Post Challenge Inhibition Of C3 And Cd14 Attenuates Escherichia Coli-Induced Inflammation In Human Whole Blood

INNATE IMMUNITY(2014)

引用 18|浏览9
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摘要
Combined inhibition of CD14 and complement, two main inducers of the inflammatory response, have proved particularly effective in attenuating Gram-negative bacteria-induced inflammation. Approaching possible clinical relevance, we investigated the effect of such inhibition in a post-challenge setting. Human whole blood was anti-coagulated with lepirudin. Anti-CD14, compstatin (C3 inhibitor) and the combination thereof were added 5min prior to or 5, 15 or 30min after adding Escherichia coli. Total incubation time with Escherichia coli was 120min. Cytokines, myeloperoxidase (MPO) and the terminal complement complex (TCC) were measured using multiplex technology and ELISA. Delayed combined inhibition significantly attenuated the inflammatory response. IL-1, IL-8 and TNF- were significantly inhibited in the range of 20-40%, even when adding the inhibitors with up to 30min delay. IL-6 was significantly inhibited with 15min delay, and MIP-1 and MPO with 5min delay. Complement activation (TCC) was blocked completely at each time point compstatin was added, whereas the cytokines and MPO increased steadily between the time points. The combined regimen was significantly more effective than single inhibition in the pre-challenge setting. The attenuation of Escherichia coli-induced inflammation in a post-challenge setting suggests a potential therapeutic window for this treatment in sepsis.
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关键词
CD14, complement, cytokines, c3, Escherichia coli, human, post-challenge
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