Cystic Fibrosis Clinical Trial
Official title:
Effect of Simvastatin on CF Airway Inflammation
Individuals with cystic fibrosis (CF) have persistent infection in the airways, which the
body attempts to fight by recruiting immune cells (neutrophils) to the lung. The immune
system and neutrophils are unable to completely kill the bacteria, and the response to the
infection leads to inflammation (swelling) of the airways and lung damage. Nitric oxide (NO)
has anti-bacterial and anti-inflammatory properties in the lung. NO production is decreased
in CF patients, and may contribute to the persistent infection and inflammation. Increasing
the production of NO in the airways of CF patients may help decrease this inflammation and
infection.
Rho GTPases are molecules in the cells that line the airways that decrease the protein that
makes nitric oxide (NOS). Rho proteins also increase inflammation in these cells. Rho
proteins are increased in CF cells, and may partially explain the low NO and high
inflammation seen in CF. Blocking the Rho protein in CF cells increases NOS, which can then
produce more NO. The Rho protein can be inhibited with a drug, simvastatin (Zocor®).
Simvastatin is used by millions of people to lower their cholesterol, is very safe, has few
side-effects and is approved for use in children greater than 10 years of age. We propose
that treating CF patients with simvastatin will increase NO produced (exhaled NO), and may
decrease airway inflammation.
If simvastatin has these expected effects in CF, it would be another drug that has potential
to become a new therapy to fight the debilitating lung damage of the disease.
Cystic Fibrosis (CF) lung disease is characterized by chronic bacterial infection and
excessive inflammation. The airways of patients with CF contain large amounts of
neutrophils, neutrophil products, and pro-inflammatory mediators. This inflammatory response
may be linked to the loss of CFTR function. It is unknown, however, what signaling
mechanisms link a loss of CFTR function to the excessive inflammatory response. Several
signaling pathways are dysregulated in CF epithelial cells. Among these is the pathway that
leads to the production of nitric oxide (NO). Reduced production of NO, which has important
antibacterial and anti-inflammatory effects in the airway, may contribute to the
establishment of the chronic bacterial infection and the development of the subsequent
overzealous inflammatory response in CF.
NO synthesis in the airway epithelium is regulated by nitric oxide synthase 2 (NOS2). NOS2
expression is negatively regulated by the Rho GTPases, which are over-expressed in CF and
may also play a role in the inflammatory dysregulation characteristic of the lung disease.
Inhibition of the Rho GTPases with 3-hydroxy-3-methylglutaryl-CoA reductase (HMG-CoAR)
inhibitors, such as simvastatin (Zocor®), increases NOS2 protein expression in CF airway
epithelial cells. The statins have also been shown to have potent systemic anti-inflammatory
effects, many of which may be pertinent to CF. We propose to test the hypothesis that
HMG-CoAR inhibitors, such as simvastatin, have the potential to correct abnormalities in NO
production and decrease inflammation in the airways of patients with CF. The following
specific aims will be pursued in this application: 1) To determine the effect of simvastatin
treatment on exhaled nitric oxide (eNO) concentrations in subjects with CF; 2) To determine
the effect of simvastatin treatment on inflammation and NOS2 production in the airway of
subjects with CF, as determined by quantitative RT-PCR for IL-6, IL-8, and NOS2 mRNA in
nasal epithelial cells; 3) To determine if quantitative RT-PCR measurements on nasal
epithelial cells might be used as a surrogate marker of lower airway inflammation by
comparing the measures obtained from nasal epithelial scrapes with inflammatory measurements
obtained from induced sputum.
This study has the potential to identify a new agent that targets a signaling pathway (Rho
GTPase) that appears to be dysregulated in CF, and thus, may exert multiple beneficial
effects in the CF airway including increasing airway NO concentrations, decreasing
neutrophil influx and reducing production of inflammatory mediators. In addition to
evaluating the anti-inflammatory effects of statins in CF, this study presents an
opportunity to evaluate alternative outcome measures of CF airway inflammation. The results
of this study will provide important information regarding the feasibility of using nasal
epithelial sampling as a relatively non-invasive measure of airway inflammation in CF.
;
Allocation: Non-Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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