The No One Waits Study: Acceptability and Feasibility of Community-based Point-of-diagnosis HCV Treatment Study

Phase 4

Completed

• Conditions: Hepatitis C, Chronic
• Interventions: Drug: Standard of care; Drug: Epclusa (SOF/VEL); Device: Fibroscan® 430 Mini Plus

• Registration Number: NCT03987503
• Lead Sponsor: University of California, San Francisco

Brief Summary

Direct-acting antiviral (DAA) therapy for hepatitis C virus (HCV) offers a cure to those with chronic HCV infection. For marginalized communities, linkage to care services often aren't enough to overcome barriers to accessing the medical system. For difficult to link populations, offering treatment at the same non-clinical community space may improve uptake and reduce loss-to-follow-up. The purpose of this 2 year study is to assess the feasibility, acceptability and effectiveness of accelerated initiation of commercially available DAA therapy targeting socially marginalized communities (e.g., medically underserved, homeless, people actively injecting drugs). The study will be carried out at two community sites that perform HCV testing: (a) fixed community site and (b) community mobile site via clinical research van. Participants (n=150) who test anti-HCV positive and HCV RNA positive (chronic infection) are invited to enroll into the no one waits (NOW) Study and begin HCV treatment at point of diagnosis. All evaluation, medication dissemination, and follow-up care will take place at the project site. The investigators will estimate the effect of on-site point-of-diagnosis (POD) treatment on (1) time from HCV testing to treatment initiation, (2) completing treatment, and (3) attaining (sustained virologic response) SVR-12; overall and by study site. A secondary product will be a lesson learned guide of recommendations for implementing a POD on-site test and treat program for dissemination beyond San Francisco.

Detailed Description

This study is a non-randomized interventional study.

NOW is an open-label study evaluating the feasibility, acceptability, and effectiveness of an accelerated community-based treatment program of SOF/VEL x 12 weeks started at time of chronic HCV diagnosis (intervention).

The purpose of the proposed study is to assess the feasibility, acceptability and effectiveness of accelerated initiation of commercially available direct-acting antiviral (DAA) therapy targeting socially marginalized communities (e.g., medically underserved, homeless, people actively injecting drugs). The proposed study will be carried out at two community sites that perform HCV testing: (a) fixed community site and (b) community mobile site. The fixed site is located in the Tenderloin Neighborhood of San Francisco: The Quaker Meeting House (QMH). The QMH is the current location for an established drop-in center for young adult (\< 30 years old) people who inject drugs, a group at highest risk for acquiring new HCV infection but representing a group with the lowest engagement in HCV treatment. The QMH site is complete with two phlebotomy stations, centrifuge, clinical exam station, interview rooms, and office space. The QMH research site will prioritize study enrollment for young adult people who inject drugs (PWID). The community mobile site (DeLIVER Van) is situated in a mobile van; a 145 sqft space equipped with a phlebotomy station, clinical exam table, centrifuge, and portable Fibroscan® 430 Mini Plus. The DeLIVER Van will serve two neighborhoods in San Francisco with high HCV burden but few community-based medical service organizations: the Bayview neighborhood and Outer Mission neighborhood.

The investigators will (1) implement new tools, notably FIBROSCANS, to measure fibrosis in an at-risk group (HCV positive patients); (2) implement a new standard of care, treatment on-demand in an at-risk group (HCV positive active drug users); (3) assess the feasibility and acceptability of expanding standard of care into non-clinical settings.

At study entry, participants will undergo a combined eligibility screening/entry visit, which includes HCV testing (antibody and RNA), rapid anti-HIV test, and HBsAG (hepatitis B virus surface antigen) testing and consent for medical record linkage. If HCV RNA reactive, participants are offered enrollment into the treatment cohort and provided 2 week supply of SOF/VEL (provided by Gilead as part of the NOW Study) upon completion of a clinical evaluation, baseline survey, and venipuncture for baseline labs. If the participant is actively insured, the study investigators will obtain insurance-authorized SOF/VEL to complete the remainder of the 12 week treatment course. If the participant is not actively insured, the study team will assist with insurance acquisition and subsequently obtain insurance-authorized SOF/VEL to complete the remainder of the 12 week treatment course. For any participants, if insurance-authorized SOF/VEL is delayed beyond the initial 2 week study-provided SOF/VEL, additional supplies of SOF/VEL as needed to ensure an uninterrupted 12 week treatment course. Participants will return every 2 weeks during treatment (12 week course) for medication dispensation and study visit activities. And for two post-treatment visits for clinical monitoring (e.g., HCV RNA testing) and research activities.

Study participants in the intervention study (cohort): Chronic HCV (anti-HCV positive and HCV RNA positive) men and women ages ≥18 years newly diagnosed or re-engaged in care at a fixed or mobile community-based site. Participants should be HBsAg negative, have no known history of decompensated cirrhosis or end stage renal disease, not be pregnant or breastfeeding, and not be taking medications that are contraindicated with SOF/VEL.

