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Dive into the research topics where Fernanda Nazaré Morgado is active.

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Featured researches published by Fernanda Nazaré Morgado.


Medical Mycology | 2007

Comparison of virulence of different Sporothrix schenckii clinical isolates using experimental murine model

Marcelly Maria dos Santos Brito; Fátima Conceição-Silva; Fernanda Nazaré Morgado; Priscila S. Raibolt; Armando de Oliveira Schubach; Tania Pacheco Schubach; Guido Vidal Schäffer; Cintia de Moraes Borba

The virulence of two strains of Sporothrix schenckii isolated from patients with lymphocutaneous or disseminated sporotrichosis were examined in BALB/c mice (Group 1 and 2, respectively). The mice were inoculated subcutaneously into the left hind footpad with 4 x 10(6) S. schenckii yeast cells in order to evaluate (i) the development of cutaneous lesions, (ii) signs of inactivity, (iii) weight loss, (iv) survival rates, (v) number of viable yeast cells in the lungs and spleen, (vi) splenic index, (vii) extent of organ lesions, and (viii) immunological responses. Comparison of the two groups showed more severe disease in Group 2 mice that developed significant weight and hair loss associated with inactivity and left hind footpad lesions that extended close to the testicular area. The histopathology and large number of viable microorganisms isolated from the spleen confirmed the higher invasive ability of this strain. Moreover, a decrease of an in vitro specific lymphoproliferative response and IFN-gamma production were observed over time in Group 2 mice. As a result, at the end of the experiment, the S. schenckii-antigen (Ss-Ag) response was considered negative with a stimulation index (SI) = 2. In contrast, Group 1 mice presented a positive response to Ss-Ag (SI = 14.1). These results confirm the existence of different virulence profiles in S. schenckii strains. In addition, the use of subcutaneous inoculation as a suitable route for verification of the pathogenicity of this fungus in the murine model was confirmed.


PLOS ONE | 2015

Parasite Load Induces Progressive Spleen Architecture Breakage and Impairs Cytokine mRNA Expression in Leishmania infantum- Naturally Infected Dogs

Amanda dos Santos Cavalcanti; Marcelo Ribeiro-Alves; Luiza de Oliveira Ramos Pereira; Gustavo Leandro Mestre; Anna Beatriz Robottom Ferreira; Fernanda Nazaré Morgado; Mariana Côrtes Boité; Elisa Cupolillo; Milton Ozório Moraes; Renato Porrozzi

Canine Visceral Leishmaniasis (CVL) shares many aspects with the human disease and dogs are considered the main urban reservoir of L. infantum in zoonotic VL. Infected dogs develop progressive disease with a large clinical spectrum. A complex balance between the parasite and the genetic/immunological background of the host are decisive for infection evolution and clinical outcome. This study comprised 92 Leishmania infected mongrel dogs of various ages from Mato Grosso, Brazil. Spleen samples were collected for determining parasite load, humoral response, cytokine mRNA expression and histopathology alterations. By real-time PCR for the ssrRNA Leishmania gene, two groups were defined; a low (lowP, n = 46) and a high parasite load groups (highP, n = 42). When comparing these groups, results show variable individual humoral immune response with higher specific IgG production in infected animals but with a notable difference in CVL rapid test optical densities (DPP) between highP and lowP groups. Splenic architecture disruption was characterized by disorganization of white pulp, more evident in animals with high parasitism. All cytokine transcripts in spleen were less expressed in highP than lowP groups with a large heterogeneous variation in response. Individual correlation analysis between cytokine expression and parasite load revealed a negative correlation for both pro-inflammatory cytokines: IFNγ, IL-12, IL-6; and anti-inflammatory cytokines: IL-10 and TGFβ. TNF showed the best negative correlation (r2 = 0.231; p<0.001). Herein we describe impairment on mRNA cytokine expression in leishmania infected dogs with high parasite load associated with a structural modification in the splenic lymphoid micro-architecture. We also discuss the possible mechanism responsible for the uncontrolled parasite growth and clinical outcome.


