154 results on '"Sosa-Estani S"'
Search Results
2. Efficacy and safety assessment of different dosage of benznidazol for the treatment of Chagas disease in chronic phase in adults (MULTIBENZ study): study protocol for a multicenter randomized Phase II superiority clinical trial
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Molina-Morant, D., Fernández, M. L., Bosch-Nicolau, P., Sulleiro, E., Bangher, M., Salvador, F., Sanchez-Montalva, A., Ribeiro, A. L. P., de Paula, A. M. B., Eloi, S., Correa-Oliveira, R., Villar, J. C., Sosa-Estani, S., and Molina, I.
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- 2020
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3. Interruption of mother-to-child transmission and detection and treatment of children of infected mothers as a contribution to eradicate Chagas disease in Europe
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Sosa-Estani, S., primary, Alvar, J., additional, Sancho, J., additional, Aparicio Azcárraga, P., additional, Ciscar, M., additional, Gold, S., additional, Labrador Cañadas, M.V., additional, Pécoul, B., additional, Rivero, M., additional, and Gerardo Castellanos, L., additional
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- 2021
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4. Frequency of the congenital transmission of Trypanosoma cruzi: a systematic review and meta-analysis
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Howard, E J, Xiong, X, Carlier, Y, Sosa-Estani, S, and Buekens, P
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- 2014
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5. Efficacy and safety assessment of different dosage of benznidazol for the treatment of Chagas disease in chronic phase in adults (MULTIBENZ study) : study protocol for a multicenter randomized Phase II non-inferiority clinical trial
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Molina-Morant, D., Fernández, M. L., Bosch-Nicolau, Pau, Sulleiro, Elena, Bangher, M., Salvador, F., Sanchez-Montalva, A., Ribeiro, A. L. P., de Paula, A. M. B., Eloi, S., Correa-Oliveira, Rodrigo, Villar, J. C., Sosa-Estani, S., Molina Romero, Israel, Universitat Autònoma de Barcelona, Molina-Morant, D., Fernández, M. L., Bosch-Nicolau, Pau, Sulleiro, Elena, Bangher, M., Salvador, F., Sanchez-Montalva, A., Ribeiro, A. L. P., de Paula, A. M. B., Eloi, S., Correa-Oliveira, Rodrigo, Villar, J. C., Sosa-Estani, S., Molina Romero, Israel, and Universitat Autònoma de Barcelona
- Abstract
Chagas disease (CD) continues to be a neglected infectious disease with one of the largest burdens globally. Despite the modest cure rates in adult chronic patients and its safety profile, benznidazole (BNZ) is still the drug of choice. Its current recommended dose is based on nonrandomized studies, and efficacy and safety of the optimal dose of BNZ have been scarcely analyzed in clinical trials. MULTIBENZ is a phase II, randomized, noninferiority, double-blind, multicenter international clinical trial. A total of 240 patients with Trypanosoma CD in the chronic phase will be recruited in four different countries (Argentina, Brazil, Colombia, and Spain). Patients will be randomized to receive BNZ 150 mg/day for 60 days, 400 mg/day for 15 days, or 300 mg/day for 60 days (comparator arm). The primary outcome is the efficacy of three different BNZ therapeutic schemes in terms of dose and duration. Efficacy will be assessed according to the proportion of patients with sustained parasitic load suppression in peripheral blood measured by polymerase chain reaction. The secondary outcomes are related to pharmacokinetics and drug tolerability. The follow-up will be 12 months from randomization to end of study participation. Recruitment was started in April 2018. This is a clinical trial conducted for the assessment of different dose schemes of BNZ compared with the standard treatment regimen for the treatment of CD in the chronic phase. MULTIBENZ may help to clarify which is the most adequate BNZ regimen in terms of efficacy and safety, predicated on sustained parasitic load suppression in peripheral blood. ClinicalTrials.gov, . Registered on 19 June 2017
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- 2020
6. Target product profile for a test for the early assessment of treatment efficacy in chagas disease patients: An expert consensus
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Generalitat de Catalunya, Instituto de Salud Carlos III, National Institutes of Health (US), National Institute of Allergy and Infectious Diseases (US), Ministerio de Economía y Competitividad (España), Ministero della Salute, Alonso-Padillaid, J., Abril, M., de Noya, B.A., Almeida, Igor C., Angheben, A., Jorge, T.A., Chatelain, E., Esteva, Monica, Gascón, Joaquim, Grijalva, M.J., Guhl, F., Hasslochermoreno, A.M., López López, Manuel Carlos, Luquetti, A., Noya, O., Pinazo, M.J., Ramsey, J.M., Ribeiro, I., Ruiz, A.M., Schijman, A.G., Sosa-Estani, S., Thomas, María del Carmen, M., Torrico, F., Zreinid, M., Picado, A., Generalitat de Catalunya, Instituto de Salud Carlos III, National Institutes of Health (US), National Institute of Allergy and Infectious Diseases (US), Ministerio de Economía y Competitividad (España), Ministero della Salute, Alonso-Padillaid, J., Abril, M., de Noya, B.A., Almeida, Igor C., Angheben, A., Jorge, T.A., Chatelain, E., Esteva, Monica, Gascón, Joaquim, Grijalva, M.J., Guhl, F., Hasslochermoreno, A.M., López López, Manuel Carlos, Luquetti, A., Noya, O., Pinazo, M.J., Ramsey, J.M., Ribeiro, I., Ruiz, A.M., Schijman, A.G., Sosa-Estani, S., Thomas, María del Carmen, M., Torrico, F., Zreinid, M., and Picado, A.
- Abstract
descripción no proporcionada por scopus
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- 2020
7. Trypanosoma cruzi Discrete Typing Units in Chagas disease patients from endemic and non-endemic regions of Argentina
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CURA, C. I., LUCERO, R. H., BISIO, M., OSHIRO, E., FORMICHELLI, L. B., BURGOS, J. M., LEJONA, S., BRUSÉS, B. L., HERNÁNDEZ, D. O., SEVERINI, G. V., VELAZQUEZ, E., DUFFY, T., ANCHART, E., LATTES, R., ALTCHEH, J., FREILIJ, H., DIEZ, M., NAGEL, C., VIGLIANO, C., FAVALORO, L., FAVALORO, R. R., MERINO, D. E., SOSA-ESTANI, S., and SCHIJMAN, A. G.
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- 2012
8. Protozoan Diseases: Chagas Disease
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Segura, E.L., primary and Sosa-Estani, S., additional
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- 2008
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9. Soluble platelet selectin (sP-selectin) and soluble vascular cell adhesion molecule-1 (sVCAM-1) decrease during therapy with benznidazole in children with indeterminate form of Chagas' disease
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LAUCELLA, S. A., SEGURA, E. L., RIARTE, A., and SOSA, ESTANI S.
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- 1999
10. Detection of Shiga toxin-producing Escherichia coli by PCR in cattle in Argentina : Evaluation of two procedures
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Gioffré, A, Meichtri, L, Miliwebsky, E, Baschkier, A, Chillemi, G, Romano, M.I, Sosa Estani, S, Cataldi, A, Rodrı́guez, R, and Rivas, M
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- 2002
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11. Advances and challenges in the treatment of Chagas disease - a global perspective
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Sosa-Estani, S., primary
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- 2018
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12. A new pediatric tablet strength of benznidazole for the treatment of chagas disease
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Terlouw, D. J., Alves, F. P., Sosa-Estani, S., Freilij, H., Altcheh, J., Brutus, Laurent, Kiechel, J. R., and Ribeiro, I.
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- 2009
13. Short Report : Use of a rapid test on umbilical cord blood to screen for Trypanosoma cruzi infection in pregnant women in Argentina, Bolivia, Honduras, and Mexico
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Sosa-Estani, S., Gamboa-Leon, M. R., del Cid-Lemus, J., Althahe, F., Alger, J., Almendares, O., Cafferata, M. L., Chippaux, Jean-Philippe, Dumonteil, E., Gibbons, L., Padilla-Raygoza, N., Schneider, D., Belizan, J. M., and Buekens, P.
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parasitic diseases - Abstract
We conducted a cross-sectional study of Chagas disease in five endemic areas in Argentina, Bolivia. Honduras, and Mexico to estimate the prevalence of Trypanosoma cruzi-specific antibodies in pregnant women, and to assess the use of a rapid test (Chagas Stat-Pak) to screen for T. cruzi infection ill the time of delivery. The prevalence of antibodies to T. cruzi measured by enzyme-linked immunosorbent assay (ELISA) in maternal blood was 5.5% (a range of 0.8-28.8% among the countries) in 2,495 women enrolled. Compared with ELISA in maternal blood samples, the Chagas Stat-Pak rapid test sensitivity and specificity in umbilical cord blood were 94.6% and 99.0%, respectively. These results show the ability for a rapid determination of the presence of T. cruzi-specific antibodies in umbilical cord blood as a pragmatic strategy to screen for infection in pregnant women.
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- 2008
14. Towards a Paradigm Shift in the Treatment of Chronic Chagas Disease
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Viotti, R., primary, Alarcón de Noya, B., additional, Araujo-Jorge, T., additional, Grijalva, M. J., additional, Guhl, F., additional, López, M. C., additional, Ramsey, J. M., additional, Ribeiro, I., additional, Schijman, A. G., additional, Sosa-Estani, S., additional, Torrico, F., additional, and Gascon, J., additional
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- 2014
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15. International study to evaluate PCR methods for detection of Trypanosoma cruzi DNA in blood samples from Chagas disease patients.
