ABSTRACT
Translational research (TR) is an interdisciplinary branch of the biomedical field that seeks to connect its three supporting pillars: basic research on the bench, the hospital beds and other health system services, and the delivery of products for the well-being and health of the community. Here, we review the five transition stages of the TR spectrum, registering the lessons learned during > 20 years leading to the first clinical trial designed and performed in Brazil for testing a complementary treatment for Chagas disease (CD): the selenium trial (STCC). Lessons learned were: (1) to consider all the TR spectrum since the beginning of the project; (2) to start simultaneously animal studies and translation to humans; (3) to ensure a harmonious interaction between clinical and basic research teams; (4) to include MSc and PhD students only in pre-clinical and basic studies (TR0) or vertical clinical studies using retrospective samples and data (TR1); (5) to identify potential suppliers in the national commercial market for a future final treatment since the pre-clinical stage; (6) to keep an international network of experts as permanent advisers on the project. In the whole process, some perspectives were created: a complementary clinical trial for the opened questions and the construction of a Brazilian clinical CD platform.
ABSTRACT
Trypanosoma cruzi infection induces diverse alterations in immunocompetent cells and organs, myocarditis and congestive heart failure. However, the physiological network of disturbances imposed by the infection has not been addressed thoroughly. Regarding myocarditis induced by the infection, we observed in our previous work that Fas-L-/- mice (gld/gld) have very mild inflammatory infiltration when compared to BALB/c mice. However, all mice from both lineages die in the early acute phase. Therefore, in this work we studied the physiological connection relating arterial pressure, renal function/damage and cardiac insufficiency as causes of death. Our results show that a broader set of dysfunctions that could be classified as a cardio/anaemic/renal syndrome is more likely responsible for cardiac failure and death in both lineages. However, gld/gld mice had very early glomerular deposition of IgM and a more intense renal inflammatory response with reduced renal filtration, which is probably responsible for the premature death in the absence of significant myocarditis in gld/gld.
Subject(s)
Animals , Male , Mice , Acute Kidney Injury , Chagas Disease/physiopathology , Fas Ligand Protein/metabolism , Myocarditis/physiopathology , Acute Kidney Injury , Chagas Disease/complications , Mice, Inbred BALB C , Mice, Mutant Strains , Myocarditis/etiology , Myocarditis/metabolismABSTRACT
Gap junction connexin-43 (Cx43) molecules are responsible for electrical impulse conduction in the heart and are affected by transforming growth factor-â (TGF-â). This cytokine increases during Trypanosoma cruzi infection, modulating fibrosis and the parasite cell cycle. We studied Cx43 expression in cardiomyocytes exposed or not to TGF-â T. cruzi, or SB-431542, an inhibitor of TGF-â receptor type I (ALK-5). Cx43 expression was also examined in hearts with dilated cardiopathy from chronic Chagas disease patients, in which TGF-â signalling had been shown previously to be highly activated. We demonstrated that TGF-â treatment induced disorganised gap junctions in non-infected cardiomyocytes, leading to a punctate, diffuse and non-uniform Cx43 staining. A similar pattern was detected in T. cruzi-infected cardiomyocytes concomitant with high TGF-â secretion. Both results were reversed if the cells were incubated with SB-431542. Similar tests were performed using human chronic chagasic patients and we confirmed a down-regulation of Cx43 expression, an altered distribution of plaques in the heart and a significant reduction in the number and length of Cx43 plaques, which correlated negatively with cardiomegaly. We conclude that elevated TGF-â levels during T. cruzi infection promote heart fibrosis and disorganise gap junctions, possibly contributing to abnormal impulse conduction and arrhythmia that characterise severe cardiopathy in Chagas disease.
