HIV Infections Clinical Trial
Official title:
STI Screening as a Combined HIV Prevention Platform for MSM in Peru
The investigators propose to develop and pilot an HIV prevention intervention based on rectal
STI testing, counseling, and treatment for MSM in Peru. The investigators will use nucleic
acid testing to screen 750 behaviorally high-risk MSM for rectal gonorrheal and/or chlamydial
(GC/CT) infection. GC/CT-positive subjects will receive single-dose antibiotic treatment and
single-session Personal Cognitive Counseling (PCC) (n=50) or standard post-test counseling
(n=50). A GC/CT-negative control group (n=50) will also be enrolled to compare biological
outcomes including changes in levels of inflammatory cytokines following rectal STI. The
intervention is based on three interrelated objectives: 1) To use periodic rectal STI nucleic
acid testing to identify the members of the MSM population at greatest short-term risk for
HIV infection; 2) To provide single-dose antibiotic treatment to control the immune
activation and mucosal inflammation caused by rectal GC/CT infection that increase cellular
risk for HIV transmission; and 3) To use Personal Cognitive Counseling (PCC) to understand
and modify recent high-risk sexual practices that led to rectal STI acquisition and that
increase future HIV risk.
The investigators propose to screen 750 behaviorally high-risk MSM for rectal GC/CT infection
to enroll 100 GC/CT-positive individuals (using a conservative 15% prevalence estimate) and
50 GC/CT-negative controls (matched by age and baseline frequency of URAI). GC/CT-infected
participants will be given single-dose antibiotic therapy and randomized to receive
single-session PCC (n=50) or standard post-test counseling (n=50). The primary outcome will
be the impact of PCC on self-reported sexual risk behavior (URAI). Secondary outcomes will
assess: 1) Feasibility/Acceptability of the STI screening program; 2) Impact of GC/CT
infection and treatment on levels of inflammatory cytokines (IL-6, IL-8, TNF-αand IL-1β) in
rectal mucosa; 3) Prevalence of persistent/recurrent rectal GC/CT; and 4) HIV incidence in
GC/CT-infected and -uninfected MSM.
Overview. The investigators plan to screen 750 behaviorally high-risk, HIV-uninfected MSM in
order to enroll 100 subjects with rectal GC/CT infection and 50 uninfected controls.
GC/CT-infected participants will receive single-dose antibiotic therapy and be randomized to
receive either PCC or standard-of-care post-test counseling. GC/CT-negative participants will
receive standard post-test counseling. Behavioral and biological assessments will be
conducted at Baseline, 3-month and 6-month Follow-up visits. The primary outcome will be the
effect of PCC on the prevalence of URAI with an HIV-infected or unknown status partner in the
preceding 3-months. Secondary outcomes include feasibility/acceptability of the intervention,
prevalence of persistent or recurrent GC/CT infection, change in rectal cytokine levels, and
incidence of HIV infection.
Recruitment. Participants will be recruited from local HIV testing sites using the methods
described above.
Screening Visit. The investigators will screen 750 MSM reporting at least one recent episode
of unprotected receptive anal intercourse (URAI) for rectal GC/CT infection with a goal of
identifying 100 GC/CT-positive participants (using a conservative 15% prevalence estimate and
assuming 10% loss to follow-up over 6 months).
i) Rapid HIV Testing: After providing informed consent, all potential participants will
undergo rapid HIV testing. Study staff will provide pre- and post-test risk reduction
counseling based on the CDC's RESPECT-2 model (24) and screen for HIV at point of care using
a 4th Generation Rapid HIV-1/2 assay (Alere Determine, Alere).
ii) Physical Examination: Potential participants will undergo routine physical examination to
assess for signs of STI. Participants with evidence of proctitis (rectal discharge or
inflammation) will be treated with Ceftriaxone 250 mg injection and Azithromycin 1 g oral and
invited to enroll in the study based on symptomatic criteria.
iii) Syphilis Testing: Potential participants will undergo syphilis testing by RPR
(RPRnosticon, Biomerieux), with positive results confirmed by TPPA (Serodia TPPA, Fujirebio).
Results will be provided within 14 days and individuals with latent syphilis infection will
be treated with three weekly doses of Penicillin G 2.4 Million IU.
iv) Rectal NAT Screening: All potential participants, regardless of symptoms, will be tested
for rectal GC/CT infection at the screening visit. A rectal swab will be obtained by clinical
staff and tested for GC/CT using a transcription mediated assay (TMA) (GenProbe Aptima,
Hologic). Results will be provided within 14 days.
v) Antibiotic Therapy: Participants with symptomatic proctitis at the screening visit will be
provided with appropriate antibiotic treatment (Ceftriaxone 250 mg IM and Azithromycin 1g PO
once), advised of the importance of partner notification, and offered antibiotic therapy
packets to deliver to their recent sexual partners (maximum of 5 packets per participant).
Each packet will include a single dose of Cefixime 400 mg and Azithromycin 1g PO as well as
printed information about GC/CT infection and local testing and treatment resources for HIV
and other STIs (including free partner testing and treatment at the Via Libre site).
Enrollment Visit. Based on results of nucleic acid testing and/or symptomatic criteria, we
will enroll 100 HIV-uninfected MSM with rectal GC/CT infection who will be randomized to
receive either PCC (n=50) or standard post-test counseling (n=50). An additional 50
GC/CT-uninfected control subjects will also be enrolled.
i) Antibiotic Therapy: Participants diagnosed with rectal GC/CT by nucleic acid testing will
receive antibiotic therapy and up to 5 partner treatment packets as described above.
ii) Randomization: Participants diagnosed with rectal GC/CT infection and/or symptomatic
proctitis will be randomized to receive either PCC or standard of care post-test counseling.
