Revised Simplified Algorithm for Treatment Eligibility for HIV (SLATEII)

Overview

In its 2017 revision of the global guidelines for HIV care and treatment, the World Health Organization called for rapid or same-day initiation of antiretroviral treatment (ART) for eligible patients testing positive for HIV. In sub-Saharan Africa, where most HIV patients are located, studies continue to document high losses of treatment-eligible patients from care before they receive their first dose of antiretroviral medications (ARVs). Among facility-level reasons for these losses are treatment initiation protocols that require multiple clinic visits and long waiting times before a patient who tests positive for HIV is dispensed an initial supply of medications. Simpler, more efficient, accelerated algorithms for ART initiation are needed, including strategies for rapid initiation in patients with symptoms of tuberculosis, most of whom do not have active TB. In July 2017, the original SLATE study (SLATE I) completed enrollment in South Africa. One of the most striking findings of the study so far is the large proportion of patients who "screened out" of the SLATE algorithm and were referred for additional services rather than started on ART immediately. Among 298 patients assigned to the intervention arm and evaluated for immediate treatment eligibility under the SLATE algorithm, 149 (50%) screened out, two thirds of these (100/149) due to symptoms of TB. The vast majority of the TB suspects (93/100, 93%) tested negative for active TB. The SLATE II study will revise the original SLATE algorithm to provide a pathway for immediate ART initiation for some patients with TB symptoms. Under SLATE II, patients with TB symptoms will be clinically evaluated by the study nurse and will receive a urine point of care LAM (lipoarabinomannan antigen of mycobacteria) test. Those with milder symptoms and a negative LAM test will be offered immediate ART. Those with more serious symptoms and/or a positive LAM test will be asked to return the next day to receive TB test results and either immediate ART or TB treatment. All intervention arm patients (symptomatic and asymptomatic) will be asked for a sputum sample for Xpert testing, and positives will be contacted on the next day. The SLATE II algorithm will also incorporate other improvements identified from SLATE I.

Full Title of Study: “Randomized Evaluation of a Revised, Simplified Clinical Algorithm for Identifying Patients Eligible for Immediate Initiation of Antiretroviral Therapy for HIV (SLATEII)”

Study Type

  • Study Type: Interventional
  • Study Design
    • Allocation: Randomized
    • Intervention Model: Parallel Assignment
    • Primary Purpose: Treatment
    • Masking: None (Open Label)
  • Study Primary Completion Date: August 19, 2019

Detailed Description

SLATE II is be a pragmatic, individually randomized evaluation to determine the effectiveness of the revised algorithm in increasing ART initiation, compared to standard care, among non-pregnant adult patients. Six hundred HIV-infected adult patients not yet on ART will be enrolled during a routine clinic visit and randomized to receive the intervention or standard care. Patients in the intervention arm will be administered a revised version of the SLATE screens, including the TB add-on; those found eligible under the algorithm will be offered immediate treatment initiation, while those who are not eligible will be referred for standard clinic care. Patients in the standard arm will be referred for ART initiation under standard clinic procedures. All care after the initial visit will be by the clinic under standard care. Primary outcomes will be ART initiation within 7 days of study enrollment and viral suppression within 8 months of study enrollment. The study is being conducted at three healthcare facilities (clinics) in South Africa. In September 2017, the South African National Department of Health instructed all clinics to offer same-day ART initiation to eligible patients but provided little guidance on determining eligibility. SLATE II will help to create such guidance. If successful, it will improve on the SLATE approach to collecting and interpreting a minimum set of patient data that will avoid delaying treatment initiation for the majority of patients who are eligible for immediate ART, while deferring initiation in the minority who should not start immediately.

Interventions

  • Procedure: SLATE II
    • The SLATE II algorithm is a series of questions and procedures that allow a study clinician to determine if antiretroviral therapy for HIV can be started immediately (same-day) or if additional care or services are needed before ART initiation.

Arms, Groups and Cohorts

  • Experimental: SLATE
    • The SLATE arm will be administered the SLATE II algorithm and initiated on ART immediately if eligible under the algorithm. Patients not eligible under the algorithm will be referred for standard care.
  • No Intervention: Standard
    • The standard arm will be referred to standard care after study enrollment.

Clinical Trial Outcome Measures

Primary Measures

  • Proportion of patients initiated on ART
    • Time Frame: 7 days after study enrollment
    • % of enrolled patients initiated onto ART within one week of study enrollment, which may occur at HIV diagnosis or at a pre-ART follow-up visit
  • Proportion of patients initiated on ART and alive, in care, and retained
    • Time Frame: 8 months after study enrollment
    • Proportion of enrolled patients initiated on ART within 28 days of study enrollment and retained in care 8 months after study enrollment, as indicated by a clinic visit no more than 7 months after ART initiation

