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Multiple Oral Doses of BI 207127 NA in Treatment naïve and Treatment-experienced Hepatitis C Virus (HCV)-Infected Patients

Primary Purpose

Hepatitis C, Chronic

Status

Completed

Phase

Phase 1

Locations

Study Type

Interventional

Intervention

BI 207127 NA

Placebo

About this trial

This is an interventional treatment trial for Hepatitis C, Chronic

Eligibility Criteria

18 Years - 70 Years (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

Adults from 18 - 70 years
Male OR female with documented hysterectomy OR menopausal female with last menstrual period at least 12 months prior to screening
Written informed consent consistent with International Conference on Harmonization/Good Clinical Practice and local legislation given prior to any study procedures
Chronic HCV infection demonstrated by positive HCV immunoglobulin G Antibody
HCV genotype 1 which has to be confirmed by central laboratory test before Visit 2
For non-cirrhotic cohorts: Liver biopsy obtained within the last 36 months consistent with HCV infection showing minimal to mild liver fibrosis and without cirrhosis (Ishak or Metavir grade ≤ 2). For cirrhotic cohorts, previous liver biopsy or Fibroscan consistent with liver cirrhosis performed at any time before screening
HCV RNA load > 100,000 IU RNA per ml serum at screening

Exclusion Criteria:

All fertile males not willing to use an adequate form of contraception (condom, sterilisation at least 6 months post operation) in case their partner is of childbearing potential and is not using an adequate form of contraception (hormonal contraceptives, oral or injectable/ implantable, intra-uterine device)
Patients who have been treated with at least one dose of any HCV-polymerase inhibitor for acute or chronic hepatitis C infection
Any other or additional plausible cause for chronic liver disease, including the presence of other viruses known or suspected to cause hepatitis
Decompensated liver disease within past 12 months, as indicated by variceal bleeding, ascites, encephalopathy, Prothrombin or International Normalized Ratio (INR) prolonged to >1.7 x upper limit of normal (ULN), serum bilirubin > 2 mg/dl or albumin < 3.5 g/dl (i.e. Child-Pugh grade B, score > 7)
For non-cirrhotic cohorts: Any previous liver biopsy consistent with cirrhosis. For cirrhotic cohorts: Any liver biopsy or fibroscan result from last 2 years excluding liver cirrhosis.
Positive test for human immunodeficiency virus (HIV) or hepatitis B antigen at screening
Current alcohol or drug abuse, or history of the same, within the past six (6) months. Exception: Occasional use of cannabis is not an exclusion criterion. The investigator must however instruct the patient that consumption of cannabis is not allowed during the treatment period.
Any concurrent disease (cardiovascular, pulmonary, renal, haematological, neurological, psychiatric, immunologic, metabolic or endocrine dysfunction) if clinically significant based on the investigator's medical assessment at screening. A clinically significant disease is defined as one which in the opinion of the investigator may either put the patient at risk because of participation in the study or may influence the results of the study or the patient's ability to participate in the study. Exclusion is also necessary for any pre-existing cardiac abnormality by history.
Clinically significant abnormalities at screening ECG, including but not limited to a QTc longer than 435 msec, Pulse Rate > 240 msec at baseline and any bundle branch block pattern, but not necessarily non-specific T wave abnormalities
History of malignancy (except for previously cured squamous cell or basal cell carcinoma)
Patients treated with any interferon (IFN) (approved or investigational) or Peg-IFN and/or Ribavirin within 3 months prior to screening
Planned or concurrent usage of any other pharmacological therapy including any antiviral therapy or vaccination from 7 days before treatment and during treatment
Usage of any investigational drug within thirty (30) days prior to enrolment or 5 halflives, whichever is longer; or the planned usage of an investigational drug during the course of the current study
Known hypersensitivity to drugs or excipients
Patients with any one of the following laboratory values at screening:
- Alanine transaminase (ALT) > 3x ULN, local lab
- Aspartate aminotransferase (AST) > 3x ULN, local lab
- Total bilirubin > 1.5x ULN, local lab, unless predominantly conjugated and reflecting Gilbert's disease
- Alkaline phosphatase > 1.5x ULN, local lab
- Prothrombin time (INR) > 1.5x ULN, central lab
- Creatinine > 1x ULN, local lab
- Urine protein / creatinine ratio > 0.3 g protein / g creatinine, central lab
- Alpha-1-microglobulin / creatinine in urine > 1x ULN, central lab
- Platelet count < 100,000 / mm3, central lab
- White Blood cell count < 2000 cells/mm3, central lab
- Absolute neutrophile count < 1500 cells, central lab
- Hemoglobin < 12 g/dL, central lab
- For patients with liver cirrhosis:
  - ALT > 5x ULN, local lab
  - AST > 5x ULN, local lab
  - Platelet count < 70,000 / mm3, central lab
Patients with any clinically significant laboratory abnormalities based on the investigator's medical assessment at screening
Positive urine test for drug abuse at screening
Prior randomisation into this trial
Inability to comply with the protocol
Patients with ongoing or historical photosensitivity or recurrent rash
Alpha fetoprotein value (AFP) > 100 ng/ml; if AFP is > 20 and ≤ 100 ng/ml, patients can be included if liver cancer is excluded by a current imaging study (i.e. ultrasound, computer tomography scan or magnetic resonance imaging)

