Clivia Maria Moraes de Oliveira
Federal University of Pará
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Featured researches published by Clivia Maria Moraes de Oliveira.
Medical Mycology | 2014
Carla Pagliari; Luciane Kanashiro-Galo; Aline Alves de Lima Silva; Tânia Cristina Barboza; Paulo Ricardo Criado; Maria Irma Seixas Duarte; Arival Cardoso de Brito; Marília Brasil Xavier; Deborah Aben-Athar Unger; Clivia Maria Moraes de Oliveira; Juarez Antonio Simões Quaresma; Mirian Nacagami Sotto
Plasmacytoid dendritic cells (pDCs) are characterized by expression of CD123 and BDCA-2 (Blood Dendritic Cell Antigen 2) (CD303) molecules, which are important in innate and adaptive immunity. Chromoblastomycosis (CBM), lacaziosis or Jorge Lobos disease (JLD), and paracoccidioidomycosis (PCM), are noteworthy in Latin America due to the large number of reported cases. The severity of lesions is mainly determined by the hosts immune status and in situ responses. The dendritic cells studied in these fungal diseases are of myeloid origin, such as Langerhans cells and dermal dendrocytes; to our knowledge, there are no data for pDCs. Forty-three biopsies from patients with CBM, 42 from those with JLD and 46 diagnosed with PCM, were evaluated by immunohistochemistry. Plasmacytoid cells immunostained with anti-CD123 and anti-CD303 were detected in 16 cases of CBM; in those stained with anti-CD123, 24 specimens were obtained from PCM. We did not detect the presence of pDCs in any specimen using either antibody in JLD. We believe that, albeit a secondary immune response in PCM and CBM, pDCs could act as a secondary source of important cytokines. The BDCA-2 (CD303) is a c-type lectin receptor involved in cell adhesion, capture, and processing of antigens. Through the expression of the c-lectin receptor, there could be an interaction with fungi, similar to other receptors of this type, namely, CD207 in PCM and CD205 and CD209 in other fungal infections. In JLD, the absence of expression of CD123 and CD303 seems to indicate that pDCs are not involved in the immune response.
Medical Mycology | 2015
Luciane Kanashiro-Galo; Carla Pagliari; Tania Cristina Barboza; Arival Cardoso de Brito; Marília Brasil Xavier; Clivia Maria Moraes de Oliveira; Deborah Aben-Athar Unger; Mirian Nacagami Sotto; Juarez Antonio Simões Quaresma; Maria Irma Seixas Duarte
Jorge Lobos disease (JLD) is a chronic granulomatous mycosis described in various Latin American countries. The main objective of the present study was to investigate the possible role of Th17 and Foxp3+ Treg cells in the pathogenesis of Jorge Lobos disease. Human skin biopsies were submitted to an immunohistochemistry protocol to detect Foxp3, interleukin (IL)-1beta, CD25, IL-6, IL-17, and IL-23. The epidermis presented acanthosis, hyperkeratosis, and frequent presence of fungi. The dermis presented inflammatory infiltrate comprising macrophages, lymphocytes, epithelioid and multinucleated cells, and an intense number of fungi. Foxp3+ Treg cells and IL-17+ cells were visualized in lymphocytes in the inflammatory infiltrate. IL-1, IL-2R (CD25), IL-6, and IL-23 were visualized in the dermis, intermingled with fungal cells, permeating or participating of the granuloma. Following IL-17, the most prominent cytokine was IL-6. IL-23 and cells expressing CD25 were present in fewer number. The comparative analysis between IL-17 and Foxp3 demonstrated a statistically significant increased number of IL-17+ cells. Th17 cells play a role in the immune response of JLD. IL-1beta and IL-6 added to the previously described increased number of TGF-beta would stimulate such pattern of response. Th17 cells could be present as an effort to modulate the local immune response; however, high levels of a Th17 profile could overcome the role of Treg cells. The unbalance between Treg/Th17 cells seems to corroborate with the less effective immune response against the fungus.
