Optimizing the Delivery of HIV Post-exposure Prophylaxis: A Randomized Controlled Trial of Text Messaging Support and Physician to Nurse Task-shifting
Overview
- Phase
- Phase 2
- Intervention
- nPEP
- Conditions
- HIV Infections
- Sponsor
- Unity Health Toronto
- Enrollment
- 434
- Locations
- 3
- Primary Endpoint
- Self-reported completion of a full course of PEP medications and receipt of a final HIV test result from their nPEP provider 12 weeks after the index exposure
- Last Updated
- 4 years ago
Overview
Brief Summary
Despite decades of traditional prevention efforts based on behavior change and condom use, Ontario has seen over 700 new HIV infections annually over the past 10 years. Post-exposure prophylaxis (PEP) is one such approach, in which uninfected persons use 28 days of antiretroviral medications (ARVs) shortly after an HIV exposure to minimize the risk of acquiring HIV. PEP is highly efficacious, is considered a standard of care intervention based on medical and ethical grounds, and is supported by treatment guidelines. Yet several implementation challenges have limited its clinical and public health impact in Ontario, where no formal PEP policy exists. Our proposal seeks to optimize two aspects of delivering PEP for sexual exposures (nPEP). Results will inform the development of a standardized approach to nPEP both province-wide and elsewhere.
Thus study has pragmatic, multicenter randomized controlled trial using a 2x2 factorial design to determine whether the proportion of nPEP patients that successfully complete follow-up:
- is higher among those receiving mobile phone-based text messaging support than among those receiving standard care; and
- is non-inferior among those receiving care from a sexual health clinic nurse compared to those receiving hospital-based physician care.
The prospective, randomized, non-blinded, 2x2 factorial trial that will enroll 318 study participants in Toronto. In Intervention A, we will randomize half of study participants to a text messaging support service ('WelTel'), in which a trained, community-based counselor provides standardized weekly 'check-in' messages during their 12-week course of PEP follow-up. The other half will receive standard care, which does not include any form of active outreach or reminders outside of scheduled appointments. In Intervention B, we will randomize half of participants to receive nurse-led care for PEP follow-up at a local sexual health clinic; the other half will receive standard care by a hospital-based ID physician. The specific activities for each follow-up visit will be clearly defined in a medical directive. In keeping with Ontario legislation on medical directives, nurses will review cases with their authorizing physician or nurse practitioner on a routine basis.
Investigators
Eligibility Criteria
Inclusion Criteria
- •Be 18 years or older
- •Be known or presumed to be HIV-uninfected at baseline
- •Be initiated on PEP by a healthcare provider in the past six days for a sexual exposure to a known or suspected HIV-infected source
- •STAGE 1 only: Own a mobile phone with text messaging capabilities on which they are willing to potentially receive messages from the text messaging service
- •Be capable of communicating verbally and via text in English
- •Be planning to continue their follow-up locally or be willing to have follow-up study visits conducted remotely; either by telephone or via an encrypted video conferencing system (such as Zoom for healthcare).
- •Be referred to a sexual assault center and provided with necessary counselling and support services if presented for nPEP following sexual assault.
Exclusion Criteria
- •Creatinine clearance \<30 mL/min (using Cockcroft-Gault formula)
- •Enrolled in any other clinical trial of an HIV prevention intervention
- •Prior participation in this clinical trial for a previous episode of nPEP
- •Known co-infection with chronic hepatitis B at enrollment
- •Current or planned pregnancy or breastfeeding
- •Use of a medication whose co-administration with Biktarvy is contraindicated (dofetilide, carbamazepine, oxcarbazepine, phenobarbital, phenytoin, rifampin, rifampicin, rifabutin, rifapentine, modafinil, dexamethasone, metformin, St. John's Wort)
- •Concomitant use of HIV pre-exposure prophylaxis (PrEP)
- •Stage 2 only: Concomitant use of any non-prescription medication, supplement, vitamin or natural remedy which the patient is unwilling to discontinue during Biktarvy® administration
Arms & Interventions
ARM 4 = ID PHYSICIAN-LED nPEP,
PEP will be delivered according to the standard of care by an infectious diseases physician.
Intervention: nPEP
ARM 1 = TEXT MESSAGING SUPPORT
PEP will be delivered by ID physician and participants will receive weekly text message "check-ins" and optional automated text appointment reminders via the WelTel system.
Intervention: nPEP
ARM 1 = TEXT MESSAGING SUPPORT
PEP will be delivered by ID physician and participants will receive weekly text message "check-ins" and optional automated text appointment reminders via the WelTel system.
Intervention: Text Messaging Support
ARM 2 = NO TEXT MESSAGING SUPPORT
PEP will be delivered according to the standard of care by an infectious diseases physician. Participants will not receive text message reminders or "check-in".
Intervention: nPEP
ARM 3 = NURSE-LED nPEP
PEP will be delivered by a sexual health clinic nurse operating under a medical directive.
Intervention: nPEP
ARM 3 = NURSE-LED nPEP
PEP will be delivered by a sexual health clinic nurse operating under a medical directive.
Intervention: Nurse-Led nPEP
Outcomes
Primary Outcomes
Self-reported completion of a full course of PEP medications and receipt of a final HIV test result from their nPEP provider 12 weeks after the index exposure
Time Frame: 12 weeks
Determined by patient completion of acceptability questionnaire and evidence of HIV test result
Secondary Outcomes
- Diagnosis of incident HIV(12 weeks)
- Patient satisfaction with their PEP experience(12 weeks)
- Self-reported sexual risk-taking behaviour(12 weeks)
- Numbers and types of linkages made by PEP providers to other forms of healthcare(Week 12)
- Incidence of Treatment-Emergent Adverse Events [Safety and Tolerability of TAF/FTC/ELV/cobi-based nPEP](12 weeks)
- Completion of each scheduled follow-up activity (blood tests and clinic visits)(12 weeks)
- Inquiries from participants to the PEP provider outside of scheduled follow-up(12 weeks)
- Sexually transmitted infections (gonorrhea, chlamydia, syphilis, hepatitis B and C)(12 weeks)
- PEP-related referrals for physician consultation(12 weeks)