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Guideline of the Brazilian Society of Cardiology on Diagnosis and Treatment of Patients with Chagas Disease Cardiomyopathy / Diretriz da Sociedade Brasileira de Cardiologia sobre Diagnóstico e Tratamento de Pacientes com Cardiomiopatia da Doença de Chagas

Marin-Neto, José Antonio; Rassi Jr., Anis; Moraes Oliveira, Gláucia M.; Lemos Correia, Luís Claudio; Novaes Ramos Jr., Alberto; Hasslocher-Moreno, Alejandro Marcel; Luquetti Ostermayer, Alejandro; Sousa, Andréa Silvestre de; Amato Vincenzo de Paola, Angelo; Sobral de Sousa, Antonio Carlos; Pinho Ribeiro, Antonio Luiz; Correia Filho, Dalmo; Moraes de Souza, Dilma do Socorro; Cunha-Neto, Edecio; J. A. Ramires, Felix; Bacal, Fernando; Pereira Nunes, Maria do Carmo; Martinelli Filho, Martino; Ibrahim Scanavacca, Maurício; Magalhães Saraiva, Roberto; Alves de Oliveira Júnior, Wilson; M. Lorga-Filho, Adalberto; de Jesus Benevides de Almeida Guimarães, Adriana; Lopes Latado Braga, Adriana; Sarmento de Oliveira, Adriana; V. L. Sarabanda, Alvaro; Yecê das Neves Pinto, Ana; Assis Lopes do Carmo, André; Schmidt, André; Costa, Andréa Rodrigues da; Ianni, Barbara Maria; Markman Filho, Brivaldo; Eduardo Rochitte, Carlos; Thé Macedo, Carolina; Mady, Charles; Chevillard, Christophe; Bittencourt das Virgens, Cláudio Marcelo; Nery de Castro, Cleudson; De Paoli de Carvalho Britto, Constança Felícia; Pisani, Cristiano; do Carmo Rassi, Daniela; C. Sobral Filho, Dario; Rodrigues Almeida, Dirceu; A. Bocchi, Edimar; T. Mesquita, Evandro; de Souza Nogueira Sardinha Mendes, Fernanda; Pereira, Francisca Tatiana; Sperandio da Silva, Gilberto Marcelo; de Lima Peixoto, Giselle; Glotz de Lima, Gustavo; H. Veloso, Henrique; Turin Moreira, Henrique; Bellotti Lopes, Hugo; Masciarelli Francisco Pinto, Ibraim; Pinto Dias, João Carlos; Bemfica, João Marcos; Silva-Nunes, João Paulo; Soares Barreto-Filho, José Augusto; Kerr Saraiva, José Francisco; Lannes-Vieira, Joseli; Menezes Oliveira, Joselina Luzia; V. Armaganijan, Luciana; Martins, Luiz Cláudio; C. Sangenis, Luiz Henrique; Barbosa, Marco Paulo; Almeida-Santos, Marcos Antônio; Simões, Marcos Vinicius; Shikanai-Yasuda, Maria Aparecida; Vieira Moreira, Maria da Consolação; Higuchi, Maria de Lourdes; Costa Monteiro, Maria Rita de Cássia; Felix Mediano, Mauro Felippe; Maia Lima, Mayara; T. Oliveira, Maykon; Moreira Dias Romano , Minna; Nitz, Nadjar; de Tarso Jorge Medeiros, Paulo; Vieira Alves, Renato; Alkmim Teixeira, Ricardo; Coury Pedrosa, Roberto; Aras, Roque; Morais Torres, Rosália; dos Santos Povoa, Rui Manoel; Rassi, Sérgio Gabriel; Salles Xavier, Sérgio; Marinho Martins Alves , Silvia; B. N. Tavares, Suelene; Lima Palmeira, Swamy; da Silva Junior, Telêmaco Luiz; da Rocha Rodrigues, Thiago; Madrini Junior, Vagner; Maia da Costa , Veruska; Dutra, Walderez.

