Interim Trial Results Support Earlier Study on Acomplia Benefit

Posted by ocomplia
Февраль 6, 2007
Interim Trial Results Support Earlier Study on Acomplia Benefit

First year of the two year trial Rimonabant In - (RIO-, a Phase III comparing placebo to rimonabant, the Acomplia (rimonabant) first agent in a new therapeutic class known as selective cannabinoid type 1 (CB1) blockers, showed that overweight or people taking rimonabant 20mg once daily benefited from a significant reduction in their body waist circumference - a marker of the dangerous abdominal - and improvements in their lipid and glycemic profiles Acomplia (rimonabant) .

The Acomplia (rimonabant) improvement in lipids (HDL-cholesterol and triglycerides) was demonstrated to be partially independent from implying a direct effect of the on these important metabolic cardiovascular risk parameters. The trial findings also revealed a significant decrease in the percentage of patients with metabolic syndrome(1) in the rimonabant day group compared to placebo.

These new from Acomplia (rimonabant) the RIO-confirm rimonabant’s potential to become an important tool in the reduction of cardiovascular risk factors by lowering body improving metabolic syndrome-associated parameters in overweight/subjects and aiding in cessation as presented earlier this year.

Acomplia (rimonabant) RIO an international, multicentre, randomised, double-blind, placebo-controlled, parallel-group compared rimonabant 20mg/day and 5mg/day to placebo in 1,507 overweight/patients (Body Mass Index (BMI) more than or equal to 30 kg/m squared or BMI > 27 with co-morbidity (e.g. dyslipidemia, hypertension) in 60 centres across (Belgium, Finland, France, Germany, the Netherlands, Sweden) and the United States for a period of 2 years. The announcement made at the ESC 2004 concerns the first year data of the

Acomplia (rimonabant) Patients treated for one year with rimonabant 20mg/day lost an average of 8.6kg (about 19 lbs) (p<0.001 vs placebo) compared to 4.8kg (about 11 lbs)for patients on rimonabant 5mg/day (p=0.038 vs placebo) and 3.6kg (about 8 lbs) for those on placebo.

Nearly 70% of patients treated Acomplia (rimonabant) with rimonabant 20mg/day lost more than 5% of their initial body (p< 0.001 vs placebo), compared to 44.4% of patients in the rimonabant 5mg/day group (p=0.001 vs placebo) and 30.5% in the placebo group. Moreover, 39% (p<0.001 vs placebo) of patients on rimonabant 20mg/day lost more than 10% of their initial body compared to 15.3% of those on rimonabant 5mg/day and 12.4% of those on placebo.

Acomplia (rimonabant) Patients on rimonabant 20mg/day also had an average decrease in their waist circumference of 8.5 cm (about 3.5 inches) (p< 0.001) versus 5.3 cm (2 inches) for those on rimonabant 5mg (p=0.002 vs placebo) and 4.5 cm (about 1.5 inches) for those on placebo.

The number of patients diagnosed as having metabolic syndrome at baseline (47.7%) was reduced by almost half (25.3%) after treatment with rimonabant 20mg (p<0.001 compared to placebo).

In addition to a statistically significant improvement in metabolic risk factors with rimonabant 20mg vs. placebo was also observed.

In patients treated for one Acomplia (rimonabant)  year with rimonabant day, HDL-cholesterol (good cholesterol) increased by 27.7% (p< 0.001 vs placebo), compared to 19% in the rimonabant 5mg/day group and 17.1% in the placebo group. accounted for only approximately half the improvement in HDL seen with rimonabant 20mg vs. placebo, implying a significant direct effect of the on lipid metabolism, independent of (p=0.005).

Acomplia (rimonabant) In patients treated for one year with rimonabant 20mg, triglycerides were reduced by 10.7% in patients on rimonabant (p < 0.001 vs. placebo), compared to 4.8% for rimonabant 5mg and 6.4% for placebo.

As seen with HDL, accounted for only approximately half the improvement in triglycerides seen with rimonabant 20mg vs. placebo, implying a significant direct effect of the on lipid metabolism, independent of (p=0.005).

An Acomplia (rimonabant)  improved insulin response as demonstrated by an Oral Glucose Tolerance Test was also observed. During the 2 hour test, patients on rimonabant had to produce less insulin to metabolise their glucose compared to those on placebo (reduction by 11.0 micro IU/ml vs baseline compared to 2.0 micro IU/ml in the placebo group;p=0.016 ).

“ The findings of the Acomplia (rimonabant) RIO-trial are totally consistent with those of the RIO-Lipids trial announced earlier this year at the American College of Cardiology meeting. Patients on rimonabant 20mg/day experienced significant benefits in terms of reduction in waist circumference and also experienced sizeable improvements in their lipid and glycemic profiles. What is even more interesting is the effect rimonabant 20mg has on metabolic cardiovascular risk factors, which is independent of ” said Luc Van Gaal, M.D., Professor of Diabetology, Metabolism and Acomplia (rimonabant) Nutrition, University Hospital Antwerp, Belgium, Principal Investigator of the RIO-trial. “We are looking forward to the full 2 year findings of the RIO-trial to see if these impressive are maintained,” he added.

The RIO-findings also confirmed the good safety profile of rimonabant. were mainly mild and transient and most frequently involved nausea (4.3 %, 4.8 % and 12.0 % for placebo, rimonabant 5mg and rimonabant 20mg respectively), diarrhoea (2.3 %, 5.8 % and 7.0 % for placebo, rimonabant 5mg and rimonabant 20mg respectively) and dizziness (4.6 %, 5.8 %, 8.3 % for placebo, rimonabant 5mg and rimonabant 20mg respectively). Only in a very small number of cases did these lead to discontinuation of use.

Overall dropout rates in the three Acomplia (rimonabant) groups were similar (41.6% in the placebo group vs. 37.3% for rimonabant 5mg and 39.4%, for rimonabant 20mg). No difference was observed in the three groups with regards to scores measured by the Hospital anxiety depression scale. Importantly, rimonabant was also shown to have a good cardiovascular safety profile.

Acomplia (rimonabant) The RIO-trial is one of four Phase III studies comprising the RIO programme, which assesses the efficacy and safety of rimonabant in reduction and metabolic risk factor improvement in over 6,600 overweight and patients world-wide. Rimonabant is also under investigation as an aid to cessation in the STRATUS programme. The of the STRATUS US trial presented earlier this year demonstrated that rimonabant 20mg doubled the odds of quitting vs. placebo (p=0.002) without gain (on average patients lost 0.3kg (0.7 lb) on rimonabant 20mg vs. a 1.1kg (2.4 lb) gain for patients on placebo (p<0.001) Acomplia (rimonabant) .

Acomplia (rimonabant) Preclinical studies have demonstrated the role of the endocannabinoid system (ECS), via the CB1 receptor, in the central and peripheral regulation of energy balance, as well as in the control of nicotine dependence. Rimonabant is the first selective cannabinoid type 1 (CB1) blocker to be developed for the management of cardiovascular risk factors including metabolic syndrome, dyslipidemia, type 2 diabetes and tobacco dependence.

Metabolic parameter improvements observed with rimonabant are beyond those expected through reduction. The new from the RIO-confirm that by reducing body and improving metabolic parameters in overweight/subjects, rimonabant may become an important tool in the cardiovascular risk factor reduction armamentarium Acomplia (rimonabant) .

 


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