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Oxidative Stress, Septic Shock, and Survival Matthew Greenwood April 29, 2015
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Hypothesis: double blockade of complement C5 and the TLR coreceptor CD14 will improve survival during polymicrobial sepsis
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Methods Use cecal ligation model to induce polymycrobial sepsis Treat C57BL/6 mice with anti-inflammatory agents – Coversin – Anti-mouse CD14 Monitor – Levels of cytokines and other biomarkers – Mouse survival
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What is Coversin? Inhibitor of complement C5 – Prevents immune chemotaxis – Prevents formation of membrane attack system Originally from Ornithodoros moubata http://www.vipimmunopharma.com/coversin/ http://lymeaware.free.fr/lyme/Websave/maladie satiques/www.maladies-a- tiques.com/Ornithodoros%20moubata.jpg
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Figure 1 Cytokine levels after 24 hours
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Figure 2 Inflammatory marker levels after 24 hours.
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Figure 3 Inflammatory marker levels after 24 hours.
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Figure 4 Subject survival
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Conclusions Combined C5 and CD14 inhibition significantly improves systemic inflammation, clinical signs, and survival rate Reducing the magnitude and duration of both the pro- and anti-inflammatory conditions improves outcome
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Future directions Correlate cytokine levels with mortality and morbidity Treat with antibiotics with the immunosupressants Testing in humans to improve patient outcomes
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Hypothesis: protecting mitochondria with mitochondrial targeted antioxidants will alleviate myocardial inflammation and rescue heart function in sepsis
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Background
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Methods Used intratracheal injection of Streptococcus pneumonia to induce sepsis Sprague-Dawley male rats served as the model organism Administered Mito-Vit-E in a 21.5 uMol/kg dose
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Figure 1 Distribution of Mito-Vit-E
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Figure 2
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Figure 3 Oxidation of molecules
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Figure 4 Mitochondrial membrane integrity
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Figure 5
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Figure 6
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Figures 7 & 8
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Conclusions Mitochondrial targeted Vitamin E – Improved antioxidant capacity – Reduced Oxidation of mitochondrial molecules – Protected mitochondrial structure – Reduced Cytokine production – Reduced neutrophil infiltration – Protected heart function
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Future Directions Survival studies Administer with antibiotics Testing in humans to improve patient outcomes
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My Experiment Hypothesis: Administration of reactive oxygen species or pro-oxidative species will improve immune response and survival following sepsis Specific Aim: Determine the reactive oxygen species or oxidants that are able to boost immune response in healthy and immunosuppressed mice to recover from sepsis.
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Experimental Approach Treat mice with oxidants and mitochondrially targeted antioxidants Determine cytokine levels Find optimal treatment for subject survival
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