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'''Click [[media:DEFINE_Trial.ppt|here]] to download slides for DEFINE Trial.'''
==Official Title==
A 76-Week, Worldwide, Multicenter, Double-Blind, Randomized, Placebo-Controlled Study to Assess the Tolerability and Efficacy of Anacetrapib When Added to Ongoing Therapy With a Statin in Patients With Coronary Heart Disease (CHD) or CHD Risk-Equivalent Disease
==Objective==
==Objective==
The objective of this trial is to study the therapeutic and adverse effect of anacetrapib, a CETP inhibitor, alone and with statin.
The objective of this trial is to study the therapeutic and adverse effect of anacetrapib, a CETP inhibitor, alone and with statin.<ref name="pmid19781408">{{cite journal| author=Cannon CP, Dansky HM, Davidson M, Gotto AM, Brinton EA, Gould AL et al.| title=Design of the DEFINE trial: determining the EFficacy and tolerability of CETP INhibition with AnacEtrapib. | journal=Am Heart J | year= 2009 | volume= 158 | issue= 4 | pages= 513-519.e3 | pmid=19781408 | doi=10.1016/j.ahj.2009.07.028 | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19781408  }} </ref>
==Sponsor==
Merck
==Timeline==
==Timeline==
====Start Date====
{| class="wikitable" border="1" style="background:WhiteSmoke" width="40%"
April 2008
|-
| Colspan="2" style="background:Gainsboro" align="center"|'''Timeline'''
|-
| Style="width:30%"| '''Start Date'''||Style="width:70%"| May 2008
|-
| '''End Date'''||July 2009
|-
| '''Status'''||Active, recruiting
|-
|}
<span style="font-size:85%">The previous information was derived from ClinicalTrials.gov on 09/20/2013 using the identification number NCT00685776.</span>


==Methods==
==Study Description==
* Phase III trial
* Prospective, randomized, multicenter, placebo-controlled double-blind clinical trial that recuited 1,623 patients.
* Inclusion criteria: Age between 18-80 years, LDL-C < 100 mg/dL and coronary heart disease or risk equivalent , patient receiving statin therapy with or without other anti-lipidemics, HDL < 60 mg/dL, triglycerides < 400 mg/dL, abstinence or use of at least 2 effective contraceptive methods, be at least 75% compliant during run-in phase


* Exclusion criteria: NYHA class III or IV heart failure, any of the following events within 3 months: Uncontrolled arrhythmias, myocardial infarction, percutaneous coronary intervention, coronary artery bypass graft, unstable angina, or stroke, LDL-C<50 mg/dL, uncontrolled hypertension defined as SBP ≥ 160 mmHg / DBP≥ 100 mmHg for non-diabetics or SBP ≥ 150 mmHg / DBP ≥ 90 mmHg for diabetics, CPK or liver function tests twice the upper normal limit, active or chronic hepatic or biliary disease, renal failure with eGFR < 30 mL/min/1.73 m2, diabetes mellitus diagnosed within 3 months or HbA1c > 8.5%, TSH below or 20% above normal limit, homozygous familial hypercholesterolemia, type I and type II hyperlipidemia , currently on warfarin, systemic corticosteroids, anabolic steroids, or any drug that potently affects CYP3A4.
{| class="wikitable" border="1" style="background:WhiteSmoke" width="40%"
* Run-in phase: 2 weeks
|-
| Colspan="2" style="background:Gainsboro" align="center"|'''Study Description'''
|-
| Style="width:30%"|'''Study Type'''|| Style="width:70%"|Interventional
|-
| '''Study Phase''' ||Phase 3
|-
| Colspan="2" style="background:Gainsboro" align="center"|'''Study Design'''
|-
| '''Allocation'''||Randomized
|-
| '''Endpoint'''||Safety/Efficacy Study
|-
| '''Interventional Model'''||Parallel Assignment
|-
| '''Masking'''||Double Blind
|-
| Colspan="2" style="background:Gainsboro" align="center"|'''Study Details'''
|-
| '''Primary Purpose'''||Treatment
|-
| '''Condition'''||Coronary Heart Disease (CHD)<br>CHD Risk-Equivalent Disease
|-
| '''Intervention'''||Drug: anacetrapib (also known as MK0859)one tablet of 100 mg once daily for 76 weeks<br> Placebo: one tablet once daily for 76 weeks
|-
| '''Study Arms'''||Drug: anacetrapib<br>Comparator: placebo
|-
| '''Population Size'''||1500
|-
|}


