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2. Serodiagnosis and therapeutic monitoring of New-World tegumentary leishmaniasis using synthetic type-2 glycoinositolphospholipid-based neoglycoproteins.

Author

Viana, Sayonara M., Montoya, Alba L., Carvalho, Augusto M., de Mendonça, Brunele S., Portillo, Susana, Olivas, Janet J., Karimi, Nasim H., Estevao, Igor L., Ortega-Rodriguez, Uriel, Carvalho, Edgar M., Dutra, Walderez O., Maldonaldo, Rosa A., Michael, Katja, de Oliveira, Camila I., and Almeida, Igor C.

Published
2022
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3. T-cell receptor variable region usage in Chagas disease: A systematic review of experimental and human studies.

Author

de Souza-Silva, Thaiany Goulart, Gollob, Kenneth J., and Dutra, Walderez O.

Subjects
CHAGAS' disease, NEGLECTED diseases, T cells, MAJOR histocompatibility complex, SCIENCE databases, BURULI ulcer
Abstract

T cells recognize their ligand, the peptide major histocompatibility complex (MHC), via the T-cell receptor (TCR), which is composed of covalently linked α and β or γ and δ chains. This recognition is critical for T-cell ontogeny and controls the selection, activation, and function of T lymphocytes. Specific TCR αβ variable regions have been associated with immunopathogenesis of Chagas disease. Here, we present a systematic review that compiles experimental in vivo and human data regarding the preferential expression of variable alpha (Vα) and variable beta (Vβ) chain regions in Trypanosoma cruzi infection. The original studies indexed in PubMed/Medline, Scopus, and Web of Science databases were screened according to the PRISMA strategy. The analysis showed that expression of TCR Vα subfamilies were evaluated in one human study, and, unlike TCR Vβ, TCR Vα presented a more restricted usage. Despite the great variability in the usage of TCR Vβ regions in human Chagas disease, a down-regulation of TCR Vβ5 expression by T cells from patients in the acute phase of the disease was shown. Opposingly, this TCR region was found overly expressed in CD4+ T cells from chronic Chagas patients. It was also demonstrated that murine Vβ9+ T cells derived from nonlymphoid organs of T. cruzi-infected animals had a modulatory profile, while splenic Vβ9+ T cells produced inflammatory cytokines, indicating that although they display the same TCR Vβ region usage, these cells are functionally distinct. Despite the limitations of few papers and year of publication of the studies, compiling the data derived from them reveals that further investigation of TCR usage will point to their potential role in protective or pathogenic responses, as biomarkers of disease progression, and in the search for dominant peptides potentially useful for the development of vaccines or therapies. Author summary: Chagas disease is a neglected tropical disease, caused by infection with Trypanosoma cruzi. Differential expression of certain T-cell receptor (TCR) variable regions has been associated with the immunopathogenesis of Chagas disease. Here, we present a systematic review that compiled experimental in vivo and human data regarding the preferential expression of TCR alpha and beta chain variable regions in Chagas disease. The original studies indexed in the PubMed/Medline, Scopus, and Web of Science databases were screened according to the PRISMA strategy. Despite the great variability in the use of TCR Vβ in T. cruzi infection, the outcomes indicate that there is a down-regulation of TCR Vβ5 expression in T cells from patients in the acute phase of Chagas disease. However, this region is preferentially expressed by CD4+ T cells from chronic Chagas patients. Additionally, it has been demonstrated that murine Vβ9+ T cells derived from nonlymphoid organs displayed a modulatory profile, while splenic Vβ9+ T cells produced inflammatory cytokines, indicating that although they express the same TCR Vβ region, these cells are functionally distinct. Information on TCR expression, specificity and function have critical impact on vaccine design. [ABSTRACT FROM AUTHOR]

Published
2022
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5. Prothymosin Alpha: A Novel Contributor to Estradiol Receptor Alpha-Mediated CD8+ T-Cell Pathogenic Responses and Recognition of Type 1 Collagen in Rheumatic Heart Valve Disease.

Author

Passos, Livia S.A., Jha, Prabhash K., Becker-Greene, Dakota BA, Blaser, Mark C., Romero, Dayanna, Lupieri, Adrien, Sukhova, Galina K., Libby, Peter, Singh, Sasha A., Dutra, Walderez O., Aikawa, Masanori, Levine, Robert A., Nunes, Maria C.P., Aikawa, Elena, and Becker-Greene, Dakota

Published
2022
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6. Crosstalk Between Plasma Cytokines, Inflammation, and Liver Damage as a New Strategy to Monitoring NAFLD Progression.

Author

Fontes-Cal, Tereza C. M., Mattos, Rafael T., Medeiros, Nayara I., Pinto, Bruna F., Belchior-Bezerra, Mayara, Roque-Souza, Bruna, Dutra, Walderez O., Ferrari, Teresa C. A., Vidigal, Paula V. T., Faria, Luciana C., Couto, Cláudia A., and Gomes, Juliana A. S.

Subjects
NON-alcoholic fatty liver disease, CYTOKINES, INFLAMMATION, LIVER
Abstract

Cytokines are involved in the immunopathogenesis of nonalcoholic fatty liver disease (NAFLD), but the relationship between them and clinical parameters of NAFLD progression is still unknown. Using flow cytometry, we evaluated the plasma levels of IL-1β, IL-6, IL-12, TNF and IL-10 and their association with clinical and biochemical parameters of liver function during simple steatosis (NAFL) and nonalcoholic steatohepatitis (NASH) in biopsy-proven patients. The NASH patients showed higher levels of IL-6 associated with a lower IL-10/IL-6 ratio. Besides heatmaps were similar in the NAFL and NASH groups, the same did not occur in signature curves, the NASH patients were high producers to IL-12 and IL-6 while the NAFL patients were not high producers of any cytokines evaluated. Integrative biomarker network analysis revealed that cytokines are differently correlated with clinical parameters, while IL-12, IL-10 presented moderate and negative correlations with glycemic and lipid profile in the NAFL group. The NASH group IL-12 and TNF revealed stronger and positive correlations with transient elastography parameters and NAFLD liver fibrosis score. These data suggest that IL-6 and IL-10 might act in chronic inflammation and insulin resistance whereas IL-12 and TNF may be involved in promoting liver damage and NAFLD progression. Plasma concentration analysis of these molecules and their association with clinical parameters can be used as new biomarkers to monitoring NAFLD progression and to reflect NASH development. [ABSTRACT FROM AUTHOR]

Published
2021
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7. A Genome-wide Association Study Identifies SERPINB10, CRLF3, STX7, LAMP3, IFNG-AS1, and KRT80 As Risk Loci Contributing to Cutaneous Leishmaniasis in Brazil.

Author

Castellucci, Léa C, Almeida, Lucas, Cherlin, Svetlana, Fakiola, Michaela, Francis, Richard W, Carvalho, Edgar M, Hora, Anadílton Santos da, Lago, Tainã Souza do, Figueiredo, Amanda B, Cavalcanti, Clara M, Alves, Natalia S, Morais, Katia L P, Teixeira-Carvalho, Andréa, Dutra, Walderez O, Gollob, Kenneth J, Cordell, Heather J, and Blackwell, Jenefer M

Subjects
PROTEINS, FLOW cytometry, LEISHMANIASIS, BIOPSY, B cells, RNA, RISK assessment, COMPARATIVE studies, NEUTROPHILS, INTERFERONS, GENES, GENOMES, DESCRIPTIVE statistics, GENOTYPES, HEMATOPOIETIC stem cells, MONOCYTES, DISEASE risk factors
Abstract

