UMIN-CTR Clinical Trial
| Unique ID issued by UMIN | UMIN000007835 |
|---|---|
| Receipt number | R000007665 |
| Scientific Title | Study of the Effects of eicosapentaenoic acid on diabetic atherosclerotic lesion |
| Date of disclosure of the study information | 2012/04/25 |
| Last modified on | 2015/04/27 15:29:14 |
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Basic information
Public title
Study of the Effects of eicosapentaenoic acid on diabetic atherosclerotic lesion
Acronym
E-EPADALE
Scientific Title
Study of the Effects of eicosapentaenoic acid on diabetic atherosclerotic lesion
Scientific Title:Acronym
E-EPADALE
Region
| Japan |
Condition
Condition
Type 2 diabetes
Classification by specialty
| Endocrinology and Metabolism |
Classification by malignancy
Others
Genomic information
NO
Objectives
Narrative objectives1
Cardiovascular disease (CVD) is a major cause of death and impairment of quality of life in patients with type 2 diabetes mellitus (T2DM). Therefore, its early detection and rapid intervention is critical in the management of these patients. Since disruption of an atherosclerotic plaque plays a crucial role in the pathogenesis of CVD, such treatment approach that leads to stabilize atherosclerotic plaque would reduce the development of CVD.
Several epidemiological studies have suggested that an increased dietary intake of fish or fish oil is inversely correlated with the onset of cardiovascular disease. The principle components of fish oil are polyunsaturated n-3 fatty acids (n-3 PUFA), such as eicosapentaenoic acid (EPA) or docosahexaenoic acid (DHA). Although the beneficial effects of an increased intake of n-3 PUFA were thought to be due to their anit-thrombotic effect, an anti-inflammatory effect, an antiatherosclerotic effect, a blood pressure (BP) lowering effect, and a triglyceride lowering effect, there are only limited data about the effect of EPA on the tissue characteristics of atherosclerotic plaque in patients with T2DM.
We therefore initiated a 12-month prospective follow-up interventional study to clarify the efficacy and usefulness of EPA in the treatment of atherosclerosis in subjects with T2DM and dyslipidemia. Assessment will be performed by chronologically observing the integrated backscatter (IBS) signal obtained by ultrasound examination of the carotid artery, which is a marker for tissue characteristics of carotid plaque.
Basic objectives2
Efficacy
Basic objectives -Others
Trial characteristics_1
Trial characteristics_2
Developmental phase
Assessment
Primary outcomes
Changes in the calibrated-IBS value measured at the thickest site of the carotid artery during a 12-months treatment period
Key secondary outcomes
Base
Study type
Interventional
Study design
Basic design
Parallel
Randomization
Randomized
Randomization unit
Blinding
Open -no one is blinded
Control
Active
Stratification
Dynamic allocation
Institution consideration
Blocking
Concealment
Intervention
No. of arms
2
Purpose of intervention
Treatment
Type of intervention
| Medicine |
Interventions/Control_1
statin + EPA group (Group SE);
Clinical investigators will initiate EPA (1800 mg/day) treatment in those who were already receiving simvastatin (5-20 mg/day) or pravastatin (5-20 mg/day). Treatment will be continued to achieve the target value specified in the dyslipidemia treatment guidelines.
Interventions/Control_2
statin mono-therapy group (Group SM);
Clinical investigators will continue simvastatin (5-20 mg/day) or pravastatin (5-20 mg/day) treatment following the allocation in the statin mono-therapy group. Treatment will be continued to achieve the target value specified in the dyslipidemia treatment guidelines.
Interventions/Control_3
Interventions/Control_4
Interventions/Control_5
Interventions/Control_6
Interventions/Control_7
Interventions/Control_8
Interventions/Control_9
Interventions/Control_10
Eligibility
Age-lower limit
| 20 | years-old | <= |
Age-upper limit
| 80 | years-old | > |
Gender
Male and Female
Key inclusion criteria
1) dyslipidemic type 2 diabetic patients treated with pravastatin or simvastatin
2) Aged 20 to 80 years of age at the time of enrollment (regardless of gender)
3) Written consent for participation in the study
Key exclusion criteria
Patients meeting one of the following conditions will be excluded:
1) type 1 and secondary diabetes, 2) severe infectious disease, before or after surgery, and severe trauma, 3) events of myocardial infarction, angina pectoris, cerebral stroke, and cerebral infarction, 4) moderate or severe renal dysfunction (serum creatinine (mg/dL): male, 1.4<; female, 1.2<), 5) severe liver dysfunction (AST: 100 IU/l or higher), 6) moderate or severe heart failure) (NYHA/New York Heart Association stage III or severer), 7) under treatment with an EPA preparation at the time of study initiation, 8) pregnant, lactating, and possibly pregnant women and those planning to become pregnant, 9) patients with bleeding (hemophilia, gastrointestinal ulceration, urinary tract bleeding, hemoptysis, vitreous hemorrhage, etc.), 10) past medical history of hypersensitivity to investigational drugs, 11) judged as ineligible by clinical investigators.
Target sample size
44
Research contact person
Name of lead principal investigator
| 1st name | |
| Middle name | |
| Last name | Taka-aki Matsuoka |
Organization
Osaka University Graduate School of Medicine
Division name
Department of Metabolic Medicine
Zip code
Address
2-2 Yamadaoka, Suita, Osaka
TEL
06-6879-3743
matsuoka@endmet.med.osaka-u.ac.jp
Public contact
Name of contact person
| 1st name | |
| Middle name | |
| Last name | Naoto Katakami |
Organization
Osaka University Graduate School of Medicine
Division name
Department of Metabolic Medicine
Zip code
Address
2-2 Yamadaoka, Suita, Osaka
TEL
06-6879-3743
Homepage URL
katakami@endmet.med.osaka-u.ac.jp
Sponsor or person
Institute
Osaka University Graduate School
Institute
Department
Personal name
Funding Source
Organization
none
Organization
Division
Category of Funding Organization
Self funding
Nationality of Funding Organization
Other related organizations
Co-sponsor
Name of secondary funder(s)
IRB Contact (For public release)
Organization
Address
Tel
Secondary IDs
Secondary IDs
NO
Study ID_1
Org. issuing International ID_1
Study ID_2
Org. issuing International ID_2
IND to MHLW
Institutions
Institutions
大阪大学医学部附属病院
Other administrative information
Date of disclosure of the study information
| 2012 | Year | 04 | Month | 25 | Day |
Related information
URL releasing protocol
Publication of results
Unpublished
Result
URL related to results and publications
Number of participants that the trial has enrolled
Results
Results date posted
Results Delayed
Results Delay Reason
Date of the first journal publication of results
Baseline Characteristics
Participant flow
Adverse events
Outcome measures
Plan to share IPD
IPD sharing Plan description
Progress
Recruitment status
Terminated
Date of protocol fixation
| 2012 | Year | 01 | Month | 30 | Day |
Date of IRB
Anticipated trial start date
| 2012 | Year | 02 | Month | 01 | Day |
Last follow-up date
| 2014 | Year | 11 | Month | 06 | Day |
Date of closure to data entry
Date trial data considered complete
Date analysis concluded
Other
Other related information
Management information
Registered date
| 2012 | Year | 04 | Month | 25 | Day |
Last modified on
| 2015 | Year | 04 | Month | 27 | Day |
Link to view the page
Value
https://center6.umin.ac.jp/cgi-open-bin/ctr_e/ctr_view.cgi?recptno=R000007665
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