Elizabeth Maria Heins-Vaccari
University of São Paulo
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Featured researches published by Elizabeth Maria Heins-Vaccari.
Revista Do Instituto De Medicina Tropical De Sao Paulo | 1998
Clarisse Martins Machado; Marilena dos Anjos Martins; Elizabeth Maria Heins-Vaccari; Carlos da Silva Lacaz; Maria Cristina M. A. Macedo; Jussara Bianchi Castelli; Rosaura S. Medeiros; Roberto L. Silva; Frederico Luiz Dulley
A forty-year-old man underwent an allogeneic BMT from his HLA identical sister. GvHD prophylaxis was done with cyclosporine (CyA), methotrexate and prednisone (PDN). On day +90 extensive GvHD was noted and higher doses of immunosuppressive drugs alternating CyA with PDN were initiated. Patients follow-up was complicated by intermittent episodes of leukopenia and monthly episodes of sinusitis or pneumonia. One year after BMT, the patient developed hoarseness and nasal voice. No etiologic agent could be identified on a biopsy sample of the vocal chord. Upon tapering the doses of immunosuppressive drugs, the patient had worsening of chronic GvHD and was reintroduced on high doses of cyclosporine alternating with prednisone on day +550. Three months later, GvHD remained out of control and the patient was started on azathioprine. On day +700, hoarseness and nasal voice recurred. Another biopsy of the left vocal chord failed to demonstrate infection. Episodes of sinusitis became more frequent and azathioprine was withheld 3 months after it was started. One month later, the patient had bloody nasal discharge and surgical drainage of maxillary sinuses was performed. Histopathology showed hyphae and cultures grew Scedosporium apiospermum. Itraconazole 800 mg/day was initiated. The patient developed progressive respiratory failure and died 15 days later.
Revista Do Instituto De Medicina Tropical De Sao Paulo | 1995
Mônica Scarpelli Martinelli Vidal; Natalina Takahashi de Melo; Nilma Maciel Garcia; Gilda Maria Barbaro Del Negro; Cezar Mendes de Assis; Elizabeth Maria Heins-Vaccari; Roberto D. Naiff; Rinaldo Poncio Mendes; Carlos da Silva Lacaz
A sample of P. brasiliensis isolated from the spleen and the liver of an armadillo (Dasipus novencinctus) has been analysed under a mycological and immunochemical viewpoint. The armadillo was captured in an area of Tucuruí (State of Pará, Brazil), the animal being already established as an enzootic reservoir of P. brasiliensis at that region of the country. This sample maintained in the fungal collection of the Tropical Medicine Institute of São Paulo (Brazil) numbered 135, has got all the characteristics of P. brasiliensis, with a strong antigenic power and low virulence for guinea-pigs and Wistar rats. The specific exoantigen of P. brasiliensis--the glycoprotein with a molecular weight of 43 kDa--was easily demonstrated with double immunodiffusion, immunoelectrophoresis, SDS-PAGE and immunobloting techniques.
Revista Do Instituto De Medicina Tropical De Sao Paulo | 2010
Liliane Alves Scheid; Débora Alves Nunes Mario; Elizabeth Maria Heins-Vaccari; Janio Morais Santurio; Sydney Hartz Alves
The aim of this study was to report the ability of killer toxins, previously used as biotyping techniques, as a new tool to differentiate C. albicans from C. dubliniensis. The susceptibility of C. albicans and C. dubliniensis to killer toxins ranged from 33.9 to 93.3% and from 6.67 to 93.3%, respectively.
Revista Do Instituto De Medicina Tropical De Sao Paulo | 1997
Carlos da Silva Lacaz; Mônica Scarpelli Martinelli Vidal; Cristiane N. Pereira; Elizabeth Maria Heins-Vaccari; Natalina Takahashi de Melo; Neusa Y. Sakai-Valente; Giovana Leticia Hernandes Arriagada
The present study concern on mycologic and immunochemical data obtained from two samples of a fungus considered as belonging to the species Paracoccidioides cerebriformis described by Moore in 1935, and maintained since then on Sabourauds agar in the mycology collection of the Instituto de Medicina Tropical de São Paulo. After 60 years, the samples exhibited the same characteristics described by MOORE (1935). However, experimental lesions did not resulted in guinea-pigs inoculated intratesticularly. The dominant antigen in Paracoccidioides brasiliensis, 43 kDa glicoprotein (gp43), could not be demonstrated by SDS PAGE and Western blotting. Immunoelectrophoresis did not demonstrated the E arch of cathodic migration using a policlonal anti gp43 serum. According to these findings, it is concluded that the fungus described by MOORE (1935) as P. cerebriformis does not belong to the genus Paracoccidioides. Paracoccidioidomycosis should therefore be considered as resulting from infection by a single species, Paracoccidioides brasiliensis (Splendore, 1912) as asserted by ALMEIDA (1930). Further studies, through molecular biology methods, could identify the mentioned fungus.
Revista Do Instituto De Medicina Tropical De Sao Paulo | 2002
Carlos da Silva Lacaz; Edward Porto; José Eduardo Costa Martins; Elizabeth Maria Heins-Vaccari; N. Takahashi De Melo
Revista Do Instituto De Medicina Tropical De Sao Paulo | 2003
José Paulo S. Nóbrega; Sergio Rosemberg; Ana Maria Adami; Elizabeth Maria Heins-Vaccari; Carlos da Silva Lacaz; Thales de Brito
Anais Brasileiros De Dermatologia | 1988
Clarisse Zaitz; C. da S. Lacaz; Alberto Salebian; L. Rangel Ruiz; Elizabeth Maria Heins-Vaccari; N. Takahashi De Melo
Anais Brasileiros De Dermatologia | 1988
Elizabeth Maria Heins-Vaccari; N. Takahashi De Melo; C. da S. Lacaz; A. Dias Pereira; G. Del Negro
Anais Brasileiros De Dermatologia | 1990
Elizabeth Maria Heins-Vaccari; C. da S. Lacaz; E. G. Rodrigues
Anais Brasileiros De Dermatologia | 1984
C. da S. Lacaz; J. Gualberto Da Silva; L. M. Buazar Sabba; N. Takahashi De Melo; Elizabeth Maria Heins-Vaccari; L. Angelo Calvis; I. De Oliveira Santos