HIV Clinical Trial
Official title:
Use of Tenofovir/Emtricitabine With Immediate or Deferred Doxycycline 100mg PO Daily for Combination HIV and Syphilis Pre-exposure Prophylaxis in HIV-negative Men Who Have Sex With Men: a Pilot Study of Dual Daily HIV and Syphilis PrEP. (The DuDHS Trial).
Men who have sex with men remain at high risk for HIV infection. Targeting prevention
interventions to MSM at highest risk of seroconversion is an important goal of combination
prevention interventions. Antecedent diagnosis of another sexually transmitted infection
(STI), particularly syphilis, may serve as an entry point for biomedical prevention as these
individuals are at highest risk for incident HIV. The use of the antiretroviral combination
of tenofovir/emtricitabine has been shown to be associated with an overall 44% reduction in
HIV acquisition in high-risk MSM when taken daily as PrEP. In those individuals with
detectable drug levels, the benefit was as high as 90% risk reduction. In real-world
evaluations of PrEP, high-risk sexual behaviour may continue as evidenced by high rates of
intercurrent sexually transmitted infections. As such, biomedical interventions that may
offer additional reduction in acquisition of common sexually transmitted infections should
also be evaluated.
Recently a small pilot study has demonstrated potential benefit from a similar strategy for
syphilis prevention. In this study 30 MSM were randomized to receive either 100mg doxycycline
once daily or contingency management strategies linked to remaining free of sexually
transmitted diseases at progressive study visits. Overall, those receiving doxycycline were
significantly less likely to be diagnosed with any STI during followup than those in the
comparator arm.
The investigators therefore propose to undertake a pilot study to evaluate the feasibility of
using both tenofovir/emtricitabine and doxycycline (immediate or deferred use) for
pre-exposure prophylaxis amongst HIV-negative MSM with recent history of syphilis infection
in Vancouver, Canada.
1. Rationale:
1.1 Men who have sex with men with antecedent diagnosis of another sexually transmitted
infection, particularly syphilis, are at high risk for HIV infection.
Men who have sex with men (MSM) continue to experience high rates of HIV incident
infections in Canada and a disproportionately high burden of disease relative to the
general population. In 2011, approximately 48% of new diagnoses occurred in MSM across
Canada, a figure that has been relatively stable for the last decade. Within British
Columbia (BC), although HIV new diagnosis rates overall have been declining over the
last decade (dropping from a rate of 10.6 cases/100,000 in 2004 to 5.9 cases/100,000 in
2013), MSM made up an increasing majority of new diagnoses (59%) within BC in 2013.
Within Vancouver Coastal Health Authority (VCH), approximately 70% of all new HIV
diagnoses annually from 2012-15 were amongst MSM.
Targeting prevention interventions to MSM at highest risk is important when determining
potential publicly funded biomedical interventions, particularly the use of HIV
pre-exposure prophylaxis (PrEP). Antecedent diagnosis of another sexually transmitted
infection (STI) may serve as an entry point for biomedical prevention as these
individuals are at highest risk for incident HIV. In an evaluation of HIV incidence
following diagnosis of syphilis infection in New York City, the annual HIV incidence was
3.6% (95% Confidence Interval [CI]: 3.27% - 3.97%), with overall HIV incidence amongst
MSM of 5.56% (1). In those males with syphilis and a subsequent additional STI the HIV
incidence was even greater at 7.89% (95% CI: 6.62% - 9.24%). A similar analysis of
clients attending STI clinics in BC has revealed that antecedent STI is predictive of an
elevated risk for subsequent HIV seroconversion with clients who ever had a diagnosis of
syphilis having an HIV incidence of 3.6% person-years (95%CI: 2.5-4.9), gonorrhea (2.0%;
95%CI: 1.6-2.5), rectal gonorrhea (4.5% person-years; 95%CI: 3.4-5.8), while individuals
with rectal gonorrhea and syphilis had an incidence rate of 12.6 % person-years (95%CI:
8.4-21.8).
Evaluating the use of PrEP in MSM with antecedent STI is an important component to
inform HIV prevention programs in BC and nationally. The STI clinics operated by the BC
Centre for Disease Control are well-positioned for this evaluation as about 15 and 25%
of all HIV diagnoses in BC and VCH, respectively are diagnosed at these clinics.
