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Trial registered on ANZCTR
Registration number
ACTRN12624000194561
Ethics application status
Approved
Date submitted
31/01/2024
Date registered
28/02/2024
Date last updated
21/07/2024
Date data sharing statement initially provided
28/02/2024
Type of registration
Prospectively registered
Titles & IDs
Public title
A Multiple Dose Study in Participants with Severe Alcohol-Associated Hepatitis to Assess the Safety and the Way the Body Absorbs, Distributes, and Eliminates the drug SZN-043.
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Scientific title
A Phase 1b Multiple Ascending Dose Study to Assess the Safety, Tolerability, and Pharmacokinetics of SZN-043 in Participants with Severe Alcohol-Associated Hepatitis
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Secondary ID [1]
311416
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CL-0043-1002
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Universal Trial Number (UTN)
U1111-1303-3987
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Trial acronym
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Linked study record
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Health condition
Health condition(s) or problem(s) studied:
Severe Alcohol-Associated Hepatitis
332697
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Condition category
Condition code
Oral and Gastrointestinal
329407
329407
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0
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Other diseases of the mouth, teeth, oesophagus, digestive system including liver and colon
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Intervention/exposure
Study type
Interventional
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Description of intervention(s) / exposure
SZN-043 is a is an antibody fusion protein that is an RSPO mimetic specifically targeted to hepatocytes through ASGR1 binding. SZN-043 will be administered via intravenous injection. Doses of 0.5mg/kg, 1.0mg/kg, and 1.5mg/kg are planned to be tested in 3 separate cohorts, twice within one week (Day 0, Day 4). The product is administered and observed by qualified staff in an in an inpatient setting. Optional cohorts are possible to test other doses and frequencies to be determined by review of available data. The frequency may increase to as much as 3x (Day 0, 4, and 7) or decrease. The determination of the frequency and of the exact dose will be made based on emerging safety data, PK data, and/or other indicators with respect to patient outcomes from the preceding cohorts. The maximum exposure will not exceed a dose equivalant of 3,0mg/kg.
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Intervention code [1]
327855
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Treatment: Drugs
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Comparator / control treatment
No control group.
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Control group
Uncontrolled
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Outcomes
Primary outcome [1]
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To evaluate the safety of MAD of SZN-043 in participants with severe alcohol-associated hepatitis.
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Assessment method [1]
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Safety at proposed doses will be assessed by monitoring adverse events reported by participants or staff as observed from analysis of blood samples, performance of ECGs, monitoring of vital signs and physical examination.
findings.
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Timepoint [1]
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Laboratory assessments are conducted from baseline and thereafter daily through Day 9, D11, D14, D18. D21, D28, d60, and D90.
Physical Examinations are conducted at baseline and at end of study.
Vital signs are monitored on days of dosing, as required on lab visit days, but at least at Day 7, Day 28, Day 60 and Day 90.
ECGs are conducted on days of dosing, and at end of study.
All adverse events, reported by participants and/or observed by clinical staff will reported through end of study participation.
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Primary outcome [2]
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To evaluate the Tolerability of MAD of SZN-043 in participants with severe alcohol-associated hepatitis
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Assessment method [2]
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Assessed through observation and subsequent report by staff and/or participant of adverse events related to the methods of administration. This includes monitoring of vital signs.
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Timepoint [2]
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Continual assessment from the start of dose through 4 hours post dose.
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Secondary outcome [1]
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To assess the change from baseline in alcohol-associated hepatitis disease progression within and across cohorts as measured by Model for End-Stage Liver Disease (MELD).
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Assessment method [1]
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Calculate MELD score from blood samples collected.
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Timepoint [1]
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Percent and absolute change in MELD score from baseline toDays 4, 7, 28, 60, and 90.
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Secondary outcome [2]
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To assess the change from baseline in functional measures of liver function within and across cohorts as measured by ALT.
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Assessment method [2]
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Percent and absolute change from baseline of ALT as measured from blood samples.
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Timepoint [2]
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Laboratory assessments are conducted from baseline and thereafter daily through Day 9, D11, D14, D18. D21, D28, d60, and D90.