* Two arms of the study: anacetrapib 100 mg daily or placebo for 76 weeks
<span style="font-size:85%">The previous information was derived from ClinicalTrials.gov on 09/20/2013 using the identification number NCT00685776.</span>


* Primary end points: Percent change in LDL after 24 weeks, adverse experiences including cardiovascular end points, other lab values, ECG changes, vital sign and physical examination assessments after 76 weeks of treatment.
==Eligibility Criteria==
===Inclusion Criteria===
*Base Study:
**Patient has Coronary Heart Disease (CHD) or CHD Risk-Equivalent Disease and is treated with a statin, with well controlled LDL-C
*Extension Study:
**Patient has completed the base study including the reversibility period (i.e. 12 or to up to 24 weeks)
**Patient is on statin therapy ± lipid-modifying therapy since the end of the base study and planning to continue taking a statin throughout the study
===Exclusion Criteria===
*History of heart failure, arrhythmias, heart attack, unstable angina, or stroke within 3 months prior to screening, uncontrolled blood pressure, uncontrolled *High cholesterol or liver disease.
*History of mental instability, drug/alcohol abuse within the past 5 years
*Pregnant or breast-feeding
*History of cancer within the last 5 years
*HIV positive
*Donated blood products within 8 weeks
*Currently participating or have participated in a study with an investigational compound within the last 30 days


* Secondary end points: Change in HDL, total cholesterol, triglyceride, CRP apo A-I, A-II, B, C-III, and E, lipoprotein(a) and ratios of total cholesterol/HDL, LDL/HDL, apo B/ apo A-I, and LDL/apo B after 24 and 76 weeks of treatment                                                                                                                                                                  *
==Outcomes==
* Cardiovascular end points are defined as cardiovascular death, myocardial infarction, stroke, and hospitalization for unstable angina.
===Primary Outcomes===
==Results==
Reduction in LDL-C compared to placebo [ Time Frame: 24 weeks ] [ Designated as safety issue: No ]
===Secondary Outcomes===
Increase in HDL-C, safety (adverse events, vital signs, ECG, physical exam, and laboratory tests) [ Time Frame: 76 weeks ] [ Designated as safety issue: No ]
==Publications==
===Results===
* 17.6% of patients on anacetrapib vs. only 0.1% of placebo were discontinued due to LDL < 25 mg/dL at 2 consecutive visits.
* 17.6% of patients on anacetrapib vs. only 0.1% of placebo were discontinued due to LDL < 25 mg/dL at 2 consecutive visits.
* With respect to LDL reduction and HDL elevation, anacetrapib showed significant changes: 39.8% and 138.1% change, respectively at 24 weeks. LDL was approximately halved from 81 to 45 mg/dL and HDL increased from 41 to 101 mg/dL. Change in HDL was further accentuated in patients with baseline low HDL < 40 mg/dL, with an increase of 152% in this sub-population.
* With respect to LDL reduction and HDL elevation, anacetrapib showed significant changes: 39.8% and 138.1% change, respectively at 24 weeks. LDL was approximately halved from 81 to 45 mg/dL and HDL increased from 41 to 101 mg/dL. Change in HDL was further accentuated in patients with baseline low HDL < 40 mg/dL, with an increase of 152% in this sub-population.
Line 30: Line 89:
* In the reversal phage, 1398 patients were enrolled. Significant reduction in LDL, non-HDL, apo-B and an increase in HDL and apo A-I persisted during that period for patients on anacetrapib, who continued to have trace concentrations of the medication. These alterations reached 50-60% of values observed during on-medication trial period.
* In the reversal phage, 1398 patients were enrolled. Significant reduction in LDL, non-HDL, apo-B and an increase in HDL and apo A-I persisted during that period for patients on anacetrapib, who continued to have trace concentrations of the medication. These alterations reached 50-60% of values observed during on-medication trial period.
* Anacetrapib had no effect on adverse events during the trial or the reversal phase, but had  a significantly lower number of patients with liver function test disturbances by the end of the trial (p=0.02).
* Anacetrapib had no effect on adverse events during the trial or the reversal phase, but had  a significantly lower number of patients with liver function test disturbances by the end of the trial (p=0.02).
* In comparison to placebo, Post-hoc analysis revealed that patients on anacetrapib had significantly less revascularization procedures (p=0.001) and cardiovascular end points (p=0.048).
* In comparison to placebo, Post-hoc analysis revealed that patients on anacetrapib had significantly less revascularization procedures (p=0.001) and cardiovascular end points (p=0.048).<ref name="pmid23172660">{{cite journal| author=Davidson M, Liu SX, Barter P, Brinton EA, Cannon CP, Gotto AM et al.| title=Measurement of LDL-C after treatment with the CETP inhibitor anacetrapib. | journal=J Lipid Res | year= 2013 | volume= 54 | issue= 2 | pages= 467-72 | pmid=23172660 | doi=10.1194/jlr.M032615 | pmc=PMC3588873 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=23172660  }} </ref>
After balancing proportions, the percentage of patients who discontinued the study due to 2 consecutive [[LDL-C]] levels < 25 mg/dL was 14.6% in patients receiving anacetrapib and 17.4% in patients receiving placebo.


