- ICH GCP
- US Clinical Trials Registry
- Clinical Trial NCT06019936
A Randomized,Double-blind, Placebo Controlled, Multicenter Study to Evaluate the Safety and Efficacy of MT2004 Capsule in DILI Subjects
A Randomized,Double-blind, Placebo Controlled, Multicenter Study to Evaluate the Safety and Efficacy of MT2004 Capsule in Treatment of Cholestatic and Mixed Drug Induced Liver Injury (DILI)
The goal of this randomized, double-blind, placebo controlled, Multicenter Phase II clinical trial is to initially evaluate the Safety and Efficacy of MT2004 Capsule in Cholestatic and Mixed drug induced liver injury (DILI) subjects.
The main questions it aims to answer are:
- The Efficacy of MT2004 Capsule in Cholestatic and Mixed DILI subjects
- The Safety and Pharmacokinetic characteristic of MT2004 Capsule in Cholestatic and Mixed DILI subjects
- The mechanism of using MT2004 Capsule on Cholestatic and Mixed DILI subjects
Study Overview
Status
Intervention / Treatment
Detailed Description
Xi'An Aolitai Pharmaceutical Technology Co Ltd is developing MT2004, a novel investigational synthetic small molecule farnesoid X receptor (FXR) agonist targeted to the liver. The MT2004 was designed as the prodrug and the metabolites MT2004-met1 of MT2004 will act to the FXR receptor to regulate a series of genes expression. It also plays an important role in the metabolism of bile acids, lipids and sugars.
The goal of this randomized, double-blind, placebo controlled, Multicenter Phase II clinical trial is to initially evaluate the Safety and Efficacy of MT2004 Capsule in Cholestatic and Mixed drug induced liver injury (DILI) subjects. The whole study will be divied to three stages including screening period (14 Days before the treatment), treatment period (the participants will be randomized to receive MT2004, or placebo orally (BID), for 12 weeks) and follow-up period. The study aims to recruit total of 80 subjects with Cholestatic and Mixed DILI, in which 12 of subjects will be firstly enrolled and allocated to the MT2004 group (Dose level: 25mg) as well as control group with the proportion of 2:1 by using the stratified randomization method. During the whole study, the adjustment of the subjects amount, the dose level as well as randomization proportion will based on the decesion of Independent Data Monitoring Board (IDMC). The highest dose will not exceed the 50mg BID.
The placebo will be used in this study, and the researchers will compare the placebo and test article to see the safety and efficacy.
Study Type
Enrollment (Estimated)
Phase
- Phase 2
Contacts and Locations
Study Contact
- Name: LanLan Song, Master
- Phone Number: +8615929300901
- Email: songlanlan@micot.cn
Study Contact Backup
- Name: DeChuang Yuan, Master
- Email: yuandechuang@micot.cn
Study Locations
-
-
Shanghai
-
Shanghai, Shanghai, China, 200001
- Recruiting
- Shanghai Jiaotong University School of Medicine,Renji Hospital
-
Contact:
- YiMin Mao, Master
- Phone Number: +8613003175438
- Email: maoym@163.com
-
Principal Investigator:
- YiMin Mao, Master
-
-
Participation Criteria
Eligibility Criteria
Ages Eligible for Study
- Adult
- Older Adult
Accepts Healthy Volunteers
Description
Inclusion Criteria:
1. 18≤ age ≤ 75 years, male or female.
2. When diagnosis of acute DILI, the liver biochemical threshold of patients must meet one of the following criteria: :(1) ALT ≥5 ×ULN;(2) ALP ≥2× ULN;(3) ALT≥3× ULN and TBil ≥2×ULN.
3. ALP ≥2× ULN, and conform to the clinical classification of cholestatic type or mixed type DILI in the Chinese Guidelines for the Diagnosis and Treatment of Drug-induced Liver Injury (2023 edition) (cholestatic type: R value ≤2; Mixed type: 2<R value <5).
4. Excluded other common causes of acute liver injury, such as acute viral hepatitis A, B, C, E, autoimmune hepatitis, biliary tract disease, PBC, etc. (Exclusive diagnostic tests completed in our hospital or other hospitals after this suspected acute DILI event or within 2 months before screening were acceptable)
5. RUCAM causality scale score ≥6 points; If the RUCAM score is between the 3-5 it is necessary to evaluate the causal relationship by three experts according to the evaluation criteria of expert opinions in the Chinese Guidelines for the Diagnosis and Treatment of Drug-induced Liver Injury (2023 edition), and at least two experts determine that the liver injury of the patients are "likely", "very likely" or "definitely" caused by drugs.
6. The serious level of DILI is within level 1-2 based on the Chinese Guidelines for the Diagnosis and Treatment of Drug-induced Liver Injury (2023 edition).
