HIV Infection Clinical Trial
Official title:
Testing and Linkage to Care for IDUs in Kenya (TLC-IDU Kenya); HCV Among PWIDs in Kenya: A Supplement to the TLC-IDU Study
Testing and Linkage to Care for Injecting Drug Users in Kenya:
Interventions for people who inject drugs (PWID) in sub-Saharan African have been almost
entirely absent, despite the fact that in countries like Kenya they contribute a growing
proportion of incident HIV infections. This study will leverage a historic decision in Kenya
to launch needle exchange program (NSP) and related services for this most-at-risk population
(MARP). The investigators will use this NSP/MARP platform to seek out PWID, deliver rapid HIV
testing, point of care CD4 count and link to ART using peer case managers, and evaluate
community viral load impact using a stepped wedge cluster-randomized design. Lessons learned
will have important applicability throughout sub-Saharan African.
HCV Among PWID in Kenya: A Supplement to the TLC-IDU study:
The prevalence of HCV in Kenya, where an increasing number of people who inject drugs (PWID)
live and are becoming HIV- as well as HCV-infected, has not been defined. We will establish
HCV prevalence among PWID in Nairobi, Western, and Coastal region by adding HCV rapid and
confirmatory tests in our parent PWID study (TLC-IDU Kenya); deliver appropriate counseling
and treatment options to those eligible; collect HCV treatment adherence data; and
disseminate study findings. These data will provide novel and relevant information about HCV
and HIV co-infection in Kenya among PWID that will be immediately applicable in terms of
public health impact to national and regional HCV testing, counseling, and clinical
management policy.
Testing and Linkage to Care for Injecting Drug Users in Kenya
The purpose of the study will be to leverage the GoK's first-ever needle and syringe program,
to implement the HIV seek, test, treat, and retain paradigm among PWID, whose parenteral and
sexual transmission networks amplify HIV epidemics. Study innovations include: (1) use of a
stepped wedge trial design; (2) intent to track community viral load in a low-income country
setting; (3) use of rapid CD4 assays to reduce time from HIV diagnosis to ART initiation; and
(4) use of conditional cash transfers to support peer case management of participant HIV
treatment retention.
Aim 1: Evaluate seek test treat retain using a stepped wedge cluster-randomized design.
Clusters will be the planned NSP service sites. The investigators will initiate
respondent-driven sampling (RDS) to reach PWID in Nairobi, Western region and coastal Mombasa
(including Malindi) for baseline HIV-1 prevalence determination, then collect waves of study
data as service sites roll out, including behavioral data. Teams will do rapid HIV and HCV
testing and refer for addiction/mental health and other services (e.g., OST). HIV-positives
will receive prevention with positives (PwP) counseling and point of care CD4 counts. Those
with CD4 <500/μL will be assigned a peer case manager to link the person to ART at
study-participating HIV clinics, support ART and PwP adherence and care retention. Both peer
case managers and subjects will receive small conditional cash transfers for subject's
adherence to HIV care visits. Primary study outcomes will include time to successful linkage
to care, time to ART, and community viral load before and after TLC-IDU initiation.
'Community viral load' will be ascertained by collecting specimens from randomly-selected
HIV-positives at each of the NASCOP NSP-IDU service sites. This sampling will be done in
waves over time, to document changes in infectivity (median viral load). With individual
viral loads collected per site per time step (for a n= of at least 1800 viral loads in total
across all sites and timewaves) the investigators will have good power to detect log10 viral
load changes of 0.23 and hazard ratios of ~1.5 when comparing pre- and post-intervention
period using linear mixed effects analysis.
Aim 1: Research hypothesis: Staggered rollout of a planned NSP/MARP program can be utilized
to collect pre- and post intervention data that will allow assessment of impact on community
viral load. Linkage to care will be higher, time to ART initiation will be reduced, and
retention in care will be higher during time periods with the TLC-IDU services as compared to
time periods with standard of care.
Aim 2: Conduct mathematical modeling to estimate community viral load in PWID injecting and
sexual networks, and to assess potential population-level impact of the TLC-IDU intervention
on Ro, numbers of infections averted, and quality-adjusted life expectancy.
Aim 2: Research hypothesis: HIV transmission dynamics models can use parameters from Aim 1
data waves, with sensitivity analyses identifying those parameters with largest impact on
effect estimation and stability.
Aim 3: Assess the incremental cost-effectiveness ratio of the TLC-IDU model, using a national
payer perspective. This study will provide among the world's first data regarding
implementation of the seek, test, treat and retain paradigm with IDUs in sub-Saharan Africa.
It will demonstrate the degree to which a combination of structural, biomedical and
behavioral interventions can reduce infectivity. Partnership with Kenya's national HIV
program will allow lessons learned from this study to inform other countries considering how
best to address the growing PWID contribution to the HIV epidemic in this high-HIV-burden
region.
Aim 3: Research hypothesis: Utilizing MARP/NSP services will result in a reduction in median
community viral load and in forward HIV transmission. Cost per quality adjusted life year
saved and HIV infection averted will be favorable as compared with the alternative of no
specific seek, test, treat and retain program directed to PWID.
HCV Among PWID in Kenya: A Supplement to the TLC-IDU study
Hepatitis C virus (HCV) is a global pandemic that leads to 500,000 preventable deaths
worldwide. People who inject drugs (PWID) are at much higher risk of HCV infection, with an
estimated 10 million HCV infections among PWID worldwide. In Kenya, PWID are at high risk of
HCV infection, yet HCV prevalence in this key population is not well-defined. The time is
ripe to establish HCV prevalence among high-risk PWID in Kenya, determine the role of sexual
transmission and risk behavior in those identified with HCV, and explore potential best
approaches to provide clinical and counseling services, especially to HCV-HIV co-infected
individuals. We therefore propose to add rapid HCV testing to our study of PWID in Kenya, the
NIDA-funded parent 'TLC-IDU study' (Kurth & Cherutich, PIs), and to collect additional
specific behavioral and clinical data relevant to HCV in this high-HIV burden setting.
These data will provide novel and highly relevant information about HCV and HIV co-infection
in Kenya among PWID that will be immediately applicable to national HCV testing and treating
policy. Our scientific objectives:
Supplement Specific Aim 1: Establish HCV prevalence in PWID in Nairobi, Western and Coastal
region, by adding a rapid HCV assay to the study panel among all participants (both HIV
infected and uninfected) recruited during the last TLC-IDU study waves. (The study involves
recruiting PWID who undergo rapid HIV testing/phenotyping and behavioral data collection, as
well as peer case management to support HIV treatment). Those testing positive with the HCV
rapid point of care assay will be given initial counseling to raise their awareness, tell
them they have been exposed, and encourage them to return for confirmatory results.
Confirmatory viral HCV testing will be done and confirmed positive participants given an
incentive to return to the study site for standardized HCV counseling and treatment referral
for those with HCV monoinfection and HIV-HCV infection. Main outcomes will include: a) HCV
prevalence determination b) HCV testing and counseling feasibility and acceptability
measures, c) unique predictors of HCV monoinfection and HIV and HCV coinfection determined in
multinomial logistic regression analysis.
Supplement Specific Aim 2: Deliver HCV counseling and available treatment, including
sofosbuvir treatment to those eligible and collect HCV treatment adherence data.
Supplement Specific Aim 3: Present study findings and program implications at a national
workshop with study partner NASCOP. Invite key stakeholders, researchers, and implementers to
discuss HCV agenda for Kenya.
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