Sites / Locations

Arms of the Study

Arm 1

Arm 2

Arm 3

Arm Type

Experimental

Placebo Comparator

Arm Label

BI 207127 in patients with cirrhosis

BI 207127 in patients without cirrhosis

Placebo in patients without cirrhosis

Arm Description

multiple rising doses

Outcomes

Primary Outcome Measures

Virologic Response (VR)

Virologic response was defined as a ≥ 1 log10 reduction in serum Hepatitis C virus (HCV) Ribonucleic acid (RNA) level from baseline at any time from the start of administration of treatment up to day 5. In this Outcome Measure the percentage of participants with virologic response is presented.

Secondary Outcome Measures

Time Dependent Change From Baseline in Viral Load (VL)

Change of VL from baseline to day 7 is presented (VL at timepoint minus VL at baseline). Acronym used within the categories: planned time (PTM). The number of participants analysed displays the number of participants included in the analysis set whereas the number of participants for each timepoint display the number of participants with available data at that timepoint.

Cmax

Maximum measured concentration of Deleobuvir in plasma (Cmax) determined after the first dose.

Cmin

Measured concentration of Deleobuvir in plasma determined immediately before the second dose (Cmin). The number of participants analysed displays the number of participants with available data at the timepoints of interest.

Tmax

Time from dosing to maximum measured concentration (tmax) of Deleobuvir determined after the first dose.

AUC0-τ

Area under the concentration-time curve of Deleobuvir in plasma over the interval 0 hour (h) to the next dose of trial medication (AUC0-τ) measured after first administration of trial drug.

Cmax,ss

The maximum measured concentration of Deleobuvir in plasma at steady state after the last dose of study drug (Cmax,ss). more detailed time frame information: 5 minutes (min) prior to the first dose of study medication of Day 5 (-0:05) and 0:30, 1:00, 2:00, 3:00*, 4:00, 6:00, 8:00*, 10:00, 12:00, 16:00, 24:00, 48:00 h thereafter; Assigned to the planned time points 95:55, 96:30, 97:00, 98:00 99:00*, 100:00, 102:00, 104:00*, 106:00, 108:00, 112:00, 120:00, 144:00 h (*At these time points, in patients with cirrhosis only)

Cmin,ss

The minimum measured concentration of Deleobuvir in plasma at steady state (Cmin,ss). more detailed time frame information: 5 minutes (min) prior to the first dose of study medication of Day 5 (-0:05) and 0:30, 1:00, 2:00, 3:00*, 4:00, 6:00, 8:00*, 10:00, 12:00, 16:00, 24:00, 48:00 h thereafter; Assigned to the planned time points 95:55, 96:30, 97:00, 98:00 99:00*, 100:00, 102:00, 104:00*, 106:00, 108:00, 112:00, 120:00, 144:00 h (*At these time points, in patients with cirrhosis only). The number of participants analysed displays the number of participants with available data at the timepoints of interest.

