- ICH GCP
- Registre américain des essais cliniques
- Essai clinique NCT00724893
Efficacy of Pegetron® Redipen™ Treatment and Treatment Compliance of Patients With Chronic Hepatitis C in Canada (P04423)
20 juillet 2015 mis à jour par: Merck Sharp & Dohme LLC
Pegetron® Redipen™ Prospective Optimal Weight-based Dosing Response Program
Treatment compliance is a key success factor in obtaining the full benefit of Pegetron (peginterferon alfa-2b [PegIFN-2b] plus ribavirin combination) therapy for patients.
Treatment-naïve patients with chronic hepatitis C (CHC) in Canada to whom Pegetron Redipen was prescribed will receive Pegetron Redipen therapy in accordance with approved labeling.
The study will assess the effect of the newly approved Pegetron Redipen on treatment compliance and its effect on sustained virologic response rates.
Sustained virologic response is defined as negative hepatitis C virus ribonucleic acid (HCV-RNA) six months post-treatment.
Aperçu de l'étude
Statut
Complété
Les conditions
Intervention / Traitement
Type d'étude
Observationnel
Inscription (Réel)
2430
Critères de participation
Les chercheurs recherchent des personnes qui correspondent à une certaine description, appelée critères d'éligibilité. Certains exemples de ces critères sont l'état de santé général d'une personne ou des traitements antérieurs.
Critère d'éligibilité
Âges éligibles pour étudier
18 ans et plus (Adulte, Adulte plus âgé)
Accepte les volontaires sains
Non
Sexes éligibles pour l'étude
Tout
Méthode d'échantillonnage
Échantillon de probabilité
Population étudiée
Treatment-naïve patients with chronic hepatitis C undergoing treatment with Pegetron Redipen at approximately 100 centers in Canada.
La description
Inclusion Criteria:
- Treatment-naïve patients with chronic hepatitis C
- Adults (>18 years of age)
- Prescribed Pegetron Redipen
- Must meet all requirements for treatment with Pegetron Redipen
- Must be able to obtain reimbursement of medication through private or provincial coverage
Exclusion Criteria:
- Active hepatitis B virus (HBV) infection (hepatitis B surface antigen [HBsAg] positive)
- HIV antibody positive
- Post liver transplant patients
- Any other exclusion criteria as per the product Monograph
Plan d'étude
Cette section fournit des détails sur le plan d'étude, y compris la façon dont l'étude est conçue et ce que l'étude mesure.
Comment l'étude est-elle conçue ?
Détails de conception
- Modèles d'observation: Cohorte
- Perspectives temporelles: Éventuel
Cohortes et interventions
Groupe / Cohorte |
Intervention / Traitement |
---|---|
Stage 1 Participants
Participants with CHC receiving PegIFN-2b using Redipen™ formulation (1.5 mcg/kg) once weekly and ribavirin capsules (800-1400 mg) daily according to routine medical practice at participating study sites.
|
PegIFN-2b powder for solution adminstered subcutaneously using the newly approved Redipen.
Dosing per approved labeling
Autres noms:
Ribavirin capsules administered orally.
Dosing in accordance with approved labelling.
Autres noms:
|
Stage 2 Participants
Participants with CHC Genotype 1 receiving PegIFN-2b using Redipen™ formulation (1.5 mcg/kg) once weekly and ribavirin capsules (800-1400 mg) daily according to routine medical practice at participating study sites.
|
PegIFN-2b powder for solution adminstered subcutaneously using the newly approved Redipen.
Dosing per approved labeling
Autres noms:
Ribavirin capsules administered orally.
Dosing in accordance with approved labelling.
Autres noms:
|
Que mesure l'étude ?
Principaux critères de jugement
Mesure des résultats |
Description de la mesure |
Délai |
---|---|---|
Number of Participants Achieving Viral Response at Any Evaluation Point (Stage 1)
Délai: Up to 72 weeks
|
This is a measure of the number of participants achieving a viral response (negative hepatitis C virus ribonucleic acid [HCV-RNA]) at either of the follow-up evaluation time points (12 weeks [window 10-14 weeks] or ≥22 weeks after the end of treatment (EOT).