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Schijman,AG, Bisio,M, Orellana,L, Sued,M, Duffy,T, Mejia Jaramillo,AM, Cura,C, Auter,F, Veron,V, Qvarnstrom,Y, Deborggraeve,S, Hijar,G, Zulantay,I, Lucero,RH, Velazquez,E, Tellez,T, Sanchez Leon,Z, Galvão,L, Nolder,D, Monje Rumi,M, Levi,JE, Ramirez,JD, Zorrilla,P, Flores,M, Jercic,MI, Crisante,G, Añez,N, De Castro,AM, Gonzalez,CI, Acosta Viana,K, Yachelini,P, Torrico,F, Robello,C, Diosque,P, Triana Chavez,O, Aznar,C, Russomando,G, Büscher,P, Assal,A, Guhl,F, Sosa Estani,S, DaSilva,A, Britto,C, Luquetti,A, Ladzins,J, Schijman,AG, Bisio,M, Orellana,L, Sued,M, Duffy,T, Mejia Jaramillo,AM, Cura,C, Auter,F, Veron,V, Qvarnstrom,Y, Deborggraeve,S, Hijar,G, Zulantay,I, Lucero,RH, Velazquez,E, Tellez,T, Sanchez Leon,Z, Galvão,L, Nolder,D, Monje Rumi,M, Levi,JE, Ramirez,JD, Zorrilla,P, Flores,M, Jercic,MI, Crisante,G, Añez,N, De Castro,AM, Gonzalez,CI, Acosta Viana,K, Yachelini,P, Torrico,F, Robello,C, Diosque,P, Triana Chavez,O, Aznar,C, Russomando,G, Büscher,P, Assal,A, Guhl,F, Sosa Estani,S, DaSilva,A, Britto,C, Luquetti,A, and Ladzins,J
- Abstract
A century after its discovery, Chagas disease still represents a major neglected tropical threat. Accurate diagnostics tools as well as surrogate markers of parasitological response to treatment are research priorities in the field. The purpose of this study was to evaluate the performance of PCR methods in detection of Trypanosoma cruzi DNA by an external quality evaluation.
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- 2011
16. Frequency of the congenital transmission ofTrypanosoma cruzi: a systematic review and meta-analysis
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Howard, EJ, primary, Xiong, X, additional, Carlier, Y, additional, Sosa-Estani, S, additional, and Buekens, P, additional
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- 2013
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17. Andes virus associated with hantavirus pulmonary syndrome in northern Argentina and determination of the precise site of infection.
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Gonzalez Della Valle, M, primary, Cortez, J, additional, Edelstein, A, additional, Cacace, M L, additional, Miguel, S, additional, Jurgelenas, G, additional, Padula, P, additional, Martinez, V, additional, and Sosa Estani, S, additional
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- 2002
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18. Efficacy of chemotherapy with benznidazole in children in the indeterminate phase of Chagas' disease.
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Sosa Estani, S, primary, Porcel, B M, additional, Segura, E L, additional, Yampotis, C, additional, Ruiz, A M, additional, and Velazquez, E, additional
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- 1998
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19. Risk factors for sporadic Shiga toxin-producing Escherichia coli infections in children, Argentina.
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Rivas M, Sosa-Estani S, Rangel J, Caletti MG, Vallés P, Roldán CD, Balbi L, Marsano de Mollar MC, Amoedo D, Miliwebsky E, Chinen I, Hoekstra RM, Mead P, Griffin PM, Rivas, Marta, Sosa-Estani, Sergio, Rangel, Josefa, Caletti, Maria G, Vallés, Patricia, and Roldán, Carlos D
- Abstract
We evaluated risk factors for sporadic Shiga toxin-producing Escherichia coli (STEC) infection among children in Argentina. We conducted a prospective case-control study in 2 sites and enrolled 150 case-patients and 299 controls. The median age of case-patients was 1.8 years; 58% were girls. Serotype O157:H7 was the most commonly isolated STEC. Exposures associated with infection included eating undercooked beef, living in or visiting a place with farm animals, and contact with a child <5 years of age with diarrhea. Protective factors included the respondent reporting that he or she always washed hands after handling raw beef and the child eating more than the median number of fruits and vegetables. Many STEC infections in children could be prevented by avoiding consumption of undercooked beef, limiting exposure to farm animals and their environment, not being exposed to children with diarrhea, and washing hands after handling raw beef. [ABSTRACT FROM AUTHOR]
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- 2008
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20. Etiological treatment in patients infected by Trypanosoma cruzi: experiences in Argentina.
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Sosa-Estani S and Segura EL
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- 2006
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21. Towards a Paradigm Shift in the Treatment of Chronic Chagas Disease
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Viotti, R., Alarcón de Noya, B., Araujo-Jorge, T., Grijalva, M. J., Guhl, F., López, M. C., Ramsey, J. M., Ribeiro, I., Schijman, A. G., Sosa-Estani, S., Torrico, F., and Gascon, J.
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ABSTRACTTreatment for Chagas disease with currently available medications is recommended universally only for acute cases (all ages) and for children up to 14 years old. The World Health Organization, however, also recommends specific antiparasite treatment for all chronic-phase Trypanosoma cruzi-infected individuals, even though in current medical practice this remains controversial, and most physicians only prescribe palliative treatment for adult Chagas patients with dilated cardiomyopathy. The present opinion, prepared by members of the NHEPACHA network (Nuevas Herramientas para el Diagnóstico y la Evaluación del Paciente con Enfermedad de Chagas/New Tools for the Diagnosis and Evaluation of Chagas Disease Patients), reviews the paradigm shift based on clinical and immunological evidence and argues in favor of antiparasitic treatment for all chronic patients. We review the tools needed to monitor therapeutic efficacy and the potential criteria for evaluation of treatment efficacy beyond parasitological cure. Etiological treatment should now be mandatory for all adult chronic Chagas disease patients.
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- 2013
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22. Characterization and Epidemiologic Subtyping of Shiga Toxin–Producing Escherichia coli Strains Isolated from Hemolytic Uremic Syndrome and Diarrhea Cases in Argentina
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Rivas, M., Miliwebsky, E., Chinen, I., Roldán, C.D., Balbi, L., García, B., Fiorilli, G., Sosa-Estani, S., Kincaid, J., Rangel, J., and Griffin, P.M.
- Abstract
Argentina has a high incidence of hemolytic uremic syndrome (HUS); 12.2 cases per 100,000 children younger than 5 years old were reported in 2002. Shiga toxin (Stx)–producing Escherichia coli (STEC) is the primary etiologic agent of HUS, and STEC O157 is the predominant serogroup isolated. The main objective of the present work was to establish the phenotypic and genotypic characteristics of the STEC strains in general isolated from Argentine children during a prospective study and the clonal relatedness of STEC O157:H7 strains using subtyping techniques. One hundred and three STEC strains isolated from 99 children were included. The phenotypic and genotypic features were established, and a polymerase chain reaction–restriction fragment length polymorphism (PCRRFLP) was performed to determine stx2 variants. The clonal relatedness of E. coli O157 isolates was established by phage typing and pulsed-field gel electrophoresis (PFGE). The 103 STEC strains belonged to 18 different serotypes, and 59% were of serotype O157:H7. Stx2 was identified in 90.3%, and stx1 in 9.7%. Among the 61 STEC O157 strains, 93.4% harbored the stx2/stx2vh-a genes; PT4 (39.3%) and PT2 (29.5%) were the predominant phage types. Using PFGE with the enzyme XbaI, a total of 41 patterns with at least 80% similarity were identified, and seven clusters with identical profiles were established. Some of the clusters were further split by PFGE using BlnI as the second enzyme. Isolates with indistinguishable PFGE patterns were with one exception also indistinguishable by phage typing and stx genotyping. These findings confirmed that some isolates were genetically related. However, no epidemiological linkages were identified. STEC strains with different genotypes and belonging to diverse serotypes were isolated in Argentina. Some STEC O157 strains could not be distinguished by applying subtyping techniques such as PFGE and phage typing.
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- 2006
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23. Short report: Use of a rapid test on umbilical cord blood to screen for trypanosoma cruzi infection in pregnant women in Argentina, Bolivia, Honduras, and México
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Sosa-Estani, S., Gamboa-León, M. R., Del Cid-Lemus, J., Althabe, F., Alger, J., Almendares, O., Cafferata, M. L., Chippaux, J. -P, Eric Dumonteil, Gibbons, L., Padilla-Raygoza, N., Schneider, D., Belizán, J. M., Buekens, P., James, M., Garbarino, G., Chahla, R., Postigo-Ignacio, J. R., Santalla, J., Amador, D., Giron, I., Ponce, C., Ponce, E., Zuniga, C., and Gonzalez-Ramirez, C.
24. Use of a rapid test on umbilical cord blood to screen for Trypanosoma cruzi infection in pregnant women in Argentina, Bolivia, Honduras, and Mexico
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Sosa-Estani S, Rubi Gamboa-León, Del Cid-Lemus J, Althabe F, Alger J, Almendares O, Ml, Cafferata, Jp, Chippaux, Dumonteil E, Gibbons L, Padilla-Raygoza N, Schneider D, Jm, Belizán, Buekens P, and Working Group
25. Benznidazol and triazol Research group for nanomedicine and innovation on Chagas disease (BERENICE). A new treatment for Chagas disease
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Molina, I., Sousa-Silva, M., Teresa Vinuesa, Veciana, J., Pedraz, J. L., Correa-Oliveira, R., Sosa-Estani, S., Ferrero, L., Melul, P. M., Esteban, E., and Gainza, E.