Preprint Pt | PREPRINT-SCIELO | ID: pps-4820

This guideline aimed to update the concepts and formulate the standards of conduct and scientific evidence that support them, regarding the diagnosis and treatment of the Cardiomyopathy of Chagas disease, with special emphasis on the rationality base that supported it. Chagas disease in the 21st century maintains an epidemiological pattern of endemicity in 21 Latin American countries. Researchers and managers from endemic and non-endemic countries point to the need to adopt comprehensive public health policies to effectively control the interhuman transmission of T. cruzi infection, and to obtain an optimized level of care for already infected individuals, focusing on diagnostic and therapeutic opportunistic opportunities. Pathogenic and pathophysiological mechanisms of the Cardiomyopathy of Chagas disease were revisited after in-depth updating and the notion that necrosis and fibrosis are stimulated by tissue parasitic persistence and adverse immune reaction, as fundamental mechanisms, assisted by autonomic and microvascular disorders, was well established. Some of them have recently formed potential targets of therapies. The natural history of the acute and chronic phases was reviewed, with enhancement for oral transmission, indeterminate form and chronic syndromes. Recent meta-analyses of observational studies have estimated the risk of evolution from acute and indeterminate forms and mortality after chronic cardiomyopathy. Therapeutic approaches applicable to individuals with Indeterminate form of Chagas disease were specifically addressed. All methods to detect structural and/or functional alterations with various cardiac imaging techniques were also reviewed, with recommendations for use in various clinical scenarios. Mortality risk stratification based on the Rassi score, with recent studies of its application, was complemented by methods that detect myocardial fibrosis. The current methodology for etiological diagnosis and the consequent implications of trypanonomic treatment deserved a comprehensive and in-depth approach. Also the treatment of patients at risk or with heart failure, arrhythmias and thromboembolic events, based on pharmacological and complementary resources, received special attention. Additional chapters supported the conducts applicable to several special contexts, including t. cruzi/HIV co-infection, risk during surgeries, in pregnant women, in the reactivation of infection after heart transplantation, and others. Finally, two chapters of great social significance, addressing the structuring of specialized services to care for individuals with the Cardiomyopathy of Chagas disease, and reviewing the concepts of severe heart disease and its medical-labor implications completed this guideline.

Esta diretriz teve como objetivo principal atualizar os conceitos e formular as normas de conduta e evidências científicas que as suportam, quanto ao diagnóstico e tratamento da CDC, com especial ênfase na base de racionalidade que a embasou. A DC no século XXI mantém padrão epidemiológico de endemicidade em 21 países da América Latina. Investigadores e gestores de países endêmicos e não endêmicos indigitam a necessidade de se adotarem políticas abrangentes, de saúde pública, para controle eficaz da transmissão inter-humanos da infecção pelo T. cruzi, e obter-se nível otimizado de atendimento aos indivíduos já infectados, com foco em oportunização diagnóstica e terapêutica. Mecanismos patogênicos e fisiopatológicos da CDC foram revisitados após atualização aprofundada e ficou bem consolidada a noção de que necrose e fibrose sejam estimuladas pela persistência parasitária tissular e reação imune adversa, como mecanismos fundamentais, coadjuvados por distúrbios autonômicos e microvasculares. Alguns deles recentemente constituíram alvos potenciais de terapêuticas. A história natural das fases aguda e crônica foi revista, com realce para a transmissão oral, a forma indeterminada e as síndromes crônicas. Metanálises recentes de estudos observacionais estimaram o risco de evolução a partir das formas aguda e indeterminada e de mortalidade após instalação da cardiomiopatia crônica. Condutas terapêuticas aplicáveis aos indivíduos com a FIDC foram abordadas especificamente. Todos os métodos para detectar alterações estruturais e/ou funcionais com variadas técnicas de imageamento cardíaco também foram revisados, com recomendações de uso nos vários cenários clínicos. Estratificação de risco de mortalidade fundamentada no escore de Rassi, com estudos recentes de sua aplicação, foi complementada por métodos que detectam fibrose miocárdica. A metodologia atual para diagnóstico etiológico e as consequentes implicações do tratamento tripanossomicida mereceram enfoque abrangente e aprofundado. Também o tratamento de pacientes em risco ou com insuficiência cardíaca, arritmias e eventos tromboembólicos, baseado em recursos farmacológicos e complementares, recebeu especial atenção. Capítulos suplementares subsidiaram as condutas aplicáveis a diversos contextos especiais, entre eles o da co-infecção por T. cruzi/HIV, risco durante cirurgias, em grávidas, na reativação da infecção após transplante cardíacos, e outros. Por fim, dois capítulos de grande significado social, abordando a estruturação de serviços especializados para atendimento aos indivíduos com a CDC, e revisando os conceitos de cardiopatia grave e suas implicações médico-trabalhistas completaram esta diretriz.