PLOS ONE | 2015

Are Neutrophil Extracellular Traps Playing a Role in the Parasite Control in Active American Tegumentary Leishmaniasis Lesions

Fernanda Nazaré Morgado; Michelle T. C. Nascimento; Elvira M. Saraiva; Carla de Oliveira-Ribeiro; Maria de Fátima Madeira; Marcela da Costa-Santos; Érica de Camargo Ferreira e Vasconcellos; Maria Inês Fernandes Pimentel; Marcelo Rosandiski Lyra; Armando de Oliveira Schubach; Fátima Conceição-Silva

Neutrophil extracellular traps (NETs) have been described as a network of extracellular fibers composed by DNA, histones and various proteins/enzymes. Studies have demonstrated that NETs could be responsible for the trapping and elimination of a variety of infectious agents. In order to verify the presence of NETs in American tegumentary leishmaniasis (ATL) and their relationship with the presence of amastigotes we evaluated active cutaneous lesions of 35 patients before treatment by the detection of parasites, neutrophils (neutrophil elastase) and histones through immunohistochemistry and confocal immunofluorescence. Intact neutrophils could be detected in all ATL lesions. NETs were present in 27 patients (median 1.1; range from 0.1 to 23.5/mm2) with lesion duration ranging from one to seven months. NETs were in close proximity with neutrophils (r = 0.586; p = 0.0001) and amastigotes (r = 0.710; p = 0.0001). Two patterns of NET formation were detected: small homogeneously distributed networks observed in all lesions; and large structures that could be visualized at a lower magnification in lesions presenting at least 20% of neutrophils. Lesions presenting the larger NET formation showed high parasite detection. A correlation between NET size and the number of intact amastigotes was observed (p=0.02). As we detected an association between NET and amastigotes, our results suggest that neutrophil migration and NET formation could be stimulated and maintained by stimuli derived from the parasite burden/parasite antigen in the extracellular environment. The observation of areas containing only antigens not intermingled with NETs (elastase and histone) suggests that the involvement of these structures in the control of parasite burden is a dynamic process in which the formation of NETs is exhausted with the destruction of the parasites. Since NETs were also associated with granulomas, this trapping would favor the activity of macrophages in order to control the parasite burden.


PLOS ONE | 2014

T-Cell Populations and Cytokine Expression Are Impaired in Thymus and Spleen of Protein Malnourished BALB/c Mice Infected with Leishmania infantum

Sergio Cuervo-Escobar; Monica Losada-Barragán; Adriana Umaña-Pérez; Renato Porrozzi; Leonardo Saboia-Vahia; Luisa Helena Monteiro de Miranda; Fernanda Nazaré Morgado; Rodrigo Caldas Menezes; Myriam Sánchez-Gómez; Patricia Cuervo

Visceral leishmaniasis (VL) is a parasitic infectious disease that causes significant morbidity and mortality in the tropical and subtropical regions of the world. Although infections with visceralizing Leishmania may be asymptomatic, factors such as undernutrition increase the likelihood of progressing to clinical disease. Protein malnutrition, the most deleterious cause of malnutrition in developing countries, has been considered as a primary risk factor for the development of clinical VL. However, data regarding the immunological basis of this association are scarce. With the aim to analyze the effects of protein malnutrition on Leishmania infantum infection, we used BALB/c mice subjected to control or low protein isocaloric diets. Each animal group was divided into two subgroups and one was infected with L. infantum resulting in four study groups: animals fed 14% protein diet (CP), animals fed 4% protein diet (LP), animals fed 14% protein diet and infected (CPi), and animals fed 4% protein diet and infected (LPi).The susceptibility to L. infantum infection and immune responses were assessed in terms of body and lymphoid organ weight, parasite load, lymphocyte subpopulations, and cytokine expression. LPi mice had a significant reduction of body and lymphoid organ weight and exhibited a severe decrease of lymphoid follicles in the spleen. Moreover, LPi animals showed a significant decrease in CD4+CD8+ T cells in the thymus, whereas there was an increase of CD4+ and CD8+ T cells percentages in the spleen. Notably, the cytokine mRNA levels in the thymus and spleen of protein malnourished-infected animals were altered compared to the CP mice. Protein malnutrition results in a drastic dysregulation of T cells and cytokine expression in the thymus and spleen of L. infantum-infected BALB/c mice, which may lead to defective regulation of the thymocyte population and an impaired splenic immune response, accelerating the events of a normal course of infection.