Tmax,ss

Time from dosing to the maximum measured concentration of Deleobuvir at steady state after the last dose of study drug (tmax,ss) more detailed time frame information: 5 minutes (min) prior to the first dose of study medication of Day 5 (-0:05) and 0:30, 1:00, 2:00, 3:00*, 4:00, 6:00, 8:00*, 10:00, 12:00, 16:00, 24:00, 48:00 h thereafter; Assigned to the planned time points 95:55, 96:30, 97:00, 98:00 99:00*, 100:00, 102:00, 104:00*, 106:00, 108:00, 112:00, 120:00, 144:00 h (*At these time points, in patients with cirrhosis only)

AUCτ,ss

Area under the concentration-time curve of Deleobuvir in plasma at steady state over a uniform dosing interval τ (AUCτ,ss) measured after last dose of trial drug. more detailed time frame information: 5 minutes (min) prior to the first dose of study medication of Day 5 (-0:05) and 0:30, 1:00, 2:00, 3:00*, 4:00, 6:00, 8:00*, 10:00, 12:00, 16:00, 24:00, 48:00 h thereafter; Assigned to the planned time points 95:55, 96:30, 97:00, 98:00 99:00*, 100:00, 102:00, 104:00*, 106:00, 108:00, 112:00, 120:00, 144:00 h (*At these time points, in patients with cirrhosis only). The number of participants analysed displays the number of participants with available data at the timepoints of interest.

AUC0-∞,ss

Area under the concentration-time curve of Deleobuvir in plasma over the interval 0 hour (h) extrapolated to infinity at steady state (AUC0-∞,ss) measured after last administration of trial drug. more detailed time frame information: 5 minutes (min) prior to the first dose of study medication of Day 5 (-0:05) and 0:30, 1:00, 2:00, 3:00*, 4:00, 6:00, 8:00*, 10:00, 12:00, 16:00, 24:00, 48:00 h thereafter; Assigned to the planned time points 95:55, 96:30, 97:00, 98:00 99:00*, 100:00, 102:00, 104:00*, 106:00, 108:00, 112:00, 120:00, 144:00 h (*At these time points, in patients with cirrhosis only). The number of participants analysed displays the number of participants with available data at the timepoints of interest.

λz,ss

Terminal rate of Deleobuvir constant in plasma at steady state (λz,ss) measured after last dose of study drug. more detailed time frame information: 5 minutes (min) prior to the first dose of study medication of Day 5 (-0:05) and 0:30, 1:00, 2:00, 3:00*, 4:00, 6:00, 8:00*, 10:00, 12:00, 16:00, 24:00, 48:00 h thereafter; Assigned to the planned time points 95:55, 96:30, 97:00, 98:00 99:00*, 100:00, 102:00, 104:00*, 106:00, 108:00, 112:00, 120:00, 144:00 h (*At these time points, in patients with cirrhosis only). The number of participants analysed displays the number of participants with available data at the timepoints of interest.

t1/2,ss

Terminal half-life of Deleobuvir in plasma at steady state (t1/2,ss) measured after the last dose of study drug. more detailed time frame information: 5 minutes (min) prior to the first dose of study medication of Day 5 (-0:05) and 0:30, 1:00, 2:00, 3:00*, 4:00, 6:00, 8:00*, 10:00, 12:00, 16:00, 24:00, 48:00 h thereafter; Assigned to the planned time points 95:55, 96:30, 97:00, 98:00 99:00*, 100:00, 102:00, 104:00*, 106:00, 108:00, 112:00, 120:00, 144:00 h (*At these time points, in patients with cirrhosis only). The number of participants analysed displays the number of participants with available data at the timepoints of interest.

CL/F,ss

Apparent clearance of Deleobuvir in plasma after oral administration at steady state (CL/F,ss) measured after the last dose of study drug. more detailed time frame information: 5 minutes (min) prior to the first dose of study medication of Day 5 (-0:05) and 0:30, 1:00, 2:00, 3:00*, 4:00, 6:00, 8:00*, 10:00, 12:00, 16:00, 24:00, 48:00 h thereafter; Assigned to the planned time points 95:55, 96:30, 97:00, 98:00 99:00*, 100:00, 102:00, 104:00*, 106:00, 108:00, 112:00, 120:00, 144:00 h (*At these time points, in patients with cirrhosis only). The number of participants analysed displays the number of participants with available data at the timepoints of interest.

Vz/F,ss

Apparent volume of Deleobuvir distribution during the terminal phase λz following an oral dose at steady state (Vz/F,ss) after the last dose of study drug. more detailed time frame information: 5 minutes (min) prior to the first dose of study medication of Day 5 (-0:05) and 0:30, 1:00, 2:00, 3:00*, 4:00, 6:00, 8:00*, 10:00, 12:00, 16:00, 24:00, 48:00 h thereafter; Assigned to the planned time points 95:55, 96:30, 97:00, 98:00 99:00*, 100:00, 102:00, 104:00*, 106:00, 108:00, 112:00, 120:00, 144:00 h (*At these time points, in patients with cirrhosis only). The number of participants analysed displays the number of participants with available data at the timepoints of interest.