Subject(s)
Adult , Animals , Female , Humans , Male , Mice , Middle Aged , Benzamides/therapeutic use , Chagas Disease/metabolism , /metabolism , Dioxoles/therapeutic use , Gap Junctions/metabolism , Myocytes, Cardiac/chemistry , Receptors, Transforming Growth Factor beta/antagonists & inhibitors , Transforming Growth Factor beta/therapeutic use , Chagas Disease/drug therapy , Fluorescent Antibody Technique , Gap Junctions/drug effects , Immunohistochemistry , Microscopy, Confocal , Myocytes, Cardiac/drug effects , Myocytes, Cardiac/metabolismABSTRACT
Em 1909, Carlos Chagas anunciou a descoberta de uma nova doença: a tripanossomíase humana, doença de Chagas. A descoberta representou não apenas uma contribuição inovadora para o campo da medicina tropical, em particular os estudos sobre as doenças parasitárias, mas também mostrou a realidade sanitária e social do interior do país, assolado pelas endemias rurais. Cem anos depois nos deparamos com uma valiosa oportunidade de reflexão sobre os múltiplos sentidos e implicações da comemoração do grande feito de Carlos Chagas, que, tal como a biografia do cientista, associam ciência, saúde pública e projetos para a nação. Comemorar, lembrar junto, significa, assim, refletir sobre as várias temporalidades imbricadas nesta data: a memória de um passado que engendou o presente e convida a pensar os desafios do futuro. A história, tecendo os fios de um tempo construído por tantos indivíduos e gerações ao longo destes cem anos, apresenta-se como caminho para congregar todos aqueles que se associam a este legado e pretendem compartilhá-lo entre as novas gerações. Diante deste cenário e do atual quadro epidemiológico de uma enfermidade que ainda afeta milhões de pessoas em toda a América Latina, evidencia-se a importância de se articular ações que permitam suprir as lacunas relacionadas ao conhecimento da doença de Chagas e às medidas efetivas para tratamento e controle. Os textos reunidos neste livro constituem um importante marco nesse sentido. Clássicos em Doença de Chagas: história e perspectivas no cenário da descoberta lança nova luz sobre os estudos da doença a partir da reunião de 15 artigos científicos comentados por renomados pesquisadores, especialmente convidados para esta homenagem. Estamos diante de um valioso acervo documental que esperamos possa estimular o avanço do conhecimento e, assim, contribuir para a busca de soluções dos problemas sociais e de saúde relacionados á enfermidade de Chagas.
Subject(s)
Chagas Disease/history , Chagas Disease/prevention & control , History of Medicine , Public Health/history , BrazilABSTRACT
Revisões históricas aos avanços científicos para o controle da doença, o Simpósio Internacional Comemorativo do Centenário da Descoberta da Doença de Chagas (1909-2009).
Subject(s)
Humans , Chagas Disease/diagnosis , Chagas Disease/epidemiology , Chagas Disease/history , Trypanosoma cruzi/parasitology , Chagas Disease/ethnology , Chagas Disease/parasitology , Chagas Disease/pathologyABSTRACT
Revisões históricas aos avanços científicos para o controle da doença, o Simpósio Internacional Comemorativo do Centenário da Descoberta da Doença de Chagas (1909-2009).
Subject(s)
Humans , Chagas Disease/diagnosis , Polysaccharides/history , Polysaccharides , History of Medicine , Serologic Tests/history , Serologic TestsABSTRACT
Revisões históricas aos avanços científicos para o controle da doença, o Simpósio Internacional Comemorativo do Centenário da Descoberta da Doença de Chagas (1909-2009).
Subject(s)
Humans , Science/trends , Chagas Disease/history , History of MedicineABSTRACT
Chagas disease is a major public health problem in Bolivia. In the city of Cochabamba, 58 percent of the population lives in peripheral urban districts ("popular zones") where the infection prevalence is extremely high. From 1995 to 1999, we studied the demographics of Chagas infections in children from five to 13 years old (n = 2218) from the South zone (SZ) and North zone (NZ) districts, which differ in social, environmental, and agricultural conditions. Information gathered from these districts demonstrates qualitative and quantitative evidence for the active transmission of Trypanosoma cruzi in urban Cochabamba. Seropositivity was high in both zones (25 percent in SZ and 19 percent in NZ). We observed a high risk of infection in children from five to nine years old in SZ, but in NZ, a higher risk occurred in children aged 10-13, with odds ratio for infection three times higher in NZ than in SZ. This difference was not due to triatomine density, since more than 1,000 Triatoma infestans were captured in both zones, but was possibly secondary to the vector infection rate (79 percent in SZ and 37 percent in NZ). Electrocardiogram abnormalities were found to be prevalent in children and pre-adolescents (SZ = 40 percent, NZ = 17 percent), indicating that under continuous exposure to infection and re-infection, a severe form of the disease may develop early in life. This work demonstrates that T. cruzi infection should also be considered an urban health problem and is not restricted to the rural areas and small villages of Bolivia.
