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A Trial to Evaluate Safety, Tolerability, PK and Antiviral Activity of MB-110 in Hepatitis C Virus Infected Patients

Primary Purpose

Chronic Hepatitis C

Status

Unknown status

Phase

Phase 1

Locations

Taiwan

Study Type

Interventional

Intervention

MB-110

Placebo

About this trial

This is an interventional treatment trial for Chronic Hepatitis C focused on measuring MB-110

Eligibility Criteria

20 Years - 65 Years (Adult, Older Adult)All SexesAccepts Healthy Volunteers

Inclusion Criteria for Part A:

To be eligible to participate in this study, subjects must meet all of the following criteria at screening:

Male or female between 20 to 55 years of age inclusive
For females, not breast-feeding, not pregnant, post-menopausal for at least 2 years, surgically sterile, or willing to use a double barrier method [intrauterine device (IUD) plus condom, spermicidal gel plus condom] of contraception, or other effective contraceptive methods from screening until 30 days after the last dose of study drug
For males, willing to use a reliable form of contraception (use of a male condom with spermicide or a partner fulfilling the above criteria), or abstinence from screening until 30 days after the last dose of study drug
Body weight ≥ 50 kg inclusive and body mass index (BMI) in the range of 19.0 to 30.0 kg/m2, extremes included
Good physical and mental health conditions on the basis of medical history and vital signs performed at screening
Healthy on the basis of clinical laboratory tests performed at screening. If the results are outside the normal reference ranges, the subject may be included only if the investigator judges the abnormalities or deviations from normal not to be clinically significant. This determination must be recorded in the subject's source document and initialed by the investigator. This is not applicable to the laboratory abnormalities listed in the exclusion criteria [using the Division of Microbiology and Infectious Diseases (DMID) Adult Toxicity criteria-see Section 13.3].
Non-smoking for at least 3 months prior to screening, to be confirmed by a urine cotinine dipstick test
12-lead electrocardiogram (ECG) consistent with normal cardiac conduction and function:
- Heart rate (HR) between 50 and 100 bpm
- QTcF interval ≤ 430 ms (male) or ≤ 450 ms (female)
- QRS interval lower than 120 ms
- PR interval ≤ 200 ms
- Willing to abstain from caffeine- or xanthine-containing beverages and food, including coffee and tea, alcohol, grapefruit juice, and bitter oranges during the study period

10. Willing to sign an Informed Consent Form (ICF) indicating that he or she understands the purpose of and procedures required for the study and is willing to participate in the study

Exclusion Criteria for Part A:

Subjects must be excluded if they meet any of the following criteria:

Breast-feeding or pregnant female
History of heart arrhythmias (any clinically relevant) or having baseline prolongation of QTcF interval > 430 ms (male) or > 450 ms (female), history of risk factors for Torsade de Pointes syndrome (hypokalemia, family history of long QT syndrome), or a HR (supine pulse as obtained from vital signs) < 50 bpm or > 100 bpm
History or suspicion of current use of alcohol, barbiturate, amphetamine, recreational or narcotic drug use, which in the investigator's opinion would compromise subject's safety and/or compliance with the study procedures
Hepatitis A, B, or C infection (confirmed by hepatitis A antibody IgM, hepatitis B surface antigen, or hepatitis C virus antibody, respectively) or HIV-1 or HIV-2 infection (confirmed by CLIA test) at study screening
Clinically relevant, currently active or underlying gastrointestinal, cardiovascular-, nervous system, psychiatric, metabolic, renal, hepatic, respiratory, inflammatory, or infectious disease
History of drug allergy such as, but not limited to, sulfonamides and penicillins, or drug allergy witnessed in previous trials with investigational drugs
Any condition that, in the opinion of the investigator, would compromise the study or the well-being of the subject or prevent the subject from meeting or performing study requirements
Use of concomitant medication, including over-the-counter product, herbal medication and dietary supplement in a period of 14 days before the study
Donation of blood or plasma over 250 mL within 60 days preceding the study
Subjects with one or more of the following laboratory abnormalities at screening as defined by DMID Adult Toxicity Table:
- Hemoglobin grade 1 or greater (≤ 10.5 gm/dL)
- Platelet count grade 1 or greater (< 100,000/mm3)
- Absolute neutrophil count grade 1 or greater (≤ 1500/mm3)
- Aspartate transaminase (AST) or alanine aminotransferase (ALT) grade 1 or greater (> 1.1x ULN [upper limit range])
- Total bilirubin grade 1 or greater (> 1.1x ULN)
- Lipase grade 1 or greater (> 1.1x ULN)
- Serum creatinine grade 1 or greater (> 1.1x ULN)
- Any other laboratory abnormality ≥ grade 1 [Note: Re-testing of abnormal lab values that may lead to exclusion will be allowed once (without prior Sponsor approval). Re-testing will take place during an unscheduled visit in the Screening phase (before admission/baseline)]
Prisoners or subjects compulsorily detained (involuntarily incarcerated) for treatment of a psychiatric illness, or having any history of suicide attempt or depression
Acute illness within 2 weeks prior to dosing, unless approved by the Sponsor's Medical Monitor