Background Our goal was to identify genetic risk factors for cutaneous leishmaniasis (CL) caused by Leishmania braziliensis. Methods Genotyping 2066 CL cases and 2046 controls using Illumina HumanCoreExomeBeadChips provided data for 4 498 586 imputed single-nucleotide variants (SNVs). A genome-wide association study (GWAS) using linear mixed models took account of genetic diversity/ethnicity/admixture. Post-GWAS positional, expression quantitative trait locus (eQTL) and chromatin interaction mapping was performed in Functional Mapping and Annotation (FUMA). Transcriptional data were compared between lesions and normal skin, and cytokines measured using flow cytometry and Bioplex assay. Results Positional mapping identified 32 genomic loci associated with CL, none achieving genome-wide significance (P < 5 × 10−8). Lead SNVs at 23 loci occurred at protein coding or noncoding RNA genes, 15 with eQTLs for functionally relevant cells/tissues and/or showing differential expression in lesions. Of these, the 6 most plausible genetic risk loci were SERPINB10 (P imputed_1000G = 2.67 × 10−6), CRLF3 (P imputed_1000G = 5.12 × 10−6), STX7 (P imputed_1000G = 6.06 × 10−6), KRT80 (P imputed_1000G = 6.58 × 10−6), LAMP3 (P imputed_1000G = 6.54 × 10−6), and IFNG-AS1 (P imputed_1000G = 1.32 × 10−5). LAMP3 (P adjusted = 9.25 × 10−12; +6-fold), STX7 (P adjusted = 7.62 × 10−3; +1.3-fold), and CRLF3 (P adjusted = 9.19 × 10−9; +1.97-fold) were expressed more highly in CL biopsies compared to normal skin; KRT80 (P adjusted = 3.07 × 10−8; −3-fold) was lower. Multiple cis-eQTLs across SERPINB10 mapped to chromatin interaction regions of transcriptional/enhancer activity in neutrophils, monocytes, B cells, and hematopoietic stem cells. Those at IFNG-AS1 mapped to transcriptional/enhancer regions in T, natural killer, and B cells. The percentage of peripheral blood CD3+ T cells making antigen-specific interferon-γ differed significantly by IFNG-AS1 genotype. Conclusions This first GWAS for CL identified multiple genetic risk loci including a novel lead to understanding CL pathogenesis through regulation of interferon-γ by IFNG antisense RNA 1. [ABSTRACT FROM AUTHOR]

Published
2021
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8. Gene expression network analyses during infection with virulent and avirulent Trypanosoma cruzi strains unveil a role for fibroblasts in neutrophil recruitment and activation.

Author

Oliveira, Antonio Edson R., Pereira, Milton C. A., Belew, Ashton T., Ferreira, Ludmila R. P., Pereira, Larissa M. N., Neves, Eula G. A., Nunes, Maria do Carmo P., Burleigh, Barbara A., Dutra, Walderez O., El-Sayed, Najib M., Gazzinelli, Ricardo T., and Teixeira, Santuza M. R.

Subjects
CHAGAS' disease, GENE regulatory networks, GENE expression, TRYPANOSOMA cruzi, ROLE conflict, INFLAMMATION
Abstract

Chagas disease is caused by Trypanosoma cruzi, a protozoan parasite that has a heterogeneous population composed of a pool of strains with distinct characteristics, including variable levels of virulence. In previous work, transcriptome analyses of parasite genes after infection of human foreskin fibroblasts (HFF) with virulent (CL Brener) and non-virulent (CL-14) clones derived from the CL strain, revealed a reduced expression of genes encoding parasite surface proteins in CL-14 compared to CL Brener during the final steps of the intracellular differentiation from amastigotes to trypomastigotes. Here we analyzed changes in the expression of host genes during in vitro infection of HFF cells with the CL Brener and CL-14 strains by analyzing total RNA extracted from cells at 60 and 96 hours post-infection (hpi) with each strain, as well as from uninfected cells. Similar transcriptome profiles were observed at 60 hpi with both strains compared to uninfected samples. However, at 96 hpi, significant differences in the number and expression levels of several genes, particularly those involved with immune response and cytoskeleton organization, were observed. Further analyses confirmed the difference in the chemokine/cytokine signaling involved with the recruitment and activation of immune cells such as neutrophils upon T. cruzi infection. These findings suggest that infection with the virulent CL Brener strain induces a more robust inflammatory response when compared with the non-virulent CL-14 strain. Importantly, the RNA-Seq data also exposed an unexplored role of fibroblasts as sentinel cells that may act by recruiting neutrophils to the initial site of infection. This role for fibroblasts in the regulation of the inflammatory response during infection by T. cruzi was corroborated by measurements of levels of different chemokines/cytokines during in vitro infection and in plasma from Chagas disease patients as well as by neutrophil activation and migration assays. Author summary: Trypanosoma cruzi is the causative agent of Chagas disease, a debilitating and often life-threatening illness that affects 6 to 7 million people mainly in Latin America. The parasite, transmitted to humans by an insect vector, needs to invade different cells from the infected person in order to multiply and spread the infection to various organs, including the heart and the gut. In this study, we investigated how the host cell responds to the infection by analyzing changes in the expression of human genes in fibroblasts infected with the CL Brener and CL-14 strains, which are strains that present highly distinct virulent phenotypes during infection in mice. We showed that human fibroblasts build a strong immune response upon infection by T. cruzi and that this response is different depending on the parasite strain: infection with the virulent CL Brener strain induces a more robust inflammatory response compared with the infection with the avirulent CL-14 strain. We also showed that, in response to the infection, fibroblasts produce molecules that can recruit and activate neutrophils, which are important immune cells that controls the infection. [ABSTRACT FROM AUTHOR]

Published
2020
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9. Diet Alters Serum Metabolomic Profiling in the Mouse Model of Chronic Chagas Cardiomyopathy.

Author

Lizardo, Kezia, Ayyappan, Janeesh Plakkal, Ganapathi, Usha, Dutra, Walderez O., Qiu, Yunping, Weiss, Louis M., and Nagajyothi, Jyothi F.

Subjects
CHAGAS' disease, CARDIOMYOPATHIES, PARASITIC diseases, PATHOLOGY, METABOLIC regulation, FORMYLATION, AMINE oxidase, LIPID metabolism
Abstract

Chagas disease is caused by Trypanosoma cruzi which is endemic in Latin America. T. cruzi infection results in a latent infection with approximately a third of latently infected patients developing chronic Chagas cardiomyopathy (CCM). CCM is a common cause of cardiomyopathy in endemic regions and has a poor prognosis compared to other cardiomyopathies. The factors responsible for the transition from the asymptomatic indeterminate latent stage of infection to CCM are poorly understood. Our previous studies demonstrated that lipid metabolism and diet are important determinants of disease progression. In the present study, we analyzed various serum metabolomic biomarkers such as acylcarnitines, amino acids, biogenic amines, glycerophospholipids, and sphingolipids in murine models of CCM, where the mice specifically develop either left or right ventricular cardiomyopathy based on the diets fed during the indeterminate stage in a murine model of Chagas disease. Our data provide new insights into the metabolic changes that may predispose patients to CCM and biomarkers that may help predict the risk of developing cardiomyopathy from T. cruzi infection. Author Summary. Chronic Chagas cardiomyopathy (CCM) is a parasitic disease prevalent in Latin America. Currently, no effective drugs or vaccines are available to prevent or cure CCM. The factors involved in the disease severity and progression are poorly understood to design new therapeutic interventions. In order to rapidly identify Chagas patients with a higher risk to develop CCM, a new set of biomarkers specific to Chagas disease is needed. We performed serum metabolomic analyses in chronic T. cruzi-infected mice fed on different diets and identified cardiac ventricular-specific metabolite biomarkers that could define CCM severity. In this paper, we present the results of serum metabolomic analyses and discuss its correlations to the diet-induced metabolic regulations in the pathogenesis of CCM in a murine model of Chagas disease. [ABSTRACT FROM AUTHOR]

Published
2019
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10. Evidence of Different IL-1β Activation Pathways in Innate Immune Cells From Indeterminate and Cardiac Patients With Chronic Chagas Disease.

Author

Medeiros, Nayara I., Pinto, Bruna F., Elói-Santos, Silvana M., Teixeira-Carvalho, Andréa, Magalhães, Luísa M. D., Dutra, Walderez O., Correa-Oliveira, Rodrigo, and Gomes, Juliana A. S.

Subjects
CARDIAC patients, CHAGAS' disease, CARDIOMYOPATHIES, MYOCARDITIS, MATRIX metalloproteinases, CASPASES
Abstract

Background: Chagas cardiomyopathy is the main fibrosing myocarditis among known heart diseases. Development of cardiomyopathy has been related to extracellular matrix (ECM) remodeling, which are controlled by matrix metalloproteinases (MMPs) and cytokines, especially interleukin (IL)-1β. The convertion of 31KDa inactive precursor, the proIL-1β in 17KDa active IL-1β peptide, is controlled by caspase-1-dependent pathway, associated with inflammasomes. Other caspase-1 independent mechanisms mediated by proteases, especially as MMPs, have already been described. Methods: We evaluated IL-1β activation pathways in neutrophils and monocyte subsets from patients with different clinical forms of Chagas disease1 after T. cruzi antigen stimulation by multiparameter flow cytometry. Results: Our data demonstrated that Chagas patients with the indeterminate clinical form (IND) showed increased levels of IL-1β post-stimulation as well as increased expression of MMP-2, NLRP3, and CASP1, which are associated with the classical caspase-1-dependent pathway. Conversely, patients with the cardiac clinical form (CARD) showed increased IL-1β after stimulation associated with MMP-9 and alternative caspase-1-independent pathway. Conclusions: We suggest some distinct molecular mechanisms for production of IL-1β in innate immune cells from patients with different clinical forms of Chagas disease. MMP-2 and MMP-9 gelatinases are associated with distinct disease outcomes and IL-1β production. [ABSTRACT FROM AUTHOR]

Published
2019
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11. A Th2-Type Response Is Associated With Exuberant Lesions in Pregnant Women Infected With Leishmania braziliensis.

