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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT03272009
Other study ID # EYP001-103
Secondary ID 2017-002211-33
Status Completed
Phase Phase 1
First received
Last updated
Start date September 21, 2017
Est. completion date July 30, 2018

Study information

Verified date August 2018
Source Enyo Pharma
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Bile acids regulating farnesoid X receptor (FXR) interact with hepatitis B virus replication. EYP001a is a selective, synthetic FXR agonist under development for the treatment of hepatitis B.

This Phase 1b study is designed primarily to determine the safety, tolerability, pharmacokinetics and pharmacodynamics of EYP001a in chronically HBV infected subjects.


Description:

This is a multicenter, randomized, double-blind, placebo-controlled two-part trial.

In Part A, EYP001a will be administered as 29 days monotherapy. Three dose-levels and 2 dosing regimens of EYP001a will be explored against placebo. The design also includes an open-label standard of care Entecavir monotherapy arm (comparator). Subjects will be randomly assigned to one of the 6 treatment arms:

- Treatment A: oral EYP001a

- Treatment B: oral EYP001a

- Treatment C: oral EYP001a

- Treatment D: oral EYP001a

- Treatment E: oral placebo

- Treatment F: oral Entecavir

In Part B, EYP001a or placebo will be administered as 29 days combination therapy with the standard of care Peg-IFNα2a. Subjects will be randomly assigned to one of the 3 treatment arms:

- Treatment G: oral EYP001a plus open label Peg-INFα2a administered as subcutaneous injection

- Treatment H: oral EYP001a plus open label Peg-INFα2a administered as subcutaneous injection

- Treatment I: oral placebo plus open label Peg-INFα2a administered as subcutaneous injection

Subjects enrolled in Part A are eligible for participation in Part B.

Participation will include a 40 day screening period, a 29 day treatment period and a 6 day follow-up evaluation period. For subjects who participate in both Parts A and B, a 14 washout period between Parts A and B will be included.

The safety and tolerability of EYP001a will be assessed by evaluating physical examinations, vital signs, ECGs, clinical laboratory parameters, and adverse events.


Recruitment information / eligibility

Status Completed
Enrollment 73
Est. completion date July 30, 2018
Est. primary completion date July 30, 2018
Accepts healthy volunteers No
Gender All
Age group 18 Years to 65 Years
Eligibility Inclusion Criteria:

1. Have given voluntary written informed consent;

2. Have a documented medical history of chronic HBV infection (within 12 months of screening visit), both results:

- Documented positive hepatitis B surface antigen (HBsAg) and

- Documented HBV DNA > 1000 IU/mL

3. Is anti-HBV treatment naive or treatment experienced (see also exclusion criterion #3).

4. Gender: male or female.

5. Age: 18 to 65 years inclusive.

6. Body mass index (BMI): 17.0-35.0 kg/m2 inclusive.

7. Has clinical chemistry, hematology, coagulation and urinalysis tests within normal, allowable limits (with the exception of alanine aminotransferase [ALT]); see inclusion criterion #10); if there is an out of range value, the result must be considered clinically non-significant by the investigator in order to be eligible.

8. Vital signs after at least 5 minutes resting in supine position at screening within the following ranges:

- systolic blood pressure: between 90 mm Hg and 145 mm Hg

- diastolic blood pressure: between 45 mm Hg and 90 mm Hg

- heart rate: between 40 bpm and 100 bpm

9. Have no clinically significant abnormal 12-lead automatic electrocardiogram (ECG) (incomplete right bundle branch block can be accepted) at screening: PR interval between 120 ms -and 210 ms, QRS-duration < 120 ms, QTc-interval (Fridericia's) = 450 msec.

10. ALT at screening = 5 x upper limit of normal (ULN).

11. Agrees to abstain from all medication, including non-prescription and prescription medication for 28 days prior to the Day 1 study visit, except for authorized medications (such as hormonal contraceptives for females, vitamins prescribed per label dosages and paracetamol). On a case-by-case basis, regular co-medication either as defined on the medication exception list or as documented by written approval from the sponsor as acceptable prior to randomization, will not be considered as a deviation from this criterion.

12. At screening, females must be non-pregnant and non-lactating, or of non-childbearing potential (either surgically sterilized or physiologically incapable of becoming pregnant, or at least 1 year post-menopausal [amenorrhea duration of 12 consecutive months); non-pregnancy will be confirmed for all females by a pregnancy test conducted at screening and at follow-up visit.

13. Female subjects of child-bearing potential, with a fertile male sexual partner, should be willing to use adequate contraception from screening until 90 days after the follow-up visit. Adequate contraception is defined as using hormonal contraceptives or an intrauterine device combined with at least 1 of the following forms of contraception: a diaphragm or cervical cap, or a condom. Also, total abstinence, in accordance with the lifestyle of the subject, is acceptable.

14. Male subjects, if not surgically sterilized, should be willing to use adequate contraception and not donate sperm from the Day 1 visit to the clinical research centre until 90 days after the follow-up visit. Adequate contraception for the male subject (and his female partner) is defined as using hormonal contraceptives or an intrauterine device combined with at least 1 of the following forms of contraception: a diaphragm or cervical cap, or a condom. Also, total abstinence, in accordance with the lifestyle of the subject is acceptable.

15. At screening, has no recent (<3 months) history of any clinically significant conditions, which, in the opinion of the investigator, would jeopardize the safety of the subject or impact the validity of the study results.