Inclusion Criteria for Part B:

To be eligible to participate in this study, subjects must meet all of the following criteria:

Male or female between 20 to 65 years of age inclusive
For females, not breast-feeding, not pregnant, post-menopausal for at least 2 years, surgically sterile, or willing to use a double barrier method [intrauterine device (IUD) plus condom, spermicidal gel plus condom] of contraception, or other effective contraceptive methods from screening until 30 days after the last dose of study drug
For males, willing to use a reliable form of contraception (use of a male condom with spermicide or a partner fulfilling the above criteria), or abstinence from screening until 30 days after the last dose of study drug
Body weight ≥ 50 kg inclusive and body mass index (BMI) in the range of 19.0 to 30.0 kg/m2, extremes included
Willing to abstain from caffeine- or xanthine-containing beverages, including coffee and tea, alcohol, grapefruit juice, and bitter oranges during the study period
Willing to sign an Informed Consent Form (ICF) indicating that he or she understands the purpose of and procedures required for the study and is willing to participate in the study
Presence of chronic hepatitis C (CHC) as documented below:
- Positive for anti-HCV antibody at least 6 months before screening; or
- A liver biopsy or Elastoscan/Fibroscan/FibroSURE performed at screening with evidence of CHC, such as the presence of fibrosis and/or inflammation
Positive for anti-HCV antibody at screening
Absence (no medical history or physical findings) of ascites, bleeding esophageal varices, hepatic encephalopathy, or other signs and symptoms of decompensated liver disease
Presence of an HCV RNA level ≥ 1x105 IU/mL at screening
Presence of genotype 1b, 2a, or 3a HCV-infection at screening
Treatment-naïve HCV-infected subjects who are eligible to receive interferon, ribavirin, and HCV protease inhibitors but have a viable HCV treatment plan established with HCV care provider

Exclusion Criteria for Part B:

Subjects must be excluded if they meet any of the following criteria:

Breast-feeding or pregnant female
History of heart arrhythmias (any clinically relevant) or having baseline prolongation of QTcF interval > 430 ms (male) or > 450 ms (female), history of risk factors for Torsade de Pointes syndrome (hypokalemia, family history of long QT syndrome), or a HR (supine pulse as obtained from vital signs) < 50 bpm or > 100 bpm
History or suspicion of current use of alcohol, barbiturate, amphetamine, recreational or narcotic drug use, which in the investigator's opinion would compromise subject's safety and/or compliance with the study procedures
Hepatitis A or B infection (confirmed by hepatitis A antibody IgM, or hepatitis B surface antigen, respectively) or HIV-1 or HIV-2 infection (confirmed by CLIA test) at study screening
Clinically relevant, currently active or underlying gastrointestinal, cardiovascular-, nervous system, psychiatric, metabolic (e.g., diabetes mellitus), renal, hepatic, respiratory, inflammatory, or infectious disease
History of drug allergy such as, but not limited to, sulfonamides and penicillins, or drug allergy witnessed in previous trials with investigational drugs
Any condition that, in the opinion of the investigator, would compromise the study or the well-being of the subject or prevent the subject from meeting or performing study requirements
Use of prohibited medications or herbal remedies within 14 days prior to first dose of study drug administration
Donation of blood or plasma over 250 mL within 60 days preceding the study
Subjects with one or more of the following laboratory abnormalities at screening as defined by Division of Microbiology and Infectious Diseases (DMID) Adult Toxicity Table:
- Hemoglobin grade 1 or greater (≤ 10.5 gm/dL)
- Platelet count grade 1 or greater (< 100,000/mm3)
- Absolute neutrophil count grade 1 or greater (≤ 1500/mm3)
- AST or ALT > 5x ULN
- Total bilirubin > 1.5x ULN
- Prothrombin time INR >1.5x ULN
- Lipase grade 1 or greater (> 1.1x ULN)
- Serum creatinine grade 1 or greater (> 1.1x ULN)
- Any other laboratory abnormality ≥ grade 2 [Note: Re-testing of abnormal lab values that may lead to exclusion will be allowed once (without prior Sponsor approval). Re-testing will take place during an unscheduled visit in the Screening phase (before admission/baseline)]
Prisoners or subjects compulsorily detained (involuntarily incarcerated) for treatment of a psychiatric illness, or having any history of suicide attempt or depression
Received any other investigational drug within 30 days prior to first dose of study drug administration
Co-infections with HIV-1, HIV-2 or other liver infection
History or evidence of cirrhosis or decompensated liver disease

Sites / Locations

Microbio Co., Ltd.