Author

Dutra, Walderez O, Barbosa, Daniela Faria, Souza, Paulo Eduardo Alencar de, Morgan, Daniel, Poetker, Shelene, Guimarães, Luiz Henrique, Bacelar, Olívia, Gollob, Kenneth J, Carvalho, Edgar M, and de Souza, Paulo Eduardo Alencar

Subjects
LEISHMANIASIS, PREGNANT women, CYTOKINES, NEUTROPHILS, CD4 antigen, INTERFERON gamma, COMPARATIVE studies, INTERFERONS, INTERLEUKINS, LEISHMANIA, RESEARCH methodology, MEDICAL cooperation, RESEARCH, SKIN, T cells, EVALUATION research
Abstract

Background: Cutaneous leishmaniasis (CL) is characterized by an exaggerated inflammatory response. During pregnancy there is a decreased inflammatory response, and we have shown that pregnant women with CL develop exuberant lesions.Methods: Cytokine production by peripheral blood mononuclear cells and the frequency of cells expressing cytokines in lesions from pregnant and nonpregnant women with CL were evaluated.Results: We observed that CL lesions from pregnant women displayed a more intense cellular infiltrate, associated with an increase in neutrophils and CD4+ cells. While no difference was observed regarding the number of interferon-gamma (IFN-γ)+ cells in lesions from pregnant compared to nonpregnant women with CL, interleukin-10 (IL-10) and IL-4 expression were approximately 3-times higher in lesions in pregnant women. Main sources of IL-4 and IL-10 were CD4+ and CD68+ cells, respectively. Expression of IL-4, but not IFN-γ or IL-10, was positively correlated with the intensity of inflammatory infiltrate in lesions from pregnant women.Conclusions: These results provide evidence of an IL-4-mediated pathology in Leishmania braziliensis-infected pregnant women. These differences in lesion pathogenesis in pregnant and nonpregnant women may open possibilities for new therapies for CL treatment during pregnancy, which are currently lacking. [ABSTRACT FROM AUTHOR]

Published
2019
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12. IL-10 and TGF-β unbalanced levels in neutrophils contribute to increase inflammatory cytokine expression in childhood obesity.

Author

Medeiros, Nayara I., Mattos, Rafael T., Menezes, Carlos A., Fares, Rafaelle C. G., Talvani, André, Dutra, Walderez O., Rios-Santos, Fabrício, Correa-Oliveira, Rodrigo, and Gomes, Juliana A. S.

Subjects
ANTIGENS, CELL receptors, CYTOKINES, FLOW cytometry, GENE expression, INFLAMMATION, INTERLEUKINS, NEUTROPHILS, CHILDHOOD obesity, TRANSFORMING growth factors-beta, TOLL-like receptors
Abstract

Purpose: Obesity is a multifactorial disease, associated with metabolic disorders, chronic low-grade inflammation, and impaired immunity. This study aimed to evaluate the childhood obesity-associated effects on neutrophil activation and cytokine production.Methods: We evaluated activation and recognition markers and cytokine production in neutrophils from the peripheral blood of children with obesity and normal weight using multicolor flow cytometry.Results: We demonstrate a higher frequency of neutrophils in childhood obesity group (CO) compared to normal-weight group (NW). Our data showed that neutrophils from CO group are capable of antigen recognition and presentation through higher expression of TLR-4 (CD284) and HLA-DR in comparison with neutrophils from NW. On the other hand, neutrophils from CO group are faulty to deliver co-stimulatory signals, through lower expression of co-stimulatory molecules. We showed an increased expression of IL-6, IL-1β, IL-12, and TNF, and decreased expression of IL-8 and IL-10 by neutrophils from CO compared to NW, while TGF-β is equivalently expressed in neutrophils from both groups. Despite this, we observed that TGF-β/inflammatory cytokine ratio was significantly higher than the IL-10/inflammatory cytokine ratio only in CO group. Our analysis showed obesity altering the correlation profile for the expression of co-stimulatory, recognition, and activation molecules, as well as for cytokines by neutrophils, suggesting an association between lower IL-10 expression and inflammation in childhood obesity.Conclusions: The unbalance between the ratio of IL-10 and TGF-β expressions, the IL-10 lower expression, and changes in correlation profile seem to contribute with an inefficient regulation of inflammatory cytokine expression in childhood obesity. However, these changes still not may be considered the sole mechanism that directs inflammation during childhood obesity, once other molecules, pathways, and cells should be evaluated. [ABSTRACT FROM AUTHOR]

Published
2018
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13. CD86 Expression by Monocytes Influence an Immunomodulatory Profile in Asymptomatic Patients with Chronic Chagas Disease.

Author

Pinto, Bruna F., Medeiros, Nayara I., Teixeira-Carvalho, Andrea, Eloi-Santos, Silvana M., Fontes-Cal, Tereza C. M., Rocha, Débora A., Dutra, Walderez O., Correa-Oliveira, Rodrigo, and Gomes, Juliana A. S.

Subjects
DIAGNOSIS of Chagas' disease, MONOCYTES, LYMPHOCYTES
Abstract

In the chronic phase of Chagas disease, 60% of the patients develop the asymptomatic form known as indeterminate (IND). The remaining 30% of the patients develop a life-threatening form in which digestive and/or cardiac (CARD) alterations take place. The mechanisms underlying the development of severe forms of Chagas disease remain poorly understood. It is well known that interactions between immune cells such as monocytes and lymphocytes drive immune responses. Further, the co-stimulatory molecules CD80 and CD86 expressed by monocytes and subsets induce lymphocyte activation, thereby triggering cellular immune response. Here, we revealed, for the first time, the functional-phenotypic profile of monocytes subsets in Chagas disease. Using flow cytometry, we evaluated the effect of in vitro stimulation with Trypanosoma cruzi antigens on the expression of the co-stimulatory molecules CD80 and CD86 in different monocyte subsets of patients with IND and CARD clinical forms of Chagas disease. We also assessed the expression of toll-like receptor (TLR)-2, TLR-4, TLR-9, HLA-DR, IL-10, and IL-12 in the monocyte subsets and of CTLA-4 and CD28, ligands of CD80 and CD86, in T lymphocytes. CD86 expression in all monocyte subsets was higher in IND patients when compared with non-infected (NI) individuals. After stimulation with T. cruzi, these patients also showed a higher frequency of CD4+CTLA-4+ T lymphocytes than NI individuals. We found an association between CD80 and CD28, and between CD86 and CTLA-4 expression, with a high frequency of regulatory T (Treg) cells in IND patients. We proposed that CD86 may be involved in immunoregulation by its association with CTLA-4 in asymptomatic patients. CD86 and CTLA-4 interaction may influence Treg activation, and this could represent a new strategy to control inflammation and tissue damage. [ABSTRACT FROM AUTHOR]

Published
2018
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14. Infection of Human Monocytes with Leishmania infantum Strains Induces a Downmodulated Response when Compared with Infection with Leishmania braziliensis.

Author

Viana, Agostinho Gonçalves, Magalhães, Luísa Mourão Dias, Giunchetti, Rodolfo Cordeiro, Dutra, Walderez O., and Gollob, Kenneth J.