26. Diferencias regionales y Síndrome Pulmonar por Hantavirus (enfermedad emergente y tropical en Argentina)
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Sosa-Estani Sergio, Salomón Oscar Daniel, Gómez Adolfo Orlando, Esquivel María Laura, and Segura Elsa Leonor
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Hantavirus ,Surtos de Enfermedades ,Ecosistema ,Salud Pública ,Salud ,Medicine ,Public aspects of medicine ,RA1-1270 - Abstract
Se describen algunos factores que habrían favorecido a caracterizar la expresión del Síndrome Pulmonar por Hantavirus en Argentina. Estos factores muestran diversos orígenes que van desde los procesos de ocupación del espacio y de producción, la estructura laboral, el patrón de migración humana, la etnia, la dinámica de reservorios y su relación con los tipos de virus, y el comportamiento del hombre. Estos factores se expresan en tres marcos ecológicos asociados a diferentes regiones geográficas de Argentina: 1) Noroeste, 2) Central (Pampa húmeda) y 3) Sur Andina. Este complejo escenario obliga a abordar con la misma complejidad las investigaciones, para identificar determinantes primarios, biológicos, sociales y ambientales, causales de salud o enfermedad en su estrecha interacción y no individualmente. Este abordaje permitirá diseñar estrategias apropiadas para mejorar las condiciones de salud. Las mismas deberían ser diseñadas y transferidas por equipos transdisciplinarios de investigación, donde la participación de la comunidad desde las primeras etapas de desarrollo es esencial para la sustentabilidad de la estrategia.
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- 2001
27. Tegumentary leishmaniasis in Northern Argentina: distribution of infection and disease, in three municipalities of Salta, 1990-1992
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Sosa-Estani Sergio, Segura Elsa Leonor, Salomón Oscar Daniel, Gómez Adolfo, Peralta Mario, Coutada Virgilio, and Ruiz Luis Medina
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Tegumentary leishmaniasis ,Leishmaniasis ,Arctic medicine. Tropical medicine ,RC955-962 - Abstract
This work describes the epidemiological pattern of tegumentary leishmaniasis in an area north of Salta, Argentina. The prevalence and incidence were estimated by means of a cross-sectional study and two follow-up studies during two consecutive years. The Montenegro Skin Test (MST) was administered to 7336 subjects at baseline. The prevalence and incidence between 1990 and 1992 of infection (MST reactive) was 38? persons and 4.5? persons/year respectively. The prevalence and incidence of tegumentary leishmaniasis (presence of clinical signs) was 1.8? and 0.8? persons/year, respectively. A physical examination performed on 264 patients with MST reactive during three years revealed that 130 cases (49.2%) had some evident sign of infection (scar and/or lesion), with a clinical presentation compatible with leishmaniasis. Our study demonstrated that after the epidemic outbreak of 1985 the transmission in the study area returned to endemic levels in 1992, and also demonstrated the presence of the asymptomatic infection in the area.
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- 2000
28. Critical analysis of Chagas disease treatment in different countries
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Andrea Angheben, Sergio Sosa-Estani, Fernanda de Souza Nogueira Sardinha Mendes, Sheba Meymandi, Israel Molina, José A. Pérez-Molina, Institut Català de la Salut, [de Souza Nogueira Sardinha Mendes F] Fundação Oswaldo Cruz-Fiocruz, Instituto Nacional de Infectologia Evandro Chagas, Rio de Janeiro, RJ, Brasil. [Perez-Molina JA] Ramón y Cajal University Hospital, Instituto Ramón y Cajal de Investigación Sanitaria, Infectious Diseases Department, National Referral Unit for Tropical Diseases, Madrid, Spain. [Angheben A] Istituto di Ricovero e Cura a Carattere Scientifico Sacro Cuore Don Calabria Hospital Department of Infectious - Tropical Diseases and Microbiology, Negrar di Valpolicella, Verona, Italy. [Meymandi SK] University of California, Center of Excellence for Chagas Disease at Olive View, Los Angeles, CA, US. [Sosa-Estani S] Drugs for Neglected Diseases initiative, Rio de Janeiro, RJ, Brasil. National Scientific and Technical Research Council, Epidemiology and Public Health Research Center, Buenos Aires, Argentina. [Molina I] Servei de Malalties Infeccioses, Vall d’Hebron Hospital Universitari, Barcelona, Spain. Programa de Salut Internacional de l’Institut Català de la Salut, Barcelona, Spain. Fundação Oswaldo Cruz-Fiocruz, Instituto René Rachou, Laboratório de Triatomíneos e Epidemiologia da Doença de Chagas, Belo Horizonte, MG, Brasil, and Vall d'Hebron Barcelona Hospital Campus
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Microbiology (medical) ,Chagas disease ,Otros calificadores::Otros calificadores::/farmacoterapia [Otros calificadores] ,Disease ,nifurtimox ,Other subheadings::Other subheadings::/drug therapy [Other subheadings] ,Geographic Locations::Europe [GEOGRAPHICALS] ,atención a la salud (salud pública)::prestación sanitaria::tratamiento de las enfermedades [SALUD PÚBLICA] ,Malalties - Presa de decisions ,enfermedades parasitarias::infecciones por protozoos::infecciones por Euglenozoa::tripanosomiasis::enfermedad de Chagas [ENFERMEDADES] ,Globalization ,Political science ,Development economics ,medicine ,Humans ,Chagas Disease ,benznidazole ,treatment ,Social environment ,medicine.disease ,Europe ,Health Care (Public Health)::Delivery of Health Care::Disease Management [PUBLIC HEALTH] ,localizaciones geográficas::Europa (continente) [DENOMINACIONES GEOGRÁFICAS] ,Americas ,Europa ,Chagas, Malaltia de - Tractament ,Parasitic Diseases::Protozoan Infections::Euglenozoa Infections::Trypanosomiasis::Chagas Disease [DISEASES] - Abstract
Chagas disease; Treatment; Benznidazole Enfermedad de Chagas; Tratamiento; Benznidazol Malaltia de Chagas; Tractament; Benznidazol As a result of globalization and constant migratory flows, Chagas disease is now present in almost all continents. The management and treatment of the disease is often influenced by the economic and social context of the societies that host patients. In this manuscript, we aim to provide a comparative review of approaches to patients with Chagas disease in the Americas and Europe.
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- 2022
29. Human Trypanosoma cruzi chronic infection leads to individual level steady-state parasitemia: Implications for drug-trial optimization in Chagas disease
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Pablo M. De Salazar, Sergio Sosa-Estani, Fernando Salvador, Elena Sulleiro, Adrián Sánchez-Montalvá, Isabela Ribeiro, Israel Molina, Caroline O. Buckee, Institut Català de la Salut, [De Salazar PM, Buckee CO] Center for Communicable Disease Dynamics, Department of Epidemiology, Harvard T.H. Chan School of Public Health, Boston, Massachusetts, United States of America. [Sosa-Estani S] Drugs for Neglected Diseases Initiative. Rio de Janeiro, Brazil. Epidemiology and Public Health Research Centre, CONICET, Buenos Aires, Argentina. [Salvador F, Sánchez-Montalvá A] Servei de Malalties Infeccioses, Vall d’Hebron Hospital Universitari, Barcelona, Spain. International Health Program of the Catalan Institute of Health (PROSICS), Barcelona, Spain. Centro de Investigación Biomédica en Red de Enfermedades Infecciosas (CIBERINFEC), Instituto de Salud Carlos III, Madrid, Spain. [Sulleiro E] Servei de Microbiologia, Vall d’Hebron Hospital Universitari, Barcelona, Spain. International Health Program of the Catalan Institute of Health (PROSICS), Barcelona, Spain. Centro de Investigación Biomédica en Red de Enfermedades Infecciosas (CIBERINFEC), Instituto de Salud Carlos III, Madrid, Spain. [Ribeiro I] Drugs for Neglected Diseases Initiative, Geneve, Switzerland. [Molina I] Servei de Malalties Infeccioses, Vall d’Hebron Hospital Universitari, Barcelona, Spain. International Health Program of the Catalan Institute of Health (PROSICS), Barcelona, Spain. Instituto René RachouFIOCRUZ Minas, Laboratório de Triatomíneos e Epidemiologia da Doença de Chagas, Belo Horizonte, Brazil. Centro de Investigación Biomédica en Red de Enfermedades Infecciosas (CIBERINFEC), Instituto de Salud Carlos III, Madrid, Spain, and Vall d'Hebron Barcelona Hospital Campus
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Clinical Trials as Topic ,Chagas, Malaltia de ,Trypanosoma cruzi ,Public Health, Environmental and Occupational Health ,Sang - Paràsits ,enfermedades parasitarias::parasitemia [ENFERMEDADES] ,Parasitemia ,Real-Time Polymerase Chain Reaction ,enfermedades parasitarias::infecciones por protozoos::infecciones por Euglenozoa::tripanosomiasis::enfermedad de Chagas [ENFERMEDADES] ,Infectious Diseases ,Parasitic Diseases::Parasitemia [DISEASES] ,Humans ,Chagas Disease ,Persistent Infection ,Parasitic Diseases::Protozoan Infections::Euglenozoa Infections::Trypanosomiasis::Chagas Disease [DISEASES] - Abstract
Currently available drugs against Trypanosoma cruzi infection, which causes 12000 deaths annually, have limitations in their efficacy, safety and tolerability. The evaluation of therapeutic responses to available and new compounds is based on parasite detection in the bloodstream but remains challenging because a substantial proportion of infected individuals have undetectable parasitemia even when using diagnostic tools with the highest accuracy. We characterize parasite dynamics which might impact drug efficacy assessments in chronic Chagas by analyzing pre- and post-treatment quantitative-PCR data obtained from blood samples collected regularly over a year. We show that parasitemia remains at a steady-state independently of the diagnostic sensitivity. This steady-state can be probabilistically quantified and robustly predicted at an individual level. Furthermore, individuals can be assigned to categories with distinct parasitological status, allowing a more detailed evaluation of the efficacy outcomes and adjustment for potential biases. Our analysis improves understanding of parasite dynamics and provides a novel background for optimizing future drug efficacy trials in Chagas disease. Trial Registration: original trial registered with ClinicalTrials.gov, number NCT01489228.
