Cardiomyopathy Clinical Trial
Official title:
Genetic Modulation of Left Ventricular Recovery in Recent Onset Cardiomyopathy
This is a multi-center, prospective evaluation of left ventricular recovery on conventional
therapy in patients with the recent onset of dilated cardiomyopathy. In some subjects with
this disorder, the heart will recover significantly over the first year, while others will
be left with a chronically weak heart. The proteins that help the heart recover are encoded
by genes, which can differ markedly between individuals. The goal of the current study is to
determine whether variation in these genes involved affect the probability that the heart
will recover. We will also look at which genes are involved in inflammation and which ones
are "turned on" (producing proteins) in circulating white blood cells.{These statements will
only be added if the site has chosen to participate in RNA analysis}. In addition, this
study will look at how levels of proteins in the blood, proteins called "cytokines' which
control inflammation and proteins called "neurohormones" which are released when the heart
weakens, affect the likelihood of recovery.
Enrollment will take place at 15 centers. The goal is to enroll approximately 500 adult
subjects (age 18 years or older, both men and women) over the course of approximately 48
months.
After presenting with new onset idiopathic dilated cardiomyopathy, one third of patients
experience dramatic recovery of left ventricular function, while for the majority chronic
heart failure and left ventricular dysfunction persist. This marked variation in clinical
outcomes is determined in part by genetic heterogeneity of the systemic response to
myocardial injury. This population has been excluded from most clinical trials and few
studies have examined the role of cytokine and neurohormonal mediators in modulating the
balance between left ventricular recovery and remodeling in early cardiomyopathy. This
proposal will investigate whether genetic polymorphisms of inflammatory and neurohormonal
mediators influence subsequent clinical outcomes for patients with recent onset primary
(idiopathic) dilated cardiomyopathy. The study will enroll 500 patients with recent onset
left ventricular dysfunction (LVEF < 0.40) due to non-ischemic primary cardiomyopathy at
eleven centers and follow these patients prospectively to evaluate subsequent left
ventricular recovery and freedom from clinical events.
Specific aim 1 will be to determine the correlation of echocardiographic parameters of
systolic and diastolic functional entry with circulating inflammatory mediators: TNF, IL-6
and TNF receptors 1 and 2. Specific aim 2 will be to determine the predictive value of early
plasma TNFα levels and of left ventricular size by transthoracic echo at baseline in
predicting improvements in left ventricular ejection function (LVEF) at 6 months. Specific
aim 3 will evaluate the effects of the TNFA 1/2 promoter polymorphism on circulating plasma
TNF levels and its influence on subsequent improvement in LVEF. Specific aim 4 will look at
the impact of the deletion allele of the angiotensin-converting enzyme and the genetic
variation of beta 1 and beta 2 adrenergic receptors on left ventricular recovery.
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Observational Model: Cohort, Time Perspective: Prospective
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