Subjects
LEISHMANIA infantum, MICROBIAL virulence, PUBLIC health administration
Abstract

Human infection with different species of Leishmania leads to distinct clinical manifestations, ranging from relatively mild cutaneous (Leishmania braziliensis) to severe visceral (Leishmania infantum) forms of leishmaniasis. Here, we asked whether in vitro infection of human monocytes by Leishmania strains responsible for distinct clinical manifestations leads to early changes in immunological characteristics and ability of the host cells to control Leishmania. We evaluated the expression of toll-like receptors and MHC class II molecules, cytokines, and Leishmania control by human monocytes following short-term infection with L. braziliensis (M2904), a reference strain of L. infantum (BH46), and a wild strain of L. infantum (wild). The induction of TLR2, TLR9, and HLA-DR were all lower in L. infantum when compared with L. braziliensis-infected cells. Moreover, L. infantum-infected monocytes (both strains) produced lower TNF-alpha and a lower TNF-alpha/IL-10 ratio, resulting in a weaker inflammatory profile and a 100-fold less effective control of Leishmania than cells infected with L. braziliensis. Our results show that L. infantum strains fail to induce a strong inflammatory response, less activation, and less control of Leishmania from human monocytes, when compared with that induced by L. braziliensis infection. This functional profile may help explain the distinct clinical course observed in patients infected with the different Leishmania species. [ABSTRACT FROM AUTHOR]

Published
2018
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15. Vasoactive intestinal peptide degradation might influence Interleukin-17 expression in cardiac chagasic patients.

Author

Beltrão Pereira, Francielle, Dutra, Walderez O., Gollob, Kenneth J., Afonso Reis, Edna, Grossi de Oliveira, Ana Laura, Otávio da Costa Rocha, Manoel, and Alves da Silva Menezes, Cristiane

Abstract

The vasoactive intestinal peptide (VIP) expression is lower in cardiac chagasic patients and is related to worse cardiac function. The reduction of VIP in patients with Chagas disease may be a result of its enhanced degradation. To test this hypothesis, the tryptase and chymase expression was evaluated. We also related VIP levels with interleukin-17 (IL- 17) expression since VIP may modulate IL-17 production. Plasma levels of chymase were higher in chagasic patients. Conversely, VIP/chymase and VIP/tryptase ratios were lower in chagasic patients when compared to non-infected individuals. Besides, the VIP/chymase ratio was lower in chagasic cardiac patients in comparison with the indeterminate group. A positive correlation between tryptase and chymase levels was observed in chagasic cardiac patients. In relation to IL-17, we observed a higher expression of this cytokine in the cardiac form of the disease than in the indeterminate form. IL-17/VIP ratio was higher in the cardiac form in comparison with non-infected or indeterminate form. These results suggest that the low levels of VIP observed in chagasic patients could be due to an increased production of chymase and/or to the additive effect of the interaction between chymase and tryptase in the cardiac form. Moreover, the decreased VIP expression may contribute to the increase of IL-17 in chagasic cardiac patients. [ABSTRACT FROM AUTHOR]

Published
2018
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16. Distinct Trypanosoma cruzi isolates induce activation and apoptosis of human neutrophils.

Author

Magalhães, Luísa M. D., Viana, Agostinho, de Jesus, Augusto C., Chiari, Egler, Galvão, Lúcia, Gomes, Juliana A., Gollob, Kenneth J., and Dutra, Walderez O.

Subjects
TRYPANOSOMA, NEUTROPHILS, GRANULOCYTES, PHAGOCYTES, PATHOGENIC microorganisms
Abstract

Neutrophils are critical players in the first line of defense against pathogens and in the activation of subsequent cellular responses. We aimed to determine the effects of the interaction of Trypanosoma cruzi with human neutrophils, using isolates of the two major discrete type units (DTUs) associated with Chagas’ disease in Latin America (clone Col1.7G2 and Y strain, DTU I and II, respectively). Thus, we used CFSE-stained trypomastigotes to measure neutrophil-T. cruzi interaction, neutrophil activation, cytokine expression and death, after infection with Col1.7G2 and Y strain. Our results show that the frequency of CFSE+ neutrophils, indicative of interaction, and CFSE intensity on a cell-per-cell basis were similar when comparing Col1.7G2 and Y strains. Interaction with T. cruzi increased neutrophil activation, as measured by CD282, CD284, TNF and IL-12 expression, although at different levels between the two strains. No change in IL-10 expression was observed after interaction of neutrophils with either strain. We observed that exposure to Y and Col1.7G2 caused marked neutrophil death. This was specific to neutrophils, since interaction of either strain with monocytes did not cause death. Our further analysis showed that neutrophil death was a result of apoptosis, which was associated with an upregulation of TNF-receptor, TNF and FasLigand, but not of Fas. Induction of TNF-associated neutrophil apoptosis by the different T. cruzi isolates may act as an effective common mechanism to decrease the host’s immune response and favor parasite survival. [ABSTRACT FROM AUTHOR]

Published
2017
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17. Differential Expression of Matrix Metalloproteinases 2, 9 and Cytokines by Neutrophils and Monocytes in the Clinical Forms of Chagas Disease.

Author

Medeiros, Nayara I., Fares, Rafaelle C. G., Franco, Eliza P., Sousa, Giovane R., Mattos, Rafael T., Chaves, Ana T., Nunes, Maria do Carmo P., Dutra, Walderez O., Correa-Oliveira, Rodrigo, Rocha, Manoel O. C., and Gomes, Juliana A. S.

Subjects
DILATED cardiomyopathy, MATRIX metalloproteinases, CYTOKINES, CHAGAS' disease, NEUTROPHILS
Abstract

Dilated cardiomyopathy, the most severe manifestation in chronic phase of Chagas disease, affects about 30% of patients and is characterized by myocardial dysfunction and interstitial fibrosis due to extracellular matrix (ECM) remodeling. ECM remodeling is regulated by proteolytic enzymes such as matrix metalloproteinases (MMPs) and cytokines produced by immune cells, including phagocytes. We evaluated by flow cytometry the expression of MMP-2, MMP-9, IL-1β, TNF-α, TGF-β and IL-10 by neutrophils and monocytes from patients with indeterminate (IND) and cardiac (CARD) clinical forms of Chagas disease and non-infected individuals (NI), before and after in vitro stimulation with Trypanosoma cruzi antigens. Our results showed an important contribution of neutrophils for MMPs production, while monocytes seemed to be involved in cytokine production. The results showed that neutrophils and monocytes from IND and CARD patients had higher intracellular levels of MMP-2 and MMP-9 than NI individuals. On the other hand, T. cruzi derived-antigens promote a differential expression of MMP-2 and MMP-9 in patients with Chagas disease and may regulate MMPs expression in neutrophils and monocytes, mainly when a cardiac alteration is not present. Our data also showed that in the presence of T. cruzi derived-antigens the production of cytokines by neutrophils and monocytes, but mainly by monocytes, may be intensified. Correlation analysis demonstrated that MMP-2 had a positive correlation with IL-10 and a negative correlation with IL-1β, whereas MMP-9 showed a negative correlation with IL-10. We also observed that IND patients presented a greater percentage of high producer cells of regulatory molecules when compared to CARD patients, indicating a different pattern in the immune response. Our data suggest that MMPs and cytokines produced by neutrophils and monocytes are important contributors for cardiac remodeling and may be an interesting target for new biomarker research. [ABSTRACT FROM AUTHOR]

Published
2017
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18. Chronic Low-Grade Inflammation in Childhood Obesity Is Associated with Decreased IL-10 Expression by Monocyte Subsets.

Author

Mattos, Rafael T., Medeiros, Nayara I., Menezes, Carlos A., Fares, Rafaelle C. G., Franco, Eliza P., Dutra, Walderez O., Rios-Santos, Fabrício, Correa-Oliveira, Rodrigo, and Gomes, Juliana A. S.

Subjects
GENETICS of childhood obesity, TREATMENT of childhood obesity, IMMUNOREGULATION, CYTOKINES, MONOCYTES
Abstract

Chronic low-grade inflammation is related to the development of comorbidities and poor prognosis in obesity. Monocytes are main sources of cytokines and play a pivotal role in inflammation. We evaluated monocyte frequency, phenotype and cytokine profile of monocyte subsets, to determine their association with the pathogenesis of childhood obesity. Children with obesity were evaluated for biochemical and anthropometric parameters. Monocyte subsets were characterized by flow cytometry, considering cytokine production and activation/recognition molecules. Correlation analysis between clinical parameters and immunological data delineated the monocytes contribution for low-grade inflammation. We observed a higher frequency of non-classical monocytes in the childhood obesity group (CO) than normal-weight group (NW). All subsets displayed higher TLR4 expression in CO, but their recognition and antigen presentation functions seem to be diminished due to lower expression of CD40, CD80/86 and HLA-DR. All subsets showed a lower expression of IL-10 in CO and correlation analyses showed changes in IL-10 expression profile. The lower expression of IL-10 may be decisive for the maintenance of the low-grade inflammation status in CO, especially for alterations in non-classical monocytes profile. These cells may contribute to supporting inflammation and loss of regulation in the immune response of children with obesity. [ABSTRACT FROM AUTHOR]

Published
2016
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19. What the Erythrocytic Nuclear Alteration Frequencies Could Tell Us about Genotoxicity and Macrophage Iron Storage?