- Published
- 2021
30. Randomized Trial of Benznidazole for Chronic Chagas' Cardiomyopathy.
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Morillo, C. A., Marin-Neto, J. A., Avezum, A., Sosa-Estani, S., Rassi Jr., A., Rosas, F., Villena, E., Quiroz, R., Bonilla, R., Britto, C., Guhl, F., Velazquez, E., Bonilla, L., Meeks, B., Rao-Melacini, P., Pogue, J., Mattos, A., Lazdins, J., Rassi, A., and Connolly, S. J.
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- *
CARDIOVASCULAR diseases , *CHRONIC diseases , *IMIDAZOLES , *LONGITUDINAL method , *CARDIOMYOPATHIES , *PARASITES , *POLYMERASE chain reaction , *PROTOZOA , *RESEARCH funding , *TREATMENT effectiveness , *ANTIPROTOZOAL agents , *PROPORTIONAL hazards models , *DISEASE progression , *GENOTYPES , *DISEASE complications , *THERAPEUTICS - Abstract
Background: The role of trypanocidal therapy in patients with established Chagas' cardiomyopathy is unproven.Methods: We conducted a prospective, multicenter, randomized study involving 2854 patients with Chagas' cardiomyopathy who received benznidazole or placebo for up to 80 days and were followed for a mean of 5.4 years. The primary outcome in the time-to-event analysis was the first event of any of the components of the composite outcome of death, resuscitated cardiac arrest, sustained ventricular tachycardia, insertion of a pacemaker or implantable cardioverter-defibrillator, cardiac transplantation, new heart failure, stroke, or other thromboembolic event.Results: The primary outcome occurred in 394 patients (27.5%) in the benznidazole group and in 414 (29.1%) in the placebo group (hazard ratio, 0.93; 95% confidence interval [CI], 0.81 to 1.07; P=0.31). At baseline, a polymerase-chain-reaction (PCR) assay was performed on blood samples obtained from 1896 patients; 60.5% had positive results for Trypanosoma cruzi on PCR. The rates of conversion to negative PCR results (PCR conversion) were 66.2% in the benznidazole group and 33.5% in the placebo group at the end of treatment, 55.4% and 35.3%, respectively, at 2 years, and 46.7% and 33.1%, respectively, at 5 years or more (P<0.001 for all comparisons). The effect of treatment on PCR conversion varied according to geographic region: in Brazil, the odds ratio for PCR conversion was 3.03 (95% CI, 2.12 to 4.34) at 2 years and 1.87 (95% CI, 1.33 to 2.63) at 5 or more years; in Colombia and El Salvador, the odds ratio was 1.33 (95% CI, 0.90 to 1.98) at 2 years and 0.96 (95% CI, 0.63 to 1.45) at 5 or more years; and in Argentina and Bolivia, the odds ratio was 2.63 (95% CI, 1.89 to 3.66) at 2 years and 2.79 (95% CI, 1.99 to 3.92) at 5 or more years (P<0.001 for interaction). However, the rates of PCR conversion did not correspond to effects on clinical outcome (P=0.16 for interaction).Conclusions: Trypanocidal therapy with benznidazole in patients with established Chagas' cardiomyopathy significantly reduced serum parasite detection but did not significantly reduce cardiac clinical deterioration through 5 years of follow-up. (Funded by the Population Health Research Institute and others; ClinicalTrials.gov number, NCT00123916; Current Controlled Trials number, ISRCTN13967269.). [ABSTRACT FROM AUTHOR]- Published
- 2015
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31. A standardized clinical database for research in Chagas disease: The NHEPACHA network.
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González Martínez A, Losada-Galván I, Gabaldón-Figueira JC, Martínez-Peinado N, Saraiva RM, Fernández ML, Ramsey JM, Noya-González O, Alarcón de Noya B, Schijman AG, Berón S, Abril M, Gascón J, Sosa-Estani S, Pinazo MJ, Alonso-Padilla J, and Hasslocher-Moreno AM
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- Humans, Latin America epidemiology, Surveys and Questionnaires, Spain epidemiology, Databases, Factual, Biomedical Research standards, Chagas Disease epidemiology, Chagas Disease drug therapy
- Abstract
The NHEPACHA Iberoamerican Network, founded on the initiative of a group of researchers from Latin American countries and Spain, aims to establish a research framework for Chagas disease that encompasses diagnosis and treatment. For this purpose, the network has created a questionnaire to gather relevant data on epidemiological, clinical, diagnostic, and therapeutic aspects of the disease. This questionnaire was developed based on a consensus of expert members of the network, with the intention of collecting high-quality standardized data, which can be used interchangeably by the different research centers that make up the NHEPACHA network. Furthermore, the network intends to offer a clinical protocol that can be embraced by other researchers, facilitating comparability among published studies, as well as the development of therapeutic response and progression markers., Competing Interests: The authors have declared that no competing interests exist., (Copyright: © 2024 González Martínez et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.)
- Published
- 2024
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32. Efficacy of three benznidazole dosing strategies for adults living with chronic Chagas disease (MULTIBENZ): an international, randomised, double-blind, phase 2b trial.
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Bosch-Nicolau P, Fernández ML, Sulleiro E, Villar JC, Perez-Molina JA, Correa-Oliveira R, Sosa-Estani S, Sánchez-Montalvá A, Del Carmen Bangher M, Moreira OC, Salvador F, Mota Ferreira A, Eloi-Santos SM, Serre-Delcor N, Ramírez JC, Silgado A, Oliveira I, Martín O, Aznar ML, Ribeiro ALP, Almeida PEC, Chamorro-Tojeiro S, Espinosa-Pereiro J, de Paula AMB, Váquiro-Herrera E, Tur C, and Molina I
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- Adult, Humans, Double-Blind Method, Treatment Outcome, Chagas Disease drug therapy, Nitroimidazoles administration & dosage
- Abstract
Background: Treatment with benznidazole for chronic Chagas disease is associated with low cure rates and substantial toxicity. We aimed to compare the parasitological efficacy and safety of 3 different benznidazole regimens in adult patients with chronic Chagas disease., Methods: The MULTIBENZ trial was an international, randomised, double-blind, phase 2b trial performed in Argentina, Brazil, Colombia, and Spain. We included participants aged 18 years and older diagnosed with Chagas disease with two different serological tests and detectable T cruzi DNA by qPCR in blood. Previously treated people, pregnant women, and people with severe cardiac forms were excluded. Participants were randomly assigned 1:1:1, using a balanced block randomisation scheme stratified by country, to receive benznidazole at three different doses: 300 mg/day for 60 days (control group), 150 mg/day for 60 days (low dose group), or 400 mg/day for 15 days (short treatment group). The primary outcome was the proportion of patients with a sustained parasitological negativity by qPCR during a follow-up period of 12 months. The primary safety outcome was the proportion of people who permanently discontinued the treatment. Both primary efficacy analysis and primary safety analysis were done in the intention-to-treat population. The trial is registered with EudraCT, 2016-003789-21, and ClinicalTrials.gov, NCT03191162, and is completed., Findings: From April 20, 2017, to Sept 20, 2020, 245 people were enrolled, and 234 were randomly assigned: 78 to the control group, 77 to the low dose group, and 79 to the short treatment group. Sustained parasitological negativity was observed in 42 (54%) of 78 participants in the control group, 47 (61%) of 77 in the low dose group, and 46 (58%) of 79 in the short treatment group. Odds ratios were 1·41 (95% CI 0·69-2·88; p=0·34) when comparing the low dose and control groups and 1·23 (0·61-2·50; p=0·55) when comparing short treatment and control groups. 177 participants (76%) had an adverse event: 62 (79%) in the control group, 56 (73%) in the low dose group, and 59 (77%) in the short treatment group. However, discontinuations were less frequent in the short treatment group compared with the control group (2 [2%] vs 11 [14%]; OR 0·20, 95% CI 0·04-0·95; p=0·044)., Interpretation: Participants had a similar parasitological responses. However, reducing the usual treatment from 8 weeks to 2 weeks might maintain the same response while facilitating adherence and increasing treatment coverage. These findings should be confirmed in a phase 3 clinical trial., Funding: European Community's 7th Framework Programme., Competing Interests: Declaration of interests We declare no competing interests., (Copyright © 2024 Elsevier Ltd. All rights reserved.)
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- 2024
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33. Efficacy and safety of fexinidazole for treatment of chronic indeterminate Chagas disease (FEXI-12): a multicentre, randomised, double-blind, phase 2 trial.