Epigenetic regulation of transcription factor binding motifs promotes Th1 response in Chagas disease cardiomyopathy.

Brochet, Pauline; Ianni, Barbara Maria; Laugier, Laurie; Frade, Amanda Farage; Silva Nunes, João Paulo; Teixeira, Priscila Camillo; Mady, Charles; Ferreira, Ludmila Rodrigues Pinto; Ferré, Quentin; Santos, Ronaldo Honorato Barros; Kuramoto, Andreia; Cabantous, Sandrine; Steffen, Samuel; Stolf, Antonio Noedir; Pomerantzeff, Pablo; Fiorelli, Alfredo Inacio; Bocchi, Edimar Alcides; Pissetti, Cristina Wide; Saba, Bruno; Cândido, Darlan da Silva; Dias, Fabrício C; Sampaio, Marcelo Ferraz; Gaiotto, Fabio Antônio; Marin-Neto, José Antonio; Fragata, Abílio; Zaniratto, Ricardo Costa Fernandes; Siqueira, Sergio; Peixoto, Giselle De Lima; Rigaud, Vagner Oliveira-Carvalho; Bacal, Fernando; Buck, Paula; Almeida, Rafael Ribeiro; Lin-Wang, Hui Tzu; Schmidt, André; Martinelli, Martino; Hirata, Mario Hiroyuki; Donadi, Eduardo Antonio; Costa Pereira, Alexandre; Rodrigues Junior, Virmondes; Puthier, Denis; Kalil, Jorge; Spinelli, Lionel; Cunha-Neto, Edecio; Chevillard, Christophe.

Front Immunol ; 13: 958200, 2022.

Article En | MEDLINE | ID: mdl-36072583

Chagas disease, caused by the protozoan Trypanosoma cruzi, is an endemic parasitic disease of Latin America, affecting 7 million people. Although most patients are asymptomatic, 30% develop complications, including the often-fatal Chronic Chagasic Cardiomyopathy (CCC). Although previous studies have demonstrated some genetic deregulations associated with CCCs, the causes of their deregulations remain poorly described. Based on bulk RNA-seq and whole genome DNA methylation data, we investigated the genetic and epigenetic deregulations present in the moderate and severe stages of CCC. Analysis of heart tissue gene expression profile allowed us to identify 1407 differentially expressed transcripts (DEGs) specific from CCC patients. A tissue DNA methylation analysis done on the same tissue has permitted the identification of 92 regulatory Differentially Methylated Regions (DMR) localized in the promoter of DEGs. An in-depth study of the transcription factors binding sites (TFBS) in the DMRs corroborated the importance of TFBS's DNA methylation for gene expression in CCC myocardium. TBX21, RUNX3 and EBF1 are the transcription factors whose binding motif appears to be affected by DNA methylation in the largest number of genes. By combining both transcriptomic and methylomic analysis on heart tissue, and methylomic analysis on blood, 4 biological processes affected by severe CCC have been identified, including immune response, ion transport, cardiac muscle processes and nervous system. An additional study on blood methylation of moderate CCC samples put forward the importance of ion transport and nervous system in the development of the disease.

Chagas Cardiomyopathy , Chagas Disease , Trypanosoma cruzi , Chagas Disease/genetics , Epigenesis, Genetic , Humans , Transcription Factors/genetics

Impairment of Multiple Mitochondrial Energy Metabolism Pathways in the Heart of Chagas Disease Cardiomyopathy Patients.

Teixeira, Priscila Camillo; Ducret, Axel; Langen, Hanno; Nogoceke, Everson; Santos, Ronaldo Honorato Barros; Silva Nunes, João Paulo; Benvenuti, Luiz; Levy, Debora; Bydlowski, Sergio Paulo; Bocchi, Edimar Alcides; Kuramoto Takara, Andréia; Fiorelli, Alfredo Inácio; Stolf, Noedir Antonio; Pomeranzeff, Pablo; Chevillard, Christophe; Kalil, Jorge; Cunha-Neto, Edecio.