Author

Gomes, Juliana M. M., Ribeiro, Heder J., Procópio, Marcela S., Alvarenga, Betânia M., Castro, Antônio C. S., Dutra, Walderez O., da Silva, José B. B., and Corrêa Junior, José D.

Subjects
ERYTHROCYTES, GENETIC toxicology, MACROPHAGES, IRON compounds, ELECTRON microscopy
Abstract

Erythrocytic nuclear alterations have been considered as an indicative of organism’s exposure to genotoxic agents. Due to their close relationship among their frequencies and DNA damages, they are considered excellent markers of exposure in eukaryotes. However, poor data has been found in literature concerning their genesis, differential occurrence and their life span. In this study, we use markers of cell viability; genotoxicity and cellular turn over in order to shed light to these events. Tilapia and their blood were exposed to cadmium in acute exposure and in vitro assays. They were analyzed using flow cytometry for oxidative stress and membrane disruption, optical microscopy for erythrocytic nuclear alteration, graphite furnace atomic absorption spectrometry for cadmium content in aquaria water, blood and cytochemical and analytical electron microscopy techniques for the hemocateretic aspects. The results showed a close relationship among the total nuclear alterations and cadmium content in the total blood and melanomacrophage centres area, mismatching reactive oxygen species and membrane damages. Moreover, nuclear alterations frequencies (vacuolated, condensed and blebbed) showed to be associated to cadmium exposure whereas others (lobed and bud) were associated to depuration period. Decrease on nuclear alterations frequencies was also associated with hemosiderin increase inside spleen and head kidney macrophages mainly during depurative processes. These data disclosure in temporal fashion the main processes that drive the nuclear alterations frequencies and their relationship with some cellular and systemic biomarkers. [ABSTRACT FROM AUTHOR]

Published
2015
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20. Differential Activation of Human Monocytes and Lymphocytes by Distinct Strains of Trypanosoma cruzi.

Author

Magalhães, Luísa M. D., Viana, Agostinho, Chiari, Egler, Galvão, Lúcia M. C., Gollob, Kenneth J., and Dutra, Walderez O.

Subjects
TRYPANOSOMA cruzi, CHAGAS' disease, MONOCYTES, LYMPHOCYTE receptors, GRANZYMES, PHYSIOLOGY
Abstract

Background: Trypanosoma cruzi strains are currently classified into six discrete typing units (DTUs) named TcI to VI. It is known that these DTUs have different geographical distribution, as well as biological features. TcI and TcII are major DTUs found in patients from northern and southern Latin America, respectively. Our hypothesis is that upon infection of human peripheral blood cells, Y strain (Tc II) and Col cl1.7 (Tc I), cause distinct immunological changes, which might influence the clinical course of Chagas disease. Methodology/Principal Findings: We evaluated the infectivity of CFSE-stained trypomastigotes of Col cl1.7 and Y strain in human monocytes for 15 and 72 hours, and determined the immunological profile of lymphocytes and monocytes exposed to the different isolates using multiparameter flow cytometry. Our results showed a similar percentage and intensity of monocyte infection by Y and Col cl1.7. We also observed an increased expression of CD80 and CD86 by monocytes infected with Col cl1.7, but not Y strain. IL-10 was significantly higher in monocytes infected with Col cl1.7, as compared to Y strain. Moreover, infection with Col cl1.7, but not Y strain, led to an increased expression of IL-17 by CD8+ T cells. On the other hand, we observed a positive correlation between the expression of TNF-alpha and granzyme A only after infection with Y strain. Conclusion/Significance: Our study shows that while Col cl1.7 induces higher monocyte activation and, at the same time, production of IL-10, infection with Y strain leads to a lower monocyte activation but higher inflammatory profile. These results show that TcI and TcII have a distinct immunological impact on human cells during early infection, which might influence disease progression. [ABSTRACT FROM AUTHOR]

Published
2015
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21. Acute Chagas Disease: New Global Challenges for an Old Neglected Disease.

Author

Andrade, Daniela V., Gollob, Kenneth J., and Dutra, Walderez O.

Subjects
CHAGAS' disease, ACUTE diseases, NEGLECTED diseases, PROTOZOAN diseases, HIV infections
Abstract

Chagas disease is caused by infection with the protozoan Trypanosoma cruzi, and although over 100 years have passed since the discovery of Chagas disease, it still presents an increasing problem for global public health. A plethora of information concerning the chronic phase of human Chagas disease, particularly the severe cardiac form, is available in the literature. However, information concerning events during the acute phase of the disease is scarce. In this review, we will discuss (1) the current status of acute Chagas disease cases globally, (2) the immunological findings related to the acute phase and their possible influence in disease outcome, and (3) reactivation of Chagas disease in immunocompromised individuals, a key point for transplantation and HIV infection management. [ABSTRACT FROM AUTHOR]

Published
2014
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22. Acute Chagas Disease: New Global Challenges for an Old Neglected Disease.

Author

Andrade, Daniela V., Gollob, Kenneth J., and Dutra, Walderez O.

Subjects
CHAGAS' disease, PROTOZOAN diseases, MEDICAL protozoology, HIV infections, IMMUNE system
Abstract

Chagas disease is caused by infection with the protozoan Trypanosoma cruzi, and although over 100 years have passed since the discovery of Chagas disease, it still presents an increasing problem for global public health. A plethora of information concerning the chronic phase of human Chagas disease, particularly the severe cardiac form, is available in the literature. However, information concerning events during the acute phase of the disease is scarce. In this review, we will discuss (1) the current status of acute Chagas disease cases globally, (2) the immunological findings related to the acute phase and their possible influence in disease outcome, and (3) reactivation of Chagas disease in immunocompromised individuals, a key point for transplantation and HIV infection management. [ABSTRACT FROM AUTHOR]

Published
2014
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23. Interleukin-6 gene polymorphism (−174 G/C) is associated with toxoplasmic retinochoroiditis.

Author

Cordeiro, Cynthia A., Moreira, Paula R., Bessa, Thais F., Costa, Germano C., Dutra, Walderez O., Campos, Wesley R., Oréfice, Fernando, Young, Lucy H., and Teixeira, Antônio L.

Subjects
INTERLEUKIN-6, GENETIC polymorphisms, TOXOPLASMA, CHOROIDITIS, RETINAL diseases, OCULAR toxoplasmosis, POLYMERASE chain reaction methodology, PATIENTS
Abstract

. Purpose: Experimental data have demonstrated a relevant role for IL-6 in the modulation of acute ocular toxoplasmosis. Therefore, we aim to investigate the possible association between the IL-6 gene polymorphism at position -174 and toxoplasmic retinochoroiditis (TR) in humans. Methods: Ninety-seven patients with diagnosed TR were recruited from the Uveitis Section, Federal University of Minas Gerais. For comparison, 83 healthy blood donors with positive serology for toxoplasmosis and without retinal signs of previous TR were included in the study. Genomic DNA was obtained from oral swabs of individuals and amplified using polymerase chain reaction (PCR) with specific primers flanking the locus −174 of IL-6 (−174G/C). PCR products were submitted to restriction endonuclease digestion and analysed by polyacrylamide gel electrophoresis to distinguish allele G and C of the IL-6 gene, allowing the detection of the polymorphism and determination of genotypes. Results: There was a significant difference in the genotype (χ2 = 12.9, p = 0.001) and allele (χ2 = 6.62, p = 0.01) distribution between TR patients and control subjects. In a subgroup analysis, there was no significant difference in genotypes and allele frequencies regarding TR recurrence. Conclusions: This study suggests that the genotypes related with a lower production of IL-6 may be associated with the occurrence of TR. [ABSTRACT FROM AUTHOR]

Published
2013
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24. High interleukin 17 expression is correlated with better cardiac function in human Chagas disease.