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Pinazo MJ, Forsyth C, Losada I, Esteban ET, García-Rodríguez M, Villegas ML, Molina I, Crespillo-Andújar C, Gállego M, Ballart C, Ramirez JC, Aden T, Hoerauf A, Pfarr K, Vaillant M, Marques T, Fernandes J, Blum B, Ribeiro I, Sosa-Estani S, Barreira F, and Gascón J
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- Adult, Humans, Adolescent, Young Adult, Middle Aged, Treatment Outcome, Nifurtimox adverse effects, Double-Blind Method, Chagas Disease drug therapy, Trypanosoma cruzi, Nitroimidazoles
- Abstract
Background: More than six million people worldwide, particularly in vulnerable communities in Latin America, are infected with Trypanosoma cruzi, the causative agent of Chagas disease. Only a small portion have access to diagnosis and treatment. Both drugs used to treat this chronic, neglected infection, benznidazole and nifurtimox, were developed more than 50 years ago, and adverse drug reactions during treatment pose a major barrier, causing 20% of patients to discontinue therapy. Fexinidazole proved efficacious in an earlier, interrupted clinical trial, but the doses evaluated were not well tolerated. The present study evaluated fexinidazole at lower doses and for shorter treatment durations., Methods: In this randomised, double-blind, phase 2 trial, we included adult patients (18-60 years old) with confirmed T cruzi infection by serology and PCR and without signs of organ involvement. We evaluated three regimens of fexinidazole-600 mg once daily for 10 days (6·0 g total dose), 1200 mg daily for 3 days (3·6 g), and 600 mg daily for 3 days followed by 1200 mg daily for 4 days (6·6 g)-and compared them with a historical placebo control group (n=47). The primary endpoint was sustained negative results by PCR at end of treatment and on each visit up to four months of follow-up. This study is registered with ClinicalTrials.gov, NCT03587766, and EudraCT, 2016-004905-15., Findings: Between Oct 16, 2017, and Aug 7, 2018, we enrolled 45 patients (n=15 for each group), of whom 43 completed the study. Eight (19%) of 43 fexinidazole-treated patients reached the primary endpoint, compared with six (13%) of 46 in the historical control group. Mean parasite load decreased sharply following treatment but rebounded beginning 10 weeks after treatment. Five participants had seven grade 3 adverse events: carpal tunnel, sciatica, device infection, pneumonia, staphylococcal infection, and joint and device dislocation. Two participants discontinued treatment due to adverse events unrelated to fexinidazole., Interpretation: The fexinidazole regimens in this study had an acceptable safety profile but did not prove effective against T cruzi infection. Development of fexinidazole monotherapy for treating T cruzi infection has been stopped., Funding: The Drugs for Neglected Diseases initiative., Competing Interests: Declaration of interests AH reports being Chair of the German Network against Neglected Tropical Diseases, a German advocacy group to fight neglected tropical diseases. All other authors declare no competing interests., (Copyright © 2024 Elsevier Ltd. All rights reserved.)
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- 2024
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34. Direct evidence gap on fixed versus adjusted-dose benznidazole for adults with chronic Chagas disease without cardiomyopathy: Systematic review and individual patient data meta-analysis.
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Ciapponi A, Barreira F, Perelli L, Bardach A, Gascón J, Molina I, Morillo C, Prado N, Riarte A, Torrico F, Villar JC, Reidel S, Gibbons L, and Sosa-Estani S
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- Adult, Humans, Evidence Gaps, Chagas Disease drug therapy, Trypanosoma cruzi, Cardiomyopathies
- Abstract
Objectives: To determine the comparative efficacy and safety of a fixed dose of benznidazole (BZN) with an adjusted-dose for Trypanosoma cruzi-seropositive adults without cardiomyopathy., Methods: We conducted a systematic review and individual participant data (IPD) meta-analysis following Cochrane methods, and the PRISMA-IPD statement for reporting. Randomised controlled trials (RCTs) allocating participants to fixed or adjusted doses of BZN for T. cruzi-seropositive adults without cardiomyopathy were included. We searched (December 2021) Cochrane, MEDLINE, EMBASE, LILACS and trial registries and contacted Chagas experts. Selection, data extraction, risk of bias assessment using the Cochrane tool, and a GRADE summary of finding tables were performed independently by pairs of reviewers. We conducted a random-effects IPD meta-analysis using the one-stage strategy, or, if that was impossible, the two-stage strategy., Results: Five RCTs (1198 patients) were included, none directly comparing fixed with adjusted doses of BZN. Compared to placebo, BZN therapy was strongly associated with negative qPCR and sustainable parasitological clearance regardless of the type of dose and subgroup analysed. For negative qPCR, the fixed/adjusted rate of odds ratios (ROR
F/A ) was 8.83 (95% CI 1.02-76.48); for sustained parasitological clearance, it was 4.60 (95% CI 0.40-52.51), probably indicating at least non-inferior effect of fixed doses, with no statistically significant interactions by scheme for global and most subgroup estimations. The RORF/A for treatment interruption due to adverse events was 0.44 (95% CI 0.14-1.38), probably indicating no worse tolerance of fixed doses., Conclusions: We found no direct comparison between fixed and adjusted doses of BZN. However, fixed doses versus placebo are probably not inferior to weight-adjusted doses of BZN versus placebo in terms of parasitological efficacy and safety. Network IPD meta-analysis, through indirect comparisons, may well provide the best possible answers in the near future., Registration: The study protocol was registered in PROSPERO (CRD42019120905)., (© 2022 John Wiley & Sons Ltd.)- Published
- 2023
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35. Human Trypanosoma cruzi chronic infection leads to individual level steady-state parasitemia: Implications for drug-trial optimization in Chagas disease.
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De Salazar PM, Sosa-Estani S, Salvador F, Sulleiro E, Sánchez-Montalvá A, Ribeiro I, Molina I, and Buckee CO
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- Humans, Parasitemia parasitology, Persistent Infection, Real-Time Polymerase Chain Reaction, Clinical Trials as Topic, Chagas Disease parasitology, Trypanosoma cruzi genetics
- Abstract
Currently available drugs against Trypanosoma cruzi infection, which causes 12000 deaths annually, have limitations in their efficacy, safety and tolerability. The evaluation of therapeutic responses to available and new compounds is based on parasite detection in the bloodstream but remains challenging because a substantial proportion of infected individuals have undetectable parasitemia even when using diagnostic tools with the highest accuracy. We characterize parasite dynamics which might impact drug efficacy assessments in chronic Chagas by analyzing pre- and post-treatment quantitative-PCR data obtained from blood samples collected regularly over a year. We show that parasitemia remains at a steady-state independently of the diagnostic sensitivity. This steady-state can be probabilistically quantified and robustly predicted at an individual level. Furthermore, individuals can be assigned to categories with distinct parasitological status, allowing a more detailed evaluation of the efficacy outcomes and adjustment for potential biases. Our analysis improves understanding of parasite dynamics and provides a novel background for optimizing future drug efficacy trials in Chagas disease. Trial Registration: original trial registered with ClinicalTrials.gov, number NCT01489228., Competing Interests: The authors have declared that no competing interests exist., (Copyright: © 2022 De Salazar et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.)
- Published
- 2022
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36. Critical analysis of Chagas disease treatment in different countries.
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Mendes FSNS, Perez-Molina JA, Angheben A, Meymandi SK, Sosa-Estani S, and Molina I
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- Americas, Europe, Humans, Chagas Disease drug therapy
- Abstract
As a result of globalization and constant migratory flows, Chagas disease is now present in almost all continents. The management and treatment of the disease is often influenced by the economic and social context of the societies that host patients. In this manuscript, we aim to provide a comparative review of approaches to patients with Chagas disease in the Americas and Europe.
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- 2022
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37. Chagas disease control-surveillance in the Americas: the multinational initiatives and the practical impossibility of interrupting vector-borne Trypanosoma cruzi transmission.
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de Arias AR, Monroy C, Guhl F, Sosa-Estani S, Santos WS, and Abad-Franch F
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- Aged, Americas epidemiology, Animals, Disease Vectors, Female, Humans, Infectious Disease Transmission, Vertical prevention & control, Pregnancy, Chagas Disease epidemiology, Chagas Disease prevention & control, Trypanosoma cruzi
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Chagas disease (CD) still imposes a heavy burden on most Latin American countries. Vector-borne and mother-to-child transmission cause several thousand new infections per year, and at least 5 million people carry Trypanosoma cruzi. Access to diagnosis and medical care, however, is far from universal. Starting in the 1990s, CD-endemic countries and the Pan American Health Organization-World Health Organization (PAHO-WHO) launched a series of multinational initiatives for CD control-surveillance. An overview of the initiatives' aims, achievements, and challenges reveals some key common themes that we discuss here in the context of the WHO 2030 goals for CD. Transmission of T. cruzi via blood transfusion and organ transplantation is effectively under control. T. cruzi, however, is a zoonotic pathogen with 100+ vector species widely spread across the Americas; interrupting vector-borne transmission seems therefore unfeasible. Stronger surveillance systems are, and will continue to be, needed to monitor and control CD. Prevention of vertical transmission demands boosting current efforts to screen pregnant and childbearing-aged women. Finally, integral patient care is a critical unmet need in most countries. The decades-long experience of the initiatives, in sum, hints at the practical impossibility of interrupting vector-borne T. cruzi transmission in the Americas. The concept of disease control seems to provide a more realistic description of what can in effect be achieved by 2030.
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- 2022
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38. The translational challenge in Chagas disease drug development.