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Secondary outcome [3]
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To characterize the PK of SZN-043
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Assessment method [3]
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Measure PK parameters after multiple doses of SZN-043, as data allow, including Cmax Maximum observed serum concentration, Clast Last measurable plasma concentration, Ctau Concentration at the end of the dosing interval, Tmax Time to maximum concentration, AUC0-last Area under the drug concentration-time curve, from time 0 to the last measurable concentration, AUCtau rea under the plasma concentration-time curve for a dosing interval, AUC0-inf Area under the drug concentration-time curve, from time 0 to infinity, CL Clearance, CLss Clearance at steady state, t½ Apparent terminal half-life, Kel Apparent terminal elimination rate constant, Vd Apparent volume of distribution, Vss Volume of distribution at steady state, Vz Volume of distribution in the terminal state, MRT Mean residence time, and Rac. Accumulation ratio.
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Timepoint [3]
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Measured from Day 0 (prior to dose) through Day 35, at least daily on Days 0 through Day 9, 11, 14, 21, 28, and end of study. Day 35 may be added if a dose on Day 7 is added based on the cohort design.
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Secondary outcome [4]
431123
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To evaluate immunogenicity (measured as ADA) to SZN-043
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Assessment method [4]
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Prevalence of ADA for SZN-043 at baseline and incidence of ADA during the study measured through collection of blood samples.
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Timepoint [4]
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Measured once Pre-Dose, and again on Day 14, 28, 60 and 90.
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Secondary outcome [5]
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To assess the change from baseline in functional measures of liver function
within and across cohorts as measured by AST.
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Assessment method [5]
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Percent and absolute change from baseline of AST as measured from blood samples.
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Timepoint [5]
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Laboratory assessments are conducted from baseline and thereafter daily through Day 9, D11, D14, D18. D21, D28, d60, and D90.
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Secondary outcome [6]
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To assess the change from baseline in functional measures of liver function within and across cohorts as measured by international normalised ratio (INR)
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Assessment method [6]
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Percent and absolute change from baseline of INR as measured from blood samples.
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Timepoint [6]
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Laboratory assessments are conducted from baseline and thereafter daily through Day 9, D11, D14, D18. D21, D28, d60, and D90.
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Secondary outcome [7]
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To assess the change from baseline in functional measures of liver function within and across cohorts as measured by albumin.
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Assessment method [7]
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Percent and absolute change from baseline of albumin as measured from blood samples.
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Timepoint [7]
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Laboratory assessments are conducted from baseline and thereafter daily through Day 9, D11, D14, D18. D21, D28, d60, and D90.
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Secondary outcome [8]
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To assess the change from baseline in alcohol-associated hepatitis disease progression within and across cohorts as measured by Lille Model for alcohol-associated hepatitis (Lille) score
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Assessment method [8]
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Calculate Lille Model Score as calculated from blood samples drawn on those days.
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Timepoint [8]
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Calculate Lille Model Score on Days 0, 4, and 7 to determine percent and absolute change from baseline to Days, 4 and 7 respectively, and percent of participants with Lille Model Score <0.45 at Days 4 and 7.
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Secondary outcome [9]
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To assess the change from baseline in alcohol-associated hepatitis disease progression within and across cohorts as measured by mortality.
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Assessment method [9]
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Collect reports received at any time on patient vital status (e.g. alive or not alive) from participant, medical records, publicly available information, and/or relations (e.g. physician, family).
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Timepoint [9]
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Calculate percent of participants alive at Days 28, 60, and 90
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Eligibility
Key inclusion criteria
1. Male or female (sex assigned at birth), 18 years of age or older AND considered to be an adult in accordance with local law.
2. BMI between 18.0 and 36.0 kg/m2, inclusive, at Screening.
3. A clinical diagnosis of AH that is anticipated to require inpatient care for a period to encompass at a minimum the first dose of study drug based on typical serum chemistry (as determined by local laboratory) meeting all of the following parameters:
a. Onset of jaundice within prior 8 weeks;
b. History of heavy alcohol abuse: >40 (female) or 60 (male) g alcohol/day for greater than or equal to 6 months;
c. Consumed alcohol within 8 weeks before study entry;
d. AST >50, AST/ALT >1.5, and both values are: <400 IU/L, and
e. Serum total bilirubin >3.0 mg/dL.
4. MELD score of 21 to 30, inclusive.
5. Willing to use acceptable methods of contraception or not physically able to conceive or impregnate others.
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Minimum age
18
Years
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Maximum age
No limit
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Sex
Both males and females
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Can healthy volunteers participate?