Subject(s)
Adolescent , Animals , Cats , Cattle , Child , Child, Preschool , Dogs , Female , Humans , Male , Rabbits , Chagas Disease/transmission , Health Knowledge, Attitudes, Practice , Insect Vectors/parasitology , Triatoma/parasitology , Trypanosoma cruzi/isolation & purification , Bolivia/epidemiology , Chagas Disease/diagnosis , Chagas Disease/epidemiology , Population Density , Prevalence , Risk Factors , Seroepidemiologic Studies , Sheep , Socioeconomic Factors , Urban PopulationABSTRACT
Biocorrosion means any process of corrosion in wich microorganisms are somehow involved. As far as the petroleum industry is concerned, the anaerobic type is the more important, with Sulphate-Reducing Bacteria (SRB) accouting for half of the described processes. SRB are obligate anaerobs that use sulphur, sulphate or other oxidized sulphur compounds as oxidizing agents when decomposing organic material. A typical product of SRB metabolism, hydrogen sulphide -H2S-, is extremely toxic. In the present work we review the literature on mechanisms underlying biocorrosive process in wich SRB are involved and summarize some of the ultrastructural and eletrochemical work developed using SRB obtained from water injection flow in wells located on PETROBRAS offshore marine plataforms, sampled directly in the field over metallic probes, or cultured under laboratory conditions. Biofilms develop when SRB adhere to inert surfaces. A high diversity of morphological types is found inside these biofilms. Their extracellular matrix is highly hydrated and mainly anionic, as shown by its avid reaction with cationic compounds like ruthenium red. We have noted that variations in iron contet lead to interesting changes in the ultrastructure of the bacterial cell coat and also in the rate of corrosion induced in metallic test cupons. Since routine methods to prevent and treat SRB contamination and biodeterioration involve the use of biocides that are toxic and always have some environmental impact, an accurate diagnosis of biocorrosion is always required prior to a treatment decision. We developed a method that detects and semi-quantifies the presence of living or dead SRB by using free silver potentials as an indicator of corrosive action by SRB-associated sulphides. We found a correlation between sulphide levels (determined either by spectrophotometry, or using a silver electrode -E(Ag)- that measured changes in free potentials induced by the presence of exogeneously added sulphide) and SRB concentration (enumerated by a culturing method). E(Ag) was characterized under a variety of conditions and was found to be relatively immune to possible interference resulting from aeration of media or from the presence of iron corrosion products. The method offers a simple, rapid, and effective means of diagnosing biocorrosive process prior to their control
Subject(s)
Bacteria, Anaerobic , Corrosion , Sulfates , SulfurABSTRACT
Macrophages and muscle cells are the main targets for invasion of Trypanosoma cruzi. Ultrastructural studies of this phenomenon in vitro showed that invasion occurs by endocytosis, with attachment and internalization being mediated by different components capable of recognizing epi-or trypomastigotes (TRY). A parasitophorus vacuole was formed in both cell types, thereafter fusing with lysosomes. Then, the mechanism of T. cruzi invasion of host cells (HC) is essentially similar (during a primary infection in the abscence of a specific immune response), regardless of wether the target cell is a professional or a non-professional phagocytic cell. Using sugars, lectins, glycosidases, proteinases and proteinase inhibitors, we observed that the relative balance between exposed sialic acid and galactose/N-acetyl galactosamine (GAL) residues on the TRY surface, determines the parasite's capacity to invade HC, and that lectin-mediated phagocytosis with GAL specificity is important for internalization of T. cruzi into macrophages. On the other hand, GAL on the surface to heart muscle cells participate on TRY adhesion. TRY need to process proteolytically both the HC and their own surface, to expose the necessary ligands and receptors that allow binding to, and internalization in the host cell. The diverse range of molecular mechanisms which the parasite could use to invade the host cell may correspond to differences in the available "receptors"on the surface of each specific cell type. Acute phase components, with lectin or proteinase inhibitory activities (a-macroglobulins), may also be involved in T. cruzi-host cell interaction