,4- dihidroxitetrahidrofuran-2-il)-9H-purin-2-il]prop-2-inil}piperidina-1-carboxÃlico; ATL313) na enterite induzida pela TxA em alÃas ileais de camundongos. O ATL313 (0,05-5 nM) e/ou o antagonista dos receptores A2A da adenosina (ZM241385; 5 nM) ou PBS foram injetados em alÃas ileais imediatamente antes da injeÃÃo de TxA (1-10 Âg/alÃa) ou PBS. As razÃes volume de secreÃÃo/comprimento da alÃa e peso/comprimento da alÃa foram calculadas 3h depois. Amostras de tecido foram coletadas para dosagem de atividade de mieloperoxidade (MPO), atividade de ADA, histopatologia, imunohistoquÃmica para apoptose (ApopTag_) e dosagem de TNF-a_ por ELISA. A injeÃÃo de TxA (1-10 Âg) nas alÃas ileais aumentou significativamente (p<0,05) as razÃes volume de secreÃÃo/comprimento da alÃa e peso/comprimento da alÃa com pico em 5Âg. O tratamento das alÃas com ATL313 (5 nM) reduziu significativamente (p<0,05) a secreÃÃo e o edema, preveniu a destruiÃÃo da mucosa e a apoptose induzidos por TxA. Tais efeitos protetores foram revertidos pelo antagonista dos receptores A2A de adenosina, o ZM241385 (5 nM). O tratamento com ATL313 (5 nM), reduziu ainda a infiltraÃÃo neutrofÃlica, avaliada pela dosagem de MPO, e reduziu o aumento da atividade de ADA induzidos pela TxA, bem como a dosagem de TNF-a no tecido das alÃas ileais. O prÃ-tratamento sistÃmico com fucoidina, mas nÃo com PBS, tambÃm reduziu o dano na mucosa e atividade de ADA no tecido das alÃas ileais tratadas com TxA. Assim, conclui-se que na enterite induzida pela TxA em camundongos, o agonista dos receptores A2A da adenosina (ATL313) possui um potente efeito antiinflamatÃrio, reduzindo consideravelmente a lesÃo tecidual e a atividade de ADA. Nossos resultados tambÃm indicam que o aumento da atividade de ADA e o dano tecidual induzido pela TxA em alÃa ileal de camundongos està relacionado com a infiltraÃÃo neutrofÃlica induzida por esta toxina. Conselho Nacional de Desenvolvimento CientÃfico e TecnolÃgicohttp://www.teses.ufc.br/tde_busca/arquivo.php?codArquivo=84application/pdfinfo:eu-repo/semantics/openAccessporreponame:Biblioteca Digital de Teses e Dissertações da UFCinstname:Universidade Federal do Cearáinstacron:UFC2019-01-21T11:13:10Zmail@mail.com -
dc.title.en.fl_str_mv Study of a new adenosine receptor A2A agonist, ATL313, on Clostridium difficile toxin A-induced enteritis in ileal pouch isolated of mice
dc.title.alternative.pt.fl_str_mv Estudo do efeito de um novo agonista do receptor a2a de adenosina, atl313, sobre a enterite induzida pela toxina a do clostridium difficile em alÃa ileal isolada de camundongos
title Study of a new adenosine receptor A2A agonist, ATL313, on Clostridium difficile toxin A-induced enteritis in ileal pouch isolated of mice
spellingShingle Study of a new adenosine receptor A2A agonist, ATL313, on Clostridium difficile toxin A-induced enteritis in ileal pouch isolated of mice
Ingrid Chaves Cavalcante
Clostridium difficile
Toxina A
InflamaÃÃo
Enterite
Adenosina
NeutrÃfilo
Clostridium difficile
Toxin Type A
Inflammation
Enteritis
Adenosine
Neutrophil Activation
FARMACOLOGIA
title_short Study of a new adenosine receptor A2A agonist, ATL313, on Clostridium difficile toxin A-induced enteritis in ileal pouch isolated of mice
title_full Study of a new adenosine receptor A2A agonist, ATL313, on Clostridium difficile toxin A-induced enteritis in ileal pouch isolated of mice
title_fullStr Study of a new adenosine receptor A2A agonist, ATL313, on Clostridium difficile toxin A-induced enteritis in ileal pouch isolated of mice
title_full_unstemmed Study of a new adenosine receptor A2A agonist, ATL313, on Clostridium difficile toxin A-induced enteritis in ileal pouch isolated of mice