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Number of Participants Achieving Viral Response at 12 Weeks After EOT (Stage 1)
Délai: Up to 62 weeks
|
This is a measure of the number of participants achieving a viral response (negative HCV-RNA) at 12 weeks (window 10-14 weeks) after EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 62 weeks
|
Number of Participants Achieving Sustained Viral Response (SVR) (Stage 1)
Délai: Up to 72 weeks
|
This is a measure of the number of participants who achieved SVR, defined as HCV-RNA negative at ≥22 weeks after EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Number of Participants Achieving SVR (Stage 2)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at six months after EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Mesures de résultats secondaires
Mesure des résultats |
Description de la mesure |
Délai |
---|---|---|
Number of Participants Discontinued From Study Treatment Due to Adverse Events (Stage 1 and Stage 2)
Délai: Up to 48 weeks
|
An adverse event is any unfavorable and unintended change in the structure, function, or chemistry of the body whether or not considered related to the study treatment
|
Up to 48 weeks
|
Number of Participants Achieving Viral Response at Any Evaluation Point, Excluding Participants Who Discontinued Treatment Prior to Early Virologic Response (EVR) Evaluation (Stage 1)
Délai: Up to 72 weeks
|
Viral response was defined as negative HCV-RNA.
EVR was defined as either HCV-RNA detectable with a ≥2 log reduction from baseline or HCV-RNA negative at Treatment Week 12. Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Number of Participants Achieving Viral Response at 12 Weeks After EOT, Excluding Participants Who Discontinued Prior to EVR Evaluation (Stage 1)
Délai: Up to 62 weeks
|
Viral response was defined as negative HCV-RNA.
EVR was defined as either HCV-RNA detectable with a ≥2 log reduction from baseline or HCV-RNA negative at Treatment Week 12. Participants with no viral response information were considered viral response "no".
|
Up to 62 weeks
|
Number of Participants Achieving SVR, Excluding Participants Who Discontinued Prior to EVR Evaluation (Stage 1)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at ≥22 weeks after EOT.
EVR was defined as either HCV-RNA detectable with a ≥2 log reduction from baseline or HCV-RNA negative at Treatment Week 12. Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
The Number of Participants Achieving Viral Response at 12 Weeks After EOT, Excluding Participants Who Discontinued Prior to EVR Evaluation and Participants With Missing Data (Stage 1)
Délai: Up to 62 weeks
|
Viral response was defined as negative HCV-RNA; evaluation was done 12 weeks (window 10-14 weeks) after EOT.
EVR was defined as either HCV-RNA detectable with a ≥2 log reduction from baseline or HCV-RNA negative at Treatment Week 12. Participants with no viral response information were considered viral response "no".
|
Up to 62 weeks
|
The Number of Participants Achieving SVR Excluding Participants Who Discontinued Prior to EVR Evaluation and Participants With Missing Data (Stage 1)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at ≥22 weeks after EOT.
EVR was defined as either HCV-RNA detectable with a ≥2 log reduction from baseline or HCV-RNA negative at Treatment Week 12. Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
The Number of Participants Achieving Viral Response at 12 Weeks After EOT by Chronic HCV Genotype (Stage 1)
Délai: Up to 62 weeks
|
Viral response was defined as negative HCV-RNA; evaluation was done 12 weeks (window 10-14 weeks) after EOT.
Participants with no viral response information were considered viral response "no".
For this analysis participants were grouped by their HCV genotype (Types 1-6); a genotype is a classification based on the differences in the genetic material within the hepatitis virus.
Knowing the HCV genotype helps with deciding what type and what duration of treatment will be needed because each genotype demonstrates a different response to treatment in infected individuals.
|
Up to 62 weeks
|
The Number of Participants Achieving Viral Response at 12 Weeks After EOT by Liver Fibrosis Stage (Stage 1)
Délai: Up to 62 weeks
|
Viral response was defined as negative HCV-RNA; evaluation was done 12 weeks (window 10-14 weeks) after EOT.
