1.Treatment of severe burn injury of 98% TBSA with 95% full-thickness burn and severe inhalation injury: a case report.
Lei YANG ; Jia-han WANG ; Yi-ping ZHOU
Chinese Journal of Traumatology 2003;6(4):249-251
Adult
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Burns
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complications
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therapy
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Humans
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Male
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Nutritional Support
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Smoke Inhalation Injury
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complications
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therapy
2.Expression and immunogenicity analysis of EsxA protein of Staphylococcus aureus isolated from cow milk.
Yuanyang YI ; Ya'nan ZHAO ; Pengrui MA ; Bin LI ; Yan SU
Chinese Journal of Biotechnology 2018;34(5):694-702
To study the immunogenicity of EsxA protein of Staphylococcus aureus, the EsxA-pET-28a recombinant plasmid was constructed and the expression product was analyzed by SDS-PAGE and Western blotting after the positive recombinant plasmid was induced by IPTG. Mice were immunized with purified EsxA protein and then the IgG, IgG1 and IgG2a antibody were detected with indirect ELISA. Then the histopathological examination, bacteria loading and immune protection of immunized mice were studied after challenge with S. aureus. The recombinant protein EsxA was successfully induced and expressed. After immunization the EsxA specific antibody titer could reach 1:900. Bacteria loading and pathological damage of liver, spleen and kidney were reduced after immunization with EsxA in the immunized mice. The protection rate of immunized mice was 75%. In conclusion, EsxA protein has good immunogenicity.
3.Comparison of immunogenicity between recombinant flagellins C and B of Salmonella abortus equi.
Hao WANG ; Yuanyang YI ; Duishanbay GULIMIRE ; Qinggeng FAN ; Yan SU
Chinese Journal of Biotechnology 2020;36(1):57-66
To evaluate and compare of the immunogenicity differences of flagellins FliC and FljB of Salmonella abortus equi, and lay the experimental foundation for the further utilization of the two recombinant proteins, FliC and FljB recombinant proteins were induced, expressed and purified. The purified FliC and FljB were used to immunize mice separately. The antibody level, titer and subtype of mice serum were detected after immunization. Immune-related receptors and histopathological changes were observed in immunized mice after challenged. The recombinant proteins FliC and FljB were successfully induced and expressed. Proteins of about 52 kDa and 42 kDa were purified. High levels of specific IgG antibodies were induced in mice immunized with these two proteins, the antibody level of FljB-immunized group was higher than that of FliC-immunized group, and IgG1 was the dominant subtype of antibody. The challenge protection rate of the FljB-immunized group was 87.5%, higher than that of FliC immunized group. Bacterial loads and observation pathological of FljB-immunized group were better than that of FliC immunized group, the levels of TCR2, TCR4, MHC-I and TCR induced by FljB-immunized group were higher than those of FliC-immunized group. The of immune response induced by FljB group was better than that of FliC group.
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