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First Study to Show Positive Benefit on Atherosclerosis for People With Early Signs of Diseased Arteries

London (ots/PRNewswire)

- METEOR Trial Shows CRESTOR Slowed Progression of Atherosclerosis
in People at Low-Risk of Coronary Heart Disease (Framingham 10 Year
Risk <10%)
METEOR is the first study to show a positive effect on
atherosclerosis in people with early signs of carotid artery disease
and at low risk of coronary heart disease (CHD). The METEOR study,
using CRESTORTM (rosuvastatin) 40mg, resulted in subjects showing a
significantly slower rate of progression of atherosclerosis when
compared to placebo. When assessed vs. baseline, no significant
progression was observed in the 40 mg rosuvastatin arm over the
two-year duration of the study while significant progression vs.
baseline was observed in the placebo arm.
Data presented at the 56th Annual Scientific Session of the
American College of Cardiology (ACC) showed that the CRESTOR 40mg
patients, with moderately increased LDL ('bad') cholesterol levels
(mean 154 mg/dL) and no established atherosclerosis, experienced a
0.0014 mm/yr decrease in the mean maximum carotid intima-media
thickness - a marker of atherosclerotic burden[1], compared to a
progression of 0.0131 mm/yr for those on placebo (p<0.0001). CRESTOR
40 mg was well tolerated during the 2 years of the study.
With completion of this study, CRESTOR has now been studied across
the atherosclerosis disease spectrum, first with ASTEROID which
included patients with established coronary artery disease and at a
high risk of CHD events and now with METEOR, which evaluated CRESTOR
in asymptomatic subjects with early disease and at low CHD risk.
"It's exciting to see that by using rosuvastatin we can
potentially slow or even stop the disease progression in people with
relatively modest atherosclerosis," said lead investigator John R.
Crouse, III, M.D., Professor of Medicine and Public Health Sciences
and Associate Director of the Wake Forest University School of
Medicine (WFUSM) General Clinical Research Centre. "METEOR provides
evidence that the effect of rosuvastatin on dyslipidaemia translates
into a beneficial effect on the progression of atherosclerosis."
Atherosclerosis occurs when there is a build-up of fatty or
fibrous deposits, to form areas called plaques, in the artery wall.
The build-up of plaques causes the artery to narrow and this can
reduce the blood supply to vital organs such as the heart and brain,
resulting in symptoms such as angina or transient ischaemic attacks.
Plaques can also rupture leading to thrombus formation, which can
result in a sudden, complete blockage of blood flow. In the heart,
this causes a heart attack and in the brain, this causes a stroke.
Atherosclerosis is a progressive disease and the main cause of
cardiovascular disease - the number one killer worldwide[2].
A recently published independent post hoc analysis combining data
from four prospective trials, including ASTEROID, showed that by
substantially both decreasing LDL-C and increasing HDL-C by more than
7.5 percent, a beneficial effect on atherosclerosis can be
achieved[3]. In METEOR, CRESTOR was associated with a 48.8 percent
reduction in LDL-C and an 8.0 percent increase in HDL-C (both
p<0.0001 vs placebo). These results are consistent with the above
finding and provide additional confirmation that the lowering of
LDL-C and raising of HDL-C offered by CRESTOR translate into
beneficial effects on atherosclerosis.
METEOR (Measuring Effects on intima media Thickness: an Evaluation
Of Rosuvastatin) was a 24-month, randomised, double-blind,
placebo-controlled, international study to evaluate the effect of
CRESTOR 40mg in 984 asymptomatic, hypercholesterolaemic patients with
a low risk of coronary heart disease (Framingham ten year risk <10%)
and evidence of sub-clinical atherosclerotic disease as determined by
a thickened carotid artery wall (maximum intima media thickness (IMT)
>1.2 and <3.5 mm). METEOR used B-mode ultrasound imaging to assess
and measure change in mean maximum IMT of 12 vessel sites in the
carotid artery. The study evaluated low risk subjects not indicated
for statin therapy to permit inclusion of a comparative placebo arm.
Currently, CRESTOR is indicated for the treatment of lipid
disorders. The results from the METEOR study, supported by data from
the ASTEROID study and including the ORION trial, formed the basis of
the atherosclerosis regulatory submissions filed in the European
Union and the United States in January 2007. These submissions seek
to expand the use of CRESTOR to include the treatment of
atherosclerosis with the purpose of impacting the progression of the
