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Active not recruitingPhase 2

Phase II Study Evaluating the Efficacy and Safety of DR10624 Injection in MASLD and MetALD Subjects

A Randomized, Double-blind, Placebo-controlled Phase II Clinical Study Evaluating the Efficacy and Safety of DR10624 Injection in Subjects at High Risk of Liver Fibrosis With Metabolic Dysfunction-associated Steatotic Liver Disease and Metabolic Dysfunction and Alcohol Associated Steatotic Liver Disease

Asset

DR10624

Subcutaneous · GLP-1 / glucagon / FGF21 triple

Listed sites

4

Recruiting sites

Enrollment

110

estimated

Study population

MASH / NAFLD / liver fibrosis, Obesity / overweight

Key I/E criterion

BMI 25-40

Primary endpoint

Changes of LFC

Footprint

Where this trial recruits

Site locations as reported to ClinicalTrials.gov. Site count is not enrollment count; per-site enrollment is not available from source.

Identifiers

Registered as

NCT IDNCT07024212
Org study IDDR10624-202

Timeline

Milestones

Study start2025-04-22actual
Study first posted2025-06-17actual
Last update posted2026-01-29actual
Primary completion2026-05-30estimated
Study completion2026-08-30estimated

Assets

Investigational agents

Study populations

Who this study enrolls

MASH / NAFLD / liver fibrosisObesity / overweight

Eligibility

Who can enroll

Minimum age18 Years
Maximum age75 Years
SexAll
Healthy volunteersNot accepted

Inclusion criteria

1. Subjects who have signed the informed consent form before the trial, and fully understood the trial content, process and possible adverse reactions;

2. Males or females aged 18-75 years (inclusive) at the time of signing the informed consent form;

3. LFC ≥ 10% assessed by MRI-PDFF (MRI-PDFF results that are obtained at the study site within 6 weeks prior to randomization are acceptable);

4. Screening FibroScan® with liver stiffness (LSM): ≥ 8 Kpa, and < 15 Kpa;

5. Have a body mass index (BMI) between 25.0 and 40.0 kg/m2 (inclusive) at screening;

6. Less than 5% change in body weight within 6 months prior to randomization;

7. If there is a history of type 2 diabetes, a stable treatment regimen must be maintained for at least 12 weeks prior to screening;

8. Females of childbearing potential and males must agree to use effective contraception during the study and for a specified period after the last dose of the investigational medicinal product (2 months for females, 3 months for males).

Exclusion criteria

1. Presence of cirrhosis on liver biopsy or imaging results, or have a history of cirrhosis;

2. Other causes of liver disease based on medical history and/or laboratory tests;

3. Previous (within 5 years before randomization) or planned (during the study period) obesity treatment with metabolic surgery or device-based therapy subjects with reversible weight-loss devices removed more than 12 months prior to randomization are eligible;

4. Type 1 diabetes;

5. History of malignancies within the last 5 years prior to screening, or malignancies that occurred more than 5 years ago but which are still currently active. Local squamous cell carcinoma of the skin or cervical intraepithelial neoplasia that has been cured without signs of recurrence is acceptable;

6. Presence of severe or uncontrolled underlying disease that, in the opinion of the investigator, renders the subject unsuitable for treatment with the investigational medicinal product or unable to complete study, or is likely to interfere with the evaluation of study results;

7. Subjects who have a history of bone trauma, fracture, or bone surgery within 2 months prior to screening, or concomitant bone disorders such as osteomalacia or known, untreated severe vitamin D deficiency (serum 25-hydroxyvitamin D ≤5 ng/mL); or a T-score ≤-2.5 for bone mineral density measured by DXA in the axial skeleton (lumbar vertebrae 1-4, femur neck, or total hip);

8. Subjects who have a history of medullary thyroid carcinoma, multiple endocrine neoplasia type 2, or a related family history;

9. Any significant abnormal laboratory findings from screening to randomization;

10. Subjects who have used or plan to use the following medications that may cause steatosis/steatohepatitis cumulatively for ≥4 weeks within 24 weeks prior to randomization or during the study: amiodarone, methotrexate, systemic corticosteroids (dose >5 mg/day prednisone equivalent), estrogens (dose greater than that used for hormone replacement therapy or contraception), tetracyclines, tamoxifen, anabolic steroids, valproic acid, or other drugs known to have hepatotoxicity, etc.;

11. Use of any of the following medications cumulatively for ≥4 weeks within 24 weeks prior to randomization or planned during the study: high-dose vitamin E (daily dose >400 IU), obeticholic acid, pioglitazone, berberine, or thyroid hormones (subjects with hypothyroidism who have received stable replacement therapy for at least 3 months prior to randomization are acceptable), etc.;

12. Use of antidiabetic drugs other than metformin, sulfonylureas, alpha-glucosidase inhibitors, glucokinase activators (GKA), or sodium-glucose cotransporter 2 (SGLT-2) inhibitors within 12 weeks prior to screening or planned during the study;