Author

Magalhaes LM, Villani FN, Nunes Mdo C, Gollob KJ, Rocha MO, Dutra WO, Magalhães, Luisa M D, Villani, Fernanda N A, Nunes, Maria do Carmo P, Gollob, Kenneth J, Rocha, Manoel O C, and Dutra, Walderez O

Abstract

This study was designed to investigate whether the expression of interleukin 17 (IL-17) is associated with the indeterminate or cardiac clinical forms of Chagas disease and whether IL-17 expression can be correlated with patients' cardiac function. Our results demonstrated that cardiac Chagas patients have a lower intensity of expression of IL-17 by total lymphocytes and lower frequency of circulating T helper 17 cells. Correlative analysis showed that high IL-17 expression was associated with better cardiac function, as determined by left ventricular ejection fraction and left ventricular diastolic diameter values. Therefore, IL-17 expression can be a protective factor to prevent myocardial damage in human Chagas disease. [ABSTRACT FROM AUTHOR]

Published
2013
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25. High Interleukin 17 Expression Is Correlated With Better Cardiac Function in Human Chagas Disease.

Author

Magalhães, Luisa M. D., Villani, Fernanda N. A., Nunes, Maria do Carmo P., Gollob, Kenneth J., Rocha, Manoel O. C., and Dutra, Walderez O.

Subjects
CHAGAS' disease, INTERLEUKIN-17, GENE expression, LYMPHOCYTES, CARDIOMYOPATHIES, DIASTOLE (Cardiac cycle), HEART function tests, PREVENTION
Abstract

This study was designed to investigate whether the expression of interleukin 17 (IL-17) is associated with the indeterminate or cardiac clinical forms of Chagas disease and whether IL-17 expression can be correlated with patients' cardiac function. Our results demonstrated that cardiac Chagas patients have a lower intensity of expression of IL-17 by total lymphocytes and lower frequency of circulating T helper 17 cells. Correlative analysis showed that high IL-17 expression was associated with better cardiac function, as determined by left ventricular ejection fraction and left ventricular diastolic diameter values. Therefore, IL-17 expression can be a protective factor to prevent myocardial damage in human Chagas disease. [ABSTRACT FROM AUTHOR]

Published
2013

28. Interleukin 17 Production among Patients with American Cutaneous Leishmaniasis.

Author

Bacellar, Olívia, Faria, Daniela, Nascimento, Márcia, Cardoso, Thiago M., Gollob, Kenneth J., Dutra, Walderez O., Scott, Phillip, and Carvalho, Edgar M.

Subjects
INTERLEUKINS, CUTANEOUS leishmaniasis, LEISHMANIASIS, LYMPHOCYTES, INFLAMMATION, AUTOIMMUNITY, PROTOZOAN diseases, PARASITIC diseases
Abstract

Interleukin 17 (IL-17) plays a critical role in inflammation and autoimmunity. Very little is known about IL- 17 in protozoa infection. Here, we show that lymphocytes obtained from patients with mucosal leishmaniasis and cutaneous leishmaniasis produce higher levels of IL-17 than do lymphocytes obtained from uninfected control subjects (P < .01). There was a tendency for tissue obtained from patients with mucosal leishmaniasis to contain a higher number of cells expressing IL-17, compared with tissue obtained from patients with cutaneous leishmaniasis, and there was a direct correlation between the number of cells expressing IL-17 and the presence of cellular inflammation at the lesion site (r² = 0.86; P < .001). These data support the role of IL-17 in the pathogenesis of the inflammatory reaction in leishmaniasis. [ABSTRACT FROM AUTHOR]

Published
2009
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29. Functional IL-10 Gene Polymorphism Is Associated with Chagas Disease Cardiomyopathy.

Author

Costa, Germano C., da Costa Rocha, Manoel Otávio, Moreira, Paula Rocha, Silva Menezes, Cristiane Alves, Silva, Micena R., Gollob, Kenneth J., and Dutra, Walderez O.

Subjects
INTERLEUKIN-10, GENETIC polymorphisms, CARDIOMYOPATHIES, HEART diseases, TRYPANOSOMA cruzi, INTERLEUKINS, CHAGAS' disease, GENE expression, DISEASE susceptibility
Abstract

This study was designed to determine whether the functional IL-10 gene polymorphism -1082G/A is associated with the development of cardiomyopathy in individuals infected with Trypanosoma cruzi and whether interleukin (IL)-10 expression can be correlated with patients' cardiac function. Our results demonstrated that the polymorphic allele, which correlates with lower expression of IL-10, was associated with the development of Chagas disease cardiomyopathy. Accordingly, correlative analysis showed that low IL-10 expression was associated with worse cardiac function, as determined by leftventricular ejection fraction values. Therefore, the IL-10 gene polymorphism and IL-10 expression are important in determining susceptibility to chagasic cardiomyopathy. [ABSTRACT FROM AUTHOR]

Published
2009
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31. Cutaneous Leishmaniasis during Pregnancy: Exuberant Lesions and Potential Fetal Complications.

Author

Morgan, Daniel J., Guimaraes, Luiz H., Machado, Paulo R. L., D'Oliveira Jr., Argemiro, Almeida, Roque P., Lago, Ednaldo L., Faria, Daniela R., Tafuri, Wagner L., Dutra, Walderez O., and Carvalho, Edgar M.

Subjects
LEISHMANIASIS, PREGNANCY complications, PREGNANT women, MEDICAL care, FETAL death
Abstract

Cutaneous leishmaniasis affects millions of people worldwide. After observations of atypical lesions in pregnant women at the health centers of Corte de Pedra, Brazil, 9 years of records were reviewed, and 26 pregnant patients were identified. A retrospective case-control study revealed that lesions in pregnant women were much larger than those in nonpregnant patients in an age- and sex-matched group (mean area, 6.08 cm² vs. 1.46 cm²;P = .008), and many lesions had an exophytic nature. Despite foregoing treatment until after delivery, response to pentavalent antimony therapy was favorable (rate of cure with 1 course of treatment, 85%). High rates of preterm births (10.5%) and stillbirths (10.5%) were reported. Cutaneous leishmaniasis during pregnancy produces distinct lesions and may have adverse fetal effects. [ABSTRACT FROM AUTHOR]

Published
2007
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32. A functional interleukin-1β gene polymorphism is associated with chronic periodontitis in a sample of Brazilian individuals.

Author

Moreira, Paula R., De Sá, Alessandra R., Xavier, Guilherme M., Costa, José E., Gomez, Ricardo S., Gollob, Kenneth J., and Dutra, Walderez O.

Subjects
INTERLEUKIN-1, GENES, PERIODONTITIS, ENDONUCLEASES, POLYMERASE chain reaction
Abstract

Background: Interleukin-1 beta (IL-1β) is a potent inflammatory mediator and an important polymorphism in the locus +3954 (C/T) of the human IL1B gene has been shown to affect the levels of this cytokine. This functional polymorphism has been associated with the establishment of inflammatory diseases, including periodontal disease, in European, Asian and North American populations. The aim of this study was to investigate the association between the IL1B (+3954) gene polymorphism and the occurrence of different clinical forms of periodontitis in a sample of Brazilian individuals. This study employed a cross-sectional design involving individuals from the State of Minas Gerais in the south-eastern region of Brazil. Genomic DNA was obtained from oral swabs of 129 individuals and amplified using the polymerase chain reaction (PCR) with specific primers flanking the locus +3954 of IL1B. PCR products were submitted to restriction endonuclease digestion and analyzed by polyacrylamide gel electrophoresis, to distinguish alleles T and C of the IL1B gene, allowing for the determination of the genotypes and detection of the polymorphism. The chronic periodontitis group displayed a higher percentage of the T allele (28%) when compared to the aggressive periodontitis group (10.7%, χ2 = 5.24, p = 0.02, OR = 0.31, CI = 0.11–0.88) and to control group (8.7%, χ2 = 7.11, p = 0.007, OR = 0.24, CI = 0.08–0.73). Our data suggested that the polymorphism in the locus +3954 of IL1B gene could be a risk factor for chronic periodontitis in a sample of Brazilian individuals. [ABSTRACT FROM AUTHOR]

Published
2005
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33. Helminthic Infection Down-Regulates Type 1 Immune Responses in Human T Cell Lymphotropic Virus Type 1 (HTLV-1) Carriers and Is More Prevalent in HTLV-1 Carriers than in Patients with HTLV-1--Associated Myelopathy/Tropical Spastic Paraparesis.

Author

Porto, Aur&aacute F., Santos, Silvane B., Muniz, André L., Basílio, Vanessa, Rodrigues Jr., Waldyr, Neva, Franklin A., Dutra, Walderez O., Gollob, Kenneth J., Jacobson, Steven, and Carvalho, Edgar M.