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Kratz JM, Gonçalves KR, Romera LM, Moraes CB, Bittencourt-Cunha P, Schenkman S, Chatelain E, and Sosa-Estani S
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- Drug Development, Drug Discovery, Humans, Neglected Diseases drug therapy, Chagas Disease drug therapy, Chagas Disease parasitology, Trypanocidal Agents pharmacology, Trypanocidal Agents therapeutic use, Trypanosoma cruzi
- Abstract
Chagas disease is a neglected tropical disease caused by the protozoan parasite Trypanosoma cruzi. There is an urgent need for safe, effective, and accessible new treatments since the currently approved drugs have serious limitations. Drug development for Chagas disease has historically been hampered by the complexity of the disease, critical knowledge gaps, and lack of coordinated R&D efforts. This review covers some of the translational challenges associated with the progression of new chemical entities from preclinical to clinical phases of development, and discusses how recent technological advances might allow the research community to answer key questions relevant to the disease and to overcome hurdles in R&D for Chagas disease.
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- 2022
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39. Geographic Variations in Test Reactivity for the Serological Diagnosis of Trypanosoma cruzi Infection.
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Truyens C, Dumonteil E, Alger J, Cafferata ML, Ciganda A, Gibbons L, Herrera C, Sosa-Estani S, and Buekens P
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- Antibodies, Protozoan, Enzyme-Linked Immunosorbent Assay, Female, Humans, Serologic Tests, Chagas Disease diagnosis, Trypanosoma cruzi
- Abstract
Chagas disease is a neglected disease caused by Trypanosoma cruzi parasites. Most diagnosis is based on serological tests, but the lack of a gold standard test complicates the measurement of test performance. To overcome this limitation, we used samples from a cohort of well-characterized T. cruzi-infected women to evaluate the reactivity of two rapid diagnostic tests and one enzyme-linked immunosorbent assay (ELISA). Our cohort was derived from a previous study on congenital transmission of T. cruzi and consisted of 481 blood/plasma samples from Argentina ( n = 149), Honduras ( n = 228), and Mexico ( n = 104), with at least one positive T. cruzi PCR. Reactivity of the three tests ranged from 70.5% for the Wiener ELISA to 81.0% for the T-Detect and 90.4% for the Stat-Pak rapid tests. Test reactivity varied significantly among countries and was highest in Argentina and lowest in Mexico. When considering at least two reactive serological tests to confirm seropositivity, over 12% of T. cruzi infection cases from Argentina were missed by serological tests, over 21% in Honduras, and an alarming 72% in Mexico. Differences in test performance among countries were not due to differences in parasitemia, but differences in antibody levels against ELISA antigens were observed. Geographic differences in T. cruzi parasite strains as well as genetic differences among human populations both may contribute to the discrepancies in serological testing. Improvements in serological diagnostics for T. cruzi infections are critically needed to ensure an optimum identification of cases.
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- 2021
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40. The Chagas disease study landscape: A systematic review of clinical and observational antiparasitic treatment studies to assess the potential for establishing an individual participant-level data platform.
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Maguire BJ, Dahal P, Rashan S, Ngu R, Boon A, Forsyth C, Strub-Wourgaft N, Chatelain E, Barreira F, Sosa-Estani S, and Guérin PJ
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- Adolescent, Antiparasitic Agents, Chagas Disease parasitology, Child, Child, Preschool, Clinical Trials as Topic, Female, Humans, Male, Observational Studies as Topic, Treatment Outcome, Trypanocidal Agents adverse effects, Trypanosoma cruzi genetics, Trypanosoma cruzi physiology, Young Adult, Chagas Disease drug therapy, Trypanocidal Agents administration & dosage, Trypanosoma cruzi drug effects
- Abstract
Background: Chagas disease (CD), caused by the parasite Trypanosoma cruzi, affects ~6-7 million people worldwide. Significant limitations still exist in our understanding of CD. Harnessing individual participant data (IPD) from studies could support more in-depth analyses to address the many outstanding research questions. This systematic review aims to describe the characteristics and treatment practices of clinical studies in CD and assess the breadth and availability of research data for the potential establishment of a data-sharing platform., Methodology/principal Findings: This review includes prospective CD clinical studies published after 1997 with patients receiving a trypanocidal treatment. The following electronic databases and clinical trial registry platforms were searched: Cochrane Library, PubMed, Embase, LILACS, Scielo, Clintrials.gov, and WHO ICTRP. Of the 11,966 unique citations screened, 109 (0.9%) studies (31 observational and 78 interventional) representing 23,116 patients were included. Diagnosis for patient enrolment required 1 positive test result in 5 (4.6%) studies (2 used molecular method, 1 used molecular and serology, 2 used serology and parasitological methods), 2 in 60 (55.0%), 3 in 14 (12.8%) and 4 or more in 4 (3.7%) studies. A description of treatment regimen was available for 19,199 (83.1%) patients, of whom 14,605 (76.1%) received an active treatment and 4,594 (23.9%) were assigned to a placebo/no-treatment. Of the 14,605 patients who received an active treatment, benznidazole was administered in 12,467 (85.4%), nifurtimox in 825 (5.6%), itraconazole in 284 (1.9%), allopurinol in 251 (1.7%) and other drugs in 286 (1.9%). Assessment of efficacy varied largely and was based primarily on biological outcome; parasitological efficacy relied on serology in 67/85 (78.8%) studies, molecular methods in 52/85 (61.2%), parasitological in 34/85 (40.0%), microscopy in 3/85 (3.5%) and immunohistochemistry in 1/85 (1.2%). The median time at which parasitological assessment was carried out was 79 days [interquartile range (IQR): 30-180] for the first assessment, 180 days [IQR: 60-500] for second, and 270 days [IQR: 18-545] for the third assessment., Conclusions/significance: This review demonstrates the heterogeneity of clinical practice in CD treatment and in the conduct of clinical studies. The sheer volume of potential IPD identified demonstrates the potential for development of an IPD platform for CD and that such efforts would enable in-depth analyses to optimise the limited pharmacopoeia of CD and inform prospective data collection., Competing Interests: The authors have declared that no competing interests exist.
- Published
- 2021
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41. New regimens of benznidazole monotherapy and in combination with fosravuconazole for treatment of Chagas disease (BENDITA): a phase 2, double-blind, randomised trial.
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Torrico F, Gascón J, Barreira F, Blum B, Almeida IC, Alonso-Vega C, Barboza T, Bilbe G, Correia E, Garcia W, Ortiz L, Parrado R, Ramirez JC, Ribeiro I, Strub-Wourgaft N, Vaillant M, and Sosa-Estani S
- Subjects
- Adult, Bolivia, Double-Blind Method, Drug Administration Schedule, Drug Therapy, Combination, Drug-Related Side Effects and Adverse Reactions epidemiology, Drug-Related Side Effects and Adverse Reactions pathology, Female, Humans, Male, Nitroimidazoles adverse effects, Parasite Load, Treatment Outcome, Triazoles adverse effects, Young Adult, Chagas Disease drug therapy, Nitroimidazoles administration & dosage, Triazoles administration & dosage
- Abstract
Background: Current treatment for Chagas disease with the only available drugs, benznidazole or nifurtimox, has substantial limitations, including long treatment duration and safety and tolerability concerns. We aimed to evaluate the efficacy and safety of new benznidazole monotherapy regimens and combinations with fosravuconazole, in the treatment of Chagas disease., Methods: We did a double-blind, double-dummy, phase 2, multicentre, randomised trial in three outpatient units in Bolivia. Adults aged 18-50 years with chronic indeterminate Chagas disease, confirmed by serological testing and positive qualitative PCR results, were randomly assigned (1:1:1:1:1:1:1) to one of seven treatment groups using a balanced block randomisation scheme with an interactive response system. Participants were assigned to benznidazole 300 mg daily for 8 weeks, 4 weeks, or 2 weeks, benznidazole 150 mg daily for 4 weeks, benznidazole 150 mg daily for 4 weeks plus fosravuconazole, benznidazole 300 mg once per week for 8 weeks plus fosravuconazole, or placebo, with a 12-month follow-up period. The primary endpoints were sustained parasitological clearance at 6 months, defined as persistent negative qualitative PCR results from end of treatment, and incidence and severity of treatment-emergent adverse events, serious adverse events, and adverse events leading to treatment discontinuation. Primary efficacy analysis was based on the intention-to-treat and per-protocol populations and secondary efficacy analyses on the per-protocol population. Safety analyses were based on the as-treated population. Recruitment is now closed. This trial is registered with ClinicalTrials.gov, NCT03378661., Findings: Between Nov 30, 2016, and July 27, 2017, we screened 518 patients, and 210 were enrolled and randomised. 30 patients (14%) were assigned to each treatment group. All 210 randomised patients were included in the intention-to-treat population, and 190 (90%) were included in the per-protocol population. In the intention-to-treat analysis, only one (3%) of 30 patients in the placebo group had sustained parasitological clearance at 6 months of follow-up. Sustained parasitological clearance at 6 months was observed in 25 (89%) of 28 patients receiving benznidazole 300 mg daily for 8 weeks (rate difference vs placebo 86% [95% CI 73-99]), 25 (89%) of 28 receiving benznidazole 300 mg daily for 4 weeks (86% [73-99]), 24 (83%) of 29 receiving benznidazole 300 mg daily for 2 weeks (79% [64-95]), 25 (83%) of 30 receiving benznidazole 150 mg daily for 4 weeks (80% [65-95]), 23 (85%) of 28 receiving benznidazole 150 mg daily for 4 weeks plus fosravuconazole (82% [67-97]), and 24 (83%) of 29 receiving benznidazole 300 mg weekly for 8 weeks plus fosravuconazole (79% [64-95]; p<0·0001 for all group comparisons with placebo). Six patients (3%) had ten serious adverse events (leukopenia [n=3], neutropenia [n=2], pyrexia, maculopapular rash, acute cholecystitis, biliary polyp, and breast cancer), eight had 12 severe adverse events (defined as interfering substantially with the patient's usual functions; elevated alanine aminotransferase [n=4], elevated gamma-glutamyltransferase [n=2], elevated aspartate aminotransferase [n=1], neutropenia [n=3], leukopenia [n=1], and breast cancer [n=1]), and 15 (7%) had adverse events that led to treatment discontinuation (most of these were in the groups who received benznidazole 300 mg daily for 8 weeks, benznidazole 300 mg once per week for 8 weeks plus fosravuconazole, and benznidazole 150 mg daily for 4 weeks plus fosravuconazole). No adverse events leading to treatment discontinuation were observed in patients treated with benznidazole 300 mg daily for 2 weeks or placebo. There were no treatment-related deaths., Interpretation: Benznidazole induced effective antiparasitic response, regardless of treatment duration, dose, or combination with fosravuconazole, and was well tolerated in adult patients with chronic Chagas disease. Shorter or reduced regimens of benznidazole could substantially improve treatment tolerability and accessibility, but further studies are needed to confirm these results., Funding: Drugs for Neglected Diseases initiative (DNDi)., Translation: For the Spanish translation of the abstract see Supplementary Materials section., Competing Interests: Declaration of interests We declare no competing interests., (Copyright © 2021 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY NC ND 4.0 license. Published by Elsevier Ltd.. All rights reserved.)