7. The duration of this liver injury is less than 6 months.
8. The female with fertility must have had a negative pregnancy test results before being enrolled, or at least 1 year after pausimenia, or permanent sterilization ≥6 weeks(There should have a recording of hysterectomy, bilateral salpingo-oophorectomy). The female and their male partners with the fertility potential agree to utilize the effective contraceptive methods(the following two methods can be selected: 1. any of the condom, diaphragm, Sponge or Cervical Cap with with Spermicide ).
9. Fully understand the study process of the clinical trial, and provide the signed ICF of joinning the clinical trial.
Exclusion Criteria:
1. Acute or chronic liver failure or liver decompensation
2. The history of liver decompensation or portal hypertension history
3. Moderate or above renal insufficiency, creatinine clearance (Ccr) < 60mL/min (according to the MDRD formula).
4. Patients with serious diabetes and had poor control of blood sugar (HbA1c>10%)
5. Serious sysmetic diseases of cardiovascular, respiratory, neurological, urinary, digestive, and for any reason which, in the opinion of the Investigator think the subject is not suitable for participating in the study.
6. The predict survival period < 6 months.
7. Utilization of Perursodeoxycholic acid within 14 days before the treatment.
8. Utilization of S-adenosylmethionine within 1 days before the treatment.
9. The patients must regularly utilize the known strong CYP3A4/3A5 inhibitors such as Clarithromycin, Itraconazole, ketoconazole, Ritonavir, rifampicin, phenytoin, carbamazepine within 1 week before the treatment or for the whole study period.
10. Allergies or intolerances to study drug ingredients
11. Patients are under the gestation, lactation, or patients have the pregnancy planning during the study period and 90 days after the end of the clinical trial
12. Patients are not willing to ban the alcohol during the study period.
13. Patients had joined the other clinical trials within 3 months before the administration.
14. Other conditions that the investigator think the subject is not suitable for participating in the study.
Study Plan
How is the study designed?
Design Details
- Primary Purpose: Treatment
- Allocation: Randomized
- Interventional Model: Parallel Assignment
- Masking: Double
Arms and Interventions
Participant Group / Arm |
Intervention / Treatment |
---|---|
Experimental: MT2004 Capsule
The MT2004 Capsule will be orally used twice daily after meal for 12 weeks.
|
The stratified randomization method will be used in this study.
In treatment period, the participants will orally receive the MT2004 (BID) for 12 weeks with the dose level of 25mg.
The adjustment of the dose level will base on the decesion of Independent Data Monitoring Board (IDMC).
The highest dose will not exceed the 50mg BID.
Other Names:
|
Placebo Comparator: MT2004 Capsule Placebo
The MT2004 Capsule Placebo will be orally used twice daily after meal for 12 weeks.
|
The stratified randomization method will be used in this study.
In treatment period, the participants will orally receive the MT2004 Capsule Placebo (BID) for 12 weeks with the dose level of 25mg.
The adjustment of the dose level will base on the decesion of Independent Data Monitoring Board (IDMC).
The highest dose will not exceed the 50mg BID.
|
What is the study measuring?
Primary Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Primary efficacy endpoint
Time Frame: On the week 4 after the administration
|
The efficacy of MT2004 will be evaluated based on the decreasing rate on serum ALP compared to baseline.
|
On the week 4 after the administration
|
Secondary Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Secondary efficacy endpoint
Time Frame: On the week 2,8,12 after the administration and the week 4 follow-up period
|
The efficacy of MT2004 will be evaluated based on the decreasing rate on ALP compared to baseline.
|
On the week 2,8,12 after the administration and the week 4 follow-up period
|
Secondary efficacy endpoint
Time Frame: On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
The efficacy of MT2004 will be evaluated based on the percentage of patients whose ALP decreased by more than 15% from baseline.
|
On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
Secondary efficacy endpoint
Time Frame: On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
The efficacy of MT2004 will be evaluated based on the recovery rate of ALP.
|
On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
Secondary efficacy endpoint
Time Frame: On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
The efficacy of MT2004 will be evaluated based on the decreasing rate on GGT compared to baseline.
|
On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
Secondary efficacy endpoint
Time Frame: On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
The efficacy of MT2004 will be evaluated based on the recovery rate of GGT.
|
On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
Secondary efficacy endpoint
Time Frame: On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
The efficacy of MT2004 will be evaluated based on the decreasing rate on ALT compared to baseline.
|
On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
Secondary efficacy endpoint
Time Frame: On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
The efficacy of MT2004 will be evaluated based on the recovery rate of ALT.
|
On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
Secondary efficacy endpoint
Time Frame: On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
The efficacy of MT2004 will be evaluated based on the decreasing rate on AST compared to baseline.
|
On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
Secondary efficacy endpoint
Time Frame: On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
The efficacy of MT2004 will be evaluated based on the recovery rate of AST.
|
On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
Secondary efficacy endpoint
Time Frame: On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
The efficacy of MT2004 will be evaluated based on the decreasing rate on TBIL compared to baseline.