1.2. STI prevention strategies may also benefit from biomedical prevention interventions
Novel biomedical strategies have been shown to be effective in preventing acquisition of
STI such as HIV, and are now considered to be standard of care for at-risk MSM in the
United States. The use of the antiretroviral combination of tenofovir/emtricitabine has
been shown to be associated with an overall 44% reduction in HIV acquisition in
high-risk MSM when taken daily as PrEP. In those individuals with detectable drug
levels, the benefit was as high as 90% risk reduction. In real-world evaluations of
PrEP, high-risk sexual behaviour may continue as evidenced by high rates of intercurrent
STI (50% of PrEP users after 12 months in a study of 657 PrEP initiators in San
Francisco). As such, biomedical interventions that may offer additional reduction in
acquisition of common sexually transmitted infections should be evaluated.
Recently a small pilot study has demonstrated potential benefit from a similar strategy
for syphilis prevention (2). In this study 30 MSM were randomized to receive either
100mg doxycycline once daily or contingency management strategies linked to remaining
free of sexually transmitted diseases at progressive study visits. Doxycycline 100mg
daily was chosen based on prior studies indicating that doses as low as once weekly
doxycycyline could serve as prophylaxis for leptospirosis, another spirochete infection.
Overall, those receiving doxycycline were significantly less likely to be diagnosed with
any STI during follow-up than those in the comparator arm (odds ratio [OR] 0.27; 95% CI
0.09 - 0.83). Specific protection against syphilis infection was not seen during the
on-treatment phase (OR 0.27; 95% CI 0.04 - 1.73), possibly reflecting the small sample
size. During the study period, no change in sexual behaviours between arms was noted,
supporting the potential role of doxycycline prophylaxis. A larger pilot evaluation of
this strategy, in combination with HIV PrEP, would be a novel syndemic approach to
addressing both the HIV and syphilis burden amongst the highest risk MSM.
The investigators therefore propose to undertake a randomized trial of immediate vs.
deferred doxycycline in conjunction with daily tenofovir/emtricitabine to determine the
feasibility of combined HIV and syphilis pre-exposure prophylaxis amongst HIV-negative
MSM with recent history of syphilis infection in Vancouver, Canada.
2. Objectives:
We propose to undertake a pilot trial of immediate vs. deferred doxycycline in conjunction
with daily tenofovir/emtricitabine to determine the feasibility of combined HIV and syphilis
pre-exposure prophylaxis amongst HIV-negative MSM with recent history of syphilis infection
in Vancouver, Canada. We will meet this aim through the following objectives:
1. To assess feasibility of using dual daily HIV and syphilis PrEP, as defined by:
a. Evaluation of feasibility of recruitment for a larger study i. Proportion of
participants approached for study who are eligible and agree to participate.
b. Adherence to 6 or 12 months of tenofovir/emtricitabine and doxycycline i. Determine
proportion of individuals with >95% adherence to dual therapy over 6 and 12 months ii.
Proportion of individuals with detectable doxycycline plasma level at each study visit.
Additional measures of feasibility will include the assessment of:
c. Tolerability of dual PrEP i. Comparison of grade 3 or 4 adverse events in those
receiving immediate vs. deferred PrEP
2. To evaluate antimicrobial resistance over time.
a. Change in proportion of participants with evidence of tetracycline class resistance
in common flora, namely Staphylococcus aureus, Streptococcus pyogenes and Streptococcus
pneumoniae from baseline to 6 and 12 months.
Secondary objectives will include:
3. To evaluate changes in sexual activity reported by study participants over the study
period.
4. To compare syphilis incidence between those in the immediate vs. deferred doxycycline
arms.
5. To describe frequency of other STI's diagnosed in study participants over the study
period.
Exploratory objectives will include:
6. To evaluate doxycycline resistance in individuals with documented T.pallidum infection.
7. To evaluate HIV incidence and syphilis re-infection rates over a 12 month period.
8. Characterize changes in the rectal microbiome from baseline to 6 and 12 months after
initiation of doxycycline
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