More recently, Hu et al. [26] also showed that a pretreatment
regimen of c-di-GMP administered alone subcutaneously three times at 2-week intervals followed by intravenous (i.v.) http://www.selleckchem.com/products/CAL-101.html methicillin-resistant S. aureus (MRSA) challenge 7 days after the last administration decreased bacterial burdens in both the liver and the spleen and also improved the 12-day survival rate after challenge [26]. To a lesser degree, i.p. injection of c-di-GMP 24 h before i.v. infection with MRSA results in some decrease in bacterial burdens in the liver but not in the spleen. Similarly, subcutaneous treatment of mice with c-di-GMP 48 and 24 h before intratracheal challenge with Klebsiella pneumoniae resulted in significantly improved survival rates over saline treatment [27]. The immunomodulatory effects of c-di-GMP are not limited to systemic administration. There also appears to be substantial immunomodulatory effects when Tanespimycin order c-di-GMP is delivered intranasally. Two separate studies in mouse models of bacterial pneumonia indicate that i.n. treatment with c-di-GMP has protective efficacy against respiratory pathogens despite
no direct bactericidal activity in vitro. c-di-GMP pretreatment is able to significantly reduce local bacterial burdens and decrease dissemination from the lungs [21] and [27]. In an S. pneumoniae mouse model of lung infection, i.n. pretreatment of mice with c-di-GMP 48 and 24 h before infection led to significant decreases in bacterial burdens 24 h
post-infection in mice challenged with Type 2 (both lung and blood bacterial burdens) or Type 4 (lung bacterial burdens) S. pneumoniae [21]. In mice challenged with bioluminescent Type 3 S. pneumoniae, i.n. c-di-GMP pretreatment showed no effect on bacterial burdens at early time points Adenosine but did result in lower lung bacterial burdens at 42 and 48 h post challenge. Similarly, when c-di-GMP was administered intranasally to mice before, at the time of, and after intratracheal challenge with K. pneumoniae, results showed that co-administration of c-di-GMP with K. pneumoniae plus treatment 6-h post-infection did not significantly affect survival rates while i.n. pretreatment 48 and 24 h before infection significantly improved survival rates. In the latter case, the bacterial burdens were lowered by 5-fold in the lung and ∼3 log in the blood on day 2 post-infection as compared to untreated mice [27]. Although the above studies convincingly demonstrate the immunomodulatory effect of c-di-GMP in the prevention of systemic and mucosal infection with various bacterial pathogens, the mechanism responsible for the immunomodulatory properties of c-di-GMP remains unknown. In an effort to begin dissecting this, Karaolis et al. [27] characterized the host immune response after c-di-GMP administration and K. pneumoniae challenge. Mice pretreated with c-di-GMP had significantly more neutrophils and αβT cells in the lung than controls (mice pretreated with cGMP) at day 2 post-infection.