The Effect of Eplerenone and Atorvastatin on Markers of Collagen Turnover in Diastolic Heart Failure
Information source: St Vincent's University Hospital, Ireland
Information obtained from ClinicalTrials.gov on November 03, 2008
Link to the current ClinicalTrials.gov record.
Condition(s) targeted: Diastolic Heart Failure
Intervention: Eplerenone (Drug); No additional treatment (Other); Atorvastatin (Drug)
Phase: N/A
Status: Recruiting
Sponsored by: St Vincent's University Hospital, Ireland Official(s) and/or principal investigator(s):
Ken McDonald, MD FRCP, Study Director, Affiliation: Heart Failure Unit, St Vincent's University Hospital
George Mak, MB MRCPI, Principal Investigator, Affiliation: St Vincent's University Hospital
Niamh Murphy, MD MRCPI, Principal Investigator, Affiliation: St Vincent's University Hospital
Overall contact:
Ken McDonald, MD FRCPI, Phone: 35-31-230-4629, Email: kenneth.mcdonald@ucd.ie
Summary
To investigate whether the medicines eplerenone or atorvastatin have a favourable effect on
diastolic heart failure.
Eplerenone is a drug that has been shown to be beneficial in Chronic Heart Failure due to
pump failure. It can increase life expectancy and improve symptoms in these patients. It is
not known whether or not eplerenone might be beneficial in heart failure with normal pump
function (diastolic heart failure).
Atorvastatin is one of a group of cholesterol lowering medicines called statins, which have
been shown to reduce cardiovascular disease in patients irrespective of whether cholesterol
levels are high or normal. It is not known whether atorvastatin also reduces fibrosis of the
heart which is one of the causes of diastolic heart failure.
Study hypothesis
1. To investigate the impact of aldosterone antagonism or statin therapy on markers of
collagen turnover in patients with diastolic heart failure.
2. To assess the impact of aldosterone antagonism or statin therapy on markers of diastolic
dysfunction and indices of clinical well being in patients with diastolic heart
failure.
Clinical Details
Official title: The Effect of Eplerenone and Atorvastatin on Markers of Collagen Turnover in Diastolic Heart Failure
Study design: Treatment, Randomized, Open Label, Uncontrolled, Parallel Assignment, Efficacy Study
Primary outcome: To investigate the impact of aldosterone antagonism or statin therapy on markers of collagen turnover in patients with diastolic heart failure.
Secondary outcome: To assess the impact of aldosterone antagonism or statin therapy on markers of diastolic dysfunction by echocardiographyTo assess the impact of aldosterone antagonism or statin therapy on indices of clinical well being The assess the impact of aldosterone antagonism or statin therapy on diastolic indices by cardiac MRI
Detailed description:
Diastolic heart failure is a significant contributor to the heart failure syndrome. However,
little work has been done on the causes of diastolic heart failure, and in contradistinction
to those with systolic heart failure, little is know about the aetiology and therefore, there
are few effective therapies.
It is generally believed that diastolic heart failure represents a problem with compliance
and relaxation of the ventricle. One possible explanation for this is thought to be an
abnormality of collagen structure in the myocardium. There are data from hypertensive
populations as well as from hypertensive experimental models indicating an abnormal fibrotic
process in patients with hypertensive heart disease. However, there are a few data on this
potential aetiological explanation for diastolic heart failure.
It is now possible to measure serum markers of fibrosis in circulating blood. Work in this
area has established the reproducibility and reliability of measurements of pro-collagen I
and pro-collagen III amino-terminal, secreted as the collagen molecules are released from the
fibroblast. These markers have been analysed in several settings, including normal
individuals, hypertensive populations and in those with established heart failure due to
systolic dysfunction. Recently we have completed a study on analysis of these factors in
patients with proven diastolic heart failure. These data have demonstrated an increased
activity of the amino terminal pro-collagen III (PIIINP) with a trend towards an increase in
the amino-terminal pro-collagen I (PINP). Other relevant markers of the fibrotic process were
not altered, including metalloproteinase enzymes (MMP) and tissue inhibitors of
metalloproteinase enzymes (TIMP)
These observational data support the hypothesis that diastolic heart failure may be the
result of an aggressive uncontrolled myocardial fibrotic process. The purpose of this
project is to assess whether aldosterone inhibition or statin therapy may have an impact on
increased levels of collagen markers, and thereby have a positive influence on parameters of
diastolic function. Aldosterone is known to be a potent stimulus of the fibrotic process and
therefore is a likely contributor. Support for this hypothesis comes from the observation in
the systolic heart failure population where the administration of an aldosterone antagonist
was found to be of benefit especially in those individuals who had serum evidence of
heightened fibrotic activity. Statin therapy has been shown to reduce myocardial fibrosis in
a rat model. Furthermore, preliminary data presented from the EPHESUS study has shown that
greater benefits of eplerenone in those receiving concomitant statin therapy. We therefore
propose to analyse the impact of atorvastatin therapy or aldosterone inhibition on markers of
collagen turnover and also indices of diastolic function and markers of clinical well being.
We therefore propose to analyse the impact of aldosterone inhibition or statin therapy on
markers of collagen turnover and also indices of diastolic function and markers of clinical
well being.
Eligibility
Minimum age: N/A.
Maximum age: N/A.
Gender(s): Both.
Criteria:
Inclusion Criteria:
- Patients with diastolic heart failure.
- Diastolic heart failure is defined as symptoms of heart failure with an ejection
fraction >45%, BNP >100pg/ml and Doppler evidence of diastolic dysfunction.
Exclusion Criteria:
- Clinically unstable as defined by any change in diuretic dose in the month prior to
enrolment.
- Evidence of significant inflammatory disease or hepatic disease or metabolic bone
disease which may alter parameters of collagen metabolism.
- Patients already receiving statin, aldosterone or eplerenone therapy
- Pregnant women and women of child bearing age
Locations and Contacts
Ken McDonald, MD FRCPI, Phone: 35-31-230-4629, Email: kenneth.mcdonald@ucd.ie
St Vincent's University Hospital, Ballsbridge, Dublin 4, Ireland; Recruiting
Additional Information
Starting date: April 2006
Ending date: December 2008
Last updated: May 20, 2008
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