16. Willingness to abstain from alcohol from 48 hours prior to each study visit to the clinical research centre.

Exclusion Criteria:

1. Employee of a CRO participating in this study or the Sponsor.

2. Has certain or probable compensated liver cirrhosis documented by at least 2 of the following:

1. Optional assessment: has documented liver histology Metavir score (F4), Ishak >5 or Scheuer (F4)

2. Mandatory assessment: has presence or history of ascites, spontaneous bacterial peritonitis, esophageal varices, hepatic encephalopathy

3. Mandatory assessment: platelet count below 90,000/uL within 12 months of screening visit

4. Optional assessment: positive indirect blood test of APRI or FIB4 or positive direct blood test Fibrosure, Fibrotest, or FibroSpect within 12 months of screening visit

5. Optional assessment: has positive elastography within 6 months of screening visit (Fibroscan or Shearwave Aixplorer)

6. Optional assessment: has abnormal liver imaging (CT/US/MRI) consistent with a lobular/nodular liver and cirrhosis or indirect signs of portal hypertension.

3. Subject is HBV treatment experienced AND currently on anti-HBV treatment during the 30 days (or 5 half-lives of the considered anti-HBV drug, whichever is longer) before the first investigational product administration and until the last study visit.

4. Co-infection with active hepatitis C virus (HCV, except for patients with sustained viral response SVR, who can be included).

5. Co-infection with human immunodeficiency virus (HIV) Note: hepatitis D virus (HDV) status is not required for randomization and if not available can be established during the Day 1 visit with baseline PD virology assessments.

6. Receives or plans to receive systemic immunosuppressive or immunomodulating medications (e.g. IFN) during the study or = 4 months prior to the first investigational product administration.

7. Has clinically relevant immunosuppression from, but not limited to immunodeficiency conditions such as common variable hypogammaglobulinemia.

8. Clinical diagnosis of substance abuse during = 12 months prior to screening with narcotics or cocaine or with alcohol (regular consumption > 21 units/week [men] and > 14 units/week [women]; 1 unit = 1/2 pint of beer, 25 mL shot of 40% spirit or a 125 mL glass of wine. Expressed in g/day: > 30 g/day [men] and > 20 g/day [women]).

9. Has a positive drug urine screen (cocaine, phencyclidine, amphetamines (incl. methamphetamines), opiates (incl. heroin, codeine and morphine), benzodiazepines, barbiturates, methadone or alcohol screen. Subjects who admit the occasional use of cannabis will not be excluded as long as they are able to abstain from cannabis when they are assessed at study visits.

10. Has any known pre-existing medical or psychiatric condition that could interfere with the subject's ability to provide informed consent or participate in study conduct, or that may confound study findings.

11. Has a history of long QT syndrome.

12. Has a history of clinically significant gastrointestinal disease, especially peptic ulcerations, gastrointestinal bleeding, ulcerative colitis, Crohn's disease or Inflammatory Bowel Syndrome, renal, hepatic, neurologic, hematologic, endocrine, oncologic, pulmonary, immunologic, or cardiovascular disease or any other condition which, in the opinion of the investigator, would jeopardize the safety of the subject or impact the validity of the study results.

13. Has participated in any drug study within 40 days prior to the first drug administration in the current study. Note: Part A participation to this study is acceptable and not an exclusion criteria when considering eligibility for Part B, under the condition that follow-up visit of Part A has been completed and no investigational product related SAEs have occurred during Part A.

14. Has an uncontrolled ongoing illness at screening (e.g., active viral infection).

15. Has had major surgery within 30 days prior to the first drug administration, or within 6 months for gastrointestinal surgery prior to the first drug administration.

16. Has a history of relevant drug and/or food allergies.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
EYP001a
Capsules administered orally. Number of morning and evening capsules depending on treatment arm
Placebo
Placebo capsules for oral administration, identical in appearance to the EYP001a capsules
Entecavir
Tablets administered orally
peg-interferon alfa-2a
Ready-to-Use pre-filled syringes for subcutaneous injection

Locations

Country Name City State
Australia Linear Clinical Research Limited Perth Western Australia
Australia Scientia Clinical Research Limited Sydney New South Wales
Netherlands Academic Medical Centre (AMC) Amsterdam
Netherlands Erasmus MC Rotterdam
Poland Klinika Chorób Zakaznych I Hepatologii UMB Bialystok
Poland Klinika Chorób Zakaznych Kielce
Poland HepID Lublin
Thailand Hospital for Tropical Diseases Bangkok
Thailand King Chulalongkorn Memorial Hospital Bangkok

Sponsors (2)

Lead Sponsor Collaborator
Enyo Pharma CPR Pharma Services Pty Ltd, Australia

Countries where clinical trial is conducted

Australia,  Netherlands,  Poland,  Thailand, 

Outcome

Type Measure Description Time frame Safety issue
Primary Type and frequencies of adverse events Day 1 through Day 35
Secondary Maximum plasma concentration (Cmax) of EYP001 Day 1 through Day 35
Secondary Time to reach maximum concentration (Tmax) after EYP001 administration Day 1 through Day 35
Secondary Area under the concentration-time curve from time 0 to last measurable concentration (AUC0-6h) of EYP001 Day 1 through Day 35
Secondary Bile acid precursor C4 (7ahydroxy-4-cholesten-3-one) Day 1 through Day 35
Secondary Fibroblast growth factor 19 (FGF19) Day 1 through Day 35
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