Arms of the Study

Arm 1

Arm 2

Arm Type

Experimental

Placebo Comparator

Arm Label

MB-110

Placebo

Arm Description

oral hard-gel capsule formulation. One dose strength, 25 mg of MB-110, will be filled into the #00 hard-gel capsule.

in the same #00 hard-gel capsules.

Outcomes

Primary Outcome Measures

Incidence of adverse events in cohort 1-4

Incidence of adverse events in cohort 6-8

Changes in vital signs from baseline in cohort 1-4

Changes in vital signs from baseline in cohort 5

vital signs will be performed

Changes in vital signs from baseline in cohort 6-8

Changes in physical examination from baseline in cohort 1-4

Changes in physical examination from baseline in cohort 5

Changes in physical examination from baseline in cohort 6-8

Changes in safety laboratory values (biochemistry, hematology, coagulation, and urinalysis) from baseline in cohort 1-4

Changes in safety laboratory values (biochemistry, hematology, coagulation, and urinalysis) from baseline in cohort 5

Changes in safety laboratory values (biochemistry, hematology, coagulation, and urinalysis) from baseline in cohort 6-8

Changes in 12-lead ECG from baseline in cohort 1-4

Changes in 12-lead ECG from baseline in cohort 5

Changes in 12-lead ECG from baseline in cohort 6-8

Change in plasma viral RNA from baseline in cohort 6-8

Blood for HCV RNA level determination will be collected at screening visit, day-1, Day 1 ( pre-1st dose (-2 to 0 hr), post-1st dose (8 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose)), Day 2 (post-2nd dose (12 hr±15 min and 24 hr±15 min)), Day 3 (post-3rd dose (12 hr±15 min, 24 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)), Day 13, and Day 17

Incidence of adverse events in cohort 5

Area under the plasma concentration time curve from 0 to the last measurable concentration (AUC0-t) in cohort 1-4

Area under the plasma concentration time curve from 0 to infinity (AUC0-inf) in cohort 1-4

Maximum plasma concentration (Cmax) in cohort 1-4

Trough plasma concentration (Cmin) in cohort 1-4

Time at which maximum plasma concentration (Tmax) is observed in cohort 1-4

Terminal elimination half-life (t1/2) in cohort 1-4

Terminal elimination rate constant (λz) in cohort 1-4

Urine PK parameters: the amount of study drug excreted into urine and urine recovery rate (Ae%) in cohort 1-4

Area under the plasma concentration time curve from 0 to the last measurable concentration (AUC0-t) in cohort 5

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3 and Day 4: pre-3rd, -4th dose (-2 to 0 hr) Day 5: pre-5th dose (-2 to 0 hr), post-5th dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Area under the plasma concentration time curve from 0 to infinity (AUC0-inf) in cohort 5

Maximum plasma concentration (Cmax) in cohort 5

Trough plasma concentration (Cmin) in cohort 5

Time at which maximum plasma concentration (Tmax) is observed in cohort 5

Terminal elimination half-life (t1/2) in cohort 5

Terminal elimination rate constant (λz) in cohort 5

Urine PK parameters: the amount of study drug excreted into urine and urine recovery rate (Ae%) in cohort 5

Area under the plasma concentration time curve from 0 to the last measurable concentration (AUC0-t) in cohort 6-8

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Area under the plasma concentration time curve from 0 to infinity (AUC0-inf) in cohort 6-8

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Maximum plasma concentration (Cmax) in cohort 6-8

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Trough plasma concentration (Cmin) in cohort 6-8

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Time at which maximum plasma concentration (Tmax) is observed in cohort 6-8

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Terminal elimination half-life (t1/2) in cohort 6-8

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Terminal elimination rate constant (λz) in cohort 6-8

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Urine PK parameters: the amount of study drug excreted into urine and urine recovery rate (Ae%) in cohort 6-8

Secondary Outcome Measures

Difference on area under the plasma concentration time curve from 0 to the last measurable concentration (AUC0-t) between cohort 1 and 3

Difference on area under the plasma concentration time curve from 0 to infinity (AUC0-inf) between cohort 1 and 3

Difference on maximum plasma concentration (Cmax) between cohort 1 and 3

Difference on trough plasma concentration (Cmin) between cohort 1 and 3

Difference on time at which maximum plasma concentration (Tmax) is observed between cohort 1 and 3

Difference on terminal elimination half-life (t1/2) between cohort 1 and 3

Difference on terminal elimination rate constant (λz) in cohort 6-8

Full Information

NCT ID

NCT02617615

First Posted

November 23, 2015

Last Updated

April 4, 2017

Sponsor

Microbio Co Ltd

1. Study Identification

Unique Protocol Identification Number

NCT02617615

Brief Title

A Trial to Evaluate Safety, Tolerability, PK and Antiviral Activity of MB-110 in Hepatitis C Virus Infected Patients

