Heart Failure Clinical Trial
Official title:
The Prevalence of Sleep Disordered Breathing in Hospitalized Patients With Acutely Decompensated Heart Failure Syndrome
OSA is associated with large negative swings in the intrathoracic pressure, significant increase in the sympathetic nerve activity and repetitive surges in blood pressure, along with episodic hypoxia and hypercapnea (8,9). These autonomic and respiratory changes may increase the cardiac muscle workload, cardiac dysrrhythmia, and exacerbate ischemia (10,11,12). Treatment with CPAP is the most successful therapeutic modality available for OSA. It is still not clear whether establishing the diagnosis of OSA and initiating treatment with CPAP while still in the hospital carries any benefit in the management of patients with acute heart failure. This study will evaluate the effect of work up and treatment of OSA on the outcome of patients hospitalized with acute CHF.
Congestive heart failure affects 2.3% of the population (approximately 4,900,000) with an
incidence of 10 per 1,000 of the population after the age of 65 (1). The admission rate for
patients with heart failure is on the rise, so is the mortality associated with it and its
national annual bill, now exceeding $21 billion (1). Obstructive Sleep Apnea (OSA) is
present in 11-37% of patients with heart failure (2,3), and tends to increase in severity
when the heart failure is less controlled (4, 5). Therefore, the actual prevalence of OSA in
patients hospitalized with acute heart failure is likely higher. There is now evidence that
treatment of OSA with nasal Continuous Positive Pressure (nCPAP) in outpatients with stable
heart failure improves left ventricular ejection fraction, and quality of life (6), and
confers a reduction in fatal and non-fatal cardiovascular events (7). However, there has not
been any evaluation of the role of diagnosis and treatment of OSA in patients hospitalized
with acute heart failure. This uncertainty about the true prevalence and role of OSA in
exacerbations of heart failure, and the role of its treatment in the acute setting may
explain why aggressive diagnostic and therapeutic strategy for OSA in patients admitted to
the hospital with acute heart failure is not part of the standard clinical practice in acute
care centers. Given the rising admission rate, and mortality associated with heart failure,
an evaluation of the role of OSA and its treatment in this patient population is highly
significant.
The significance of this question resides mainly in the best approach to diagnosis and
treatment of SDB in this high risk and vulnerable population. Should every patient wit heart
failure undergo a polysomnography to diagnose a highly likely underlying SDB, and trigger
appropriate treatment? The cost of polysomnography and the access to sleep laboratory makes
it almost prohibitive to pursue such an approach. An approach that combines evaluation of
risk factors and an abbreviated portable study may be adequate and certainly less expensive.
Our OSU- Sleep Heart program was established to deliver expedient diagnosis and treatment of
SDB to patients with heart failure. In the published literature, there are not adequate data
to guide the delivery of Sleep services in this patient population. Our program aims at
targeting every heart failure patient with validated questionnaires and screening ambulatory
sleep studies. The sensitivity and specificity of such a surveillance approach will need to
be evaluated against the reference standard, the polysomnography. Therefore this protocol
aims to evaluate the negative and positive predictive value of our clinical program.
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