Journal of Physics: Conference Series | 2006
T. A. Girard; F. Giuliani; T. Morlat; J. I. Collar; D. Limagne; G. Waysand; J Puibasset; Harry S. Miley; M. Auguste; Doug M. Boyer; A. Cavaillou; J.G. Marques; Clivia Maria Moraes de Oliveira; Ana C. Fernandes; A.R. Ramos; M. Felizardo; R.C. Martins
An improved SIMPLE experiment comprising four superheated droplet detectors with a total exposure of 0.42 kg.d yields ~factor 10 improvement in the previously-reported results. Despite the low exposure, the result provides restrictions on the allowed phase space of spin-dependent coupling strengths almost equivalent to those from the significantly larger exposure NAIAD-CDMS/ZEPLIN searches.
Contributed to IDM 2004: 5th International Workshop on the I | 2005
T. A. Girard; F. Giuliani; J. I. Collar; T. Morlat; D. Limagne; G. Waysand; M. Auguste; Doug M. Boyer; A. Cavaillou; Harry S. Miley; M. Da Costa; R.C. Martins; J.G. Marques; A.R. Ramos; Ana C. Fernandes; J. Puibasset; Clivia Maria Moraes de Oliveira
We present the results of the recent Phase II SIMPLE search effort, comprising two stages each of ~14 kgd exposure of 15 Superheated Droplet Detectors with ~0.2 kg active mass and recoil energy threshold of 8 keV. In the second stage, the neutron shielding was increased to reduce the on-detector rate by a factor 3.5. Combined with an improved nucleation efficiency and analysis of the detector pressure evolution during the measurements, the results yield improved results in the phase space of both spin -dependent and -independent WIMP interactions.
Medical Mycology | 2017
Ariane Fernandes Alexandre; Juarez Antonio Simões Quaresma; Tânia Cristina Barboza; Arival Cardoso de Brito; Marília Brasil Xavier; Clivia Maria Moraes de Oliveira; Deborah Aben-Athar Unger; Luciane Kanashiro-Galo; Mirian Nacagami Sotto; Maria Irma Seixas Duarte; Carla Pagliari
Abstract Jorge Lobos Disease (JLD) is a cutaneous chronic granulomatous disease caused by the pathogenic fungus Lacazia loboi. It is characterized by a granulomatous reaction with multinucleated giant cells and high number of fungal cells. In order to contribute to the comprehension of immune mechanisms in JLD human lesions, we studied the cytotoxic immune response, focusing on TCD8+ and NK cells, and granzyme B. Forty skin biopsies of lower limbs were selected and an immunohistochemistry protocol was developed to detect CD8+ T cells, NK cells and Granzyme B. In order to compare the cellular populations, we also performed a protocol to visualize TCD4+ cells. Immunolabeled cells were quantified in nine randomized fields in the dermis. Lesions were characterized by inflammatory infiltrate of macrophages, lymphocytes, epithelioid and multinucleated giant cells with intense number of fungal forms. There was a prevalence of CD8 over CD4 cells, followed by NK cells. Our results suggest that in JLD the cytotoxic immune response could represent another important mechanism to control Lacazia loboi infection. We may suggest that, although CD4+ T cells are essential for host defense in JLD, CD8+ T cells could play a role in the elimination of the fungus.
Human Pathology | 2008
Marília Brasil Xavier; Rosana Maria Feio Libonati; Débora Unger; Clivia Maria Moraes de Oliveira; Carlos Eduardo Pereira Corbett; Arival Cardoso de Brito; Juarez Antonio Simões Quaresma
Anais Brasileiros De Dermatologia | 1996
Domingos Silva; Célia Macêdo; Clivia Maria Moraes de Oliveira; Deborah Aben-Athar Unger
Mycopathologia | 2015
Tania Cristina Barboza; Juarez Antonio Simões Quaresma; Arival Cardoso de Brito; Marília Brasil Xavier; Clivia Maria Moraes de Oliveira; Deborah Aben-Athar Unger; Maria Irma Seixas Duarte; Mirian Nacagami Sotto; Carla Pagliari
American Journal of Agricultural and Biological Sciences | 2008
Maurimélia Mesquita da Costa; Silvia Helena Marques da Silva; Hugo J. R. Almeida; Clivia Maria Moraes de Oliveira; Marília Brasil Xavier; Arival Cardoso de Brito; Juarez Antonio Simões Quaresma
Rev. para. med | 2000
Tarcísio Carvalho; Adriana C. L Simões; Arival Cardoso de Brito; Clivia Maria Moraes de Oliveira