bèta
Trial Radar AI
De klinische studie NCT06539624 voor Ziekte van Fabry is rekruterend. Bekijk de kaartweergave van de Klinische Studies Radar en de AI-ontdekkingstools voor alle details. Of stel hier een vraag.
Eén studie komt overeen met de filtercriteria
Kaartweergave
Terug naar zoekresultaten

Evaluate the Safety and Preliminary Efficacy of EXG110 in Subjects With Fabry Disease 12

Rekruterend
Informatie over klinische studies is voornamelijk in het Engels beschikbaar. Trial Radar AI kan echter helpen! Klik op 'Leg studie uit' om de informatie over de studie te bekijken en te bespreken in de taal van uw keuze.
De klinische studie NCT06539624 is een interventioneel studie bij Ziekte van Fabry met de status rekruterend. Het doel is om 12 deelnemers te includeren vanaf 16 oktober 2024. De studie wordt geleid door The Children's Hospital of Zhejiang University School of Medicine en de voltooiing is gepland op 9 april 2027. Laatste update op ClinicalTrials.gov: 27 februari 2026.
Beknopte samenvatting
Objective: To explore the safety and tolerability of different doses of EXG110 with Fabre disease
Uitgebreide beschrijving
An open-label, multicenter, single-arm, non-randomized, dose-escalation, and recommended dose-extension clinical design was used to evaluate the safety and efficacy of a single intravenous administration of different doses of EXG110 in patients
Officiële titel

A Multicenter, Non-randomized, Open-label, Dose-finding Study to Evaluate the Safety and Preliminary Efficacy of Gene Therapy With EXG110 in Subjects With Fabry Disease

Aandoeningen
Ziekte van Fabry
Andere studie-ID's
  • EXG110-011
NCT-ID
NCT06539624
Startdatum (Werkelijk)
2024-10-16
Laatste update geplaatst
2026-02-27
Verwachte einddatum
2027-04-09
Inschrijving (Geschat)
12
Studietype
Interventioneel
FASE
N.v.t.
Status
Rekruterend
Primaire doel
Behandeling
Toewijzing
Niet-gerandomiseerd
Interventiemodel
Sequentieel
Blindering
Geen (Open-label)
Armen / Interventies
Deelnemersgroep/StudiearmInterventie/Behandeling
ExperimenteelDose escalation-Cohort 1
Genetic : EXG110
EXG110 injection
EXG110 is a recombinant adeno-associated virus (rAAV) that not only significantly increases plasma AGA activity, but is also highly expressed in target organs such as the heart and kidneys.EXG110 will be administered in a single dose by intravenous infusion.
ExperimenteelDose escalation-Cohort 2
Genetic : EXG110
EXG110 injection
EXG110 is a recombinant adeno-associated virus (rAAV) that not only significantly increases plasma AGA activity, but is also highly expressed in target organs such as the heart and kidneys.EXG110 will be administered in a single dose by intravenous infusion.
ExperimenteelDose escalation-Cohort 3
Genetic : EXG110
EXG110 injection
EXG110 is a recombinant adeno-associated virus (rAAV) that not only significantly increases plasma AGA activity, but is also highly expressed in target organs such as the heart and kidneys.EXG110 will be administered in a single dose by intravenous infusion.
ExperimenteelDose escalation-Cohort 4
Genetic : EXG110
EXG110 injection
EXG110 is a recombinant adeno-associated virus (rAAV) that not only significantly increases plasma AGA activity, but is also highly expressed in target organs such as the heart and kidneys.EXG110 will be administered in a single dose by intravenous infusion.
Primaire uitkomst
UitkomstmaatBeschrijving van de uitkomstmaatTijdsbestek
Incidence and severity of adverse events
Safety and tolerability of EXG110 following a single IV dose, as assessed by incidence and severity of adverse events, serious adverse events and dose limiting toxicities, including clinically significant changes from baseline to scheduled time points in safety parameters
52 weeks following EXG110 administration
Secundaire uitkomst
UitkomstmaatBeschrijving van de uitkomstmaatTijdsbestek
eGFR change from baseline in mL/min/(1.73m^2);
eGFR change from baseline in mL/min/(1.73m\^2)
52 weeks following EXG110 administration
NYHA cardiac function grade changed from baseline;
NYHA cardiac function grade changed from baseline;
52 weeks following EXG110 administration
Changed from baseline: region and area in mm^2 of skin angiokeratoma The number of Gb3 deposition in skin biopsy under the microscope
Changed from baseline: region and area in mm\^2 of skin angiokeratoma The number of Gb3 deposition in skin biopsy under the microscope
52 weeks following EXG110 administration
Change from baseline in serum AGA activity
Change from baseline in serum AGA activity
52 weeks following EXG110 administration
Change from baseline serum lysoGb3
Change from baseline serum lysoGb3
52 weeks following EXG110 administration
Deelname-assistent
Geschiktheidscriteria