Official Title

A Phase 1, First-in-Human Study to Evaluate the Safety, Tolerability, and Pharmacokinetic Profiles of Single Ascending and Multiple Oral Doses of MB-110 and to Evaluate the Antiviral Activity in Hepatitis C Virus Infected Patients

Study Type

Interventional

2. Study Status

Record Verification Date

April 2017

Overall Recruitment Status

Unknown status

Study Start Date

December 1, 2017 (Anticipated)

Primary Completion Date

June 2018 (Anticipated)

Study Completion Date

December 2018 (Anticipated)

3. Sponsor/Collaborators

Responsible Party, by Official Title

Sponsor

Name of the Sponsor

Microbio Co Ltd

4. Oversight

Studies a U.S. FDA-regulated Drug Product

Yes

Studies a U.S. FDA-regulated Device Product

Data Monitoring Committee

5. Study Description

Brief Summary

A Phase 1, First-in-Human, Randomized, Placebo-Controlled, Double-Blind Study to Evaluate the Safety, Tolerability, and Pharmacokinetic Profiles of Single Ascending and Multiple Oral Doses of MB-110 in Healthy Volunteers and to Evaluate the Antiviral Activity of MB-110 in Hepatitis C Virus Infected Subjects

Detailed Description

The present study is divided into 2 parts. Part A is a randomized, double blind, placebo controlled, sequential ascending single and multiple oral doses design to evaluate the safety, tolerability, PK, and food effect of MB-110 in healthy volunteers.Part A will recruit 2 groups (Groups 1 and 2) of 8 healthy volunteers in each group. Within each group, 8 subjects will be randomized 6:2 to receive MB-110 versus placebo.Subjects in Group 1 will receive either 50 mg of MB-110 or placebo under fasted conditions during the first visit (Cohort 1); and either 50 mg of MB-110 or placebo under fed conditions during the second visit (Cohort 3) where food effect will be evaluated. Subjects in Group 2 will receive either 100 mg of MB-110 or placebo under fasted condition during the first visit (Cohort 2); or 200 mg of MB-110 or placebo under fasted condition during the second visit (Cohort 4). In Cohort 5, 8 subjects will be selected from Group 1, Group 2, or new recruitment if the washout time is insufficient from the previous cohort. Subjects in Cohort 5 will be randomized 6:2 to receive MB-110 at dose of 200 mg or placebo once daily for 5 consecutive days. Part B is a randomized, double-blind, placebo-controlled, multiple ascending oral dose design to evaluate the safety, tolerability, PK, and antiviral activity of MB-110 in subjects infected with Hepatitis C virus genotype 1b, 2a, and 3a.Part B will recruit 3 cohorts (Cohorts 6, 7, and 8) of treatment-naïve HCV infected subjects in each cohort. In Cohort 6, 12 subjects infected with Hepatitis C virus genotype 1b will be randomized 5:5:2 to receive two dose levels of MB-110 or placebo once daily for 3 consecutive days. In Cohort 7, 6 subjects infected with Hepatitis C virus genotype 2a will be randomized 5:1 to receive MB-110 or placebo once daily for 3 consecutive days. In Cohort 8, 6 subjects infected with Hepatitis C virus genotype 3a will be randomized 5:1 to receive MB-110 or placebo once daily for 3 consecutive days.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study

Chronic Hepatitis C

Keywords

MB-110

7. Study Design

Primary Purpose

Treatment

Study Phase

Phase 1

Interventional Study Model

Parallel Assignment

Masking

ParticipantInvestigator

Allocation

Randomized

Enrollment

40 (Anticipated)

8. Arms, Groups, and Interventions

Arm Title

MB-110

Arm Type

Experimental

Arm Description

oral hard-gel capsule formulation. One dose strength, 25 mg of MB-110, will be filled into the #00 hard-gel capsule.

Arm Title

Placebo

Arm Type

Placebo Comparator

Arm Description

in the same #00 hard-gel capsules.

Intervention Type

Drug

Intervention Name(s)

MB-110

Other Intervention Name(s)

DBPR110, NSFA10003S0

Intervention Description

MB-110 is a novel, potent, and selective HCV inhibitor against the NS5A protein. In the preclinical studies, MB-110 demonstrated picomolar EC50s towards various genotypes and favorable pharmacokinetic properties to support the once daily dosing regimen.

Intervention Type

Drug

Intervention Name(s)

Placebo

Other Intervention Name(s)

Placebo of MB-110

Intervention Description

It will be identical in appearance and similar in weight to the MB-110 hard-gel capsule.