Participants with no viral response information were considered viral response "no".
Liver fibrosis stage was measured with the METAVIR scoring system (F0=no fibrosis or liver damage, F1 = beginning of liver damage with some slight scarring, F2 = moderate liver damage, scarring advancing in liver and surrounding blood vessels, F3 =significant liver damage, the liver becomes fibrotic [scarred] and connects with other scarred areas, and F4 = severe damage [cirrhosis] and liver no longer functions properly).
|
Up to 62 weeks
|
Number of Participants Achieving SVR by Liver Fibrosis Stage (Stage 1)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at ≥22 weeks after EOT.
Participants with no viral response information were considered viral response "no".
Liver fibrosis stage was measured with the METAVIR scoring system (F0=no fibrosis or liver damage, F1 = beginning of liver damage with some slight scarring, F2 = moderate liver damage, scarring advancing in liver and surrounding blood vessels, F3 = significant liver damage, the liver is fibrotic [scarred] and connects with other scarred areas, and F4 = severe damage [cirrhosis] and liver no longer functions properly).
|
Up to 72 weeks
|
Number of Participants Achieving SVR by Chronic HCV Genotype (Stage 1)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at ≥22 weeks following EOT.
Participants with no viral response information were considered viral response "no".
For this analysis participants were grouped by their HCV genotype (Types 1-6); a genotype is a classification based on the differences in the genetic material within the hepatitis virus.
Knowing the HCV genotype helps with deciding what type and what duration of treatment will be needed because each genotype demonstrates a different response to treatment in infected individuals.
|
Up to 72 weeks
|
Number of Participants Achieving SVR by Viral Load (Stage 1)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at ≥22 weeks after EOT.
Participants with no viral response information were considered viral response "no".
Viral load categories were defined as High (≥100,000 Iu/mL) or Low (<100,000 Iu/mL).
|
Up to 72 weeks
|
Number of Participants Achieving SVR by Weight (Stage 1)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at ≥22 weeks after EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Number of Participants Achieving SVR by Chronic HCV Genotype + Liver Fibrosis Stage (Stage 1)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at ≥22 weeks after EOT.
Participants with no viral response information were considered viral response "no".
Liver fibrosis stage was measured with the METAVIR scoring system (F0=no fibrosis or liver damage, F1 = beginning of liver damage with some slight scarring, F2 = moderate liver damage, scarring advancing in liver and surrounding blood vessels, F3 =significant liver damage, the liver becomes fibrotic [scarred] and connects with other scarred areas, and F4 = severe damage [cirrhosis] and liver no longer functions properly).
For this analysis participants were grouped by their HCV genotype (Types 1-6); a genotype is a classification based on the differences in the genetic material within the hepatitis virus.
Knowing the HCV genotype helps with deciding what type and what duration of treatment will be needed because each genotype demonstrates a different response to treatment in infected individuals.
|
Up to 72 weeks
|
Number of Participants Achieving SVR by Chronic HCV Genotype + Viral Load (Stage 1)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at ≥22 weeks after EOT.
Participants with no viral response information were considered viral response "no".
Viral load categories were defined as High (≥100,000 Iu/mL) or Low (<100,000 Iu/mL).
For this analysis participants were grouped by their HCV genotype (Types 1-6); a genotype is a classification based on the differences in the genetic material within the hepatitis virus.
Knowing the HCV genotype helps with deciding what type and what duration of treatment will be needed because each genotype demonstrates a different response to treatment in infected individuals.
|
Up to 72 weeks
|
Number of Participants Achieving SVR by Weight + Chronic HCV Genotype (Stage 1)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at ≥22 weeks after EOT.
Participants with no viral response information were considered viral response "no".
For this analysis participants were grouped by their HCV genotype (Types 1-6); a genotype is a classification based on the differences in the genetic material within the hepatitis virus.