Randomization assignments will be constructed in a random permuted block allocation (block
size = 7, alternating 4/3 ratio). Computer-generated assignments will be stored in opaque,
sealed envelopes and opened sequentially at the time of allocation.
iii) Behavioral Survey: GC/CT-infected participants in both arms will be asked to complete a
CASI-administered behavioral survey. The survey instrument will be self-administered using an
iPad device and will ask participants about their sexual practices during the previous 3
months, including number and type of sexual partners (primary/stable partner,
casual/recurrent contact, casual/single contact, anonymous contact, and commercial sex client
or worker), frequency of sexual intercourse (oral, anal, and vaginal), frequency of
unprotected intercourse, and frequency of unprotected intercourse with HIV-infected or
unknown serostatus partners. To collect additional detail on partner-level risk factors,
participants will be asked to provide information about their most recent sexual contacts (up
to a maximum of three contacts within 6 months). For each contact, participants will be asked
to describe the partner's age, gender, sexual orientation, sexual role, partnership type,
length of partnership, partner HIV serostatus, and sexual practices, including act-specific
condom use. Additional questions will address demographics, STI symptoms (e.g., dysuria,
urethral or rectal discharge, etc.), drug and alcohol use, depression, anxiety, and
self-efficacy for negotiating condom use.
iv) Personal Cognitive Counseling (PCC): After completing the survey, participants diagnosed
with GC/CT-infection will receive either PCC or standard of care post-test counseling,
according to randomization arm.
PCC Procedures: i) SJEI Completion: Participants will first be asked to complete the SJEI
instrument independently. ii) SJEI Review: A study counselor will meet with the participant
to review their responses to the SJEI and ask them to recount a recent sexual encounter
involving URAI. Participants will be asked to tell their story in context, paying attention
to the environmental cues, interpersonal interactions, and individual emotions and cognitive
processes occurring at each step of the encounter. After narrating their story, the
participant will review together with the counselor the self-justifications employed during
the interaction, using objective, "offline" analysis to explore the "online" cognitive
processes they used to justify sexual risk behavior during the episode. iii) Risk Counseling:
The counselor will work with the participant to highlight moments where critical behavioral
decision points occurred, identify the self-justifications used for engaging in risk behavior
at those moments, and develop a strategy to control risk behavior in future interactions. A
key component of the counseling will involve linking the prior episode of URAI with the
current diagnosis of rectal GC/CT, as a strategy to highlight flaws in previously used
self-justifications. iv) Role-Play: The counselor and the participant will rehearse risk
reduction strategies by role-playing typical interactions where high-risk sexual behavior may
occur. After completing the session, the participant will be asked to discuss their
satisfaction with the PCC model, including their comfort in discussing the cognitive
processes occurring during a sexual encounter, the perceived usefulness of the counseling,
and any important issues that were not addressed.
v) Standard of Care Post-Test Counseling. GC/CT-infected participants in the standard of care
arm (and all GC/CT-negative participants screened for infection) will receive standard
post-test counseling in accordance with Peruvian Ministry of Health guidelines. Counseling
will include a discussion of recent sexual risk behavior, condom use to reduce the risk of
future HIV/STI acquisition, partner notification, and follow-up testing.
vi) Rectal Cytokine Measurements. GC/CT-infected participants randomized to the standard
post-test counseling arm will be matched 1-to-1 with GC/CT-negative controls. Matching will
be based on age and number of episodes of URAI reported in the previous 30 days (categorized
as 1, 2-3, or >3 episodes).
GC/CT-infected participants and matched GC/CT-negative controls will be asked to provide a
swab sample of the rectal mucosa to monitor changes in levels of inflammatory cytokines from
the time of diagnosis to after antibiotic treatment. To collect the sample, a physician will
insert a sponge swab 4 cm into the participant's rectum and leave it in place for 30 seconds
prior to removal. Samples will be stored in liquid transport media at -4°C until completion
of the study, at which time all samples will be sent to the UCLA Mucosal Immunology Core
(MIC) Laboratory. Levels of IL-1β, IL-6, IL-8, and TNF-α in rectal mucosa will be measured.
Repeat measurements will be collected at 3- and 6-month Follow-up visits to assess changes
from initial diagnosis to post-treatment. Results will be used to establish baseline values
and changes in levels of key cytokines following STI treatment to define the parameters for
intermediate biological outcomes in a projected RCT.
Follow-up Visits. All participants will be asked to return for 3-month and 6-month Follow-up
assessments.
i) Behavioral Survey. All participants diagnosed with rectal GC/CT infection at Enrollment
will be asked to complete a CASI-administered Follow-up survey at each visit. Similar to the
Baseline survey, the Follow-up instrument will assess sexual risk behavior, substance use,
and other mediating factors (depression, anxiety, condom self-efficacy) over the previous
3-month period as well as partner notification and treatment outcomes.
ii) Repeat HIV Testing. Rapid HIV testing will be provided at each follow-up visit using the
above procedures.
iii) Repeat GC/CT Testing. All participants will receive repeat nucleic acid testing for
rectal GC/CT at each follow-up visit. Results of repeat testing will be provided by telephone
or in person within two weeks. Participants with new, recurrent, or persistent infection will
be treated with Ceftriaxone 250 mg IM and Azithromycin 1g PO once. Post-test counseling for
new, persistent, or recurrent infection will be provided according to the participant's
original randomization assignment (PCC or standard of care counseling).
iv) Repeat Cytokine Testing. Rectal swab measurements will be obtained from GC/CT-positive
participants randomized to the standard of care arm and matched GC/CT-negative controls at
each follow-up to monitor changes in inflammatory cytokine levels in rectal mucosa after
antibiotic treatment and in GC/CT-negative controls over the same time period. Samples will
be stored for testing in the UCLA MIC laboratory.
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