UMIN-CTR Clinical Trial
| Unique ID issued by UMIN | UMIN000004582 |
|---|---|
| Receipt number | R000005474 |
| Scientific Title | A Comparative Study of Insulin Secretagogue (SU Agent) and Insulin sensitizers (TZD) |
| Date of disclosure of the study information | 2010/11/18 |
| Last modified on | 2010/11/18 12:01:48 |
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Basic information
Public title
A Comparative Study of Insulin Secretagogue
(SU Agent) and Insulin sensitizers (TZD)
Acronym
Sulfonylurea vs Glitazone for HbA1c Reduction (SUGAR study)
Scientific Title
A Comparative Study of Insulin Secretagogue
(SU Agent) and Insulin sensitizers (TZD)
Scientific Title:Acronym
Sulfonylurea vs Glitazone for HbA1c Reduction (SUGAR study)
Region
| Japan |
Condition
Condition
Type2 diabetes
Classification by specialty
| Endocrinology and Metabolism |
Classification by malignancy
Others
Genomic information
NO
Objectives
Narrative objectives1
To evaluate the effect of monotherapy with an insulin secretagogue (SU agent) or insulin sensitizers (TZD) on blood glucose (BG) control in patients with type 2 diabetes mellitus (DM) in whom the BG level is not well controlled only with diet and exercise.
Basic objectives2
Efficacy
Basic objectives -Others
Trial characteristics_1
Trial characteristics_2
Developmental phase
Assessment
Primary outcomes
The rate for achieving the HbA1c level of < 6.5% at Month 6
Key secondary outcomes
Secondary endpoints in Step 1
1)Change in the HbA1c level at Month 6.
2)Changes in the FPG level, fasting insulin level, lipid metabolism, body weight, BMI, blood pressure and BNP at Month 6.
Secondary endpoints in Step 2
1)The rate for achieving the HbA1c level of 6.5% in the total subjects in each randomized group in Step 1.
2)The rates for achieving the target HbA1c level in the monotherapy groups.
3)Change in the HbA1c level in the monotherapy groups.
4)Changes in the FPG level, fasting insulin level, lipid metabolism, body weight, BMI, blood pressure and BNP at Month 12.5.
5)Changes in the dose of the drug and the HbA1c level.
6)Medical economic evaluation (medical expenses, new expenses for treatment and tests/ examinations required at the onset of adverse reactions, drugs necessary for lowering the HbA1c level by 1%, and drugs and medical care necessary for improving the DTSQ score by 1 point).
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
[Step 1]
The assigned study drug will be administered alone.
Insulin secretagogue (SU agent)
Treatment with the insulin secretagogue should be started at a half of the usual dose when the HbA1c level just before administration is  6.5% to < 7.0%, and at the usual dose when the HbA1c level is  7.0% to < 10.0%. Thereafter, the dose should be adjusted as necessary for achieving the morning FPG level of < 120 mg/dL.
[Step 2]
Combination therapy will be started or monotherapy will be continued according to the directions in Table 1 taking account of an evaluation of the HbA1c level at Month 6 and the dose level of the study drug. The treatment method is as follows: The maximum doses of the insulin secretagogue (SU agent) and insulin sensitizer (TZD) are the same as those specified for Step 1.
(1)When monotherapy with the insulin secretagogue (SU agent) is continued
The dose should be adjusted for achieving the morning FPG level of < 120 mg/dL.
If the subjects do not achieve the HbA1c < 6.5% after reaching the maximum dose during the treatment period, coadministration with the insulin sensitizer (TZD) should be started as in Item (2).
(2)When the insulin secretagogue (SU agent) is combined with the insulin sensitizer (TZD)
The dose of the insulin sensitizer (TZD) should be adjusted for achieving the morning FPG level of < 120 mg/dL.
Interventions/Control_2
[Step 1]
The assigned study drug will be administered alone.
Insulin sensitizer (TZD)
The doses of pioglitazone should be as follows: 15 mg/day as the starting dose, 30 mg/day as the usual dose, 45 mg/day as the maximum dose for men, and 30 mg/day as the maximum dose for women.
The dose should be adjusted for achieving the morning FPG level of < 120 mg/dL.
[Step 2]
Combination therapy will be started or monotherapy will be continued according to the directions in Table 1 taking account of an evaluation of the HbA1c level at Month 6 and the dose level of the study drug. The treatment method is as follows: The maximum doses of the insulin secretagogue (SU agent) and insulin sensitizer (TZD) are the same as those specified for Step 1.