Knowing the HCV genotype helps with deciding what type and what duration of treatment will be needed because each genotype demonstrates a different response to treatment in infected individuals.
|
Up to 72 weeks
|
Number of Participants Achieving EVR (Stage 1)
Délai: From Week 10 to Week 14
|
EVR was defined as either HCV-RNA detectable with a ≥2 log reduction from baseline or HCV-RNA negative after 12 weeks of treatment.
Participants with no viral response information were considered viral response "no".
|
From Week 10 to Week 14
|
Number of Participants Achieving SVR by EVR Type (Stage 1)
Délai: Up to 72 weeks
|
EVR was defined as either HCV-RNA detectable with a ≥2 log reduction from baseline or HCV-RNA negative after 12 weeks of treatment.
SVR was defined as HCV-RNA negative at ≥22 weeks after EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Number of Participants Achieving SVR by Gender (Stage 1)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at ≥22 weeks after EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Number of Participants Achieving SVR by Race (Stage 1)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at ≥22 weeks after EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Number of Participants Achieving SVR by Human Immunodeficiency Virus (HIV) Status (Stage 1)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at ≥22 weeks after EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Number of Participants With End of Treatment (EOT) Response (Stage 1)
Délai: Up to 48 weeks
|
EOT response was defined as HCV-RNA negative after 24 weeks of treatment in participants with HCV Genotype 2 or 3, and after 48 weeks of treatment in participants with Genotype 1, 4, 5, or 6.
If there was no EOT information or if it was marked as "not done" then EOT was set to "no".
|
Up to 48 weeks
|
Number of Participants With EOT Response by Chronic HCV Genotype (Stage 1)
Délai: Up to 72 weeks
|
EOT response was defined as HCV-RNA negative after 24 weeks of treatment in participants with HCV-RNA Genotype 2 or 3, and after 48 weeks of treatment in participants with Genotype 1, 4, 5, or 6.
If there was no EOT information or if it was marked as "not done" then EOT was set to "no".
For this analysis participants were grouped by their HCV genotype (Types 1-6); a genotype is a classification based on the differences in the genetic material within the hepatitis virus.
Knowing the HCV genotype helps with deciding what type and what duration of treatment will be needed because each genotype demonstrates a different response to treatment in infected individuals.
|
Up to 72 weeks
|
Number of Participants With EVR by Selected Chronic HCV Genotypes (Stage 1)
Délai: Week 12
|
EVR was defined as either HCV-RNA detectable with a ≥2 log reduction from baseline or HCV-RNA negative at TW12.
Participants with no viral response information were considered viral response "no".
For this analysis participants were grouped by their HCV genotype (Types 1-6); a genotype is a classification based on the differences in the genetic material within the hepatitis virus.
Knowing the HCV genotype helps with deciding what type and what duration of treatment will be needed because each genotype demonstrates a different response to treatment in infected individuals.
|
Week 12
|
Relapse Rate by HCV Genotype (Stage 1)
Délai: Up to 48 weeks
|
The relapse rate was calculated with these parameters: EOT "yes", EVR evaluation valid, and ≥22 weeks of follow-up data.
There were no imputations for EOT or SVR.
Participants with no viral response information were considered viral response "no".
For this analysis participants were grouped by their HCV genotype (Types 1-6); a genotype is a classification based on the differences in the genetic material within the hepatitis virus.
Knowing the HCV genotype helps with deciding what type and what duration of treatment will be needed because each genotype demonstrates a different response to treatment in infected individuals.
|
Up to 48 weeks
|
Number of Participants Discontinued From Study Drug Due to Adverse Events by Chronic HCV Genotype (Stage 1)
Délai: Up to 48 weeks
|
An adverse event is any unfavorable and unintended change in the structure, function, or chemistry of the body whether or not considered related to the study treatment.
For this analysis participants were grouped by their HCV genotype (Types 1-6); a genotype is a classification based on the differences in the genetic material within the hepatitis virus.