Subjects
T cells, IMMUNOLOGY, CYTOKINES, IMMUNOREGULATION, ANTINEOPLASTIC agents, ANTIVIRAL agents
Abstract

Human T cell lymphotropic virus type 1 (HTLV-1) infection is associated with an exacerbated type 1 immune response and secretion of high levels of proinflammatory cytokines. In contrast, helminthic infection induces a type 2 immune response. In the present study, the cytokine profile in HTLV-1 carriers coinfected with helminths (Strongyloides stercoralis and/or Schistosoma mansoni) was compared with that in HTLV-1 carriers not coinfected with helminths. Levels of interferon (IFN)-γ were higher in HTLV-1 carriers not coinfected with helminths than in HTLV-1 carriers coinfected with helminths (p<.05). The overall frequency of IFN-γ-P<.05 expressing CD8+ and CD4+ cells was decreased in HTLV-1 carriers coinfected with helminths (p<.05). The P<.05 percentage of interleukin (IL)-5- and IL-10-expressing T cells in HTLV-1 carriers coinfected with helminths was higher than that in HTLV-1 carriers not coinfected with helminths (p<.05). Moreover, we found that the prevalence of helminthic infection was 7-fold higher in HTLV-1 carriers than in patients with HTLV-1- associated myelopathy/tropical spastic paraparesis (p<.05). These data show that helminthic infection decreases activation of type 1 cells, which may influence the clinical outcome of HTLV-1 infection. [ABSTRACT FROM AUTHOR]

Published
2005
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34. Exacerbated inflammatory cellular immune response characteristics of HAM/TSP is observed in a large proportion of HTLV-I asymptomatic carriers.

Author

Santos, Silvane Braga, Porto, Aurélia Fonseca, Muniz, André Luiz, De Jesus, Amélia Ribeiro, Magalhães, Elza, Melo, Ailton, Dutra, Walderez O., Gollob, Kenneth J., and Carvalho, Edgar M.

Subjects
IMMUNE response, DISEASES, HTLV-I, BIOMARKERS, IMMUNOLOGY
Abstract

Background: A small fraction of Human T cell Leukemia Virus type-1 (HTLV-I) infected subjects develop a severe form of myelopathy. It has been established that patients with HTLV-I associated myelopathy/tropical spastic paraparesis (HAM/TSP) show an exaggerated immune response when compared with the immunological response observed in HTLV-I asymptomatic carriers. In this study the immunological responses in HAM/TSP patients and in HTLV-I asymptomatic carriers were compared using several immunological assays to identify immunological markers associated with progression from infection to disease. Methods: Immunoproliferation assays, cytokine levels of unstimulated cultures, and flow cytometry analysis were used to evaluate the studied groups. Nonparametric tests (Mann-Whitney U test and Wilcoxon matched-pairs signed ranks) were used to compare the difference between the groups. Results: Although both groups showed great variability, HAM/TSP patients had higher spontaneous lymphoproliferation as well as higher IFN-γ levels in unstimulated supernatants when compared with asymptomatic carriers. Flow cytometry studies demonstrated a high frequency of inflammatory cytokine (IFN-γ and TNF-α) producing lymphocytes in HAM/TSP as compared to the asymptomatic group. This difference was accounted for mainly by an increase in CD8 cell production of these cytokines. Moreover, the HAM/TSP patients also expressed an increased frequency of CD28-/CD8+ T cells. Since forty percent of the asymptomatic carriers had spontaneous lymphoproliferation and IFN-γ production similar to HAM/TSP patients, IFN-γ levels were measured eight months after the first evaluation in some of these patients to observe if this was a transient or a persistent situation. No significant difference was observed between the means of IFN-γ levels in the first and second evaluation. Conclusions: The finding that a large proportion of HTLV-I carriers present similar immunological responses to those observed in HAM/TSP, strongly argues for further studies to evaluate these parameters as markers of HAM/TSP progression. [ABSTRACT FROM AUTHOR]

Published
2004
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35. Polarized Th2 like cells, in the absence of Th0 cells, are responsible for lymphocyte produced IL-4 in high IgE-producer schistosomiasis patients.

Author

Dutra, Walderez O., Correa-Oliveira, Rodrigo, Dunne, David, Cecchini, Luiza Fosenca, Fraga, Lúcia, Roberts, Morven, Soares-Silveira, Alda Maria, Webster, Michelle, Yssel, Hans, and Gollob, Kenneth J.

Subjects
INTERLEUKIN-4, INTERFERONS, INTERLEUKIN-5, INTERLEUKIN-2, LYMPHOCYTES, SCHISTOSOMIASIS, IMMUNOGLOBULIN E, CELL proliferation, PATIENTS
Abstract

Background: Human resistance to re-infection with S. mansoni is correlated with high levels of anti-soluble adult worm antigens (SWAP) IgE. Although it has been shown that IL-4 and IL-5 are crucial in establishing IgE responses in vitro, the active in vivo production of these cytokines by T cells, and the degree of polarization of Th2 vs. Th0 in human schistosomiasis is not known. To address this question, we determined the frequency of IL-4 and IFN-γ or IL-5 and IL-2 producing lymphocytes from schistosomiasis patients with high or low levels of IgE anti-SWAP. Results: Our analysis showed that high and low IgE-producers responded equally to schistosomiasis antigens as determined by proliferation. Moreover, patients from both groups displayed similar percentages of circulating lymphocytes. However, high IgE-producers had an increased percentage of activated CD4+ T cells as compared to the low IgE-producers. Moreover, intracellular cytokine analysis, after short-term stimulation with anti-CD3/CD28 mAbs, showed that IgE high-producers display an increase in the percentage of T lymphocytes expressing IL-4 and IL-5 as compared to IgE low-responders. A coordinate control of the frequency of IL-4 and IL-5 producing lymphocytes in IgE high, but not IgE low-responders, was observed. Conclusions: High IgE phenotype human schistosomiasis patients exhibit a coordinate regulation of IL-4 and IL-5 producing cells and the lymphocyte derived IL-4 comes from true polarized Th2 like cells, in the absence of measurable Th0 cells as measured by co-production of IL-4 and IFN-γ. [ABSTRACT FROM AUTHOR]

Published
2002
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37. Activated T and B lymphocytes in peripheral blood of patients with Chagas' disease.

Author

Dutra, Walderez O., Martins-Filho, Olindo A., Can¸ado, Jose R., Pinto-Dias, Joao Carlos, Brener, Zigman, Freeman, George L., Colley, Daniel G., Gazzinelll, Giovanni, and Parra, Jupara C.

Abstract

Whole blood preparations from patients with either the indeterminate (asymptomatic) or cardiac clinical forms of chronic infection were analyzed by flow cytometry using double-labeling to identify subsets of circulating lymphocytes. Several significant differences were demonstrated between the blood lymphocyte profiles of chagaslc patients and non-chagaslc controls. Clear increase in the percentages and actual numbers of double-positive cells of the phenotype CD3/HLA-DR, as well as decrease in the percentage of CD45RA/CD4 and CD45RA/CD8 T cells, Indicate greater numbers of activated T cells circulating in the blood of infected patients. Consistent parallel increases were seen also in the B lymphocyte subset which stained double-positive for CD19/CD5. There were no significant differences in the circulation of these chronic chagaslc patients in the CD4:CD8 ratios. Also, no substantive phenotyplc differences were observed in the lymphocyte populations between the two ends of the clinical spectrum (Indeterminate versus cardiac) in chronic human Chagas' disease. These observations demonstrate that increased levels of activated T cells and CD5 B cells are present in the circulation of people with chronic Chagas' disease. These are cell phenotypes that have been associated in other conditions with autoimmune, polyclonal, and hyperlmmune responses. The specificities of these activated cells and the roles they may play in resistance or pathogenesis during chronic Chagas' disease need now to be determined. [ABSTRACT FROM PUBLISHER]

Published
1994

40. Co‐infection with distinct Trypanosoma cruzi strains induces an activated immune response in human monocytes.

Author

Magalhães, Luísa M.D., Passos, Lívia S.A., Chiari, Egler, Galvão, Lúcia M.C., Koh, Carolina C., Rodrigues‐Alves, Marina L., Giunchetti, Rodolfo C., Gollob, Kenneth, and Dutra, Walderez O.

