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dc.rights.licenseReconocimiento-NoComercial-SinObraDerivada 4.0 Internacional. (CC BY-NC-ND)-
dc.contributor.authorChiesa, Camilaes
dc.contributor.authorPerez-Torrado, Valentinaes
dc.contributor.authorMezzano, Rossanaes
dc.contributor.authorVazquez, Carolinaes
dc.contributor.authorCriscuolo, Zelikaes
dc.contributor.authorSerra, Marceloes
dc.contributor.authorMarambaud, Philippees
dc.contributor.authorEscande, Carloses
dc.contributor.authorRuiz, Santiagoes
dc.date.accessioned2026-06-08T15:56:42Z-
dc.date.available2026-06-08T15:56:42Z-
dc.date.issued2026-06-03-
dc.identifier.urihttps://hdl.handle.net/20.500.12381/5572-
dc.description.abstractObjective HHT is caused by loss-of-function mutations in BMP9-ALK1-SMAD signaling in endothelial cells (ECs) and leads to arteriovenous malformations (AVMs). Using a drug repurposing approach, we sought to identify SMAD1/5/8 activators in ECs capable of ameliorating HHT pathology. Here, we identified nitazoxanide and investigated its therapeutic potential. Methods Cell lines and human ECs were treated with nitazoxanide. SMAD1/5/8 activation, ID1 expression and mTOR signaling were assessed by Western blot, immunofluorescence, and flow cytometry. Mechanistic studies included pharmacological inhibition and siRNA-mediated silencing. In vivo efficacy was evaluated in BMP9/10-immunoblocked neonatal mice by analyzing retinal vascular abnormalities and pathway modulation. Results Nitazoxanide induced a robust, dose-dependent increase in SMAD1/5/8 phosphorylation and ID1 expression, with maximal effects at 1 μM, without affecting cell viability. This effect was ALK1-dependent, as pharmacological inhibition or genetic silencing of ALK1 abolished pathway activation, whereas ALK2 silencing had no effect. Under pro-angiogenic conditions, nitazoxanide sustained SMAD1/5/8 activation and inhibited mTOR signaling, as indicated by reduced S6 phosphorylation. In vivo, nitazoxanide significantly reduced AVM number and size, venous dilation, and hypervascularization in the retina. These effects were associated with restoration of SMAD1/5/8 signaling in the lung and normalization of mTOR activity in the liver. Importantly, nitazoxanide restored SMAD signaling in BOECs derived from HHT patients carrying ALK1 or SMAD4 mutations. Conclusion Nitazoxanide prevents HHT vascular pathology in vivo by activating SMAD1/5/8 signaling and inhibiting mTOR. These findings support its potential as a therapeutic strategy for HHT.es
dc.description.sponsorshipAgencia Nacional de Investigación e Innovaciónes
dc.description.sponsorshipBrain vascular malformation Consorsiumes
dc.description.sponsorshipNational Institute of Healthes
dc.language.isoenges
dc.rightsAcceso abierto*
dc.sourceHHT International Scientific Conferencees
dc.subjectvascular pathologyes
dc.subjectBMP9-ALK1-SMAD signalinges
dc.subjectendothelial celles
dc.subjectHereditary Hemorrhagic Telangiectasiaes
dc.subjectarteriovenous malformationes
dc.titleNitazoxanide activates BMP9-ALK1-SMAD signaling cascade and improves HHT vascular pathology.es
dc.typeDocumento de conferenciaes
dc.subject.aniiCiencias Médicas y de la Salud
dc.subject.aniiMedicina Clínica
dc.subject.aniiSistemas Cardíaco y Cardiovascular
dc.identifier.aniiFMV_1_2021_1_166595es
dc.type.versionEnviadoes
dc.anii.institucionresponsableInstitut Pasteur de Montevideoes
dc.anii.subjectcompleto//Ciencias Médicas y de la Salud/Medicina Clínica/Sistemas Cardíaco y Cardiovasculares
Aparece en las colecciones: Institut Pasteur de Montevideo

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