No
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Key exclusion criteria
1. Previous receipt of antibody or biologic therapy within the past 6 months
2. Treatment with any experimental drug within 30 days, or within 5 half-lives (whichever is longer), before Day 0 visit (Baseline).
3. Other causes of liver disease
4. Recent start of liver toxic medications
5. Have a portosystemic shunt or scheduled for transjugular intrahepatic portosystemic shunt placement or highly likely to receive a liver transplant during the study.
6. Dependent upon inotropic support (including selepressin or terlipressin) or ventilatory or vasopressor support.
7. Organ failure (as defined by hepatic encephalopathy >stage 3) or requires renal replacement therapy or creatinine >2.5 mg/dL (or 221 mmol/L).
8. Uncontrolled hyperthyroidism, history of Paget's disease, osteomalacia, or fracture within 4 weeks of Screening.
9. Uncontrolled bacterial infections, as determined by the investigator's judgment after a minimum of 2 days of antibiotic therapy.
10. History of a previous severe allergic reaction with generalised urticaria, angioedema, or anaphylaxis.
11. A QT duration corrected for heart rate by Fridericia's formula (QTcF) >450 msec for males and >470 msec for females based on either single or averaged QTcF values of triplicate ECGs before study drug administration.
12. A history of malignant neoplasm, evidence of recurrence of certain skin cancers, or under investigation for a malignancy.
13. Gastrointestinal (GI) bleeding within 2 days of Screening requiring transfusion of more than 3 units of blood.
14. Grade 3 or higher encephalopathy by West Haven Criteria.
15. Acute kidney injury defined as an increase in serum creatinine (sCr) greater than or equal to 0.3 mg/dL within 48 h or increase in sCr greater than or equal to 50% from baseline known or presumed
16. Presence of portal vein thrombosis.
17. Presence of acute pancreatitis.
18. Cerebral hemorrhage, extensive retinal hemorrhage, acute myocardial infarction (within
the last 6 weeks) or severe cardiac arrhythmias (not including atrial fibrillation).
19. Evidence of GI bleeding or renal failure after 7 days of treatment within 8 weeks of screening.
20. Liver imaging at screening showing any lesions (except benign lesions, i.e., hemangiomas).
21. Known infection with HIV or HIV Ab positive at screening .
22. Organ transplantation (such as liver, kidney, lung, heart, bone marrow, or stem cell etc.), other than cornea transplant.
23. Positive urine screen for amphetamines, cocaine, or non-prescribed opiates.
24. Pregnant or lactating at Screening or planning to become pregnant (self or partner) at any time during the study.
25. Planning to donate sperm (male) or ovum (female) within 90 days after the last dose of study drug.
26. Current use of anticoagulants that affect prothrombin time or international normalised ratio (INR).
27. Eligibility: All participants where HepQuant SHUNT test kit use is specified:
a. Extensive resection of large segments of small intestine (short gut) or severe
gastroparesis; On either a non-selective beta blocker or an angiotensin-converting
enzyme inhibitor or angiotensin II receptor blockers who are unwilling or unable
to delay taking their normal dose the morning of the HepQuant SHUNT test;
b. Allergy to any ingredient in the formulations or components in the HepQuant Lab
Developed kit.
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Study design
Purpose of the study
Treatment
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Allocation to intervention
Non-randomised trial
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Procedure for enrolling a subject and allocating the treatment (allocation concealment procedures)
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Methods used to generate the sequence in which subjects will be randomised (sequence generation)
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Masking / blinding
Open (masking not used)
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Who is / are masked / blinded?
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Intervention assignment
Other
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Other design features
Multiple Ascending Dose
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Phase
Phase 1
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Type of endpoint/s
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Statistical methods / analysis
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Recruitment
Recruitment status
Recruiting
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Date of first participant enrolment
Anticipated
30/03/2024
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Actual
23/05/2024
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Date of last participant enrolment
Anticipated
31/12/2024
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Actual
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Date of last data collection
Anticipated
31/03/2025
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Actual
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Sample size
Target
18
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Accrual to date
3
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Final
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Recruitment in Australia
Recruitment state(s)
NSW,QLD
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Recruitment outside Australia
Country [1]
26113
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New Zealand
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State/province [1]
26113
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Country [2]
26114
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Canada
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State/province [2]
26114
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Country [3]
26115
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Korea, Republic Of
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State/province [3]
26115
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Country [4]
26116
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United Kingdom
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State/province [4]
26116
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Funding & Sponsors
Funding source category [1]
315676
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Commercial sector/Industry
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Name [1]
315676
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Surrozen Operating, Inc.