Plasma Concentration Time Profiles

Individual drug plasma concentrations of Deleobuvir after multiple oral administration. Within the categories PTM means planned time. The number of participants analysed displays the number of participants included in the analysis data set whereas the number of participants for each timepoint displays the number of participants with available data at that timepoint. Below the limit of quantification (BLQ) is abbreviated.

Number of Patients With Clinically Significant Changes in Vital Signs (Pulse Rate, Systolic and Diastolic Blood Pressure).

Number of patients with clinically significant changes in vital signs (pulse rate, systolic and diastolic blood pressure) presents the number of patients with an reported adverse event which has a symptom in changes in vital signs. Vascular disorders was identified as changes in vital signs. The number of participant with vascular disorders is presented in this outcome measure

Number of Patients With Abnormal Findings in 12-lead ECG (Electrocardiogram)

Number of patients with a new onset of an abnormal finding by central assessment are presented.

Number of Patients With Abnormal Changes in Laboratory Tests

Number of patients with abnormal changes in safety laboratory tests including urine protein diagnostics, and adrenocorticotropic hormone (ACTH) and cortisol measurements resulted in adverse events.

Number of Patients With Adverse Events

Number of patients with any adverse event (AE)

Number of Patients With Abnormal Findings in Physical Examination

The number of patients with abnormal findings in physical examination presents the number of patients with any treatment-emergent adverse events in this study.

Assessment of Global Tolerability on a 4-point Scale

The global tolerability was presented on a four item scale: good, satisfactory, not satisfactory and bad. Rating was done by the investigator.

Body Temperature

The body temperature will be presented as the mean values in visit 1 and visit 7. The number of participants analysed displays the number of participants included in the analysis set whereas the numbers for each timepoint display the number of participants with available data at that timepoint.

Full Information

NCT ID

NCT02176525

First Posted

June 26, 2014

Last Updated

April 28, 2016

Sponsor

Boehringer Ingelheim

1. Study Identification

Unique Protocol Identification Number

NCT02176525

Brief Title

Multiple Oral Doses of BI 207127 NA in Treatment naïve and Treatment-experienced Hepatitis C Virus (HCV)-Infected Patients

Official Title

Safety, Antiviral Activity, and Pharmacokinetics of Multiple Oral Doses of BI 207127 NA Administered q8H for 5 Days as Monotherapy, a Randomised, Double-blind, Placebo Controlled Study

Study Type

Interventional

2. Study Status

Record Verification Date

April 2016

Overall Recruitment Status

Completed

Study Start Date

December 2007 (undefined)

Primary Completion Date

December 2009 (Actual)

Study Completion Date

undefined (undefined)

3. Sponsor/Collaborators

Responsible Party, by Official Title

Sponsor

Name of the Sponsor

Boehringer Ingelheim

4. Oversight

5. Study Description

Brief Summary

The purpose of this study was to investigate antiviral activity, safety and pharmacokinetics of 5 days of monotherapy with BI 207127 in HCV genotype 1 (GT1) infected patients. Both treatment-naïve patients and patients previously treated with peginterferon and ribavirin were included. In addition, the effect of study medication was examined in a group of patients with liver cirrhosis.

6. Conditions and Keywords

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

Hepatitis C, Chronic

7. Study Design

Primary Purpose

Treatment

Study Phase

Phase 1

Interventional Study Model

Parallel Assignment

Masking

Double

Allocation

Randomized

Enrollment

75 (Actual)

8. Arms, Groups, and Interventions

Arm Title

BI 207127 in patients with cirrhosis

Arm Type

Experimental

Arm Description

multiple rising doses

Arm Title

BI 207127 in patients without cirrhosis

Arm Type

Experimental

Arm Description

multiple rising doses

Arm Title

Placebo in patients without cirrhosis

Arm Type

Placebo Comparator

Intervention Type

Drug

Intervention Name(s)

BI 207127 NA

Intervention Type

Drug

Intervention Name(s)

Placebo

Primary Outcome Measure Information:

Title

Virologic Response (VR)

Description

Time Frame

Baseline (Visit 2_2 at planned time 5 minutes prior to first administration of trial drug), up to day 5

Secondary Outcome Measure Information:

Title

Time Dependent Change From Baseline in Viral Load (VL)

Description

Time Frame

Baseline, up to day 7

Title

Cmax

Description

Maximum measured concentration of Deleobuvir in plasma (Cmax) determined after the first dose.