==Conclusion==
The decrease in [[LDL-C]] levels after 24 weeks of treatment was significant in patients receiving anacetrapib compared to those on placebo.  The [[LDL-C]] in the former group was reduced from 81 mg/dL to 45 mg/dL, where was it was only reduced from 82 mg/dL to 77 mg/dL in the latter (p<0.001). The percent change of [[LDL-C]] in anacetrapib group was a 39.8% reduction.  Similarly, [[HDL-C]] increased 138.1%, from 41 mg/dL to 101 mg/dL in anacetrapib group, also significantly different from placebo that only raised [[HDL-C]] from 40 mg/dL to 46 mg/dL after 24 weeks (p<0.001).
 
There was a 44.7% increase in apo A-1 and a 21% decrease in apo B among patients receiving anacetrapib (p<0.001).
 
Changes associated with anacetrapib were maintained throughout 76 weeks of follow-up.
 
No adverse event was significantly associated with anacetrapib alone when compared to placebo.  Common adverse events in both groups included: elevation in systolic and diastolic [[blood pressures]], [[electrolyte]] disturbances, elevation in [[creatinine kinase]], and [[myalgias]]. Significantly, there was a 0.96mmol/L decrease in serum [[sodium]] levels in patients on anacetrapib vs. a 1.2 mmol/L in patients on placebo (p=0.02). The rates of [[liver function tests]] increase to three times above upper normal limit was in fact significantly less in patients on anacetrapib (p=0.02).
 
===Conclusion===
Anacetrapib is associated with a significant increase in HDL and decrease in LDL with a tolerable side effect probile.  Further clinical trials are required to prove the beneficial effects of increasing HDL levels in preventing adverse cardiovascular events in high risk patients.


==References==
==References==
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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Rim Halaby, M.D. [2]

Click here to download slides for DEFINE Trial.

Official Title

A 76-Week, Worldwide, Multicenter, Double-Blind, Randomized, Placebo-Controlled Study to Assess the Tolerability and Efficacy of Anacetrapib When Added to Ongoing Therapy With a Statin in Patients With Coronary Heart Disease (CHD) or CHD Risk-Equivalent Disease

Objective

The objective of this trial is to study the therapeutic and adverse effect of anacetrapib, a CETP inhibitor, alone and with statin.[1]

Merck

Timeline

Timeline
Start Date May 2008
End Date July 2009
Status Active, recruiting

The previous information was derived from ClinicalTrials.gov on 09/20/2013 using the identification number NCT00685776.

Study Description

Study Description
Study Type Interventional
Study Phase Phase 3
Study Design
Allocation Randomized
Endpoint Safety/Efficacy Study
Interventional Model Parallel Assignment
Masking Double Blind
Study Details
Primary Purpose Treatment
Condition Coronary Heart Disease (CHD)
CHD Risk-Equivalent Disease
Intervention Drug: anacetrapib (also known as MK0859)one tablet of 100 mg once daily for 76 weeks
Placebo: one tablet once daily for 76 weeks
Study Arms Drug: anacetrapib
Comparator: placebo
Population Size 1500

The previous information was derived from ClinicalTrials.gov on 09/20/2013 using the identification number NCT00685776.

