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Impact of oral simvastatin therapy on acute lung injury in mice during pneumococcal pneumonia.

BMC microbiology
January 1, 1970
Angela R Boyd et al. (4 authors)
Journal ArticleResearch Support, N.I.H., ExtramuralAnimal Study
Extracted Claims (16)
InterventionDirectionEndpointPopulationDosageImpactClaim #
high simvastatin diet (HSD)
decrease
lung consolidation
BALB/c mice
-
had reduced
#1
high simvastatin diet (HSD)
decrease
chemokines MCP-1
BALB/c mice
P = 0.03
significant reduction in
#2
high simvastatin diet (HSD)
decrease
chemokines KC
BALB/c mice
P = 0.02
significant reduction in
#3
high simvastatin diet (HSD)
decrease
ICAM-1 in the lungs
BALB/c mice
-
reduction in
#4
high simvastatin diet (HSD)
decrease
bacterial titers in the blood
BALB/c mice
P = 0.007 at 36 hours
significantly lower
#5
high simvastatin diet (HSD)
decrease
bacterial titers in the blood
BALB/c mice
P = 0.03 at 42 hours
significantly lower
#6
low simvastatin diet (LSD)
decrease
bacterial titers in the lungs
BALB/c mice
-
resulted in reduced
#7
low simvastatin diet (LSD)
decrease
bacterial titers in the blood
BALB/c mice
-
resulted in reduced
#8
low simvastatin diet (LSD)
decrease
number of infiltrated neutrophils
BALB/c mice
-
reduced
#9
low simvastatin diet (LSD)
no change
mortality
BALB/c mice
-
had no reduced
#10
high simvastatin diet (HSD)
no change
mortality
BALB/c mice
-
had no reduced
#11
prolonged oral simvastatin therapy
decrease
neutrophil infiltration
mice
-
had a strong dose-dependent effect on protection against S. pneumoniae as evidenced by reduced
#12
prolonged oral simvastatin therapy
neutral
maintenance of vascular integrity
mice
-
had a strong dose-dependent effect on protection against S. pneumoniae as evidenced by
#13
prolonged oral simvastatin therapy
decrease
chemokine production in the lungs
mice on HSD
-
had a strong dose-dependent effect on protection against S. pneumoniae as evidenced by lowered
#14
statin therapy
decrease
bacterial burden in the lungs
-
-
protected through reduced
#15
oral simvastatin at physiologically relevant doses
neutral
pneumococcal pneumonia
-
-
only modestly protects against
#16
Abstract

BACKGROUND: Recent studies suggest that the reported protective effects of statins (HMG-CoA reductase inhibitors) against community-acquired pneumonia (CAP) and sepsis in humans may be due to confounders and a healthy user-effect. To directly test whether statins are protective against Streptococcus pneumoniae, the leading cause of CAP, we examined the impact of prolonged oral simvastatin therapy at physiologically relevant doses in a mouse model of pneumococcal pneumonia. BALB/c mice were placed on rodent chow containing 0 mg/kg (control), 12 mg/kg (low simvastatin diet [LSD]; corresponds to 1.0 mg/kg/day), or 120 mg/kg (high simvastatin diet [HSD]; corresponds to 10 mg/kg/day) simvastatin for four weeks, infected intratracheally with S. pneumoniae serotype 4 strain TIGR4, and sacrificed at 24, 36, or 42 h post-infection for assessment of lung histology, cytokine production, vascular leakage and edema, bacterial burden and bloodstream dissemination. Some mice received ampicillin at 12-h intervals beginning at 48 h post-infection and were monitored for survival. Immunoblots of homogenized lung samples was used to assess ICAM-1 production. RESULTS: Mice receiving HSD had reduced lung consolidation characterized by less macrophage and neutrophil infiltration and a significant reduction in the chemokines MCP-1 (P = 0.03) and KC (P = 0.02) and ICAM-1 in the lungs compared to control mice. HSD mice also had significantly lower bacterial titers in the blood at 36 (P = 0.007) and 42 (P = 0.03) hours post-infection versus controls. LSD had a more modest effect against S. pneumoniae but also resulted in reduced bacterial titers in the lungs and blood of mice after 42 h and a reduced number of infiltrated neutrophils. Neither LSD nor HSD mice had reduced mortality in a pneumonia model where mice received ampicillin 48 h after challenge. CONCLUSIONS: Prolonged oral simvastatin therapy had a strong dose-dependent effect on protection against S. pneumoniae as evidenced by reduced neutrophil infiltration, maintenance of vascular integrity, and lowered chemokine production in the lungs of mice on HSD. Statin therapy also protected through reduced bacterial burden in the lungs. Despite these protective correlates, mortality in the simvastatin-receiving cohorts was equivalent to controls. Thus, oral simvastatin at physiologically relevant doses only modestly protects against pneumococcal pneumonia.

Medical Subject Headings (MeSH)
Acute Lung InjuryAdministration, OralAnimalsAnticholesteremic AgentsCytokinesDisease Models, AnimalEdemaFemaleHistocytochemistryLungMiceMice, Inbred BALB CPneumonia, PneumococcalSimvastatinStreptococcus pneumoniaeSurvival Analysis
Study Links
PubMed ID22587610
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