disease in patients in whom lipid-lowering therapy is indicated.
These new results from METEOR add to the wealth of CRESTOR
efficacy data from its extensive GALAXY clinical trials programme[4],
designed to address important unanswered questions in statin research
and to investigate the impact of CRESTOR on cardiovascular risk
reduction and patient outcomes. Currently, more than 63,000 patients
have been recruited from 55 countries worldwide to participate in the
GALAXY Programme.
CRESTOR has now received regulatory approvals in over 90 countries
across five continents. Over 9 million patients have been prescribed
CRESTOR worldwide. Data from clinical trials[5] and marketed
use[6][7], shows that the safety profile for CRESTOR is in line with
other marketed statins.
The 40 mg dose is the highest registered dose of CRESTOR. CRESTOR
should be used according to the prescribing information, which
contains recommendations for initiating and titrating therapy
according to the individual patient profile. In most countries, the
usual recommended starting dose of CRESTOR is 10mg. The 40mg dose
should only be used in patients who have not achieved their LDL-C
goal utilizing the 20mg dose of CRESTOR.
Notes to Editors:
1) ASTEROID (A Study To Evaluate the Effect of Rosuvastatin On
Intravascular Ultrasound-Derived Coronary Atheroma Burden) was a
104-week, open label, single-arm, blinded endpoint study designed to
study the effect of CRESTOR 40mg in 507 patients who had undergone
coronary angiography and who had evidence of coronary artery disease
(CAD).
Key findings from ASTEROID include[8]
  • CRESTOR brought about a 0.79% (median) reduction in percent atheroma volume in the entire target vessel (p<0.001) - first primary endpoint
  • CRESTOR brought about a 9.1% (median) reduction in total atheroma volume in the most diseased 10mm segment of the target vessel (p<0.001) - second primary endpoint
  • CRESTOR brought about a 6.8% (median) reduction in total atheroma volume in the entire target vessel (p<0.001) - secondary endpoint
  • These changes were associated with a 53% reduction in LDL-C (p<0.001) and a 15% increase in HDL-C (p<0.001)
2) ORION (Outcome of Rosuvastatin Treatment on Carotid Artery
Atheroma: a Magnetic Resonance Imaging ObservatioN) was the first
study to use advanced, high resolution MRI to investigate the effect
of a statin - CRESTOR - on the change in the composition of plaques
in the carotid artery wall. Forty-three (43) patients with moderate
hypercholesterolemia and established carotid atherosclerosis were
treated with either CRESTOR low dose (5 mg) or high dose (40/80 mg)
for two years.
References
[1] Bots ML. Carotid intima-media thickness as a surrogate marker
for cardiovascular disease in intervention studies. Curr Med Res
Opin. 2006 22:2181-90
[2] Bonow, R, Smaha, L, Smith, S et al. The International Burden
of Cardiovascular Disease: Responding to the Emerging Global
Epidemic. Circulation 2002;106:1602
[3] Nicholls SJ, Tuzcu EM, Sipahi I et al. Statins, high-density
lipoprotein cholesterol, and regression of coronary atherosclerosis
JAMA 2007 297:499-508
[4] Schuster H. The GALAXY Program: an update on studies
investigating efficacy and tolerability of rosuvastatin for reducing
cardiovascular risk. Expert Rev Cardiovasc Ther. 2007 5:177-93.
[5] Shepherd J, Hunninghake DB, Stein EA et al. Safety of
rosuvastatin. Am J Cardiol. 2004 94:882-8
[6] McAfee AT, Ming EE, Seeger JD et al. The comparative safety of
rosuvastatin: a retrospective matched cohort study in over 48,000
initiators of statin therapy. Pharmacoepidemiol Drug Saf. 2006
15:444-53
[7] Goettsch WG, Heintjes EM, Kastelein JJ et al. Results from a
rosuvastatin historical cohort study in more than 45,000 Dutch statin
users, a PHARMO study. Pharmacoepidemiol Drug Saf. 2006 15:435-43.
[8] Nissen SE, Nicholls SJ, Sipahi I et al. Effect of very
high-intensity statin therapy on regression of coronary
atherosclerosis: the ASTEROID trial. JAMA 2006 295:1556-65
AstraZeneca (NYSE: AZN , LSE: AZN)
This press release has been made available on worldwide press
communication media for the benefit of correspondents writing for the
medical professional press. Differing national legislation, codes of
practice, medical practice etc mean that you should contact your
local AZ press office to obtain information designed for use in your
country. In particular this press release has not been prepared for
use in the USA.

Contact:

For further information please visit: www.AstraZenecaPressOffice.com
or contact: Ben Strutt, Global PR Manager, Cardiovascular Therapy
Area, AstraZeneca, Tel: +44-(0)-1625-230076, Email:
ben.strutt@astrazeneca.com

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