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   cbpm and cbpg of streptococcus pneumoniae elicit a high protection in mice challenged with a serotype 19f pneumococcus  
   
نویسنده kazemian hamid ,afshar davoud ,garcia ernesto ,pourmand mohammad reza ,jeddi-tehrani mahmood ,aminharati farzaneh ,shokri fazel ,yazdi mohammad hossein
منبع iranian journal of allergy, asthma and immunology - 2018 - دوره : 17 - شماره : 6 - صفحه:574 -585
چکیده    Among many pneumococcal antigens, choline-binding proteins (cpbs) display a high immunogenicity in animal models. this study aims to determine the immunogenicity of cbpm, cbpg and cbpl proteins of streptococcus pneumoniae in a mice model. the genes were cloned into pet21a expression vector and the recombinant proteins were produced. mice were immunized with the purified recombinant proteins. subsequently, the mice were challenged with s. pneumoniae atcc 49619 (2×106 cfu) and their survival and bacterial clearances were followed 24 hours after infection. the antibody responses of the mice were determined by elisa assay. the opsonophagocytosis assay was performed using rabbit’s sera. passive immunization was carried out using two doses of anti-cbps antibodies. finally, these mice were experimentally infected with virulent bacteria and the protective effects of two doses of 10 and 100 µg/ml by monitoring the survival rate and bacterial clearance were determined at 2, 3 and 7 days after bacterial challenge. the mice actively immunized with cbpm, cbpg and cbpl recombinant proteins showed survival rate of 100%, 85% and 75%, respectively. the survival rates among passively immunized mice groups which received 100 µg/ml dose of anti-cbpm, anti-cbpg and anti- cbpl were 50%, 50% and 25%, respectively. the rates of opsonization with rabbit’s antibodies against cbpm, cbpg, and cbpl at 100 µg/ml doses was 45.6%, 14.7% and 82.3%, and at 10 µg/ml was 12.9%, 12.2% and 9.35%, respectively. our findings suggest that the recombinant proteins particularly cbpm and cbpg can protect the mice against pneumococcus19f serotype and effectively induce a protective antibody response. thus, cbpg and cbpm proteins might be used as suitable vaccine candidate in pneumococcal vaccine formulations.
کلیدواژه cholinebinding proteins ,pneumococcal vaccine ,streptococcus pneumoniae
آدرس tehran university of medical sciences, school of public health, department of pathobiology, ایران, tehran university of medical sciences, school of public health, department of pathobiology, ایران, centro de investigación biomédica en red de enfermedades respiratorias, spain, tehran university of medical sciences, school of public health, urology research center, department of pathobiology, ایران, academic center for education, culture and research (acecr), monoclonal antibody research center, avicenna research institute, ایران, tehran university of medical sciences, school of public health, department of pathobiology, ایران, tehran university of medical sciences, school of public health, department of immunology, ایران, tehran university of medical sciences, faculty of pharmacy, biotechnology research center, department of pharmaceutical biotechnology, ایران
پست الکترونیکی mh-yazdi@tums.ac.ir
 
     
   
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