Leeftijd van deelnemers
Kind, Volwassene, Oudere volwassene
Minimumleeftijd
7 Years
Geslachten die in aanmerking komen voor de studie
Allen
  1. At the time of signing the informed consent, age ≥7, male or female
  2. Clinical symptoms (at least one Fabry disease related symptom) and genetic diagnosis of Fabry disease,
  3. Prior or no prior ERT treatment
  4. Have renal or cardiac involvement (adults only)
  5. All subjects of reproductive age voluntarily took effective contraception and prohibited sperm donation from entering the screening period until 52 weeks after dosing (main study period)
  6. The subjects voluntarily participate and are fully informed, fully understand the research, can comply with the requirements of the research protocol, and are willing to complete the research as planned, and voluntarily provide biological samples for testing according to the requirements of the protocol

  1. Screening period laboratory test results: a) aspartate aminotransferase or alanine aminotransferase > 1.5× upper limit of normal (ULN);b) Total bilirubin > 1.5× upper limit of normal (ULN);c) Alkaline phosphatase > 2× upper limit of normal (ULN);d) Albumin < lower limit of normal (LLN)
  2. There was a clinically significant increase in AFP during the screening period
  3. Serum virology test: a) Hepatitis B: Hepatitis B virus surface antigen (HBsAg) positive, and hepatitis B virus-deoxyribonucleic acid (HBV-DNA) higher than the upper limit of normal detection;b) Hepatitis C: if the hepatitis C virus (HCV) antibody is positive, and the hepatitis C virus-ribonucleic acid (HCV-RNA) is higher than the upper limit of normal test value;c) Syphilis: positive for syphilis screening (Tp-Ab) and positive for syphile-specific antibodies;d) HIV: Known human immunodeficiency virus (HIV) positive history or HIV screening positive
  4. AVT917 (>1:50), anti-AGA antibody positive(>1:2560)
  5. C3 lower than the normal range, C5b-9 higher than the normal range, anti-AVT917 IgM positive
  6. Current or have a history of serious cardiovascular disease and surgical history
  7. Current underlying liver disease or history of liver disease, as assessed by the investigator, that may affect the safety assessment of the drug
  8. Renal disease in adult and the slope of kidney >5 mL/min/1.73m²/year
  9. Subjects with poorly controlled diabetes after drug treatment (e.g., HbA1c≥8%);
  10. Acute/chronic infection or other chronic disease that the investigator determines will increase the risk of participants participating in the study
  11. Patients with a history of malignant tumor or currently suffering from any malignant tumor (except for the following tumor diseases: skin basal cell carcinoma, cervical carcinoma in situ, breast carcinoma in situ, skin squamous cell carcinoma has been controlled after treatment);
  12. Have malignancy cancer
  13. Patients with active autoimmune diseases (such as rheumatoid arthritis, systemic lupus erythematosus, multiple sclerosis, immune vasculitis, inflammatory bowel disease, etc.);
  14. known history of allergy to the components of the investigational products
  15. Patients with a history of drug use or drug abuse or alcoholism
  16. Use of systemic (intravenous or oral) immunomodulators within the past 6 months or currently
  17. Initiation of treatment with blood pressure lowering drugs that affect proteinuria levels (such as angiotensin-converting enzyme inhibitors, angiotensin-receptor blockers, or angiotensin-receptor/enkephalin inhibitors) within 4 weeks prior to screening, or changes in the therapeutic dose of these drugs within 4 weeks prior to screening;
  18. Has received, or is currently receiving, a clinical trial of another investigational drug/medical device or treatment (other than vitamins and minerals) within 3 months prior to signing the informed consent (or within 5 half-lives of the investigational drug, whichever is longer)
  19. Previous treatment with gene therapy products
  20. Those who had received live attenuated vaccine/vaccine within 12 weeks prior to screening or planned to receive it during the study
  21. Other clinical conditions that the investigators felt needed to be ruled out
The Children's Hospital of Zhejiang University School of Medicine logoThe Children's Hospital of Zhejiang University School of Medicine
Verantwoordelijke instantie
Mao Jianhua, Hoofdonderzoeker, Vice President of the hospital, The Children's Hospital of Zhejiang University School of Medicine
Centraal Contactpersoon
Contact: Jianhua Mao, PhD, 13516819071, [email protected]
2 Studielocaties in 1 landen

Shanghai Municipality

Shanghai Children's Medical Center, Shanghai, Shanghai Municipality, China
Lei Yin, PhD, Contact, 13641673203, [email protected]
Lei Yin, PhD, Hoofdonderzoeker
Rekruterend

Zhejiang

Children's Hospital, Zhejiang University School of Medicine, Hangzhou, Zhejiang, China
Mao Jianhua, MD, Contact, 13616819071, [email protected]
Rekruterend