Front Immunol ; 12: 755782, 2021.

Article En | MEDLINE | ID: mdl-34867990

Chagas disease cardiomyopathy (CCC) is an inflammatory dilated cardiomyopathy occurring in 30% of the 6 million infected with the protozoan Trypanosoma cruzi in Latin America. Survival is significantly lower in CCC than ischemic (IC) and idiopathic dilated cardiomyopathy (DCM). Previous studies disclosed a selective decrease in mitochondrial ATP synthase alpha expression and creatine kinase activity in CCC myocardium as compared to IDC and IC, as well as decreased in vivo myocardial ATP production. Aiming to identify additional constraints in energy metabolism specific to CCC, we performed a proteomic study in myocardial tissue samples from CCC, IC and DCM obtained at transplantation, in comparison with control myocardial tissue samples from organ donors. Left ventricle free wall myocardial samples were subject to two-dimensional electrophoresis with fluorescent labeling (2D-DIGE) and protein identification by mass spectrometry. We found altered expression of proteins related to mitochondrial energy metabolism, cardiac remodeling, and oxidative stress in the 3 patient groups. Pathways analysis of proteins differentially expressed in CCC disclosed mitochondrial dysfunction, fatty acid metabolism and transmembrane potential of mitochondria. CCC patients' myocardium displayed reduced expression of 22 mitochondrial proteins belonging to energy metabolism pathways, as compared to 17 in DCM and 3 in IC. Significantly, 6 beta-oxidation enzymes were reduced in CCC, while only 2 of them were down-regulated in DCM and 1 in IC. We also observed that the cytokine IFN-gamma, previously described with increased levels in CCC, reduces mitochondrial membrane potential in cardiomyocytes. Results suggest a major reduction of mitochondrial energy metabolism and mitochondrial dysfunction in CCC myocardium which may be in part linked to IFN-gamma. This may partially explain the worse prognosis of CCC as compared to DCM or IC.

Chagas Cardiomyopathy/metabolism , Chagas Cardiomyopathy/physiopathology , Heart/physiopathology , Mitochondria/metabolism , Myocardium/metabolism , Adolescent , Adult , Energy Metabolism/physiology , Female , Humans , Male , Middle Aged , Mitochondria/pathology , Myocardium/pathology , Young Adult

Long Pentraxin 3-Mediated Fibroblast Growth Factor Trapping Impairs Fibrosarcoma Growth.

Rodrigues, Priscila Fabiana; Matarazzo, Sara; Maccarinelli, Federica; Foglio, Eleonora; Giacomini, Arianna; Silva Nunes, João Paulo; Presta, Marco; Dias, Adriana Abalen Martins; Ronca, Roberto.

Front Oncol ; 8: 472, 2018.

Article En | MEDLINE | ID: mdl-30443492

Fibrosarcomas are soft tissue mesenchymal tumors originating from transformed fibroblasts. Fibroblast growth factor-2 (FGF2) and its tyrosine-kinase receptors (FGFRs) play pivotal roles in fibrosarcoma onset and progression, FGF2 being actively produced by fibroblasts in all stages along their malignant transformation to the fibrosarcoma stage. The soluble pattern recognition receptor long pentraxin-3 (PTX3) is an extrinsic oncosuppressor whose expression is reduced in different tumor types, including soft tissue sarcomas, via hypermethylation of its gene promoter. PTX3 interacts with FGF2 and other FGF family members, thus acting as a multi-FGF antagonist able to inhibit FGF-dependent neovascularization and tumor growth. Here, PTX3 overexpression significantly reduced the proliferative and tumorigenic potential of fibrosarcoma cells in vitro and in vivo. In addition, systemic delivery of human PTX3 driven by the Tie2 promoter inhibited the growth of fibrosarcoma grafts in transgenic mice. In a translational perspective, the PTX3-derived small molecule FGF trap NSC12 prevented activation of the FGF/FGFR system in fibrosarcoma cells and reduced their tumorigenic activity in vivo. In conclusion, impairment of the FGF/FGFR system by FGF trap molecules may represent a novel therapeutic approach for the treatment of fibrosarcoma.