Primary Outcome Measure Information:

Title

Incidence of adverse events in cohort 1-4

Time Frame

Up to 8 days (plus or minus 1 day)

Title

Incidence of adverse events in cohort 6-8

Time Frame

Up to 17 days (14 days plus or minus 1 day after dosing for 3 consecutive days)

Title

Changes in vital signs from baseline in cohort 1-4

Time Frame

at screening visit, day-1, pre-dose (-2 to 0 hr), and post-dose (2 hr, 4 hr, 6 hr, 8 hr, 12 hr, 16 hr, 24 hr, 48 hr, 72 hr, and 96 hr) and Day 8 (plus or minus 1 day)

Title

Changes in vital signs from baseline in cohort 5

Description

vital signs will be performed

Time Frame

at screening visit, day-1, post-1st, -2nd, -3rd, -4th, -5th dose (4 hr±15 min and 6 hr±15 min), discharge day (Day 9), Day 12, and Day 19 (14 days plus or minus 1 day after dosing for 5 consecutive days)

Title

Changes in vital signs from baseline in cohort 6-8

Time Frame

at screening visit, day-1, post-1st, -2nd, -3rd dose (4 hr±15 min and 6 hr±15 min), discharge day (Day 7), Day 13, and Day 17 (14 days plus or minus 1 day after dosing for 3 consecutive days)

Title

Changes in physical examination from baseline in cohort 1-4

Time Frame

at screening visit, day-1, discharge day (Day 5), and Day 8 (plus or minus 1 day)

Title

Changes in physical examination from baseline in cohort 5

Time Frame

at screening visit, day-1, discharge day (Day 9), Day 12, and Day 19 (14 days plus or minus 1 day after dosing for 5 consecutive days)

Title

Changes in physical examination from baseline in cohort 6-8

Time Frame

at screening visit, day-1, discharge day (Day 7), Day 13, and Day 17 (14 days plus or minus 1 day after dosing for 3 consecutive days)

Title

Changes in safety laboratory values (biochemistry, hematology, coagulation, and urinalysis) from baseline in cohort 1-4

Time Frame

at screening visit, day-1, and post-dose (12 hr±30 min, 48 hr±30 min, and 96 hr±30 min), and Day 8 (plus or minus 1 day)

Title

Changes in safety laboratory values (biochemistry, hematology, coagulation, and urinalysis) from baseline in cohort 5

Time Frame

at screening visit, day-1, post-1st, -3rd, and -5th dose (12 hr±30 min), Day 7, discharge day (Day 9), and Day 12 (7 days plus or minus 1 day after dosing for 5 consecutive days)

Title

Changes in safety laboratory values (biochemistry, hematology, coagulation, and urinalysis) from baseline in cohort 6-8

Time Frame

at screening visit, day-1, 12 hr±30 min post-1st, 12 hr±30 min post-3rd, Day 5, discharge day (Day 7), and Day 13 (10 days plus or minus 1 day after dosing for 3 consecutive days)

Title

Changes in 12-lead ECG from baseline in cohort 1-4

Time Frame

at screening visit, day-1, pre-dose (-2 to 0 hr), and post-dose (2 hr, 4 hr, 6 hr, 8 hr, 12 hr, 16 hr, 24 hr, 48 hr, 72 hr, and 96 hr), and Day 8 (plus or minus 1 day)

Title

Changes in 12-lead ECG from baseline in cohort 5

Time Frame

at screening visit, day-1, post-1st, -2nd, -3rd, -4th, -5th dose (4 hr±15 min and 6 hr±15 min), discharge day (Day 9), and Day 12 (7 days plus or minus 1 day after dosing for 5 consecutive days)

Title

Changes in 12-lead ECG from baseline in cohort 6-8

Time Frame

at screening visit, day-1, post-1st, -2nd, -3rd dose (4 hr±15 min and 6 hr±15 min), discharge day (Day 7), and Day 13 (10 days plus or minus 1 day after dosing for 3 consecutive days)

Title

Change in plasma viral RNA from baseline in cohort 6-8

Description

Time Frame

Up to 17 days

Title

Incidence of adverse events in cohort 5

Time Frame

Up to 19 days (14 days plus or minus 1 day after dosing for 5 consecutive days)

Title

Area under the plasma concentration time curve from 0 to the last measurable concentration (AUC0-t) in cohort 1-4

Time Frame

pre-dose (-2 to 0 hr) and post-dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Title

Area under the plasma concentration time curve from 0 to infinity (AUC0-inf) in cohort 1-4

Time Frame

Title

Maximum plasma concentration (Cmax) in cohort 1-4

Time Frame

Title

Trough plasma concentration (Cmin) in cohort 1-4

Time Frame

Title

Time at which maximum plasma concentration (Tmax) is observed in cohort 1-4

Time Frame

Title

Terminal elimination half-life (t1/2) in cohort 1-4

Time Frame

Title

Terminal elimination rate constant (λz) in cohort 1-4

Time Frame

Title

Urine PK parameters: the amount of study drug excreted into urine and urine recovery rate (Ae%) in cohort 1-4

