Sara Mina
University of Angers
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Featured researches published by Sara Mina.
Clinical and Vaccine Immunology | 2015
Sara Mina; Agnes Marot-Leblond; Bernard Cimon; Maxime Fleury; Gérald Larcher; Jean-Philippe Bouchara; Raymond Robert
ABSTRACT Scedosporium boydii is an opportunistic filamentous fungus which may be responsible for a wide variety of infections in immunocompetent and immunocompromised individuals. This fungus belongs to the Scedosporium apiospermum species complex, which usually ranks second among the filamentous fungi colonizing the airways of patients with cystic fibrosis (CF) and may lead to allergic bronchopulmonary mycoses, sensitization, or respiratory infections. Upon microbial infection, host phagocytic cells release reactive oxygen species (ROS), such as hydrogen peroxide, as part of the antimicrobial response. Catalases are known to protect pathogens against ROS by detoxification of the hydrogen peroxide. Here, we investigated the catalase equipment of Scedosporium boydii, one of the major pathogenic species in the S. apiospermum species complex. Three catalases were identified, and the mycelial catalase A1 was purified to homogeneity by a three-step chromatographic process. This enzyme is a monofunctional tetrameric protein of 460 kDa, consisting of four 82-kDa glycosylated subunits. The potential usefulness of this enzyme in serodiagnosis of S. apiospermum infections was then investigated by an enzyme-linked immunosorbent assay (ELISA), using 64 serum samples from CF patients. Whatever the species involved in the S. apiospermum complex, sera from infected patients were clearly differentiated from sera from patients with an Aspergillus fumigatus infection or those from CF patients without clinical and biological signs of a fungal infection and without any fungus recovered from sputum samples. These results suggest that catalase A1 is a good candidate for the development of an immunoassay for serodiagnosis of infections caused by the S. apiospermum complex in patients with CF.
Fungal Biology | 2015
Sara Mina; C. Staerck; Sènan M. d'Almeida; Agnès Marot; Yves Delneste; Alphonse Calenda; Julie Tabiasco; Jean-Philippe Bouchara; Maxime Fleury
Scedosporium boydii is an opportunistic filamentous fungus which may be responsible for a large variety of infections in both immunocompetent and immunocompromised individuals. This fungus belongs to the Scedosporium apiospermum species complex which usually ranks second among the filamentous fungi colonizing the airways of patients with cystic fibrosis (CF). Species of the S. apiospermum complex are able to chronically colonize the CF airways suggesting pathogenic mechanisms allowing persistence and growth of these fungi in the respiratory tract. Few putative virulence factors have been purified and characterized so far in the S. apiospermum complex including a cytosolic Cu,Zn-superoxide dismutase (SOD) and a monofunctional catalase (catalase A1). Upon microbial infection, host phagocytes release reactive oxygen species (ROS), such as hydrogen peroxide, as part of the antimicrobial response. Catalases are known to protect pathogens against ROS by degradation of the hydrogen peroxide. Here, we identified the S. boydii catalase A1 gene (CATA1) and investigated its expression in response to the environmental conditions encountered in the CF airways and to the oxidative stress. Results showed that S. boydii CATA1 gene expression is not affected by hypoxia, hypercapnia or pH changes. In contrast, CATA1 gene was overexpressed in response to a chemically induced oxidative stress with a relative gene expression 37-fold higher in the presence of 250 μM H(2)O(2), 20-fold higher with 250 μM menadione and 5-fold higher with 2 mM paraquat. Moreover, S. boydii CATA1 gene expression progressively increased upon exposure to activated THP-1-derived macrophages, reaching a maximum after 12 h (26 fold). Activated HL60-derived neutrophils and activated human peripheral blood neutrophils more rapidly induced S. boydii CATA1 gene overexpression, a maximum gene expression level being reached at 75 min (17 fold) and 60 min (15 fold), respectively. In contrast expression of the gene encoding the Cu,Zn-SOD (SODC gene) was not affected by H(2)O(2), menadione, paraquat or in co-culture with phagocytic cells. These results suggest that S. boydii CATA1 gene is highly stimulated by the oxidative burst response whereas SODC gene is constitutively expressed.
9th European CF Young Investigator Meeting | 2015
Sara Mina; C. Staerck; Agnès Marot; Charlotte Godon; Sandrine Giraud; Jean-Philippe Bouchara; Maxime Fleury
19th Congress of the International Society for Human and Animal Mycology | 2015
C. Staerck; Sara Mina; Agnès Marot; Charlotte Godon; Jean-Philippe Bouchara; Maxime Fleury
19th Congress of the International Society for Human and Animal Mycology | 2015
C. Staerck; Sara Mina; S. d'Almeida; Agnès Marot; Sandrine Giraud; Yves Delneste; Jean-Philippe Bouchara; Julie Tabiasco; Maxime Fleury
16ème colloque français des jeunes chercheurs en mucoviscidose | 2015
Sara Mina; C. Staerck; Charlotte Godon; Agnès Marot; Jean-Philippe Bouchara; Maxime Fleury
11ème Congrès National de la Société Française de Microbiologie | 2015
Sara Mina; C. Staerck; Charlotte Godon; Agnès Marot; Jean-Philippe Bouchara; Maxime Fleury
11ème Congrès National de la Société Française de Microbiologie | 2015
C. Staerck; Sara Mina; S. d'Almeida; Agnès Marot; Jean-Philippe Bouchara; Julie Tabiasco; Maxime Fleury
15ème colloque Français des jeunes chercheurs en mucoviscidose | 2014
Sara Mina; C. Staerck; Agnès Marot; Charlotte Godon; Raymond Robert; Jean-Philippe Bouchara; Maxime Fleury
4th International Workshop on Scedosporium Infections | 2013
Sara Mina; Agnès Marot; Maxime Fleury; Bernard Cimon; Jean-Philippe Bouchara; Raymond Robert