| CTRI Number |
CTRI/2025/10/095555 [Registered on: 01/10/2025] Trial Registered Prospectively |
| Last Modified On: |
23/03/2026 |
| Post Graduate Thesis |
No |
| Type of Trial |
Interventional |
|
Type of Study
|
Drug |
| Study Design |
Randomized, Parallel Group Trial |
|
Public Title of Study
|
Chronic hepatitis C treatment with eigth weeks of Sofosobuvir-daclatasvir in people without cirrhosis |
|
Scientific Title of Study
|
Reduced duration of eight versus twelve weeks of Sofosbuvir-daclatasvir in treatment naive non-cirrhotic patients with chronic hepatitis C virus infection: An open-label, randomized pilot trial
|
| Trial Acronym |
NIL |
|
Secondary IDs if Any
|
| Secondary ID |
Identifier |
| NIL |
NIL |
|
|
Details of Principal Investigator or overall Trial Coordinator (multi-center study)
|
| Name |
Dr Amit Goel |
| Designation |
Professor and Head, Department of hepatology, SGPGIMS |
| Affiliation |
SGPGIMS lucknow |
| Address |
LTU building, 5th floor SGPGIMS , Lucknow
SGPGIMS, raebarelli road Lucknow, UP, INDIA, 226014
Lucknow
UTTAR PRADESH
226014
India |
| Phone |
9936275741 |
| Fax |
|
| Email |
agoe.ag@gmail.com |
|
Details of Contact Person
Scientific Query
|
| Name |
Dr Amit Goel |
| Designation |
Professor and Head, Department of hepatology, SGPGIMS |
| Affiliation |
SGPGIMS lucknow |
| Address |
LTU building, 5th floor SGPGIMS , Lucknow
SGPGIMS, raebarelli road Lucknow, UP, INDIA, 226014
Lucknow
UTTAR PRADESH
226014
India |
| Phone |
9936275741 |
| Fax |
|
| Email |
agoe.ag@gmail.com |
|
Details of Contact Person
Public Query
|
| Name |
Dr Amit Goel |
| Designation |
Professor and Head, Department of hepatology, SGPGIMS |
| Affiliation |
SGPGIMS lucknow |
| Address |
LTU building, 5th floor SGPGIMS , Lucknow
SGPGIMS, raebarelli road Lucknow, UP, INDIA, 226014
Lucknow
UTTAR PRADESH
226014
India |
| Phone |
9936275741 |
| Fax |
|
| Email |
agoe.ag@gmail.com |
|
|
Source of Monetary or Material Support
|
| Sanjay Gandhi Postgraduate Institute of Medical Sciences, Rae Bareili Road,Lucknow-226014, Uttar Pradesh, India |
|
|
Primary Sponsor
|
| Name |
Sanjay Gandhi Postgraduate Institute of Medical Sciences Uttar Pradesh India |
| Address |
Department of Hepatology
Sanjay Gandhi Postgraduate Institute of Medical Sciences, Rae Bareili Road, Lucknow-226014, Uttar Pradesh, India |
| Type of Sponsor |
Research institution and hospital |
|
|
Details of Secondary Sponsor
|
|
|
Countries of Recruitment
|
India |
|
Sites of Study
|
| No of Sites = 1 |
| Name of Principal
Investigator |
Name of Site |
Site Address |
Phone/Fax/Email |
| Dr Amit goel |
Sanjay Gandhi Postgraduate Institute of Medical Sciences |
Department of hepatology, Liver Transplant Building, 4th Floor, SGPGIMS
Lucknow
Lucknow
UTTAR PRADESH |
9936275741
agoel.ag@gmail.com |
|
Details of Ethics Committee
Modification(s)
|
| No of Ethics Committees= 3 |
| Name of Committee |
Approval Status |
| Institutional Ethics Committee |
Approved |
| Institutional Ethics Committee |
Approved |
| Institutional Ethics Committee, SGPGIMS |
Approved |
|
|
Regulatory Clearance Status from DCGI
|
|
|
Health Condition / Problems Studied
|
| Health Type |
Condition |
| Patients |
(1) ICD-10 Condition: K732||Chronic active hepatitis, not elsewhere classified, |
|
|
Intervention / Comparator Agent
|
| Type |
Name |
Details |
| Comparator Agent |
Sofosbuvir plus Daclatasvir |
Sofosbuvir 400 mg once daily along with Daclatasvir 60 mg once daily for 12 weeks |
| Intervention |
Sofosbuvir plus Daclatasvir |
Sofosbuvir 400 mg once daily along with Daclatasvir 60 mg once daily for 8 weeks |
|
|
Inclusion Criteria
|
| Age From |
18.00 Year(s) |
| Age To |
80.00 Year(s) |
| Gender |
Both |
| Details |
1. Age 18 years or more
2. HCV mono-infection
3. Detectable HCV RNA (more than 10,000 IU/mL)