title_sort Study of a new adenosine receptor A2A agonist, ATL313, on Clostridium difficile toxin A-induced enteritis in ileal pouch isolated of mice
author Ingrid Chaves Cavalcante
author_facet Ingrid Chaves Cavalcante
author_role author
dc.contributor.advisor1.fl_str_mv Gerly Anne de Castro Brito
dc.contributor.advisor1ID.fl_str_mv 24198846391
dc.contributor.advisor1Lattes.fl_str_mv http://lattes.cnpq.br/8991062042568398
dc.contributor.referee1.fl_str_mv ArmÃnio Aguiar dos Santos
dc.contributor.referee1ID.fl_str_mv 21268789372
dc.contributor.referee1Lattes.fl_str_mv http://lattes.cnpq.br/6367176618425888
dc.contributor.referee2.fl_str_mv Marcus Raimundo Vale
dc.contributor.referee2ID.fl_str_mv 07574169420
dc.contributor.referee2Lattes.fl_str_mv http://buscatextual.cnpq.br/buscatextual/visualizacv.jsp?id=K4783813Z0
dc.contributor.authorID.fl_str_mv 67871747304
dc.contributor.author.fl_str_mv Ingrid Chaves Cavalcante
contributor_str_mv Gerly Anne de Castro Brito
ArmÃnio Aguiar dos Santos
Marcus Raimundo Vale
dc.subject.por.fl_str_mv Clostridium difficile
Toxina A
InflamaÃÃo
Enterite
Adenosina
NeutrÃfilo
topic Clostridium difficile
Toxina A
InflamaÃÃo
Enterite
Adenosina
NeutrÃfilo
Clostridium difficile
Toxin Type A
Inflammation
Enteritis
Adenosine
Neutrophil Activation
FARMACOLOGIA
dc.subject.eng.fl_str_mv Clostridium difficile
Toxin Type A
Inflammation
Enteritis
Adenosine
Neutrophil Activation
dc.subject.cnpq.fl_str_mv FARMACOLOGIA
dc.description.sponsorship.fl_txt_mv Conselho Nacional de Desenvolvimento CientÃfico e TecnolÃgico
dc.description.abstract.por.fl_txt_mv C. difficile toxin A (TxA) plays an important pathogenic role in antibiotic-induced diarrhea and pseudomembranous colitis, a condition characterized by intense mucosal inflammation and secretion. Agonist activity at A2A adenosine receptors (A2A ARs) attenuates inflammation and damage in many tissues. This study evaluated the effect of a new selective A2A AR agonist (4-{3-[6-amino-9-(5-cyclopropylcarbamoyl-3,4-dihydroxytetrahydrofuran-2-yl)-9H-purin-2-yl]prop-2-ynyl}piperidine-1-carboxylic acid methyl ester; ATL313) on TxA-induced enteritis in murine ileal loops. ATL313 (0.05-5 nM) and/or the A2A AR antagonist (ZM241385; 5 nM) or PBS were injected inside ileal loops immediately prior to challenge with TxA (1-10 mg/loop) or PBS. Intestinal fluid volume/length and weight/length ratios were calculated 3 h later. Ileal tissue samples were collected for measurement of myeloperoxidase (MPO) content, evaluation of ADA activity, for histopathology and apoptotic immunohistochemistry (ApopTagÃ) and for assessment of TNF-&#945; levels by ELISA. TxA (1-10 Âg/loop) significantly (p<0.05) increased volume/length and weight/length, reaching maximum values at 5Âg/loop dosage. ATL313 (5 nM) treatment significantly (p<0.05) reduced TxA-induced volume/length and weight/length, as well as prevented mucosal disruption and TxA-induced apoptosis. These protective effects were reversed by ZM241385 (5 nM), the A2A AR antagonist. ATL313 (5 nM) also reduced neutrophil infiltration, as measured by MPO content; reduced the toxin A-induced increase in ADA activity. Prior to the challenge with TxA, a systemic injection of fucoidin, but not PBS, also reduced tissue destruction and toxin A-induced increase in ADA activity. In conclusion, the A2A AR agonist ATL313 has a great antiinflammatory effect in TxA-induced mice enteritis, significantly reducing tissue destruction and ADA activity. In addition, our data suggested that TxA-induced increase in ADA activity and tissue damage in murine ileal loops are related to the neutrophil infiltration induced by this toxin.