Time Frame

5 minutes (min) prior to the first dose of study medication and 30 minutes and 1:00, 2:00, 3:00, 4:00, 6:00, 7:55, 10:00, 12:00, 15:55, 18:00 hours (h) thereafter on day 1

Title

Cmin

Description

Time Frame

5 minutes (min) prior to the first dose of study medication and 30 minutes and 1:00, 2:00, 3:00, 4:00, 6:00, 7:55, 10:00, 12:00, 15:55, 18:00 hours (h) thereafter on day 1

Title

Tmax

Description

Time from dosing to maximum measured concentration (tmax) of Deleobuvir determined after the first dose.

Time Frame

5 minutes (min) prior to the first dose of study medication and 30 minutes and 1:00, 2:00, 3:00, 4:00, 6:00, 7:55, 10:00, 12:00, 15:55, 18:00 hours (h) thereafter on day 1

Title

AUC0-τ

Description

Area under the concentration-time curve of Deleobuvir in plasma over the interval 0 hour (h) to the next dose of trial medication (AUC0-τ) measured after first administration of trial drug.

Time Frame

5 minutes (min) prior to the first dose of study medication and 30 minutes and 1:00, 2:00, 3:00, 4:00, 6:00, 7:55, 10:00, 12:00, 15:55, 18:00 hours (h) thereafter on day 1

Title

Cmax,ss

Description

Time Frame

5 min prior to the first dose of study medication of Day 5; 0:30, 1:00, 2:00, 3:00*, 4:00, 6:00, 8:00*, 10:00, 12:00, 16:00, 24:00, 48:00, 95:55, 96:30, 97:00, 98:00 99:00*, 100:00, 102:00, 104:00*, 106:00, 108:00, 112:00, 120:00, 144:00 h thereafter

Title

Cmin,ss

Description

Time Frame

Title

Tmax,ss

Description

Time Frame

Title

AUCτ,ss

Description

Time Frame

Title

AUC0-∞,ss

Description

Time Frame

Title

λz,ss

Description

Time Frame

Title

t1/2,ss

Description

Time Frame

Title

CL/F,ss

Description

Time Frame

Title

Vz/F,ss

Description

Time Frame

Title

Plasma Concentration Time Profiles

Description

Time Frame

up to day 7

Title

Number of Patients With Clinically Significant Changes in Vital Signs (Pulse Rate, Systolic and Diastolic Blood Pressure).

Description

Time Frame

Baseline, up to day 14

Title

Number of Patients With Abnormal Findings in 12-lead ECG (Electrocardiogram)

Description

Number of patients with a new onset of an abnormal finding by central assessment are presented.

Time Frame

up to 14 days

Title

Number of Patients With Abnormal Changes in Laboratory Tests

Description

Number of patients with abnormal changes in safety laboratory tests including urine protein diagnostics, and adrenocorticotropic hormone (ACTH) and cortisol measurements resulted in adverse events.

Time Frame

Baseline, up to day 14

Title

Number of Patients With Adverse Events

Description

Number of patients with any adverse event (AE)

Time Frame

up to 14 days

Title

Number of Patients With Abnormal Findings in Physical Examination

Description

The number of patients with abnormal findings in physical examination presents the number of patients with any treatment-emergent adverse events in this study.

Time Frame

up to day 14

Title

Assessment of Global Tolerability on a 4-point Scale

Description

The global tolerability was presented on a four item scale: good, satisfactory, not satisfactory and bad. Rating was done by the investigator.

