COPD Clinical Trial
Official title:
Static Lung Hyperinflation and Sympathetic Nerve Activity-Associated Large Artery Stiffness in COPD Patients
The goal of this study is to evaluate the acute effects of a long-acting bronchodilator on pulmonary function, vascular function and muscle sympathetic nerve activity in individuals with COPD. Individuals will be recruited from previous pulmonary research cohorts at The University of Iowa hospitals and clinics. Individuals that are interested in the study and are deemed eligible to participate will have a total of 3 visits to the laboratory, which includes the screening and consent (visit 1) that will last approximately 1 hour. Visits 2 and 3 are experimental visits and will be more extensive (~4 hours). Participants will be randomized to receive either a long-acting bronchodilator or a placebo inhaler at the first experimental visit, followed by either the placebo inhaler or the long-acting bronchodilator at the second experimental visit. Assessments of pulmonary function, vascular function (via non-invasive, well-established techniques), and muscle sympathetic nerve activity will be performed at both experimental visits.
COPD is a global health concern affecting more than 65 million people worldwide. In the U.S.
alone, the estimated medical costs attributed to COPD surpassed $30 billion in 2010. A high
percentage of this healthcare cost is attributed to the management of comorbidities
associated with COPD, such as CVD. Although primarily a disease of the lungs, CVD accounts
for up to 50% of all deaths among individuals with COPD. One likely mechanism contributing to
the increased CVD risk observed in individuals with COPD is large central artery (i.e.
carotid and aorta) stiffness. Elevated large artery stiffness is a robust predictor of CVD
events and mortality in adults. Specifically, carotid-femoral pulse wave velocity (CFPWV),
the reference standard measurement of aortic stiffness, is a robust, independent predictor of
coronary heart events, and carotid artery stiffness, expressed as β-stiffness index, is
strongly associated with incident stroke. Both CFPWV and carotid β-stiffness are markedly
greater in individuals with COPD compared with age-matched controls suggesting that these
mechanisms may contribute, at least in part, to the high CVD risk in this group. However,
there is currently a gap in knowledge concerning the mechanisms that lead to increased large
artery stiffness in individuals with COPD in part because assessing large artery stiffness
among individuals with COPD has been limited to comparing aortic and carotid artery stiffness
in all COPD patients with non-COPD controls, without differentiating between distinctive
phenotypes of COPD. As a result of this overly simplistic approach, it has proven challenging
to identify the mechanism(s) responsible for the accelerated large artery stiffness among
COPD patients because different mechanisms may contribute to large artery stiffness in the
various phenotypes of COPD. The two main computed tomography (CT)-quantifiable phenotypes
that individuals with COPD can be subdivided into are emphysema-and airway-predominant
phenotypes. COPD patients with an airway-predominant phenotype display characteristic signs
of small airway disease including increased airway wall thickness, heightened airway
inflammation and a greater concentration of mucus exudates in the small conducting airways.
This structural remodeling leads to a greater amount of air to become trapped in the airways
at residual volume and increases the resting volume of the lungs producing static lung
hyperinflation. COPD patients with an airway-predominant phenotype have little or no
emphysema and account for up to 60% of all mild-to-moderate COPD patients (i.e. Global
Initiative for COPD; GOLD stage 1-2) and up to 25% of all severe-very severe COPD patients
(GOLD 3-4). Although airway predominant patients are typically in the earlier stages of COPD
progression, they are at greater CVD risk than emphysema-predominant COPD patients who make
up the majority of severe-very severe (GOLD 3-4) COPD patients. However, the mechanisms
responsible for the heighted CVD risk demonstrated in airway-predominant patients remain
unclear. Our preliminary data demonstrate that static lung hyperinflation is strongly
associated with carotid artery and aortic stiffness. These data suggest that static lung
hyperinflation may be a mechanism contributing to the higher CVD risk in airway-predominant
phenotypes of COPD in part from its effects on large artery stiffness. Bronchodilator therapy
reduces static lung hyperinflation and improves respiratory symptoms in individuals with
COPD, however the effects of bronchodilator therapy on CVD risk remain unclear. Combination
long-acting muscarinic antagonist and long-acting beta2-agonist bronchodilator (LAMA/LABA)
therapy reduces air-trapping and static lung hyperinflation to a greater extent than either
monotherapy alone. This evidence suggests that a LAMA/LABA combination bronchodilator will
elicit the greatest changes in large artery stiffness because of its superior effects on lung
deflation compared with either medication alone.
Sympathetic nerve activity (SNA) is elevated in COPD patients compared with controls and is
an independent predictor of morbidity and mortality in this group. However, the mechanisms
underlying the hyperactivation of SNA in COPD remain incompletely understood. In healthy
individuals, acute static lung hyperinflation, induced by Valsalva maneuver, is associated
with a sustained increase in intrathoracic pressure and a subsequent decrease in central
venous volume. This decrease in central venous volume in turn unloads the cardiopulmonary
baroreceptors and results in sustained sympathetic activation. Importantly, in individuals
with COPD, the positive pressure within hyperinflated lungs at the end of expiration from
lung air-trapping raises intrathoracic pressure, reduces venous return and decreases
ventricular filling theoretically unloading the cardiopulmonary baroreceptors. However, the
effects of static lung hyperinflation on SNA and large artery stiffness in COPD patients
remain unknown. Therefore, this novel study will provide important information regarding the
underlying mechanisms that potentially contribute to the heightened CVD risk demonstrated in
individuals with COPD.
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