13. Use of Schisandra preparations (e.g., bifendate, bicyclol) within 6 weeks prior to randomization, or use of the following hepatoprotective drugs (including but not limited to reduced glutathione, glucuronolactone, glycyrrhizic acid preparations, polyene phosphatidylcholine, ursodeoxycholic acid, nicotinamide, liver-protecting tablets, silymarin, etc.) or other hepatoprotective Chinese proprietary medicines or health products within 2 weeks prior to randomization; or planned use of such drugs during the study;

14. Use of weight-loss drugs such as orlistat or GLP-1 receptor agonists, or other drugs with the same target as the investigational medicinal product [e.g., fibroblast growth factor-21 (FGF21) analogs, glucagon receptor (GCGR) agonists, etc.], within 6 weeks prior to screening or planned during the study;

15. Use of anti-tumor necrosis factor α (TNF-α) drugs, such as adalimumab or etanercept, etc., within 6 weeks prior to screening or planned during the study;

16. Known or suspected intolerance or hypersensitivity to the investigational medicinal product or any of its excipients; or known intolerance or hypersensitivity to drugs with the same target (e.g., FGF21 analogs, GLP-1 receptor agonists, GCGR agonists, etc.);

17. Subjects who have participated in clinical trials of other drugs and used investigational medicinal product within 12 weeks or 5 half-lives (whichever is longer) prior to screening, or those who have participated in medical device or vaccine clinical trials;

18. Alcohol consumption for at least 12 consecutive weeks within 1 year prior to screening, defined as any of the following: > 210 grams of ethanol per week for males on average, > 140 grams per week for females on average;

19. History of drug abuse or use of illicit drugs within 3 years prior to screening;

20. Pregnant or breastfeeding females, or females with a positive serum pregnancy test prior to randomization;

21. Subjects who, in the investigator's opinion, are otherwise not suitable for participation in this clinical trial.

Endpoints (19)

What's being measured

Protocol endpoints and posted registry outcome measures, grouped into outcome categories. Composite endpoints show their component event types. Standard codes (LOINC, SNOMED CT) are shown where available.

Coverage by outcome category

Other (unclassified)
7
MASH / liver
4
Weight & body composition
3
Safety / tolerability / PK
3
Glycemic / diabetes
1
Cardiometabolic biomarkers
1

Weight & body composition

3 endpoints
Secondary/protocol endpoint

Changes of body weight

Time frame:From baseline to Week 16

descriptive

Secondary/protocol endpoint

Changes of BMI

Time frame:From baseline to Week 16

descriptive

Secondary/protocol endpoint

Changes of waist-to-hip ratio

Time frame:From baseline to Week 16

ratio, improvement

Glycemic / diabetes

1 endpoint
Secondary/protocol endpoint

Changes of glucose metabolism-related parameters

Time frame:From baseline to Week 12

descriptive

MASH / liver

4 endpoints
Secondary/protocol endpoint

Changes of Liver Stiffness Measurement (LSM)

Time frame:From baseline to Week 12

descriptive

Secondary/protocol endpoint

Proportion of subjects with ≥17 U/L reduction of ALT

Time frame:From baseline to week 16

threshold achievement, improvement

Secondary/protocol endpoint

Changes of fibrosis biomarkers

Time frame:From Baseline to Week 12

descriptive

Secondary/protocol endpoint

Changes of hepatic inflammation markers

Time frame:From baseline to week 12

descriptive

Cardiometabolic biomarkers

1 endpoint
Secondary/protocol endpoint

Changes of lipid profiles

Time frame:From baseline to Week 16

descriptive

Safety / tolerability / PK

3 endpoints
Secondary/protocol endpoint

Analysis of Safety Endpoints

Time frame:From baseline to week 16

descriptive

Secondary/protocol endpoint

Immunogenicity analysis

Time frame:From baseline to Week 16

descriptive

Secondary/protocol endpoint

Pharmacokinetics profiles of DR10624 Injection

Time frame:From baseline to Week 12

descriptive

Other (unclassified)

7 endpoints
Primary/protocol endpoint/low confidence

Changes of LFC

Time frame:From baseline to Week 12

descriptive

Secondary/protocol endpoint/low confidence

Changes of Controlled Attenuation Parameter (CAP)

Time frame:From baseline to Week 12

descriptive

Secondary/protocol endpoint/low confidence

Changes of LFC

Time frame:From baseline to Week 12

descriptive

Secondary/protocol endpoint/low confidence

Proportion of subjects achieving a relative reduction of LFC

Time frame:From baseline to Week 12

threshold achievement, improvement

Secondary/protocol endpoint/low confidence

Proportion of subjects with LFC <5%

Time frame:From baseline to Week 12

threshold achievement, improvement

Secondary/protocol endpoint/low confidence

Changes of liver enzymes

Time frame:From baseline to Week 16

descriptive

Secondary/protocol endpoint/low confidence

Changes of hip circumference

Time frame:From baseline to Week 16

descriptive

Provenance

Sources

Trial identity, design, statusClinicalTrials.gov API v2
Snapshot dateJuly 1, 2026
Endpoint classificationDelfa endpoint taxonomy v2 (May 13, 2026)
Results tableno registry results posted yet

Trial facts come from public ClinicalTrials.gov records. Endpoint categories are Delfa's classification of those records, not a ClinicalTrials.gov field. All figures reflect the July 1, 2026 snapshot.