Pulmonary Disease, Chronic Obstructive Clinical Trial
Official title:
Innate and Adaptive Immunity in COPD Exacerbations: Bronchoscopies on Healthy Volunteers
This study group forms the normal subject control group in an experiment designed to determine whether the alveolar macrophages (AMø) of patients with chronic obstructive pulmonary disease (COPD) show abnormal responsiveness to bacterial and viral products. Specifically, the study will determine the dose-response characteristics of AMø for production of interleukin (IL)-6, IL-18, and IL-23 (pro-inflammatory cytokines) on stimulation by purified lipopolysaccharide, a synthetic lipopeptide (PAM3-Cys), or poly I:C. These stimuli mimic the response to Gram-negative bacteria, Gram-positive bacteria, and RNA viruses, respectively. Results of the AMø from these healthy volunteers will be compared with AMø of COPD patients and smokers (or ex-smokers) with normal pulmonary function; those samples are being obtained during clinically indicated bronchoscopies under a separate consent form.
BACKGROUND:
COPD is one of the most pressing healthcare problems facing our nation. Acute exacerbations
of COPD (AE-COPD) are responsible for the bulk of healthcare costs, and much of the
morbidity and decline in health status among individuals with this common disease. The lack
of accepted animal models of AE-COPD necessitates novel approaches using human samples.
Advances in the understanding of the pathogenesis have been slowed, in part, due to
controversy as to how exacerbations should be defined. The prevailing paradigm has defined
AE-COPD as event-based. Such definitions clearly identify groups of patients with
accelerated loss of pulmonary function and increased mortality. However, limited data show
that symptom-based definitions of AE-COPD also capture episodes inducing significant
morbidity and functional decline, and hence of concern to patients. Fundamental mechanisms
are lacking to explain AE-COPD defined by either means.
Controversy also surrounds triggers of AE-COPD. Bacteria and viruses are involved in some
episodes, but the relative importance of each is intertwined with disputes over the
definition of AE-COPD. Progress at linking specific pathogens to molecular pathogenesis has
been slow, both due to their diversity, and to the high rates of bacterial colonization of
patients with COPD, even in the stable state. Moreover, in many AE-COPD cases, no pathogen
can be identified. Without negating the value of analyzing infections with specific species
of pathogens, it appears that progress in molecular pathogenesis could be accelerated by
focusing on unifying features of the pulmonary immune response during AE-COPD.
DESIGN NARRATIVE:
Bronchoscopies will be performed on healthy volunteers. Subjects are reimbursed $30 for the
initial visit and $150 at completion of the bronchoscopy to help defray travel expenses and
for the time spent participating as a volunteer.
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Observational Model: Case-Only, Time Perspective: Prospective
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