A toxina A do Clostridium difficile (TxA) desempenha um importante papel na patogÃnese da diarrÃia induzida por antibiÃticos e na colite pseudomembranosa, uma condiÃÃo caracterizada por intensa secreÃÃo e inflamaÃÃo da mucosa. A estimulaÃÃo de receptores A2A da adenosina reduz a inflamaÃÃo e o dano tecidual. Neste estudo, avaliou-se o efeito de um novo agonista seletivo para receptores A2A da adenosina (metil Ãster do Ãcido 4-{3-[6-amino-9-(5-ciclopropilcarbamoil-3,4- dihidroxitetrahidrofuran-2-il)-9H-purin-2-il]prop-2-inil}piperidina-1-carboxÃlico; ATL313) na enterite induzida pela TxA em alÃas ileais de camundongos. O ATL313 (0,05-5 nM) e/ou o antagonista dos receptores A2A da adenosina (ZM241385; 5 nM) ou PBS foram injetados em alÃas ileais imediatamente antes da injeÃÃo de TxA (1-10 Âg/alÃa) ou PBS. As razÃes volume de secreÃÃo/comprimento da alÃa e peso/comprimento da alÃa foram calculadas 3h depois. Amostras de tecido foram coletadas para dosagem de atividade de mieloperoxidade (MPO), atividade de ADA, histopatologia, imunohistoquÃmica para apoptose (ApopTag_) e dosagem de TNF-a_ por ELISA. A injeÃÃo de TxA (1-10 Âg) nas alÃas ileais aumentou significativamente (p<0,05) as razÃes volume de secreÃÃo/comprimento da alÃa e peso/comprimento da alÃa com pico em 5Âg. O tratamento das alÃas com ATL313 (5 nM) reduziu significativamente (p<0,05) a secreÃÃo e o edema, preveniu a destruiÃÃo da mucosa e a apoptose induzidos por TxA. Tais efeitos protetores foram revertidos pelo antagonista dos receptores A2A de adenosina, o ZM241385 (5 nM). O tratamento com ATL313 (5 nM), reduziu ainda a infiltraÃÃo neutrofÃlica, avaliada pela dosagem de MPO, e reduziu o aumento da atividade de ADA induzidos pela TxA, bem como a dosagem de TNF-a no tecido das alÃas ileais. O prÃ-tratamento sistÃmico com fucoidina, mas nÃo com PBS, tambÃm reduziu o dano na mucosa e atividade de ADA no tecido das alÃas ileais tratadas com TxA. Assim, conclui-se que na enterite induzida pela TxA em camundongos, o agonista dos receptores A2A da adenosina (ATL313) possui um potente efeito antiinflamatÃrio, reduzindo consideravelmente a lesÃo tecidual e a atividade de ADA. Nossos resultados tambÃm indicam que o aumento da atividade de ADA e o dano tecidual induzido pela TxA em alÃa ileal de camundongos està relacionado com a infiltraÃÃo neutrofÃlica induzida por esta toxina.
description C. difficile toxin A (TxA) plays an important pathogenic role in antibiotic-induced diarrhea and pseudomembranous colitis, a condition characterized by intense mucosal inflammation and secretion. Agonist activity at A2A adenosine receptors (A2A ARs) attenuates inflammation and damage in many tissues. This study evaluated the effect of a new selective A2A AR agonist (4-{3-[6-amino-9-(5-cyclopropylcarbamoyl-3,4-dihydroxytetrahydrofuran-2-yl)-9H-purin-2-yl]prop-2-ynyl}piperidine-1-carboxylic acid methyl ester; ATL313) on TxA-induced enteritis in murine ileal loops. ATL313 (0.05-5 nM) and/or the A2A AR antagonist (ZM241385; 5 nM) or PBS were injected inside ileal loops immediately prior to challenge with TxA (1-10 mg/loop) or PBS. Intestinal fluid volume/length and weight/length ratios were calculated 3 h later. Ileal tissue samples were collected for measurement of myeloperoxidase (MPO) content, evaluation of ADA activity, for histopathology and apoptotic immunohistochemistry (ApopTagÃ) and for assessment of TNF-&#945; levels by ELISA. TxA (1-10 Âg/loop) significantly (p<0.05) increased volume/length and weight/length, reaching maximum values at 5Âg/loop dosage. ATL313 (5 nM) treatment significantly (p<0.05) reduced TxA-induced volume/length and weight/length, as well as prevented mucosal disruption and TxA-induced apoptosis. These protective effects were reversed by ZM241385 (5 nM), the A2A AR antagonist. ATL313 (5 nM) also reduced neutrophil infiltration, as measured by MPO content; reduced the toxin A-induced increase in ADA activity. Prior to the challenge with TxA, a systemic injection of fucoidin, but not PBS, also reduced tissue destruction and toxin A-induced increase in ADA activity. In conclusion, the A2A AR agonist ATL313 has a great antiinflammatory effect in TxA-induced mice enteritis, significantly reducing tissue destruction and ADA activity. In addition, our data suggested that TxA-induced increase in ADA activity and tissue damage in murine ileal loops are related to the neutrophil infiltration induced by this toxin.
publishDate 2005
dc.date.issued.fl_str_mv 2005-04-29
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/masterThesis
status_str publishedVersion
format masterThesis
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language por
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dc.publisher.none.fl_str_mv Universidade Federal do CearÃ
dc.publisher.program.fl_str_mv Programa de PÃs-GraduaÃÃo em Farmacologia
dc.publisher.initials.fl_str_mv UFC
dc.publisher.country.fl_str_mv BR
publisher.none.fl_str_mv Universidade Federal do CearÃ
dc.source.none.fl_str_mv reponame:Biblioteca Digital de Teses e Dissertações da UFC
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reponame_str Biblioteca Digital de Teses e Dissertações da UFC
collection Biblioteca Digital de Teses e Dissertações da UFC
instname_str Universidade Federal do Ceará
instacron_str UFC
institution UFC
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