4. No evidence of cirrhosis based upon a combination of history, examination, ultrasound, Transient elastography, APRI, FIB-4, Upper GI endoscopy |
|
| ExclusionCriteria |
| Details |
1. Presence of cirrhosis
2. HBsAg or HIV coinfection
3. Estimated GFR below 30 ml/ minute
4. Prior exposure to oral anti-HCV drugs, i.e, DAAs
5. Hepatocellular carcinoma or any other malignancy
6. High-risk population such as people living with HIV, people on maintenance hemodialysis, thalassaemic or haemophiliacs, people who inject drugs, men have sex with men, high risk sexual behaviour |
|
|
Method of Generating Random Sequence
|
Permuted block randomization, variable |
|
Method of Concealment
|
Centralized |
|
Blinding/Masking
|
Not Applicable |
|
Primary Outcome
|
| Outcome |
TimePoints |
| Proportion of participants who achieved the sustained virological response after the completion of 8 weeks or 12 weeks of sofosbuvir/daclatasvir treatment |
Proportion of participants who achieved the sustained virological response after the completion of 8 weeks or 12 weeks of sofosbuvir/daclatasvir treatment |
|
|
Secondary Outcome
|
| Outcome |
TimePoints |
| None |
Not applicable |
|
|
Target Sample Size
|
Total Sample Size="180"
Sample Size from India="180"
Final Enrollment numbers achieved (Total)= "Applicable only for Completed/Terminated trials"
Final Enrollment numbers achieved (India)="Applicable only for Completed/Terminated trials" |
|
Phase of Trial
|
Phase 3 |
|
Date of First Enrollment (India)
|
01/11/2025 |
| Date of Study Completion (India) |
Applicable only for Completed/Terminated trials |
| Date of First Enrollment (Global) |
Date Missing |
| Date of Study Completion (Global) |
Applicable only for Completed/Terminated trials |
|
Estimated Duration of Trial
|
Years="3"
Months="0"
Days="0" |
Recruitment Status of Trial (Global)
Modification(s)
|
Not Applicable |
| Recruitment Status of Trial (India) |
Open to Recruitment |
|
Publication Details
|
N/A |
|
Individual Participant Data (IPD) Sharing Statement
|
Will individual participant data (IPD) be shared publicly (including data dictionaries)?
Response - NO
|
|
Brief Summary
|
Background: HCV is a hepatotropic virus and all those
with HCV viremia need treatment. In absence of cirrhosis, HCV is treated with
pan-genotypic drug, sofosbuvir/daclatasvir, for 12 weeks and the treatment is
successful if HCV RNA is remained undetectable at 12 weeks (SVR12) after
stopping the drugs. Recent data and our own experience have shown that the
treatment duration can be reduced from 12 to 8 weeks for without compromising
the response. Large, good quality data are required on effectiveness of 8 weeks
of sofosbuvir/daclatasvir combination.
Research question: Can anti-HCV treatment duration be reduced
from 12 weeks to 8 weeks without compromising the virological response?
Primary objective: Compare the sustained virological
response (SVR12) in non-cirrhotic HCV infected patients treated with 8 weeks
versus 12 weeks of sofosbuvir/daclatasvir combination
Methodology: This open label, randomized pilot study will
include 180 treatments naïve, viraemic, non-cirrhotic HCV patients.
Participants will be randomized to receive either 8- or 12-week treatment
followed by HCV RNA testing at 12 weeks after treatment completion for SVR12 to
define treatment success or failure. A blood specimen will also be collected at
baseline (for HCV genotype determination), at 4 weeks of treatment (for early
virological response).
Proposed outcome: The study will provide data on efficacy of 8
weeks of treatment as compared to standard of care (12 weeks) in non-cirrhotic
patients with active HCV infection.
Future plan: If the results of our study will
support, we will plan a double-blind, multicentric, RCT to provide a reliable
evidence and reach the final conclusion. |