Knowing the HCV genotype helps with deciding what type and what duration of treatment will be needed because each genotype demonstrates a different response to treatment in infected individuals.
|
Up to 48 weeks
|
Number of Participants Achieving Rapid Virologic Response (RVR) (Stage 2)
Délai: Week 4
|
RVR was defined as undetectable HCV-RNA after 4 weeks of treatment (window of 2 to 6 weeks).
Participants with no viral response information were considered viral response "no".
|
Week 4
|
Number of Participants Achieving EVR (Stage 2)
Délai: Week 12
|
EVR was defined as either HCV-RNA undetectable with a ≥2 log reduction in HCV-RNA from baseline or HCV-RNA undetectable after 12 weeks of treatment.
Participants with no viral response information were considered viral response "no".
|
Week 12
|
Number of Participants Achieving RVR by Race (Stage 2)
Délai: Week 4
|
RVR was defined as undetectable HCV-RNA after 4 weeks of treatment (window of 2 to 6 weeks).
Participants with no viral response information were considered viral response "no".
|
Week 4
|
Number of Participants Achieving EVR by Race (Stage 2)
Délai: Week 12
|
EVR was defined as either HCV-RNA undetectable with a ≥2 log reduction in HCV-RNA from baseline or HCV-RNA undetectable after 12 weeks of treatment.
Participants with no viral response information were considered viral response "no".
|
Week 12
|
Number of Participants Achieving SVR by Race (Stage 2)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at six months after EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Number of Participants Achieving RVR Who Achieved SVR (Stage 2)
Délai: Week 4
|
RVR was defined as undetectable HCV-RNA after four weeks of treatment.
SVR was defined as HCV-RNA negative at 24 weeks after EOT.
Participants with no viral response information were considered viral response "no".
|
Week 4
|
Number of Participants Achieving EVR Who Achieved SVR (Stage 2)
Délai: Week 12
|
EVR was defined as either HCV-RNA undetectable with a ≥2 log reduction in HCV-RNA from baseline or HCV-RNA undetectable after 12 weeks of treatment.
SVR was defined as HCV-RNA negative at 24 weeks after EOT.
Participants with no viral response information were considered viral response "no".
|
Week 12
|
Number of Participants Achieving RVR by Liver Fibrosis Stage (Stage 2)
Délai: Week 4
|
RVR was defined as undetectable HCV-RNA after four weeks of treatment.
SVR was defined as HCV-RNA negative at 24 weeks after EOT.
Participants with no viral response information were considered viral response "no".
Liver fibrosis stage was measured with the METAVIR scoring system (F0=no fibrosis or liver damage, F1 = beginning of liver damage with some slight scarring, F2 = moderate liver damage, scarring advancing in liver and surrounding blood vessels, F3 =significant liver damage, the liver becomes fibrotic [scarred] and connects with other scarred areas , and F4 = severe damage [cirrhosis] and liver no longer functions properly).
|
Week 4
|
Number of Participants Achieving EVR by Liver Fibrosis Stage (Stage 2)
Délai: Week 12
|
EVR was defined as either HCV-RNA undetectable with a ≥2 log reduction in HCV-RNA from baseline or HCV-RNA undetectable after 12 weeks of treatment.SVR was defined as HCV-RNA negative at 24 weeks after EOT.
Participants with no viral response information were considered viral response "no".
Liver fibrosis stage was measured with the METAVIR scoring system (F0=no fibrosis or liver damage, F1 = beginning of liver damage with some slight scarring, F2 = moderate liver damage, scarring advancing in liver and surrounding blood vessels, F3 =significant liver damage, the liver becomes fibrotic [scarred] and connects with other scarred areas , and F4 = severe damage [cirrhosis] and liver no longer functions properly).
|
Week 12
|
Number of Participants Achieving SVR by Liver Fibrosis Score (Stage 2)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at 24 weeks after EOT.
Participants with no viral response information were considered viral response "no".
