UMIN-CTR Clinical Trial
| Unique ID issued by UMIN | UMIN000029975 |
|---|---|
| Receipt number | R000034211 |
| Scientific Title | Effect of SGLT2 inhibitor (Lusefi) on diabetic nephropathy Stratified analysis based on different original renal function category |
| Date of disclosure of the study information | 2018/01/04 |
| Last modified on | 2023/04/07 10:44:44 |
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Basic information
Public title
Effect of SGLT2 inhibitor (Lusefi) on diabetic nephropathy
Stratified analysis based on different original renal function category
Acronym
CHAT-Lu
Scientific Title
Effect of SGLT2 inhibitor (Lusefi) on diabetic nephropathy
Stratified analysis based on different original renal function category
Scientific Title:Acronym
CHAT-Lu
Region
| Japan |
Condition
Condition
Type 2 diabetes mellitus
Classification by specialty
| Endocrinology and Metabolism |
Classification by malignancy
Others
Genomic information
NO
Objectives
Narrative objectives1
Long term time course effect of SGLT2 inhibitor (Lusefi) on renal function (eGFR)
Basic objectives2
Efficacy
Basic objectives -Others
Trial characteristics_1
Trial characteristics_2
Developmental phase
Assessment
Primary outcomes
Renal function at 104th week post SGLT2 inhibitor treatment
Stratified analysis based on different original renal function category
Key secondary outcomes
Base
Study type
Interventional
Study design
Basic design
Single arm
Randomization
Non-randomized
Randomization unit
Blinding
Open -no one is blinded
Control
Uncontrolled
Stratification
Dynamic allocation
Institution consideration
Blocking
Concealment
Intervention
No. of arms
1
Purpose of intervention
Treatment
Type of intervention
| Medicine |
Interventions/Control_1
Oral treatment of SGLT2 inhibitor(Lusefi)2.5mg once a day for 104 weeks
Interventions/Control_2
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
| Not applicable |
Gender
Male and Female
Key inclusion criteria
Type 2 diabetes mellitus(HbA1c 6.5%<=)
pre eGFR(30-90ml/min/1.73m2)
age 20 years old <=
Key exclusion criteria
past use of SGLT2 inhibitor
severe ketoacidosis,diabetes coma,type1diabetes
severe infection,pre and post operation,severe in injury
pregnancy,lactation,potential pregnancy
Target sample size
100
Research contact person
Name of lead principal investigator
| 1st name | Hidenori |
| Middle name | |
| Last name | Urata |
Organization
Fukuoka University Chikushi Hospital
Division name
Cardiovascular internal medicine
Zip code
8188502
Address
1-1-1,Zokumyoin,Chikushino Fukuoka
TEL
092-921-1011
uratah@fukuoka-u.ac.jp
Public contact
Name of contact person
| 1st name | Hidenori |
| Middle name | |
| Last name | Urata |
Organization
Fukuoka University Chikushi Hospital
Division name
Cardiovascular internal medicine
Zip code
8188502
Address
1-1-1,Zokumyoin,Chikushino Fukuoka
TEL
092-921-1011
Homepage URL
uratah@fukuoka-u.ac.jp
Sponsor or person
Institute
Fukuoka University Chikushi Hospital
Institute
Department
Personal name
Funding Source
Organization
Tisho Toyama Pharmaceutical co,Ltd
Organization
Division
Category of Funding Organization
Other
Nationality of Funding Organization
Other related organizations
Co-sponsor
Name of secondary funder(s)
IRB Contact (For public release)
Organization
Kyoto Prefectural University of Medicine, Clinical Research Review Board
Address
465 Kajii-cho, Kawaramachi-Hirokoji, Kamigyo-ku, Kyoto
Tel
0752515337
rinri@koto.kpu-m.ac.jp
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
| 2018 | Year | 01 | Month | 04 | Day |
Related information
URL releasing protocol
https://jrct.niph.go.jp
Publication of results
Published
Result
URL related to results and publications
https://jrct.niph.go.jp
Number of participants that the trial has enrolled
53
Results
There was no significant decrease in eGFR over 2 years, demonstrating renoprotective effects of luseogliflozin in patients with type 2 diabetes. Changes in eGFR were not correlated with changes in HbA1c. On the other hand, luseogliflozin had lesser renal protective effect in patients with overt proteinuria. In this study, blood sugar lowering effect, blood pressure lowering effect, liver function improving effect, and weight loss effect were also observed.
Results date posted
| 2023 | Year | 04 | Month | 07 | Day |
Results Delayed
Results Delay Reason
Date of the first journal publication of results
Baseline Characteristics
Luseogliflozin was administered to type 2diabetes mellitus patients who received written consent from the patient during outpatient visits to Fukuoka University Chikushi Hospital or to
the registered practitioners with the Chikushi Cardiovascular Clinical Research Network (Chikushi-JRN). From 3 April 2018 to 23 December 2019, 53 patients were enrolled at 5 sites and 46 patients who were able to continue Luseogliflozin up to 104 weeks were analyzed. The mean age was 66.2 years, 56.6% of men, and the mean duration of diabetes was 8.1 years. Averaged
BMI was 27, so that rather obesity patients were entered. As for complicated diseases, hypertension and dyslipidemia were found in about 60% of cases. DPP-4 inhibitors were the most common hypoglycemic drugs used at the start at 41.5%, followed by biguanides at 22.6%.
