A Prospective, Single-center, Open-label, Single-arm Clinical Study to Evaluate the Safety and Efficacy of a Single Intravenous Infusion of LY-M001 Injection in Pediatric and Adolescent Patients With Type 1 Gaucher Disease
Overview
- Phase
- Early Phase 1
- Intervention
- LY-M001
- Conditions
- Gaucher Disease
- Sponsor
- Shanghai Jiao Tong University School of Medicine
- Enrollment
- 9
- Locations
- 1
- Primary Endpoint
- Incidence of adverse events (AE) and serious adverse events (SAE) within 52 weeks after LY-M001 infusion
- Status
- Active, Not Recruiting
- Last Updated
- 2 months ago
Overview
Brief Summary
The purpose of this study was to evaluate the safety, tolerability, efficacy, immunogenicity, PD and PK characteristics of LY-M001 injection in children with GD1 aged 6 years ≤ age < 18 years. This study mainly includes the main study stage and the long-term follow-up study stage.
Detailed Description
The study planned to enroll 6-9 patients with GD1 for 5 years, with a total of 34 follow-up visits. The main study period was 52 weeks, and the long-term follow-up period was 53 weeks to 5 years after administration. In this study, three dose groups were preset, and the first subject was enrolled with 1.0× 10\^13 vg/kg as the initial dose (the first dose group). After the safety was determined by DLT observation, subsequent subjects were enrolled. Based on safety and efficacy data, it will be decided by SRC discussion to increase to the next dose group. This is an open clinical study without blindness.
Investigators
Xiumin Wang, PhD
Director
Shanghai Jiao Tong University School of Medicine
Eligibility Criteria
Inclusion Criteria
- •The subject and/or parent, caregiver, or legal representative must be willing and able to provide written informed consent/consent for the study in accordance with applicable regulations and guidelines and comply with all study access and procedures, including the use of any data collection devices that can be used to directly record participant data.
- •Gender is not limited, 6 years old ≤ 18 years old.
- •Patients with double allele mutation of glucocerebrosidase gene (GBA1) and decreased glucocerebrosidase activity were confirmed by laboratory tests and met the clinical manifestations of type I Gaucher disease.
- •Subjects were newly treated or treated patients with type I Gaucher disease; For patients treated with enzyme replacement therapy (ERT) or substrate clearance therapy (SRT) before screening, 5 drug half-lives are required before administration.
- •The subject is willing to participate in all study follow-up and comply with all study procedures and evaluations.
- •The subject must be willing to refrain from donating blood, organs, tissues, or cells at any time after receiving treatment.
- •Pregnant Women (WOCBP) subjects tested negative for pregnancy.
Exclusion Criteria
- •Positive AAV8 neutralizing antibody (antibody titer \> 1:10).
- •Patients with type II or III Gaucher disease (GD2 or GD3), or with suspected Gaucher disease as assessed by the investigator (e.g., subjects with Gaucher disease-related central nervous system manifestations or abnormal electroencephalogram \[EEG\] examination).
- •Active and progressive bone diseases that are expected to require surgical treatment within the next 6 months.
- •The subjects were judged by the investigator to have idiopathic thrombocytopenic purpura (ITP), thrombotic thrombocytopenic purpura (TTP), thrombocytopenia, anemia, hepatomeglia, splenomeglia, and/or osteoporosis unrelated to GD (bone mineral density z-score ±2).
- •Treatment with an investigational drug in another clinical study within 28 days prior to screening or 5 half-lives, whichever is older.
- •Evidence of a history of clinically significant liver disease or hepatotoxin exposure that meets, but is not limited to, any of the following at the time of screening:
- •① Progressive hepatomegaly larger than 3 times the normal volume;
- •② History of stage 2 or above hepatic fibrosis;
- •③ AST, ALT, or TBIL were 1.5 times higher than the upper limit of normal (ULN);
- •④ Immune hepatitis;
Arms & Interventions
LY-M001 Backdose
Participants receive a single, peripheral intravenous (IV) infusion of LY-M001 at backdose.
Intervention: LY-M001
LY-M001 Dose group 1
Participants receive a single, peripheral intravenous (IV) infusion of LY-M001 at dose group 1.
Intervention: LY-M001
LY-M001 Dose group 2
Participants receive a single, peripheral intravenous (IV) infusion of LY-M001 at dose group 2.
Intervention: LY-M001
Outcomes
Primary Outcomes
Incidence of adverse events (AE) and serious adverse events (SAE) within 52 weeks after LY-M001 infusion
Time Frame: Within 52 weeks of infusion
Number of participants with treatment-related adverse events as assessed by CTCAE v5.0.
Incidence rate of dose-limiting toxicity (DLT) events determined by the data safety review committee (SRC) within at least 28 days after LY-M001 infusion
Time Frame: Within 52 weeks of infusion
Number of participants with treatment-related adverse events as assessed by CTCAE v5.0.The adverse events defined as dose-limiting toxicity (DLT) have been clearly specified in the protocol.
Liver function levels (including alanine aminotransferase [ALT], aspartate aminotransferase [AST], total bilirubin [TBIL], alkaline phosphatase [ALP], gamma-glutamyl transferase [GGT]) within 52 weeks after LY-M001 infusion.
Time Frame: Within 52 weeks of infusion
Incidence rate of liver function-related adverse events evaluated by CTCAE V5.0.
Secondary Outcomes
- Pharmacodynamics on blood glucocerebrosidase(Within 52 weeks of infusion)
- Pharmacodynamics on Blood glucosesphingosine(Within 52 weeks of infusion)
- Effectiveness of symptom improvement on Liver volume(Within 52 weeks of infusion)
- Effectiveness of symptom improvement on spleen volume(Within 52 weeks of infusion)
- Effectiveness of symptom improvement on Hemoglobin levels(Within 52 weeks of infusion)
- Effectiveness of symptom improvement on platelet counts(Within 52 weeks of infusion)
- Effectiveness of symptom improvement on bone mineral density (BMD) after administration(Within 52 weeks of infusion)
- Effectiveness of symptom improvement on bone marrow load (BMB) after administration(Within 52 weeks of infusion)
- Effectiveness of symptom improvement on GD patient Quality of Life scale score(Within 52 weeks of infusion)