Time Frame

-2-0 hr, 0-6 hr, 6-12 hr, 12-24 hr, 24-36 hr, 36-48 hr, 48-72 hr, 72-96 hr post-dose

Title

Area under the plasma concentration time curve from 0 to the last measurable concentration (AUC0-t) in cohort 5

Description

Time Frame

Up to 8 days

Title

Area under the plasma concentration time curve from 0 to infinity (AUC0-inf) in cohort 5

Description

Time Frame

Up to 8 days

Title

Maximum plasma concentration (Cmax) in cohort 5

Description

Time Frame

Up to 8 days

Title

Trough plasma concentration (Cmin) in cohort 5

Description

Time Frame

Up to 8 days

Title

Time at which maximum plasma concentration (Tmax) is observed in cohort 5

Description

Time Frame

Up to 8 days

Title

Terminal elimination half-life (t1/2) in cohort 5

Description

Time Frame

Up to 8 days

Title

Terminal elimination rate constant (λz) in cohort 5

Description

Time Frame

Up to 8 days

Title

Urine PK parameters: the amount of study drug excreted into urine and urine recovery rate (Ae%) in cohort 5

Time Frame

Day 1: pre-1st dose (-2-0 hr), post-1st dose (0-6 hr, 6-12 hr, 12-24 hr) Day 5: post-5th dose (0-6 hr, 6-12 hr, 12-24 hr, 24-36 hr, 36-48 hr, 48-72 hr, and 72-96 hr)

Title

Area under the plasma concentration time curve from 0 to the last measurable concentration (AUC0-t) in cohort 6-8

Description

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Time Frame

Up to 6 days

Title

Area under the plasma concentration time curve from 0 to infinity (AUC0-inf) in cohort 6-8

Description

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Time Frame

Up to 6 days

Title

Maximum plasma concentration (Cmax) in cohort 6-8

Description

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Time Frame

Up to 6 days

Title

Trough plasma concentration (Cmin) in cohort 6-8

Description

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Time Frame

Up to 6 days

Title

Time at which maximum plasma concentration (Tmax) is observed in cohort 6-8

Description

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Time Frame

Up to 6 days

Title

Terminal elimination half-life (t1/2) in cohort 6-8

Description

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Time Frame

Up to 6 days

Title

Terminal elimination rate constant (λz) in cohort 6-8

Description

Day 1: pre-1st dose (-2 to 0 hr), post-1st dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min before the 2nd dose) Day 3: pre-3rd dose (-2 to 0 hr), post-3rd dose (1 hr±3 min, 2 hr±5 min, 3 hr±10 min, 4 hr±10 min, 6 hr±15 min, 8 hr±15 min, 12 hr±15 min, 16 hr±15 min, 24 hr±15 min, 36 hr±15 min, 48 hr±15 min, 72 hr±15 min, 96 hr±15 min)

Time Frame

Up to 6 days

Title

Urine PK parameters: the amount of study drug excreted into urine and urine recovery rate (Ae%) in cohort 6-8

Time Frame

Day 1: pre-1st dose (-2-0 hr), post-1st dose (0-4 hr, 4-8 hr, 8-12 hr, 12-16 hr, and 16-24 hr) Day 3: post-3rd dose (0-4 hr, 4-8 hr, 8-12 hr, 12-16 hr, 16-24 hr, 24-36 hr, 36-48 hr, 48-72 hr, and 72-96 hr)

Secondary Outcome Measure Information:

Title

Difference on area under the plasma concentration time curve from 0 to the last measurable concentration (AUC0-t) between cohort 1 and 3

Time Frame

Title

Difference on area under the plasma concentration time curve from 0 to infinity (AUC0-inf) between cohort 1 and 3

Time Frame

Title

Difference on maximum plasma concentration (Cmax) between cohort 1 and 3

Time Frame

Title

Difference on trough plasma concentration (Cmin) between cohort 1 and 3

Time Frame

Title

Difference on time at which maximum plasma concentration (Tmax) is observed between cohort 1 and 3