|
On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
Secondary efficacy endpoint
Time Frame: On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
The efficacy of MT2004 will be evaluated based on the decreasing rate on TBA compared to baseline.
|
On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
Secondary efficacy endpoint
Time Frame: On the week 2,4,8,12 after the administration
|
The efficacy of MT2004 will be evaluated based on the area of serum ALP decreasing rate-time curve.
|
On the week 2,4,8,12 after the administration
|
Secondary efficacy endpoint
Time Frame: On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
The efficacy of MT2004 will be evaluated based on the percentage of patients developed to DILI level 3-4 after the administration.
|
On the week 2,4,8,12 after the administration and the week 4 follow-up period
|
Other Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Safety endpoint
Time Frame: From the date of screening until the date of last follow-up visit or early termination and end of study, assessed up to 12 weeks.
|
Adverse Events(AEs) will be recorded and evaluated for their seriousness, severity, and relationship to the study drug.
|
From the date of screening until the date of last follow-up visit or early termination and end of study, assessed up to 12 weeks.
|
Collaborators and Investigators
Investigators
- Principal Investigator: YiMin Mao, Master, Shanghai Jiaotong University School of Medicine,Renji Hospital
Study record dates
Study Major Dates
Study Start (Actual)
Primary Completion (Estimated)
Study Completion (Estimated)
Study Registration Dates
First Submitted
First Submitted That Met QC Criteria
First Posted (Actual)
Study Record Updates
Last Update Posted (Actual)
Last Update Submitted That Met QC Criteria
Last Verified
More Information
Terms related to this study
Keywords
Additional Relevant MeSH Terms
Other Study ID Numbers
- MT2004-II-C01
- CTR20232066 (Other Identifier: Center For Drug Evaluation, NMPA)
Drug and device information, study documents
Studies a U.S. FDA-regulated drug product
Studies a U.S. FDA-regulated device product
This information was retrieved directly from the website clinicaltrials.gov without any changes. If you have any requests to change, remove or update your study details, please contact register@clinicaltrials.gov. As soon as a change is implemented on clinicaltrials.gov, this will be updated automatically on our website as well.
Clinical Trials on Drug-Induced Liver Injury
-
Kennon HeardMcNeil Consumer & Specialty Pharmaceuticals, a Division of McNeil-PPC, Inc.CompletedDrug Induced Liver InjuryUnited States
-
Korea Institute of Oriental MedicineDongGuk University; Korean Medicine Hospital of Pusan National University; Semyung... and other collaboratorsActive, not recruitingDrug Induced Liver Injury | Drug-Induced Kidney Injury | Herbal Medicine Adverse ReactionKorea, Republic of
-
Institute of Liver and Biliary Sciences, IndiaTerminatedDrug Induced Liver InjuryIndia
-
Beijing 302 HospitalUnknownDrug-Induced Liver InjuryChina
-
Beijing 302 HospitalUnknownDrug-Induced Liver InjuryChina
-
Beijing 302 HospitalUnknown
-
Beijing 302 HospitalCompletedDrug-induced Liver Injury,ChronicChina
-
University of Electronic Science and Technology...Chengdu Nuoen Biotechnologies, Inc.; Sichuan Cancer Hospital & InstituteUnknownComparative Study of Circulating microRNA Changes in Patients With Liver Injury and Healthy SubjectsLiver Failure | Drug-Induced Liver InjuryChina
-
Duke UniversityNational Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)RecruitingDrug Induced Liver InjuryUnited States
-
Beijing 302 HospitalUnknownDrug-Induced Liver InjuryChina
Clinical Trials on MT2004 Capsule
-
Xi'an Biocare Pharma Ltd.Completed
-
Quan JiangUnknown
-
Guizhou Bailing Group Pharmaceutical Co LtdWangjing Hospital, China Academy of Chinese Medical Sciences; The First Affiliated... and other collaboratorsUnknownKnee OsteoarthritisChina
-
Jonsson Comprehensive Cancer CenterWithdrawnAcute Graft Versus Host Disease | Gastrointestinal Tract Acute Graft Versus Host Disease | Severe Gastrointestinal Tract Acute Graft Versus Host Disease | Steroid Resistant Gastrointestinal Tract Acute Graft Versus Host DiseaseUnited States
-
Yung Shin Pharm. Ind. Co., Ltd.Changhua Christian HospitalCompletedHot Flashes | PMSTaiwan
-
Chipscreen Biosciences, Ltd.Not yet recruiting
-
Burapha UniversityCompletedAsparagus Capsule ConsumptionThailand
-
Vibrant Ltd.CompletedConstipationUnited States
-
Vibrant Ltd.UnknownConstipationUnited States
-
Hanmi Pharmaceutical Company LimitedUnknownChronic Obstructive Pulmonary Disease