Parasite Immunology | 2010

Signs of an in situ inflammatory reaction in scars of human American tegumentary leishmaniasis

Fernanda Nazaré Morgado; Armando de Oliveira Schubach; Érica de Camargo Ferreira e Vasconcellos; Rilza Beatriz Gayoso de Azeredo-Coutinho; Cláudia Maria Valete-Rosalino; Leonardo Pereira Quintella; Ginelza Peres Lima dos Santos; Mariza de Matos Salgueiro; M. R. Palmeiro; Fátima Conceição-Silva

Skin inflammation plays an important role during the healing of American tegumentary leishmaniasis (ATL), the distribution of cells in active lesions may vary according to disease outcome and parasite antigens in ATL scars have already been shown. We evaluated by immunohistochemistry, 18 patients with 1‐ or 3‐year‐old scars and the corresponding active lesions and compared them with healthy skin. Small cell clusters in scars organized as in the active lesions spreaded over the fibrotic tissue were detected, as well as close to vessels and cutaneous glands, despite a reduction in the inflammatory process. Analysis of 1‐year‐old scar tissue showed reduction of NOS2, E‐selectin, Ki67, Bcl‐2 and Fas expression. However, similar percentages of lymphocytes and macrophages were detected when compared to active lesions. Only 3‐year‐old scars showed reduction of CD3+, CD4+ and CD8+T cells, in addition to reduced expression of NOS2, E‐selectin, Ki67 and BCl‐2. These results suggest that the pattern of cellularity of the inflammatory reaction observed in active lesions changes slowly even after clinical healing. Analysis of 3‐year‐old scars showed reduction of the inflammatory reaction as demonstrated by decrease in inflammatory cells and in the expression of cell‐activity markers, suggesting that the host–parasite balance was only established after that period.


Parasite Immunology | 2012

Comparative study of the in situ immune response in oral and nasal mucosal leishmaniasis

M. R. Palmeiro; Fernanda Nazaré Morgado; Cláudia Maria Valete-Rosalino; Ana Cristina da Costa Martins; João Soares Moreira; Leonardo Pereira Quintella; A. De Oliveira Schubach; Fátima Conceição-Silva

Mucosal Leishmaniasis (ML) may occur in both nasal and oral mucosa. However, despite the impressive tissue destruction, little is known about the oral involvement. To compare some changes underlying inflammation in oral and nasal ML, we performed immunohistochemistry on mucosal tissue of 20 patients with ML (nasal [n = 12]; oral [n = 8] lesions) and 20 healthy donors using antibodies that recognize inflammatory markers (CD3, CD4, CD8, CD22, CD68, neutrophil elastase, CD1a, CLA, Ki67, Bcl‐2, NOS2, CD62E, Fas and FasL). A significantly larger number of cells, mainly T cells and macrophages, were observed in lesions than in healthy tissue. In addition, high nitric oxide synthase 2 (NOS2) expression was associated with a reduced detection of parasites, highlighting the importance of NOS2 for parasite elimination. Oral lesions had higher numbers of neutrophils, parasites, proliferating cells and NOS2 than nasal lesions. These findings, together with the shorter duration of oral lesions and more intense symptoms, suggest a more recent inflammatory process. It could be explained by lesion‐induced oral cavity changes that lead to eating difficulties and social stigma. In addition, the frequent poor tooth conservation and gingival inflammation tend to amplify tissue destruction and symptoms and may impair and confuse the correct diagnosis, thus delaying the onset of specific treatment.


Medical Mycology | 2011

The in situ inflammatory profile of lymphocutaneous and fixed forms of human sporotrichosis

Fernanda Nazaré Morgado; Armando de Oliveira Schubach; Mônica Bastos de Lima Barros; Fátima Conceição-Silva

The most common clinical presentations of sporotrichosis are the lymphocutaneous (LC) and fixed cutaneous (F) forms, but little is known about the immunopathologic differences between them. The aim of this study was to evaluate through immunohistochemistry the composition of the in situ inflammatory reaction so as to correlate the results with the clinical presentation of the disease. The following two groups of patients were involved in the studies, i.e., LC (n=19) and F (n=11) patients. Those with the LC form, in contrast to F patients, were found to have a larger number of lesions (P=0.001), of longer duration (P=0.026) and require a more extended course of treatment (P=0.049). LC patients also presented a greater fungal burden (LC:0-6.5; F:0-1.5; P=0.021), a higher percentage of neutrophils (median LC:24.7%; F:6.7%, P=0.002), CD4(+) cells (median LC:40.9%; F:30.0%, P=0.0024), CD22(+) cells (median LC:15.3%; F:2.9%, P=0.048), and higher intensity of NOS2 expression (P=0.009). Thus, our data identified differences in cell profile and inflammatory activity in lesions of LC and F forms of human sporotrichosis.


