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1.
Rev Bras Hematol Hemoter ; 33(1): 55-64, 2011.
Artigo em Inglês | MEDLINE | ID: mdl-23284245

RESUMO

Malaria is an acute infectious disease caused by the protozoa of the genus Plasmodium. The antigens of the Duffy Blood Group System, in addition to incompatibilities in transfusions and hemolytic disease of the newborn, are of great interest in medicine due to their association with the invasion of red blood cells by the parasite Plasmodium vivax. For invasions to occur an interaction between the parasites and antigens of the Duffy Blood Group System is necessary. In Caucasians six antigens are produced by the Duffy locus (Fya, Fyb, F3, F4, F5 and F6). It has been observed that Fy(a-b-) individuals are resistant to Plasmodium knowlesi and P. vivax infection, because the invasion requires at least one of these antigens. The P. vivax Duffy Binding Protein (PvDBP) is functionally important in the invasion process of these parasites in Duffy / DARC positive humans. The proteins or fractions may be considered, therefore, an important and potential inoculum to be used in immunization against malaria.

2.
Rev. bras. hematol. hemoter ; 33(1): 55-64, Feb. 2011. graf, tab
Artigo em Inglês | LILACS | ID: lil-582749

RESUMO

Malaria is an acute infectious disease caused by the protozoa of the genus Plasmodium. The antigens of the Duffy Blood Group System, in addition to incompatibilities in transfusions and hemolytic disease of the newborn, are of great interest in medicine due to their association with the invasion of red blood cells by the parasite Plasmodium vivax. For invasions to occur an interaction between the parasites and antigens of the Duffy Blood Group System is necessary. In Caucasians six antigens are produced by the Duffy locus (Fya, Fyb, F3, F4, F5 and F6). It has been observed that Fy(a-b-) individuals are resistant to Plasmodium knowlesi and P. vivax infection, because the invasion requires at least one of these antigens. The P. vivax Duffy Binding Protein (PvDBP) is functionally important in the invasion process of these parasites in Duffy / DARC positive humans. The proteins or fractions may be considered, therefore, an important and potential inoculum to be used in immunization against malaria.


Assuntos
Humanos , Plasmodium vivax , Proteínas de Protozoários , Quimiocinas , Sistema do Grupo Sanguíneo Duffy , Malária , Antígenos de Protozoários
3.
Sci. med ; 20(1)jan.-mar. 2010. ilus
Artigo em Português | LILACS | ID: lil-567170

RESUMO

Objetivos: fazer uma revisão dos aspectos básicos da ultraestrutura do taquizoíto de Toxoplasma gondii, agente etiológico da toxoplasmose. Fonte de dados: os dados apresentados tomam como referência resultados recentes obtidos pelos principais grupos de pesquisadores no mundo, que se dedicam ao estudo do Toxoplasma gondii, incluindo-se dados do próprio grupo de autores. Síntese dos dados: os taquizoítos de Toxoplasma gondii são responsáveis pela fase aguda da infecção, penetrando ativamente, através do complexo apical, em células dos hospedeiros onde se multiplicam. São abordadas características ultraestruturais e moleculares particulares da película, do citoesqueleto, de organelas secretórias (róptrias, micronemas e grânulos densos) e não secretórias (apicoplasto) exclusivas do filo Apicomplexa, além das peculiaridades do núcleo, mitocôndria, acidocalcisomas, retículo endoplasmático e complexo de Golgi desses parasitos intracelulares. Conclusões: estas características confirmam que o sucesso nas etapas de adesão, invasão e multiplicação do parasito possui clara correlação com suas características morfofuncionais.


Aims: To review basic aspects on the ultrastructure of the tachyzoite of Toxoplasma gondii, the causative agent of toxoplasmosis. Source of data: The data presented are based on recent publications by the most distinguished research groups in the area dedicated to the study of Toxoplasma gondii, including studies from the present authors. Summary of findings: The tachyzoites are responsible for the acute phase of the infection by actively penetrating, through the parasites? apical complex, the host cells where they multiply. Both ultrastructural and molecular particularities of the pellicle, the cytoskeleton, secretory (rhoptries, micronemas and dense granules) and non secretory (apicoplast) organelles, specific to Apicomplexa phylum, besides peculiar features of the nucleus, mitochondrion, acidocalcisomes, endoplasmic reticulum and Golgi complex of these intracellular parasites. Conclusions: These characteristics confirm that the success in the process of adhesion, invasion and multiplication of this parasite is clearly correlated to its morphology.


Assuntos
Anticorpos Antiprotozoários , Antígenos de Protozoários , Apicomplexa , Reação de Fase Aguda , Toxoplasma/ultraestrutura , Toxoplasmose
4.
Rev. cuba. med. trop ; 48(3): 178-183, sep.-dic. 1996.
Artigo em Espanhol | LILACS | ID: lil-629268

RESUMO

Se caracterizó un anticuerpo monoclonal específico a Toxoplasma gondii. El hibridoma produjo inmunoglobulinas IgG. El análisis por Western Blot demostró que el anticuerpo monoclonal fue específico para el antígeno de masa molecular aparente de 30 kd, presente en la superficie del parásito. El anticuerpo monoclonal se purificó a partir de fluido ascítico de ratón y se acopló a Sefarosa 4B. Este inmunoabsorbente fue utilizado con el fin de purificar el antígeno parasitario específico. El anticuerpo monoclonal estudiado puede ser de utilidad para las técnicas que contribuyan con el diagnóstico de la toxoplasmosis.


A specific monoclonal antibody was characterized to Toxoplasma gondii. The hybridoma produced IgG immunoglobulins. The Western Blot analysis showed that the monoclonal antibody was specific for the antigen of an apparent mollecular mass of 30 kd, which was present on the antigen surface. The monoclonal antibody was purified starting from mouse´s ascitic fluid and it was matched with Sepharose 4B. This immunoabsorbent was used to purify the specific parasitary antigen. The monoclonal antibody studied may be useful for those tecniques contributing to the toxoplasmosis diagnosis.

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