- Published
- 2021
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42. Benznidazole in Chagas disease study: do the data justify progression to phase 3? - Authors' reply.
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Torrico F, Barreira F, Strub-Wourgaft N, Ribeiro I, and Sosa-Estani S
- Subjects
- Humans, Chagas Disease drug therapy, Nitroimidazoles therapeutic use
- Published
- 2021
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43. Prospective multicenter evaluation of real time PCR Kit prototype for early diagnosis of congenital Chagas disease.
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Benatar AF, Danesi E, Besuschio SA, Bortolotti S, Cafferata ML, Ramirez JC, Albizu CL, Scollo K, Baleani M, Lara L, Agolti G, Seu S, Adamo E, Lucero RH, Irazu L, Rodriguez M, Poeylaut-Palena A, Longhi SA, Esteva M, Althabe F, Rojkin F, Bua J, Sosa-Estani S, and Schijman AG
- Subjects
- Adult, Chagas Disease congenital, Early Diagnosis, Female, Humans, Infant, Newborn, Male, Reagent Kits, Diagnostic standards, Real-Time Polymerase Chain Reaction standards, Sensitivity and Specificity, Chagas Disease diagnosis, Real-Time Polymerase Chain Reaction methods
- Abstract
Background: Current algorithm for Congenital Chagas Disease (cCD) diagnosis is unsatisfactory due to low sensitivity of the parasitological methods. Moreover, loss to follow-up precludes final serodiagnosis after nine months of life in many cases. A duplex TaqMan qPCR kit for Trypanosoma cruzi DNA amplification was prospectively evaluated in umbilical cord (UCB) and peripheral venous blood (PVB) of infants born to CD mothers at endemic and non-endemic sites of Argentina., Methods: We enrolled and followed-up 370 infants; qPCR was compared to gold-standard cCD diagnosis following studies of diagnostic accuracy guidelines., Findings: Fourteen infants (3·78%) had cCD. The qPCR sensitivity and specificity were higher in PVB (72·73%, 99·15% respectively) than in UCB (66·67%, 96·3%). Positive and negative predictive values were 80 and 98·73% and 50 and 98·11% for PVB and UCB, respectively. The Areas under the Curve (AUC) of ROC analysis for qPCR and micromethod (MM) were 0·81 and 0·67 in UCB and 0·86 and 0·68 in PVB, respectively. Parasitic loads ranged from 37·5 to 23,709 parasite equivalents/mL. Discrete typing Unit Tc V was identified in five cCD patients and in six other cCD cases no distinction among Tc II, Tc V or Tc VI was achieved., Interpretation: This first prospective field study demonstrated that qPCR was more sensitive than MM for early cCD detection and more accurate in PVB than in UCB. Its use, as an auxiliary diagnostic tool to MM will provide more accurate records on cCD incidence., Funding: FITS SALUD 001-CHAGAS (FONARSEC, MINCyT, Argentina) to the Public-Private Consortium (INGEBI-CONICET, INP-ANLIS MALBRAN and Wiener Laboratories); ERANET-LAC-HD 328 to AGS and PICT 2015-0074 (FONCYT, MinCyT) to AGS and FA., Competing Interests: Declaration of Competing Interest None of the authors received payment or service from a third part at any time. None of the authors have any patents relevant to the work., (Copyright © 2021 The Authors. Published by Elsevier B.V. All rights reserved.)
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- 2021
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44. COVID-19: Implications for People with Chagas Disease.
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Zaidel EJ, Forsyth CJ, Novick G, Marcus R, Ribeiro ALP, Pinazo MJ, Morillo CA, Echeverría LE, Shikanai-Yasuda MA, Buekens P, Perel P, Meymandi SK, Ralston K, Pinto F, and Sosa-Estani S
- Subjects
- COVID-19 therapy, Chagas Cardiomyopathy diagnosis, Chagas Cardiomyopathy epidemiology, Chagas Disease therapy, Comorbidity, Cross-Sectional Studies, Follow-Up Studies, Forecasting, Health Services Accessibility trends, Health Services Needs and Demand trends, Humans, Risk Factors, COVID-19 diagnosis, COVID-19 epidemiology, Chagas Disease diagnosis, Chagas Disease epidemiology, Neglected Diseases
- Abstract
As the global COVID-19 pandemic advances, it increasingly impacts those vulnerable populations who already bear a heavy burden of neglected tropical disease. Chagas disease (CD), a neglected parasitic infection, is of particular concern because of its potential to cause cardiac, gastrointestinal, and other complications which could increase susceptibility to COVID-19. The over one million people worldwide with chronic Chagas cardiomyopathy require special consideration because of COVID-19's potential impact on the heart, yet the pandemic also affects treatment provision to people with acute or chronic indeterminate CD. In this document, a follow-up to the WHF-IASC Roadmap on CD, we assess the implications of coinfection with SARS-CoV-2 and Trypanosoma cruzi , the etiological agent of CD. Based on the limited evidence available, we provide preliminary guidance for testing, treatment, and management of patients affected by both diseases, while highlighting emerging healthcare access challenges and future research needs., Competing Interests: The authors have no competing interests to declare., (Copyright: © 2020 The Author(s).)
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- 2020
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45. A new patient registry for Chagas disease.
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Hotez P, Bottazzi ME, Strub-Wourgaft N, Sosa-Estani S, Torrico F, Pajín L, Abril M, and Sancho J
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- Chagas Disease therapy, Humans, Neglected Diseases, Trypanosoma cruzi, Chagas Disease epidemiology, Registries
- Abstract
Competing Interests: The authors have declared that no competing interests exist.
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- 2020
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46. Short-course Benznidazole treatment to reduce Trypanosoma cruzi parasitic load in women of reproductive age (BETTY): a non-inferiority randomized controlled trial study protocol.
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Cafferata ML, Toscani MA, Althabe F, Belizán JM, Bergel E, Berrueta M, Capparelli EV, Ciganda Á, Danesi E, Dumonteil E, Gibbons L, Gulayin PE, Herrera C, Momper JD, Rossi S, Shaffer JG, Schijman AG, Sosa-Estani S, Stella CB, Klein K, and Buekens P
- Subjects
- Argentina, Chagas Disease diagnosis, Female, Humans, Parasite Load, Postpartum Period, Pregnancy, Randomized Controlled Trials as Topic, Real-Time Polymerase Chain Reaction, Retrospective Studies, Trypanosoma cruzi genetics, Chagas Disease drug therapy, Nitroimidazoles therapeutic use, Trypanosoma cruzi drug effects
- Abstract
Background: Retrospective observational studies suggest that transmission of Trypanosoma cruzi does not occur in treated women when pregnant later in life. The level of parasitemia is a known risk factor for congenital transmission. Benznidazole (BZN) is the drug of choice for preconceptional treatment to reduce parasitic load. The fear of treatment-related side effects limits the implementation of the Argentine guideline recommending BZN 60d/300 mg (or equivalent) treatment of T. cruzi seropositive women during the postpartum period to prevent transmission in a future pregnancy. A short and low dose BZN treatment might reduce major side effects and increase compliance, but its efficacy to reduce T. cruzi parasitic load compared to the standard 60d/300 mg course is not yet established. Clinical trials testing alternative BZN courses among women of reproductive age are urgently needed., Methods and Design: We are proposing to perform a double-blinded, non-inferiority randomized controlled trial comparing a short low dose 30-day treatment with BZN 150 mg/day (30d/150 mg) vs. BZN 60d/300 mg. We will recruit not previously treated T. cruzi seropositive women with a live birth during the postpartum period in Argentina, randomize them at 6 months postpartum, and follow them up with the following specific aims: Specific aim 1: to measure the effect of BZN 30d/150 mg compared to 60d/300 mg preconceptional treatment on parasitic load measured by the frequency of positive Polymerase Chain Reaction (PCR) (primary outcome) and by real-time quantitative PCR (qPCR), immediately and 10 months after treatment. Specific aim 2: to measure the frequency of serious adverse events and/or any adverse event leading to treatment interruption., Trial Registration: ClinicalTrials.gov . Identifier: NCT03672487 . Registered 14 September 2018.