PLOS Neglected Tropical Diseases | 2013

Two women presenting worsening cutaneous ulcers during pregnancy: diagnosis, immune response, and follow-up.

Fátima Conceição-Silva; Fernanda Nazaré Morgado; Maria Inês Fernandes Pimentel; Érica de Camargo Ferreira e Vasconcellos; Armando de Oliveira Schubach; Cláudia Maria Valete-Rosalino; Pascale Kropf; Ingrid Müller

1 Laboratório de Imunoparasitologia, Instituto Oswaldo Cruz, Fiocruz, Brasil, 2 Laboratório de Vigilância em Leishmanioses, Instituto de Pesquisa Clinica Evandro Chagas, Fiocruz, Brasil, 3 Departamento de Otorrino e Oftalmologia, Faculdade de Medicina, Universidade Federal do Rio de Janeiro, Rio de Janeiro, Brasil, 4 Imperial College London, Faculty of Medicine, Section of Immunology, London, United Kingdom, 5 Imperial College London, Faculty of Medicine, Section of Immunology, London, United Kingdom


Medical Mycology | 2015

Severe feline sporotrichosis associated with an increased population of CD8low cells and a decrease in CD4⁺ cells.

Luisa Helena Monteiro de Miranda; Marta de Almeida Santiago; Tânia Maria Pacheco Schubach; Fernanda Nazaré Morgado; Sandro Antonio Pereira; Raquel V. C. Oliveira; Fátima Conceição-Silva

Sporotrichosis is a subcutaneous mycosis with worldwide distribution, especially in tropical and subtropical areas. Zoonotic transmission is described with cats being the main animal species involved. The occurrence of severe feline sporotrichosis with high fungal levels demonstrates the susceptibility of cats to this disease and the importance of studying its pathogenesis. This study describes the leukocytes profile in blood of cats with sporotrichosis by flow cytometry and its correlation with histopathology and fungal load. The cats with sporotrichosis were separated into groups L1, L2, and L3 (lesions at one, two, and three or more noncontiguous skin locations, respectively) and were classified as good, fair, or poor general conditions. The highest percentage of CD4+ cells was associated to L1 (P = .04) and to good general condition (P = .03). The percentage of CD8+ cells was greater in L2 and L3 (P = .01). CD8(low) expression occurred in 20 animals with sporotrichosis, mainly in L3 (P = .01) and was not observed in healthy controls. This expression was related to macrophage granulomas (P = .01) and predominated in cases with high fungal load. Altogether, the results indicated that control over feline sporotrichosis, with maintenance of a good general condition, fixed lesions, well-organized response and lower fungal load, is associated with increased CD4+ cells percentages. In contrast, a poor general condition, disseminated lesions and high fungal load were related to increased CD8+ cell percentages and increased expression of CD8(low). As conclusion these results point to an important role of the CD4:CD8 balance in determining the clinical outcome in feline sporotrichosis.


Mycoses | 2011

Characteristics of Paecilomyces lilacinus infection comparing immunocompetent with immunosuppressed murine model

Marcelly Maria dos Santos Brito; Mariana da Silva Lima; Fernanda Nazaré Morgado; Priscila S. Raibolt; Rodrigo Caldas Menezes; Fátima Conceição-Silva; Cintia de Moraes Borba

The characteristics of Paecilomyces lilacinus infection were evaluated using two murine experimental models: immunocompetent and immunosuppressed. The evaluation criteria for characteristics of infection were clinical signs, weight loss, survival rates, histopathological alterations and the number of viable fungal cells re‐isolated from different organs; and those for immunological status were in vitro lymphoproliferative response, cell surface phenotyping and IFN‐γ production. Morphological evaluation showed that P. lilacinus isolates presented morphological characteristics consistent with those described in the literature. The immunocompetent mice could be infected by the fungi, but they did not develop the disease, unlike the immunosuppressed mice, which showed clinical signs of mycosis in an environment of suppressed cellular immune response. The hypothesis of latent infection reactivation in mice was not confirmed. The difference observed in the infection rate of the two fungi isolates points to an intrinsic variation between strains of P. lilacinus and led us to hypothesise that even in the presence of immunosuppressed environment, the fungus virulence can play a role in the pathogenesis of hyalohyphomycosis.

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Cláudia Maria Valete-Rosalino

Federal University of Rio de Janeiro

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