Liver fibrosis stage was measured with the METAVIR scoring system (F0=no fibrosis or liver damage, F1 = beginning of liver damage with some slight scarring, F2 = moderate liver damage, scarring advancing in liver and surrounding blood vessels, F3 =significant liver damage, the liver becomes fibrotic [scarred] and connects with other scarred areas , and F4 = severe damage [cirrhosis] and liver no longer functions properly).
|
Up to 72 weeks
|
Number of Participants Achieving RVR by Weight (Stage 2)
Délai: Week 4
|
RVR was defined as undetectable HCV-RNA after 4 weeks of treatment.
Participants with no viral response information were considered viral response "no".
|
Week 4
|
Number of Participants Achieving EVR by Weight (Stage 2)
Délai: Week 12
|
EVR was defined as either HCV-RNA undetectable with a ≥2 log reduction in HCV-RNA from baseline or HCV-RNA undetectable after 12 weeks of treatment.
Participants with no viral response information were considered viral response "no".
|
Week 12
|
Number of Participants Achieving SVR by Weight (Stage 2)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at 24 weeks after EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Number of Participants Achieving RVR by Chronic HCV Genotype 1 Subtype (Stage 2)
Délai: Week 4
|
RVR was defined as undetectable HCV-RNA after 4 weeks of treatment.
SVR was defined as HCV-RNA negative at 24 weeks after EOT.
Participants with no viral response information were considered viral response "no".
For this analysis participants were grouped by their HCV genotype subcategory (1a or 1b); subcategories are the result of a change in the genetic material in the viruses within the genotype.
|
Week 4
|
Number of Participants Achieving EVR by Chronic HCV Genotype 1 Subtype (Stage 2)
Délai: Week 12
|
EVR was defined as either HCV-RNA undetectable with a ≥2 log reduction in HCV-RNA from baseline or HCV-RNA undetectable after 12 weeks of treatment.SVR was defined as HCV-RNA negative at 24 weeks after EOT.
Participants with no viral response information were considered viral response "no".
For this analysis participants were grouped by their HCV genotype subcategory (1a or 1b); subcategories are the result of a change in the genetic material in the viruses within the genotype.
|
Week 12
|
Number of Participants Achieving SVR by Chronic HCV Genotype 1 Subtype (Stage 2)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at 24 weeks after EOT.
Participants with no viral response information were considered viral response "no".
For this analysis participants were grouped by their HCV genotype subcategory (1a or 1b); subcategories are the result of a change in the genetic material in the viruses within the genotype.
|
Up to 72 weeks
|
Number of Participants Achieving RVR by Gender (Stage 2)
Délai: Week 4
|
RVR was defined as undetectable HCV-RNA after 4 weeks of treatment.
Participants with no viral response information were considered viral response "no".
|
Week 4
|
Number of Participants Achieving EVR by Gender (Stage 2)
Délai: Week 12
|
EVR was defined as either HCV-RNA undetectable with a ≥2 log reduction in HCV-RNA from baseline or HCV-RNA undetectable after 12 weeks of treatment.
Participants with no viral response information were considered viral response "no".
|
Week 12
|
Number of Participants Achieving SVR by Gender (Stage 2)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at 24 weeks after EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Number of Participants Achieving RVR by HIV Status (Stage 2)
Délai: Week 4
|
RVR was defined as undetectable HCV-RNA after 4 weeks of treatment (window of 2 to 6 weeks).
Participants with no viral response information were considered viral response "no".
|
Week 4
|
Number of Participants Achieving EVR by HIV Status (Stage 2)
Délai: Week 12
|
EVR was defined as either HCV-RNA undetectable with a ≥2 log reduction in HCV-RNA from baseline or HCV-RNA undetectable after 12 weeks of treatment.