Subjects
CHAGAS' disease, MIXED infections, TRYPANOSOMA cruzi, IMMUNE response, MONOCYTES
Abstract

Aims: The aim of the study was to evaluate the immune response triggered by the first contact of human monocytes with two T cruzi strains from distinct discrete typing units (DTUs) IV and V, and whether co‐infection with these strains leads to changes in monocyte immune profiles, which could in turn influence the subsequent infection outcome. Methods and results: We evaluated the influence of in vitro single‐ and co‐infection with AM64 and 3253 strains on immunological characteristics of human monocytes. Single infection of monocytes with AM64 or 3253 induced opposing anti‐inflammatory and inflammatory responses, respectively. Co‐infection was observed in over 50% of monocytes after 15 hours of culture, but this percentage dropped ten‐fold after 72 hours. Co‐infection led to high monocyte activation and an increased percentage of both IL‐10 and TNF. The decreased percentage of co‐infected cells observed after 72 hours was associated with a decreased frequency of TNF‐expressing cells. Conclusion: Our results show that the exacerbated response observed in co‐infection with immune‐polarizing strains is associated with a decreased frequency of co‐infected cells, suggesting that the activated response favours parasite control. These findings may have implications for designing new Chagas disease preventive strategies. [ABSTRACT FROM AUTHOR]

Published
2019
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41. MMP-2 and MMP-9 plasma levels are potential biomarkers for indeterminate and cardiac clinical forms progression in chronic Chagas disease.

Author

Medeiros, Nayara I., Gomes, Juliana A. S., Fiuza, Jacqueline A., Sousa, Giovane R., Almeida, Eliane F., Novaes, Renata O., Rocha, Virgínia L. S., Chaves, Ana T., Dutra, Walderez O., Rocha, Manoel O. C., and Correa-Oliveira, Rodrigo

Subjects
BIOLOGICAL tags, CHRONIC diseases, IMMUNOASSAY, CARDIAC patients, GELATINASES
Abstract

One of the major challenges in chronic Chagas disease is to understand the mechanisms that predict the clinical evolution from asymptomatic to severe cardiac clinical forms. Our cohort consisted of twenty-eight Chagas disease patients followed for twenty years. Plasma levels of MMP-2 and MMP-9 gelatinases and TIMPs were evaluated by multiplexed immunoassay at two points in time with an average interval of six years. MMP-2 plasma levels, but not MMP-9, increased in cardiac patients over time. TIMP-1 levels diminished in cardiac patients, while TIMP-3 dropped in asymptomatic patients in the course of the evaluated interval. An inversion of time lines was observed relative to the clinical asymptomatic and cardiac forms for MMP-2. Receiver Operating Characteristic (ROC) curve analysis identified MMP-2 as a biomarker to distinguish asymptomatic from cardiac clinical forms, while MMP-9 is a biomarker that segregates infected from non-infected patients. We have pointed out that MMP-2 and MMP-9 together can predict clinical evolution in Chagas disease. MMP-2 was suggested as a biomarker for fibrosis replacement in early remodeling and a sensitive predictor for initial changes in asymptomatic patients that may evolve into the cardiac clinical form. MMP-9 seems to be a biomarker for late fibrosis and severe cardiac remodeling in cardiac patients. [ABSTRACT FROM AUTHOR]

Published
2019
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42. Leishmania infantum induces expression of the negative regulatory checkpoint, CTLA‐4, by human naïve CD8+ T cells.

Author

Viana, Agostinho Gonçalves, Magalhães, Luísa Mourão Dias, Giunchetti, Rodolfo Cordeiro, Dutra, Walderez O., and Gollob, Kenneth J.

Subjects
T cells, LEISHMANIA infantum, CYTOTOXIC T lymphocyte-associated molecule-4, VISCERAL leishmaniasis, LEISHMANIASIS, INTRACELLULAR pathogens, INTERLEUKIN-4, PROGRAMMED cell death 1 receptors
Abstract

Aims: CD8+ T cells are important in mediating protective responses to intracellular pathogens. However, an uncontrolled response may lead to pathology. The role of CD8+ T cells in different clinical manifestations of human leishmaniasis is controversial and poorly understood. We aim to study the response of CD8+ T cells to the first exposure to different strains of Leishmania, seeking to correlate these findings with clinical manifestations of disease. Methods and results: We have evaluated the expression of granzyme A, inflammatory and anti‐inflammatory cytokines, as well as CTLA‐4 by human naïve CD8+ T cells exposed to Leishmania braziliensis and two different strains of Leishmania infantum in vitro. We observed that while exposure to L braziliensis induced an inflammatory profile, as measured by the expression of granzyme A, IFN‐gamma and IL‐17, as well as a higher IFN/IL‐10 ratio, exposure to L infantum led to a regulatory profile, as measured by lower IFN/IL‐10 ratio and higher expression of CTLA‐4. Conclusion: These results may help explain why patients with the visceral clinical form present a weaker cellular response and, consequently, a worse outcome of the disease. The use of CTLA‐4 checkpoint inhibitors may emerge as a potential immunotherapy to ameliorate the immune response in visceral leishmaniasis patients. [ABSTRACT FROM AUTHOR]

Published
2019
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43. The Role of Co-Stimulatory Molecules in Chagas Disease.

Author

Pinto, Bruna F., Medeiros, Nayara I., Fontes-Cal, Tereza C. M., Naziazeno, Isabela M., Correa-Oliveira, Rodrigo, Dutra, Walderez O., and Gomes, Juliana A. S.

Subjects
CHAGAS' disease, TRYPANOSOMA cruzi, MONOCYTES, LYMPHOCYTES, T cells
Abstract

Chagas disease, caused by Trypanosoma cruzi, is a potentially life-threatening tropical disease endemic to Latin American countries that affects approximately 8 million people. In the chronic phase of the disease, individuals are classified as belonging to the indeterminate clinical form or to the cardiac and/or digestive forms when clinical symptoms are apparent. The relationship between monocytes and lymphocytes may be an important point to help clarify the complexity that surrounds the clinical symptoms of the chronic phase of Chagas disease. The co-stimulatory signals are essential to determining the magnitude of T cell response to the antigen. The signals are known to determine the regulation of subsequent adaptive immune response. However, little is known about the expression and function of these molecules in Chagas disease. Therefore, this review aims to discuss the possible role of main pathways of co-stimulatory molecule-receptor interactions in this pathology that could be crucial to understand the disease dynamics. [ABSTRACT FROM AUTHOR]

Published
2018
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44. Chagas Cardiomyopathy: An Update of Current Clinical Knowledge and Management: A Scientific Statement From the American Heart Association.

Author

Nunes, Maria Carmo Pereira, Beaton, Andrea, Acquatella, Harry, Bern, Caryn, Bolger, Ann F., Echeverría, Luis E., Dutra, Walderez O., Gascon, Joaquim, Morillo, Carlos A., Oliveira-Filho, Jamary, Ribeiro, Antonio Luiz Pinho, Marin-Neto, Jose Antonio, Echeverría, Luis E, and American Heart Association Rheumatic Fever, Endocarditis and Kawasaki Disease Committee of the Council on Cardiovascular Disease in the Young; Council on Cardiovascular and Stroke Nursing; and Stroke Council

Published
2018
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45. Histopathological outcome of Leishmania major -infected BALB/c mice is improved by oral treatment with N-acetyl-l-cysteine.

Author

Rocha-Vieira, Etel, Ferreira, Ellen, Vianna, Priscila, De Faria, Daniela R., Gaze, Soraya T., Dutra, Walderez O., and Gollob, Kenneth J.

Subjects
LEISHMANIA, GLUTATHIONE
Abstract

Summary Leishmania major infected BALB/c mice were treated with N-acetyl-l-cysteine (NAC), a glutathione precursor, to evaluate the role of in vivo glutathione on lesion pathology and cytokine profiles following infection. Mice were maintained on NAC-containing water 2 days before infection for a total of 14 weeks. The BALB/c response to L. major infection was improved by oral administration of NAC, at the level of histopathological outcome, lesion progression and cytokine profile. A significantly improved histopathological outcome of the footpad lesion, characterized by a mixed inflammatory infiltrate organized in a focal pattern with little tissue destruction and a reduced parasite load, was observed in NAC-treated BALB/c mice. Histopathological modulation was accompanied by a modified cytokine pattern from popliteal lymph node cells, demonstrated by a sustained higher frequency of interferon-γ (IFN-γ) and tumour necrosis factor-α (TNF-α)-producing cells. This work points to an important role for glutathione in the modulation of effector responses in BALB/c mice. [ABSTRACT FROM AUTHOR]

Published
2003
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