Study Timeline

• Study First Submitted: 2019-06-12
• Study First Submitted QC: 2019-06-14
• Study First Posted: 2019-06-17
• Study Start: 2020-07-01
• Primary Completion: 2022-10-30
• Study Completion: 2022-12-29
• Status Verified: 2023-01
• Last Update Submitted: 2023-01-17
• Last Update Posted: 2023-01-19

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 86

Inclusion Criteria

• ≥18 years of age
• anti-HCV and HCV RNA positive,
• interested in starting HCV treatment at the time of diagnosis
• Women of childbearing potential engaged in sexual activity that could lead to pregnancy
• must consent to use contraception and agree to pregnancy testing during treatment
• If currently not enrolled in insurance, agree to assistance to enroll in insurance

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Exclusion Criteria

• HBsAg positive from pre-screening visit and no medically controlled hepatitis B virus (HBV) condition
• History of hepatic decompensation (ascites, hepatic encephalopathy, or variceal hemorrhage).
• Current use of medications that is not compatible with SOF/VEL use, according to current prescribing guidelines, including amiodarone or a proton pump inhibitor exceeding 20 mg of omeprazole equivalent.
• Prior treatment with an NS5a based HCV treatment regimen with subsequent viral rebound. Participants who have clear HCV reinfection as defined by an HCV GT that is different from the original genotype may enroll. If genotype results are not available from the initial and subsequent HCV infection, the individual will not be enrolled unless participant can provide SVR-12 record confirming HCV cure.
• Pregnancy or breastfeeding.
• Life expectancy of < 12 months as assessed by study clinical health provider.
• Late exclusion criteria: Participants with the following lab values at week 0 will be evaluated on a case by case basis for continuation of SOF/VEL at the week 2 visit
• Albumin < 3.0
• Hemoglobin < 8.0 (women) and < 9.0 g/dl ( men)
• Platelet count < 50,000
• creatinine (Cr) clearance (estimated by Cockcroft-Gault) < 30 ml/min
• aspartate aminotransferase (AST) or Alanine Aminotransferase (ALT) > 10 x ULN
• Total bilirubin > 1.5x ULN (for participants on atazanavir, > 3 x ULN), international normalized ratio (INR) > 1. 5 x ULN

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Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
at Point-of-Diagnosis HCV treatment	Fibroscan® 430 Mini Plus	At the point of HCV infection diagnosis, (HCV RNA positive and anti-HCV positive) individuals who meet eligibility criteria and elect to start HCV treatment at the same visit and monitored at two-week intervals at the community-site.
Passive observation	Standard of care	Participants who test positive for HCV chronic infection (HCV RNA positive, and anti-HCV positive) but elect to not enroll in the intervention arm. Electronic medical record data will be reviewed for up to 2 years for HCV related care information (e.g., HCV treatment start date, end date, SVR-12).
at Point-of-Diagnosis HCV treatment	Epclusa (SOF/VEL)	At the point of HCV infection diagnosis, (HCV RNA positive and anti-HCV positive) individuals who meet eligibility criteria and elect to start HCV treatment at the same visit and monitored at two-week intervals at the community-site.

Primary Outcome Measures

Name	Time	Method
SVR-12	24 weeks from the start of treatment	The number and proportion attaining SVR12 after POD HCV treatment, overall,using a modified intention to treat analysis (participants taking one or more doses of SOF/VEL).
SVR-12, by project site	24 weeks from the start of treatment	The number and proportion attaining SVR12 after POD HCV treatment, by site, using a modified intention to treat analysis (participants taking one or more doses of SOF/VEL).

Secondary Outcome Measures

Name	Time	Method
Time from HCV testing to treatment initiation	24 weeks	Time from HCV testing visit to treatment initiation
Time from HCV testing to SVR-12.	24 weeks	Time from HCV testing visit to SVR-12
Treatment adherence at 12 weeks	12 weeks from treatment initiation	Adherence as estimated by pill count estimated as the average using self-report pill count taken divided by 84 pills.
Time from HCV testing to treatment completion	24 weeks	Time from HCV testing visit to treatment completion
Treatment adherence	12 weeks from treatment initiation	Adherence as estimated by HCV viral load test (PCR) at 12 weeks
Treatment adherence at 4 weeks	4 weeks from treatment initiation	Adherence as estimated by pill count estimated as the average using self-report pill count taken divided by 28 pills.
Treatment adherence at 8 weeks	8 weeks from treatment initiation	Adherence as estimated by pill count estimated as the average using self-report pill count taken divided by 56 pills.
Acceptability: Number of persons who decline POD treatment	1 day	Number of persons who decline POD treatment
Acceptability: median age by declined	1 day	Comparison of median age by declined POD treatment group vs POD treatment initiate group.
Acceptability: percent female by declined	1 day	Comparison of percent female by declined POD treatment group vs POD treatment initiate group.
Acceptability: percent non-white race/ethnicity by	1 day	Comparison of percent non-white race/ethnicity by declined POD treatment group vs POD treatment initiate group.
Acceptability: percent homeless in past 30 days	1 day	Comparison of percent homeless in past 30 days by declined POD treatment group vs POD treatment initiate group.
Acceptability: percent injected drugs in past 30 days	1 day	Comparison of percent injected drugs in past 30 days by declined POD treatment group vs POD treatment initiate group.
Acceptability: percent jail/prison stay in past 30 days	1 day	Comparison of percent jail/prison stay in past 30 days by declined POD treatment group vs POD treatment initiate group.

Trial Locations

Locations (1)

University of California, San Francisco; 🇺🇸 San Francisco, California, United States