Participant flow
Due to the fact that it was a fairly late start of sales as an SGLT2 inhibitor and the delay in the start of case enrollment due to the overlap of this study at a time when it had to be performed as Specified Clinical Research, the case registration was sluggish and the target number of cases of 100 cases could not be reached, resulting in 53 cases being registered. Since this is a prospective clinical single-arm study without a control group, it proves the hypothesis that renal function does not decrease significantly after initiation of SGLT2 inhibitors.
Although the number of registered cases was about half, stratified analysis by renal function at the start of the study determined that it was possible to conclude and judge whether this
drug could be used for the purpose of maintaining renal function for at least 2 years even in the group with relatively low renal function. The recruitment ended during the scheduled recruitment period and was observed for 2 years. During that period, as shown in 9, a total of seven patients were canceled, including 3 cases of discontinuation due to disease outbreaks, 1 case of protocol dropout, 1 case of discontinuation due to transfer, and 2 cases of discontinuation due to no visit.
Adverse events
There were three cases of illness in total. There was one death, one worsening of HbA1c, and one stroke. There were no mild or serious adverse events attributable to the drug. The details are as follows.
Case 1: Death Death from malignant lymphoma not related to medication of the study.
Case 2: Worsening of HbA1c After receiving Luseoglifrogin, it was discontinued due to continued increase in Hba1c levels, despite good improvement in factors other than HbA1c. The cause is
unknown, and the causal relationship with the administered drug is not clear.
Case 3: Cerebral infarction There is no clinical report that the appearance of stroke in cases using SGLT-2 inhibitors decreases compared to the placebo group, and the cerebral infarction in this case is considered to be a spontaneous onset with a consistent course of occurrence. This case has a history of diabetes, dyslipidemia, and administration of
Luseoglifrogin has been started since April 5, 2019. At the start of treatment, HbA1 was 6.8%, blood pressure was normal, and other laboratory tests showed no renal dysfunction or dehydration except for a high triglyceride level of 252 mg/dL. The onset of cerebral infarction occurred on December 12, 2019, eight months after the start of Luseoglifrogin administration.
According to a report from a practicing physician, this case had a speech disorder and paralysis of the right lower limb when he woke up, so he was examined by a nearby brain surgeon and was transferred to a local core hospital with a diagnosis of cerebral infarction with JCS 1st degree. He showed hemiplegia including the right face and cerebral infarction in the left radiating crown at MRI. After that, the clinical findings improved and he was discharged, and after home treatment, he went to a nearby doctor who was a field doctor and is currently doing well. There are no data on the onset of cerebral infarction, and it is not clear whether dehydration occurred.
Outcome measures
There was no significant reduction in eGFR74.6ml/min/1.73m2 at the start, 74.4 plus orminus 21.5 ml/min/l. 73 m2 after 52 weeks, and75.8 plus or minus 20.8 ml/min/l. 73 m2 after 104 weeks compared to that at the start of treatment (n.s.). eGFR at start less than 60m1/min/ 1. 73 m2 was only 4 cases, and most of them were normal renal function. Stratified analysis of changes in eGFR with or without overt proteinuria showed that the changes in eGFR from the start at 52 weeks were those without the overt proteinuria (n=34, 0.6 ml/min/l. 73m2, 74.4 plus or minus 15.4
ml/min/l. 73m2 at the start) versus the overt proteinuria group (n = 7, -9.86 ml/min/l. 73m2, 74.0 plus or minus 7.9 ml/min/l. 73m2 at the start). It was significantly less compared to the
group without the overt proteinuria (p<0.01). The change in eGFR from the onset at week 104 was small without the overt proteinuria group (n=36), but did not reach to a significant difference (0.66 vs. overt proteinuria (+) group (n=6)), but did not reach to a significant difference (p=0.15). Changes in eGFR at 52 and 104 weeks were not correlated with initiation HbAIc or HbA1c decline. HbA1c at the start was 7.5%, significantly decreased at 52W and 104W (52W: 7.0%, 104W: 7.0%, p<0.01 vs. start, respectively). The weight reduction 52W was -3.6kg and this effect was maintained up to 104W. Diastolic blood pressure significantly decreased to 52W and 104W. Liver function improved significantly at 52W and 104W (p<0.01 vs. 0M, respectively) . lipid profile also
tended to be improved.
Plan to share IPD
IPD sharing Plan description
Progress
Recruitment status
Completed
Date of protocol fixation
| 2017 | Year | 06 | Month | 15 | Day |
Date of IRB
| 2017 | Year | 11 | Month | 17 | Day |
Anticipated trial start date
| 2018 | Year | 01 | Month | 04 | Day |
Last follow-up date
| 2022 | Year | 03 | Month | 31 | Day |
Date of closure to data entry
Date trial data considered complete
Date analysis concluded
Other
Other related information
Management information
Registered date
| 2017 | Year | 11 | Month | 15 | Day |
Last modified on
| 2023 | Year | 04 | Month | 07 | Day |
Link to view the page
Value
https://center6.umin.ac.jp/cgi-open-bin/ctr_e/ctr_view.cgi?recptno=R000034211