Time Frame

Title

Difference on terminal elimination half-life (t1/2) between cohort 1 and 3

Time Frame

Title

Difference on terminal elimination rate constant (λz) in cohort 6-8

Time Frame

10. Eligibility

Sex

All

Minimum Age & Unit of Time

20 Years

Maximum Age & Unit of Time

65 Years

Accepts Healthy Volunteers

Eligibility Criteria

Inclusion Criteria for Part A: To be eligible to participate in this study, subjects must meet all of the following criteria at screening: Male or female between 20 to 55 years of age inclusive For females, not breast-feeding, not pregnant, post-menopausal for at least 2 years, surgically sterile, or willing to use a double barrier method [intrauterine device (IUD) plus condom, spermicidal gel plus condom] of contraception, or other effective contraceptive methods from screening until 30 days after the last dose of study drug For males, willing to use a reliable form of contraception (use of a male condom with spermicide or a partner fulfilling the above criteria), or abstinence from screening until 30 days after the last dose of study drug Body weight ≥ 50 kg inclusive and body mass index (BMI) in the range of 19.0 to 30.0 kg/m2, extremes included Good physical and mental health conditions on the basis of medical history and vital signs performed at screening Healthy on the basis of clinical laboratory tests performed at screening. If the results are outside the normal reference ranges, the subject may be included only if the investigator judges the abnormalities or deviations from normal not to be clinically significant. This determination must be recorded in the subject's source document and initialed by the investigator. This is not applicable to the laboratory abnormalities listed in the exclusion criteria [using the Division of Microbiology and Infectious Diseases (DMID) Adult Toxicity criteria-see Section 13.3]. Non-smoking for at least 3 months prior to screening, to be confirmed by a urine cotinine dipstick test 12-lead electrocardiogram (ECG) consistent with normal cardiac conduction and function: Heart rate (HR) between 50 and 100 bpm QTcF interval ≤ 430 ms (male) or ≤ 450 ms (female) QRS interval lower than 120 ms PR interval ≤ 200 ms Willing to abstain from caffeine- or xanthine-containing beverages and food, including coffee and tea, alcohol, grapefruit juice, and bitter oranges during the study period 10. Willing to sign an Informed Consent Form (ICF) indicating that he or she understands the purpose of and procedures required for the study and is willing to participate in the study Exclusion Criteria for Part A: Subjects must be excluded if they meet any of the following criteria: Breast-feeding or pregnant female History of heart arrhythmias (any clinically relevant) or having baseline prolongation of QTcF interval > 430 ms (male) or > 450 ms (female), history of risk factors for Torsade de Pointes syndrome (hypokalemia, family history of long QT syndrome), or a HR (supine pulse as obtained from vital signs) < 50 bpm or > 100 bpm History or suspicion of current use of alcohol, barbiturate, amphetamine, recreational or narcotic drug use, which in the investigator's opinion would compromise subject's safety and/or compliance with the study procedures Hepatitis A, B, or C infection (confirmed by hepatitis A antibody IgM, hepatitis B surface antigen, or hepatitis C virus antibody, respectively) or HIV-1 or HIV-2 infection (confirmed by CLIA test) at study screening Clinically relevant, currently active or underlying gastrointestinal, cardiovascular-, nervous system, psychiatric, metabolic, renal, hepatic, respiratory, inflammatory, or infectious disease History of drug allergy such as, but not limited to, sulfonamides and penicillins, or drug allergy witnessed in previous trials with investigational drugs Any condition that, in the opinion of the investigator, would compromise the study or the well-being of the subject or prevent the subject from meeting or performing study requirements Use of concomitant medication, including over-the-counter product, herbal medication and dietary supplement in a period of 14 days before the study Donation of blood or plasma over 250 mL within 60 days preceding the study Subjects with one or more of the following laboratory abnormalities at screening as defined by DMID Adult Toxicity Table: Hemoglobin grade 1 or greater (≤ 10.5 gm/dL) Platelet count grade 1 or greater (< 100,000/mm3) Absolute neutrophil count grade 1 or greater (≤ 1500/mm3) Aspartate transaminase (AST) or alanine aminotransferase (ALT) grade 1 or greater (> 1.1x ULN [upper limit range]) Total bilirubin grade 1 or greater (> 1.1x ULN) Lipase grade 1 or greater (> 1.1x ULN) Serum creatinine grade 1 or greater (> 1.1x ULN) Any other laboratory abnormality ≥ grade 1 [Note: Re-testing of abnormal lab values that may lead to exclusion will be allowed once (without prior Sponsor approval). Re-testing will take place during an unscheduled visit in the Screening phase (before admission/baseline)] Prisoners or subjects compulsorily detained (involuntarily incarcerated) for treatment of a psychiatric illness, or having any history of suicide attempt or depression Acute illness within 2 weeks prior to dosing, unless approved by the Sponsor's Medical Monitor Inclusion Criteria for Part B: To be eligible to participate in this study, subjects must meet all of the following criteria: Male or female between 20 to 65 years of age inclusive For females, not breast-feeding, not