Participants with no viral response information were considered viral response "no".
|
Week 12
|
Number of Participants Achieving SVR by HIV Status (Stage 2)
Délai: Up to 72 weeks
|
SVR was defined as HCV-RNA negative at six months following EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Percentage of Compliance for Participants Achieving SVR Based on Medication Adherence Questionnaire (MAQ) (Stage 2)
Délai: Up to 72 weeks
|
Compliance was defined as participants taking ≥80% versus <80% of their doses; compliance ≥80% was derived from participants who answered "always" or "most of the time" to Questions 4 (How often do you stick to your medication schedule for your Ribavirin?) and 5 (How often do you stick to your medication schedule for your Redipen [peginterferon] injections?) of the 6-question compliance questionnaire.
Percentages are based on the total number of participants within each compliance category.
SVR was defined as HCV-RNA negative at 24 weeks after EOT.
Participants with no viral response information were considered viral response "no".
|
Up to 72 weeks
|
Collaborateurs et enquêteurs
C'est ici que vous trouverez les personnes et les organisations impliquées dans cette étude.
Parrainer
Dates d'enregistrement des études
Ces dates suivent la progression des dossiers d'étude et des soumissions de résultats sommaires à ClinicalTrials.gov. Les dossiers d'étude et les résultats rapportés sont examinés par la Bibliothèque nationale de médecine (NLM) pour s'assurer qu'ils répondent à des normes de contrôle de qualité spécifiques avant d'être publiés sur le site Web public.
Dates principales de l'étude
Début de l'étude
1 août 2005
Achèvement primaire (Réel)
1 août 2012
Achèvement de l'étude (Réel)
1 août 2012
Dates d'inscription aux études
Première soumission
25 juillet 2008
Première soumission répondant aux critères de contrôle qualité
25 juillet 2008
Première publication (Estimation)
30 juillet 2008
Mises à jour des dossiers d'étude
Dernière mise à jour publiée (Estimation)
14 août 2015
Dernière mise à jour soumise répondant aux critères de contrôle qualité
20 juillet 2015
Dernière vérification
1 juillet 2015
Plus d'information
Termes liés à cette étude
Termes MeSH pertinents supplémentaires
- Maladies du système digestif
- Infections par virus à ARN
- Maladies virales
- Infections
- Infections transmissibles par le sang
- Maladies transmissibles
- Maladies du foie
- Infections à Flaviviridae
- Hépatite, virale, humaine
- Infections à entérovirus
- Infections à Picornaviridae
- Hépatite chronique
- Hépatite
- Hépatite A
- Hépatite C
- Hépatite C chronique
- Effets physiologiques des médicaments
- Mécanismes moléculaires de l'action pharmacologique
- Agents anti-infectieux
- Agents antiviraux
- Antimétabolites
- Agents antinéoplasiques
- Facteurs immunologiques
- Interférons
- Interféron-alpha
- Ribavirine
- Interféron alpha-2
- Peginterféron alfa-2b
Autres numéros d'identification d'étude
- P04423
- MK-4031-267 (Autre identifiant: Merck Study Number)
Ces informations ont été extraites directement du site Web clinicaltrials.gov sans aucune modification. Si vous avez des demandes de modification, de suppression ou de mise à jour des détails de votre étude, veuillez contacter register@clinicaltrials.gov. Dès qu'un changement est mis en œuvre sur clinicaltrials.gov, il sera également mis à jour automatiquement sur notre site Web .
Essais cliniques sur PegIFN-2b
-
Foundation for Liver ResearchComplété
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Merck Sharp & Dohme LLCRésilié
-
Merck Sharp & Dohme LLCComplété
-
Janssen Pharmaceutical K.K.ComplétéHépatite C chroniqueJapon
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Merck Sharp & Dohme LLCRésilié
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Amsterdam UMC, location VUmcMerck Sharp & Dohme LLC; Novartis; Uppsala University HospitalRésiliéLa leucémie myéloïde chroniquePays-Bas, Danemark, Suède, Finlande, Norvège
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Suzhou Ribo Life Science Co. Ltd.Recrutement
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Merck Sharp & Dohme LLCComplétéInfections à VIH | Hépatite C | Infection par le VHC