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Address [1]
315676
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Country [1]
315676
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United States of America
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Primary sponsor type
Commercial sector/Industry
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Name
Surrozen Operating, Inc.
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Address
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Country
United States of America
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Secondary sponsor category [1]
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Commercial sector/Industry
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Name [1]
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Novotech (Australia) Pty Limited
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Address [1]
317780
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Country [1]
317780
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Australia
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Secondary sponsor category [2]
317783
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Commercial sector/Industry
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Name [2]
317783
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Novotech (New Zealand) Limited
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Address [2]
317783
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Country [2]
317783
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New Zealand
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Secondary sponsor category [3]
317784
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Commercial sector/Industry
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Name [3]
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Novotech Asia Korea Co., Limited
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Address [3]
317784
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Country [3]
317784
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Korea, Republic Of
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Ethics approval
Ethics application status
Approved
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Ethics committee name [1]
314555
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Northern B Health and Disability Ethics Committee
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Ethics committee address [1]
314555
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https://ethics.health.govt.nz/about/northern-b-health-and-disability-ethics-committee/
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Ethics committee country [1]
314555
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New Zealand
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Date submitted for ethics approval [1]
314555
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19/01/2024
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Approval date [1]
314555
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23/02/2024
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Ethics approval number [1]
314555
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Ethics committee name [2]
314556
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Metro North Health Human Research Ethics Committee A
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Ethics committee address [2]
314556
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https://metronorth.health.qld.gov.au/research/ethics-and-governance/human-research-ethics-committee
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Ethics committee country [2]
314556
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Australia
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Date submitted for ethics approval [2]
314556
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30/01/2024
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Approval date [2]
314556
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27/03/2024
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Ethics approval number [2]
314556
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Summary
Brief summary
Severe alcohol-associated hepatitis (SAH) is a huge unmet medical need, associated with high mortality. Corticosteroids have not been associated with improved long-term survival benefit and there has been no improvement in survival in SAH with medical management during the last 60 years. SAH is associated with impaired growth of new cells in your liver (known as hepatocyte proliferation). Elevated Wnt signaling and increased hepatocyte proliferation have been linked to greater survival, suggesting that therapies that can enhance hepatocyte proliferation can benefit patients. R-spondins (RSPOs) are known enhancers of Wnt signaling. SZN-043 is a bispecific fusion protein and hepatocyte-specific RSPO mimetic shown to bring on hepatocyte-targeted Wnt signaling and hepatocyte proliferation in research studies performed in laboratories. SZN-043 was evaluated for safety and how the drug behaves in the human body in a single center, first-in-human study in healthy volunteers and patients with mild cirrhosis of the liver. This second study will evaluate the same things in patients who have severe AH.
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Trial website
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Trial related presentations / publications
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Public notes
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Contacts
Principal investigator
Name
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Prof Juan Pablo Arab
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Address
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Division of Gastroenterology and Hepatology, Multiorgan Transplant Program, 339 Windermere Road, Room A10-224, Western University & London Health Sciences Centre, London, Ontario N6A 5A5
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Country
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Canada
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Phone
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+15196633946
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Fax
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Email
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[email protected]
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Contact person for public queries
Name
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Joshua Koons
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Address
131999
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Surrozen Operating, Inc., 171 Oyster Point Blvd, Ste 400, South San Francisco, CA 94708
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Country
131999
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United States of America
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Phone
131999
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+16504207056
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Fax
131999
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Email
131999
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[email protected]
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Contact person for scientific queries
Name
132000
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Craig Parker
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Address
132000
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Surrozen Operating, Inc., 171 Oyster Point Blvd, Ste 400, South San Francisco, CA 94708
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Country
132000
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United States of America
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Phone
132000
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+16504437353
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Fax
132000
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Email
132000
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[email protected]
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Data sharing statement
Will individual participant data (IPD) for this trial be available (including data dictionaries)?
No
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No/undecided IPD sharing reason/comment
Privacy and intellectual property considerations
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What supporting documents are/will be available?
No Supporting Document Provided
Results publications and other study-related documents
Documents added manually
No documents have been uploaded by study researchers.
Documents added automatically
No additional documents have been identified.
Download to PDF