pregnant, post-menopausal for at least 2 years, surgically sterile, or willing to use a double barrier method [intrauterine device (IUD) plus condom, spermicidal gel plus condom] of contraception, or other effective contraceptive methods from screening until 30 days after the last dose of study drug For males, willing to use a reliable form of contraception (use of a male condom with spermicide or a partner fulfilling the above criteria), or abstinence from screening until 30 days after the last dose of study drug Body weight ≥ 50 kg inclusive and body mass index (BMI) in the range of 19.0 to 30.0 kg/m2, extremes included Willing to abstain from caffeine- or xanthine-containing beverages, including coffee and tea, alcohol, grapefruit juice, and bitter oranges during the study period Willing to sign an Informed Consent Form (ICF) indicating that he or she understands the purpose of and procedures required for the study and is willing to participate in the study Presence of chronic hepatitis C (CHC) as documented below: Positive for anti-HCV antibody at least 6 months before screening; or A liver biopsy or Elastoscan/Fibroscan/FibroSURE performed at screening with evidence of CHC, such as the presence of fibrosis and/or inflammation Positive for anti-HCV antibody at screening Absence (no medical history or physical findings) of ascites, bleeding esophageal varices, hepatic encephalopathy, or other signs and symptoms of decompensated liver disease Presence of an HCV RNA level ≥ 1x105 IU/mL at screening Presence of genotype 1b, 2a, or 3a HCV-infection at screening Treatment-naïve HCV-infected subjects who are eligible to receive interferon, ribavirin, and HCV protease inhibitors but have a viable HCV treatment plan established with HCV care provider Exclusion Criteria for Part B: Subjects must be excluded if they meet any of the following criteria: Breast-feeding or pregnant female History of heart arrhythmias (any clinically relevant) or having baseline prolongation of QTcF interval > 430 ms (male) or > 450 ms (female), history of risk factors for Torsade de Pointes syndrome (hypokalemia, family history of long QT syndrome), or a HR (supine pulse as obtained from vital signs) < 50 bpm or > 100 bpm History or suspicion of current use of alcohol, barbiturate, amphetamine, recreational or narcotic drug use, which in the investigator's opinion would compromise subject's safety and/or compliance with the study procedures Hepatitis A or B infection (confirmed by hepatitis A antibody IgM, or hepatitis B surface antigen, respectively) or HIV-1 or HIV-2 infection (confirmed by CLIA test) at study screening Clinically relevant, currently active or underlying gastrointestinal, cardiovascular-, nervous system, psychiatric, metabolic (e.g., diabetes mellitus), renal, hepatic, respiratory, inflammatory, or infectious disease History of drug allergy such as, but not limited to, sulfonamides and penicillins, or drug allergy witnessed in previous trials with investigational drugs Any condition that, in the opinion of the investigator, would compromise the study or the well-being of the subject or prevent the subject from meeting or performing study requirements Use of prohibited medications or herbal remedies within 14 days prior to first dose of study drug administration Donation of blood or plasma over 250 mL within 60 days preceding the study Subjects with one or more of the following laboratory abnormalities at screening as defined by Division of Microbiology and Infectious Diseases (DMID) Adult Toxicity Table: Hemoglobin grade 1 or greater (≤ 10.5 gm/dL) Platelet count grade 1 or greater (< 100,000/mm3) Absolute neutrophil count grade 1 or greater (≤ 1500/mm3) AST or ALT > 5x ULN Total bilirubin > 1.5x ULN Prothrombin time INR >1.5x ULN Lipase grade 1 or greater (> 1.1x ULN) Serum creatinine grade 1 or greater (> 1.1x ULN) Any other laboratory abnormality ≥ grade 2 [Note: Re-testing of abnormal lab values that may lead to exclusion will be allowed once (without prior Sponsor approval). Re-testing will take place during an unscheduled visit in the Screening phase (before admission/baseline)] Prisoners or subjects compulsorily detained (involuntarily incarcerated) for treatment of a psychiatric illness, or having any history of suicide attempt or depression Received any other investigational drug within 30 days prior to first dose of study drug administration Co-infections with HIV-1, HIV-2 or other liver infection History or evidence of cirrhosis or decompensated liver disease

Central Contact Person:

First Name & Middle Initial & Last Name or Official Title & Degree

Ashley Hung

Phone

+886-2-2570-2088

Ext

390

ashley.hung@microbio.com.tw

First Name & Middle Initial & Last Name or Official Title & Degree

Karen Wang

Phone

+886-2-2570-2088

Ext

316

karen.wang@onenessbio.com.tw

Overall Study Officials:

First Name & Middle Initial & Last Name & Degree

Kai-Min Chu

Organizational Affiliation

Tri-Service General Hospital

Official's Role

Principal Investigator

Facility Information:

Facility Name

Microbio Co., Ltd.

City

Taipei

Country

Taiwan

Facility Contact:

First Name & Middle Initial & Last Name & Degree

Ashley Hung

Phone

+886-2-2570-2088

Ext

390

ashley.hung@microbio.com.tw

12. IPD Sharing Statement

Learn more about this trial

A Trial to Evaluate Safety, Tolerability, PK and Antiviral Activity of MB-110 in Hepatitis C Virus Infected Patients

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