(1)When the insulin sensitizer (TZD) is combined with the insulin secretagogue (SU agent)
The dose of the insulin secretagogue (SU agent) should be adjusted for achieving the morning FPG level of < 120 mg/dL.
(2)When monotherapy with the insulin sensitizer (TZD) is continued
The dose should be adjusted for achieving the morning FPG level of < 120 mg/dL.
If the subjects do not achieve the HbA1c level of < 6.5% after reaching the maximum dose during the treatment period, coadministration with the insulin secretagogue should be started as in Item (1).
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
| 30 | years-old | <= |
Age-upper limit
| 73 | years-old | > |
Gender
Male and Female
Key inclusion criteria
At preliminary registration
(1)Being treated only with dietary management and/or therapeutic exercise.
(2)HbA1c >= 6.5% to < 10.0% at preliminary registration.
(3)Age at treatment initiation:
30 to 73 years*
(4)Sex: Male and female
(5)Inpatient or outpatient
(6)Being capable of providing informed consent to participate in the study, reading the informed consent document and understanding its contents.
At formal registration
(1)Being treated only with diet and exercise.
(2)HbA1c >= 6.5% to < 10.0% at formal registration
(3)A < 1.0% difference in HbA1c from the level at preliminary registration.
Key exclusion criteria
At preliminary registration
(1)Type 1 DM
(2)The use of insulin preparations or oral hypoglycemic agents (including a-GI) within 4 weeks prior to the start of observation period.
(3)Cardiac failure at present or in the past
(4)Concurrent serious cardiac, renal, hepatic, pancreatic or blood disease.
(5)Women who are pregnant, wishing to become pregnant, or lactating.
(6)Excessive alcohol drinking.
(7)Past history of drug allergies.
(8)Those who are participating in other clinical studies (excluding epidemiological studies).
(9)Those who are determined inappropriate for the study by the investigator.
At formal registration
(1)The use of insulin preparations or oral hypoglycemic agents (including a-GI) within 4 weeks prior to the start of observation period.
(2)Cardiac failure at present or in the past
(3)Concurrent serious cardiac, renal, hepatic, pancreatic or blood disease.
(4)Women who are pregnant, wishing to become pregnant, or lactating.
(5)Excessive alcohol drinking.
(6)Past history of drug allergies.
(7)Those who are participating in other clinical studies (excluding epidemiological studies).
(8)Those who are determined inappropriate for the study by the investigator.
Target sample size
200
Research contact person
Name of lead principal investigator
| 1st name | |
| Middle name | |
| Last name | Masashi Kitaoka |
Organization
Japan Association for Diabetes Education and Care
Division name
Academic Committee
Zip code
Address
4-2-1 Kojimachi Chiyoda-ku Tokyo
TEL
Public contact
Name of contact person
| 1st name | |
| Middle name | |
| Last name | Nobuyuki Shihara |
Organization
Japan Association for Diabetes Education and Care
Division name
secretariat
Zip code
Address
4-2-1 Kojimachi Chiyoda-ku Tokyo
TEL
03-3514-1721
Homepage URL
http://www.nittokyo.or.jp/chousakenkyu_10001.html
shihara@nittokyo.or.jp
Sponsor or person
Institute
Japan Association for Diabetes Education and Care
Institute
Department
Personal name
Funding Source
Organization
Sanofi Aventis
Organization
Division
Category of Funding Organization
Profit organization
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
Other administrative information
Date of disclosure of the study information
| 2010 | Year | 11 | Month | 18 | 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
Completed
Date of protocol fixation
| 2007 | Year | 07 | Month | 13 | Day |
Date of IRB
Anticipated trial start date
| 2007 | Year | 09 | Month | 01 | Day |
Last follow-up date
| 2010 | Year | 01 | Month | 01 | Day |
Date of closure to data entry
| 2010 | Year | 02 | Month | 01 | Day |
Date trial data considered complete
| 2010 | Year | 03 | Month | 01 | Day |
Date analysis concluded
| 2010 | Year | 09 | Month | 01 | Day |
Other
Other related information
Management information
Registered date
| 2010 | Year | 11 | Month | 18 | Day |
Last modified on
| 2010 | Year | 11 | Month | 18 | Day |
Link to view the page
Value
https://center6.umin.ac.jp/cgi-open-bin/ctr_e/ctr_view.cgi?recptno=R000005474