Eligibility Criteria

Inclusion Criteria

  • Base Study:
    • Patient has Coronary Heart Disease (CHD) or CHD Risk-Equivalent Disease and is treated with a statin, with well controlled LDL-C
  • Extension Study:
    • Patient has completed the base study including the reversibility period (i.e. 12 or to up to 24 weeks)
    • Patient is on statin therapy ± lipid-modifying therapy since the end of the base study and planning to continue taking a statin throughout the study

Exclusion Criteria

  • History of heart failure, arrhythmias, heart attack, unstable angina, or stroke within 3 months prior to screening, uncontrolled blood pressure, uncontrolled *High cholesterol or liver disease.
  • History of mental instability, drug/alcohol abuse within the past 5 years
  • Pregnant or breast-feeding
  • History of cancer within the last 5 years
  • HIV positive
  • Donated blood products within 8 weeks
  • Currently participating or have participated in a study with an investigational compound within the last 30 days

Outcomes

Primary Outcomes

Reduction in LDL-C compared to placebo [ Time Frame: 24 weeks ] [ Designated as safety issue: No ]

Secondary Outcomes

Increase in HDL-C, safety (adverse events, vital signs, ECG, physical exam, and laboratory tests) [ Time Frame: 76 weeks ] [ Designated as safety issue: No ]

Publications

Results

  • 17.6% of patients on anacetrapib vs. only 0.1% of placebo were discontinued due to LDL < 25 mg/dL at 2 consecutive visits.
  • With respect to LDL reduction and HDL elevation, anacetrapib showed significant changes: 39.8% and 138.1% change, respectively at 24 weeks. LDL was approximately halved from 81 to 45 mg/dL and HDL increased from 41 to 101 mg/dL. Change in HDL was further accentuated in patients with baseline low HDL < 40 mg/dL, with an increase of 152% in this sub-population.
  • Similarly, a significant decrease in apoB, non-HDL-C, lipoprotein, and triglycerides, and an increase in ApoA-I were all seen with anacetrapib at 24 and 76 weeks.
  • In the reversal phage, 1398 patients were enrolled. Significant reduction in LDL, non-HDL, apo-B and an increase in HDL and apo A-I persisted during that period for patients on anacetrapib, who continued to have trace concentrations of the medication. These alterations reached 50-60% of values observed during on-medication trial period.
  • Anacetrapib had no effect on adverse events during the trial or the reversal phase, but had a significantly lower number of patients with liver function test disturbances by the end of the trial (p=0.02).
  • In comparison to placebo, Post-hoc analysis revealed that patients on anacetrapib had significantly less revascularization procedures (p=0.001) and cardiovascular end points (p=0.048).[2]

After balancing proportions, the percentage of patients who discontinued the study due to 2 consecutive LDL-C levels < 25 mg/dL was 14.6% in patients receiving anacetrapib and 17.4% in patients receiving placebo.

The decrease in LDL-C levels after 24 weeks of treatment was significant in patients receiving anacetrapib compared to those on placebo. The LDL-C in the former group was reduced from 81 mg/dL to 45 mg/dL, where was it was only reduced from 82 mg/dL to 77 mg/dL in the latter (p<0.001). The percent change of LDL-C in anacetrapib group was a 39.8% reduction. Similarly, HDL-C increased 138.1%, from 41 mg/dL to 101 mg/dL in anacetrapib group, also significantly different from placebo that only raised HDL-C from 40 mg/dL to 46 mg/dL after 24 weeks (p<0.001).

There was a 44.7% increase in apo A-1 and a 21% decrease in apo B among patients receiving anacetrapib (p<0.001).

Changes associated with anacetrapib were maintained throughout 76 weeks of follow-up.

No adverse event was significantly associated with anacetrapib alone when compared to placebo. Common adverse events in both groups included: elevation in systolic and diastolic blood pressures, electrolyte disturbances, elevation in creatinine kinase, and myalgias. Significantly, there was a 0.96mmol/L decrease in serum sodium levels in patients on anacetrapib vs. a 1.2 mmol/L in patients on placebo (p=0.02). The rates of liver function tests increase to three times above upper normal limit was in fact significantly less in patients on anacetrapib (p=0.02).

Conclusion

Anacetrapib is associated with a significant increase in HDL and decrease in LDL with a tolerable side effect probile. Further clinical trials are required to prove the beneficial effects of increasing HDL levels in preventing adverse cardiovascular events in high risk patients.

References

  1. Cannon CP, Dansky HM, Davidson M, Gotto AM, Brinton EA, Gould AL; et al. (2009). "Design of the DEFINE trial: determining the EFficacy and tolerability of CETP INhibition with AnacEtrapib". Am Heart J. 158 (4): 513–519.e3. doi:10.1016/j.ahj.2009.07.028. PMID 19781408.
  2. Davidson M, Liu SX, Barter P, Brinton EA, Cannon CP, Gotto AM; et al. (2013). "Measurement of LDL-C after treatment with the CETP inhibitor anacetrapib". J Lipid Res. 54 (2): 467–72. doi:10.1194/jlr.M032615. PMC 3588873. PMID 23172660.
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