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- 2020
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47. New Scheme of Intermittent Benznidazole Administration in Patients Chronically Infected with Trypanosoma cruzi: Clinical, Parasitological, and Serological Assessment after Three Years of Follow-Up.
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Álvarez MG, Ramírez JC, Bertocchi G, Fernández M, Hernández Y, Lococo B, Lopez-Albizu C, Schijman A, Cura C, Abril M, Laucella S, Tarleton RL, Natale MA, Castro Eiro M, Sosa-Estani S, and Viotti R
- Subjects
- Follow-Up Studies, Humans, Pilot Projects, Chagas Disease drug therapy, Nitroimidazoles therapeutic use, Trypanocidal Agents therapeutic use, Trypanosoma cruzi
- Abstract
In a pilot study, we showed that the intermittent administration of benznidazole in chronic Chagas disease patients resulted in a low rate of treatment suspension and therapeutic failure, as assessed by quantitative PCR (qPCR) at the end of treatment. Here, a 3-year posttreatment follow-up study of the same cohort of patients is presented. The treatment scheme consisted of 12 doses of benznidazole at 5 mg/kg of body weight/day in two daily doses every 5 days. Parasite load, Trypanosoma cruzi -specific antibodies, and serum chemokine levels were measured prior to treatment and after a median follow-up of 36 months posttreatment by DNA minicircle kinetoplastid and nuclear DNA satellite sequence qPCR methods, conventional serological techniques, a Luminex-based assay with recombinant T. cruzi proteins, and a cytometric bead array. At the end of follow-up, 14 of 17 (82%) patients had negative qPCR findings, whereas three of 17 (18%) had detectable nonquantifiable findings by at least one of the qPCR techniques. A decline in parasite-specific antibodies at 12 months posttreatment was confirmed by conventional serological tests and the Luminex assays. Monocyte chemoattractant protein 1 levels increased after treatment, whereas monokine induced by gamma interferon levels decreased. New posttreatment electrocardiographic abnormalities were observed in only one patient who had cardiomyopathy prior to treatment. Together, these data strengthen our previous findings by showing that the intermittent administration of benznidazole results in a low rate of treatment suspension, with treatment efficacy comparable to that of a daily dose of 5 mg/kg for 60 days., (Copyright © 2020 American Society for Microbiology.)
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- 2020
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48. Fixed vs adjusted-dose benznidazole for adults with chronic Chagas disease without cardiomyopathy: A systematic review and meta-analysis.
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Ciapponi A, Barreira F, Perelli L, Bardach A, Gascón J, Molina I, Morillo C, Prado N, Riarte A, Torrico F, Ribeiro I, Villar JC, and Sosa-Estani S
- Subjects
- Adult, Databases, Factual, Humans, Nifurtimox therapeutic use, Patient Safety, Randomized Controlled Trials as Topic, Treatment Outcome, Triazoles therapeutic use, Trypanosoma cruzi drug effects, Cardiomyopathies, Chagas Disease drug therapy, Nitroimidazoles administration & dosage, Nitroimidazoles therapeutic use
- Abstract
Chagas disease is a neglected disease that remains a public health threat, particularly in Latin America. The most important treatment options are nitroimidazole derivatives, such as nifurtimox and benznidazole (BZN). Some studies suggest that for adults seropositive to T. cruzi but without clinically evident chronic Chagas cardiomyopathy (CCC), a simple fixed-dose scheme of BZN could be equivalent to a weight-adjusted dose. We compared the efficacy and safety of a fixed dose of BZN with an adjusted dose for T. cruzi seropositive adults without CCC. We used the Cochrane methods, and reported according to the PRISMA statement. We included randomized controlled trials (RCTs) allocating participants to fixed and/or adjusted doses of BZN for T. cruzi seropositive adults without CCC. We searched (December 2019) Cochrane, MEDLINE, EMBASE, LILACS, Clinicaltrials.gov, and International Clinical Trials Registry Platform (ICTRP), and contacted Chagas experts. Selection, data extraction, and risk of bias assessment, using the Cochrane tool, were performed independently by pairs of reviewers. Discrepancies were solved by consensus within the team. Primary outcomes were parasite-related outcomes and efficacy or patient-related safety outcomes. We conducted a meta-analysis using RevMan 5.3 software and used GRADE summary of finding tables to present the certainty of evidence by outcome. We identified 655 records through our search strategy and 10 studies (four of them ongoing) met our inclusion criteria. We did not find any study directly comparing fixed vs adjusted doses of BZN, however, some outcomes allowed subgroup comparisons between fixed and adjusted doses of BZN against placebo. Moderate-certainty evidence suggests no important subgroup differences for positive PCR at one year and for three safety outcomes (drug discontinuation, peripheral neuropathy, and mild rash). The same effect was observed for any serious adverse events (low-certainty evidence). All subgroups showed similar effects (I2 0% for all these subgroup comparisons but 32% for peripheral neuropathy), supporting the equivalence of BZN schemes. We conclude that there is no direct evidence comparing fixed and adjusted doses of BZN. Based on low to very low certainty of evidence for critical clinical outcomes and moderate certainty of evidence for important outcomes, fixed and adjusted doses may be equivalent in terms of safety and efficacy. An individual patient data network meta-analysis could better address this issue., Competing Interests: The authors have declared that no competing interests exist.
- Published
- 2020
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49. Trypanosoma cruzi loop-mediated isothermal amplification (Trypanosoma cruzi Loopamp) kit for detection of congenital, acute and Chagas disease reactivation.
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Besuschio SA, Picado A, Muñoz-Calderón A, Wehrendt DP, Fernández M, Benatar A, Diaz-Bello Z, Irurtia C, Cruz I, Ndung'u JM, Cafferata ML, Montenegro G, Sosa Estani S, Lucero RH, Alarcón de Noya B, Longhi SA, and Schijman AG
- Subjects
- Chagas Disease cerebrospinal fluid, Chagas Disease congenital, Coinfection, DNA, Protozoan analysis, Female, HIV Infections, Humans, Infant, Infant, Newborn, Male, Real-Time Polymerase Chain Reaction methods, Retrospective Studies, Sensitivity and Specificity, Transplant Recipients, Trypanosoma cruzi physiology, Chagas Disease blood, Chagas Disease diagnosis, Nucleic Acid Amplification Techniques methods, Trypanosoma cruzi isolation & purification
- Abstract
A Trypanosoma cruzi Loopamp kit was recently developed as a ready-to-use diagnostic method requiring minimal laboratory facilities. We evaluated its diagnostic accuracy for detection of acute Chagas disease (CD) in different epidemiological and clinical scenarios. In this retrospective study, a convenience series of clinical samples (venous blood treated with EDTA or different stabilizer agents, heel-prick blood in filter paper or cerebrospinal fluid samples (CSF)) from 30 infants born to seropositive mothers (13 with congenital CD and 17 noninfected), four recipients of organs from CD donors, six orally-infected cases after consumption of contaminated guava juice and six CD patients coinfected with HIV at risk of CD reactivation (N = 46 patients, 46 blood samples and 1 CSF sample) were tested by T. cruzi Loopamp kit (Tc LAMP) and standardized quantitative real-time PCR (qPCR). T. cruzi Loopamp accuracy was estimated using the case definition in the different groups as a reference. Cohen's kappa coefficient (κ) was applied to measure the agreement between Tc LAMP (index test) and qPCR (reference test). Sensitivity and specificity of T. cruzi Loopamp kit in blood samples from the pooled clinical groups was 93% (95% CI: 77-99) and 100% (95% CI: 80-100) respectively. The agreement between Tc LAMP and qPCR was almost perfect (κ = 0.92, 95% CI: 0.62-1.00). The T. cruzi Loopamp kit was sensitive and specific for detection of T. cruzi infection. It was carried out from DNA extracted from peripheral blood samples (via frozen EDTA blood, guanidine hydrochloride-EDTA blood, DNAgard blood and dried blood spots), as well as in CSF specimens infected with TcI or TcII/V/VI parasite populations. The T. cruzi Loopamp kit appears potentially useful for rapid detection of T. cruzi infection in congenital, acute and CD reactivation due to HIV infection., Competing Interests: The authors have declared that no competing interests exist.
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- 2020
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50. Implications of asymptomatic infection for the natural history of selected parasitic tropical diseases.
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Alvar J, Alves F, Bucheton B, Burrows L, Büscher P, Carrillo E, Felger I, Hübner MP, Moreno J, Pinazo MJ, Ribeiro I, Sosa-Estani S, Specht S, Tarral A, Wourgaft NS, and Bilbe G
- Subjects
- Asymptomatic Infections, Humans, Incidence, Chagas Disease diagnosis, Chagas Disease epidemiology, Parasitic Diseases diagnosis, Parasitic Diseases epidemiology
- Abstract
Progress has been made in the control or elimination of tropical diseases, with a significant reduction of incidence. However, there is a risk of re-emergence if the factors fueling transmission are not dealt with. Although it is essential to understand these underlying factors for each disease, asymptomatic carriers are a common element that may promote resurgence; their impact in terms of proportion in the population and role in transmission needs to be determined. In this paper, we review the current evidence on whether or not to treat asymptomatic carriers given the relevance of their role in the transmission of a specific disease, the efficacy and toxicity of existing drugs, the Public Health interest, and the benefit at an individual level, for example, in Chagas disease, to prevent irreversible organ damage. In the absence of other control tools such as vaccines, there is a need for safer drugs with good risk/benefit profiles in order to change the paradigm so that it addresses the complete infectious process beyond manifest disease to include treatment of non-symptomatic infected persons.
- Published
- 2020
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