Time Frame

day 6

Title

Body Temperature

Description

Time Frame

Visit 1, Visit 7

10. Eligibility

Sex

All

Minimum Age & Unit of Time

18 Years

Maximum Age & Unit of Time

70 Years

Accepts Healthy Volunteers

Eligibility Criteria

Inclusion Criteria: Adults from 18 - 70 years Male OR female with documented hysterectomy OR menopausal female with last menstrual period at least 12 months prior to screening Written informed consent consistent with International Conference on Harmonization/Good Clinical Practice and local legislation given prior to any study procedures Chronic HCV infection demonstrated by positive HCV immunoglobulin G Antibody HCV genotype 1 which has to be confirmed by central laboratory test before Visit 2 For non-cirrhotic cohorts: Liver biopsy obtained within the last 36 months consistent with HCV infection showing minimal to mild liver fibrosis and without cirrhosis (Ishak or Metavir grade ≤ 2). For cirrhotic cohorts, previous liver biopsy or Fibroscan consistent with liver cirrhosis performed at any time before screening HCV RNA load > 100,000 IU RNA per ml serum at screening Exclusion Criteria: All fertile males not willing to use an adequate form of contraception (condom, sterilisation at least 6 months post operation) in case their partner is of childbearing potential and is not using an adequate form of contraception (hormonal contraceptives, oral or injectable/ implantable, intra-uterine device) Patients who have been treated with at least one dose of any HCV-polymerase inhibitor for acute or chronic hepatitis C infection Any other or additional plausible cause for chronic liver disease, including the presence of other viruses known or suspected to cause hepatitis Decompensated liver disease within past 12 months, as indicated by variceal bleeding, ascites, encephalopathy, Prothrombin or International Normalized Ratio (INR) prolonged to >1.7 x upper limit of normal (ULN), serum bilirubin > 2 mg/dl or albumin < 3.5 g/dl (i.e. Child-Pugh grade B, score > 7) For non-cirrhotic cohorts: Any previous liver biopsy consistent with cirrhosis. For cirrhotic cohorts: Any liver biopsy or fibroscan result from last 2 years excluding liver cirrhosis. Positive test for human immunodeficiency virus (HIV) or hepatitis B antigen at screening Current alcohol or drug abuse, or history of the same, within the past six (6) months. Exception: Occasional use of cannabis is not an exclusion criterion. The investigator must however instruct the patient that consumption of cannabis is not allowed during the treatment period. Any concurrent disease (cardiovascular, pulmonary, renal, haematological, neurological, psychiatric, immunologic, metabolic or endocrine dysfunction) if clinically significant based on the investigator's medical assessment at screening. A clinically significant disease is defined as one which in the opinion of the investigator may either put the patient at risk because of participation in the study or may influence the results of the study or the patient's ability to participate in the study. Exclusion is also necessary for any pre-existing cardiac abnormality by history. Clinically significant abnormalities at screening ECG, including but not limited to a QTc longer than 435 msec, Pulse Rate > 240 msec at baseline and any bundle branch block pattern, but not necessarily non-specific T wave abnormalities History of malignancy (except for previously cured squamous cell or basal cell carcinoma) Patients treated with any interferon (IFN) (approved or investigational) or Peg-IFN and/or Ribavirin within 3 months prior to screening Planned or concurrent usage of any other pharmacological therapy including any antiviral therapy or vaccination from 7 days before treatment and during treatment Usage of any investigational drug within thirty (30) days prior to enrolment or 5 halflives, whichever is longer; or the planned usage of an investigational drug during the course of the current study Known hypersensitivity to drugs or excipients Patients with any one of the following laboratory values at screening: Alanine transaminase (ALT) > 3x ULN, local lab Aspartate aminotransferase (AST) > 3x ULN, local lab Total bilirubin > 1.5x ULN, local lab, unless predominantly conjugated and reflecting Gilbert's disease Alkaline phosphatase > 1.5x ULN, local lab Prothrombin time (INR) > 1.5x ULN, central lab Creatinine > 1x ULN, local lab Urine protein / creatinine ratio > 0.3 g protein / g creatinine, central lab Alpha-1-microglobulin / creatinine in urine > 1x ULN, central lab Platelet count < 100,000 / mm3, central lab White Blood cell count < 2000 cells/mm3, central lab Absolute neutrophile count < 1500 cells, central lab Hemoglobin < 12 g/dL, central lab For patients with liver cirrhosis: ALT > 5x ULN, local lab AST > 5x ULN, local lab Platelet count < 70,000 / mm3, central lab Patients with any clinically significant laboratory abnormalities based on the investigator's medical assessment at screening Positive urine test for drug abuse at screening Prior randomisation into this trial Inability to comply with the protocol Patients with ongoing or historical photosensitivity or recurrent rash Alpha fetoprotein value (AFP) > 100 ng/ml; if AFP is > 20 and ≤ 100 ng/ml, patients can be included if liver cancer is excluded by a current imaging study (i.e. ultrasound, computer tomography scan or magnetic resonance imaging)

12. IPD Sharing Statement

Links:

URL

http://trials.boehringer-ingelheim.com

Description

Learn more about this trial

Multiple Oral Doses of BI 207127 NA in Treatment naïve and Treatment-experienced Hepatitis C Virus (HCV)-Infected Patients

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