Secondary Measures

  • Proportion of TB suspects initiated on ART within 14 days of study enrollment
    • Time Frame: 14 days after study enrollment
    • Proportion of TB suspects initiated on ART within 14 days of study enrollment
  • Proportions of patients initiated on ART within 1, 14, and 28 days of study enrollment
    • Time Frame: 28 days after study enrollment
    • Proportions of patients initiated on ART within 1, 14, and 28 days of study enrollment
  • Proportions of all patients and of TB suspects who initiate ART and are virally suppressed eight months after having an HIV test or enrolling in HIV care
    • Time Frame: 8 months after study enrollment
    • Viral suppression stratified by TB symptom status at baseline
  • Proportions of all patients and of TB suspects who initiate ART and are alive, in care, and retained on ART 14 months after having an HIV test or enrolling in HIV care
    • Time Frame: 14 months after study enrollment
    • Retention 12 months after enrollment, allowing 1 month for initiation and 1 month for making and recording data from 12-month visit.
  • Proportions of HIV-positive patients presenting at study clinics and not yet on ART who are eligible and ineligible for immediate initiation using SLATE algorithm criteria
    • Time Frame: 1 day after study enrollment
    • Patients who screen in and screen out of algorithm in intervention arm
  • Reasons for ineligibility for immediate initiation
    • Time Frame: 1 day after study enrollment
    • Reasons for ineligibility for immediate initiation, among those found ineligible in the intervention arm
  • Median time to ART initiation (days) for each arm
    • Time Frame: 28 days after study enrollment
    • Median and IQR time to ART initiation (days) for each arm
  • Adverse events
    • Time Frame: 1, 7, 14, and 28 days after enrollment; 8 and 14 months after enrollment
    • Frequency and types of adverse events reported in medical records after ART initiation for each follow up period
  • Patient preferences
    • Time Frame: 1 day after enrollment
    • Patient self-reported preferences on the speed and timing of ART initiation, from questionnaires
  • LAM test results
    • Time Frame: 1 day after enrollment
    • Proportion of symptomatic patients who test positive for TB using the LAM test
  • Xpert test results
    • Time Frame: 1 week after enrollment
    • Proportions of symptomatic and asymptomatic patients who test positive for TB using Xpert MTB/RIF, among those able to produce a sputum sample
  • Costs to patients
    • Time Frame: 14 months after study enrollment (end of followup)
    • Costs to patients of ART initiation under standard and intervention procedures
  • Costs to providers
    • Time Frame: 14 months after study enrollment (end of followup)
    • Costs to providers of ART initiation under standard and intervention procedures
  • Differences from SLATE I
    • Time Frame: 14 months after study enrollment (end of followup)
    • Comparison of results of SLATE II study to SLATE I study

Participating in This Clinical Trial

Inclusion Criteria

  • Adult patients (>18 years) (initiating children and adolescents on ART is likely to require additional information and adherence support, making the SLATE algorithm less applicable to pediatric populations) – Confirmed HIV-positive test result at any time (may have been diagnosed previously) – Self-report that patient is not currently on ART and has not been prescribed ART in the past three months – Presented at the study clinic for any HIV-related reason or other reason that led to referral for HIV testing or care Exclusion Criteria:

  • Pregnant (pregnancy is an exclusion criterion because treatment guidelines for pregnant women differ from those for non-pregnant adults; most pregnant women are diagnosed with HIV and initiated on ART in antenatal clinics, not general adult HIV clinics) – Not intending to return to this clinic for further HIV care in the coming year (i.e. intends to seek further care somewhere else) – Not willing to be traced by phone or in person for follow-up care if test results received after the enrollment visit indicate that further care is needed – Not physically, mentally, or emotionally able to participate in the study, in the opinion of the investigators or study staff – Not willing or able to provide written informed consent to participate in the study – Previously enrolled in the same study or the SLATE I study

Gender Eligibility: All

Minimum Age: 18 Years

Maximum Age: N/A

Are Healthy Volunteers Accepted: No

Investigator Details

  • Lead Sponsor
    • Boston University
  • Collaborator
    • University of Witwatersrand, South Africa
  • Provider of Information About this Clinical Study
    • Principal Investigator: Sydney Rosen, Professor, BUSPH – Boston University
  • Overall Official(s)
    • Sydney B Rosen, Principal Investigator, Boston University

References

Brennan AT, Maskew M, Larson BA, Tsikhutsu I, Bii M, Vezi L, Fox MP, Venter WD, Ehrenkranz P, Rosen S. Who is seeking antiretroviral treatment for HIV now? Characteristics of patients presenting in Kenya and South Africa in 2017-2018. J Int AIDS Soc. 2019 Sep;22(9):e25358. doi: 10.1002/jia2.25358.

Brennan A, Maskew M, Larson BA, Tsikhutsu I, Bii M, Vezi L, Fox M, Venter WDF, Ehrenkranz PD, Rosen S. Prevalence of TB symptoms, diagnosis and treatment among people living with HIV (PLHIV) not on ART presenting at outpatient clinics in South Africa and Kenya: baseline results from a clinical trial. BMJ Open. 2020 Sep 6;10(9):e035794. doi: 10.1136/bmjopen-2019-035794.

Scott NA, Maskew M, Fong RM, Olson IE, Brennan AT, Fox MP, Vezi L, Ehrenkranz PD, Rosen S. Patient Perspectives of Quality of the Same-Day Antiretroviral Therapy Initiation Process in Gauteng Province, South Africa: Qualitative Dominant Mixed-Methods Analysis of the SLATE II Trial. Patient. 2021 Mar;14(2):175-186. doi: 10.1007/s40271-020-00437-4.

Rosen S, Maskew M, Brennan AT, Fox MP, Vezi L, Ehrenkranz PD, Venter WDF. Improved simplified clinical algorithm for identifying patients eligible for immediate initiation of antiretroviral therapy for HIV (SLATE II): protocol for a randomized evaluation. Trials. 2018 Oct 11;19(1):548. doi: 10.1186/s13063-018-2928-5.

Citations Reporting on Results

Maskew M, Brennan AT, Fox MP, Vezi L, Venter WDF, Ehrenkranz P, Rosen S. A clinical algorithm for same-day HIV treatment initiation in settings with high TB symptom prevalence in South Africa: The SLATE II individually randomized clinical trial. PLoS Med. 2020 Aug 27;17(8):e1003226. doi: 10.1371/journal.pmed.1003226. eCollection 2020 Aug.

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