Tuberculosis Clinical Trial
— XPRESOfficial title:
Evaluating Performance, Impact, and Operational Challenges of GeneXpert Use for TB Case Finding Among HIV-infected Persons in Botswana During 2012-2013: The Xpert Package Rollout Evaluation Study (XPRES)
Verified date | July 2017 |
Source | Centers for Disease Control and Prevention |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
Background: In Botswana, as in the rest of sub-Saharan Africa, undiagnosed TB or TB diagnosed
late in the course of disease is thought to be the most common cause of death among
HIV-infected persons.
Interventions for Evaluation: The Xpert MTB/RIF assay for the GeneXpert platform (Xpert) has
a TB diagnostic sensitivity of 82.4%, significantly superior to that of smear microscopy
(44.6%). In line with WHO guidelines, the Botswana Ministry of Health (MOH) and CDC rapidly
rolled out the Xpert device and a new Xpert-based diagnostic algorithm in service of 22 HIV
care and treatment clinics. To maximize impact of the Xpert device in improving detection of
active TB, Xpert rollout was preceded by strengthening of TB screening procedures by: (1)
adopting the WHO-recommended 4-symptom TB screen for adults; (2) situating trained TB
case-finding nurses in facilities; and (3) training health facility personnel in TB
diagnostic algorithms. The combination of these strengthened TB screening procedures and
rollout of the Xpert device is referred to as the "Xpert package" in this protocol.
Key Evaluation Objectives: The protocol has two key objectives: (1) to evaluate whether the
new MOH-recommended Xpert-based TB diagnostic algorithm for new adult HIV clinic enrollees is
more sensitive than the pre-Xpert smear-microscopy-based algorithm in diagnosing
culture-positive TB disease; and (2) to evaluate the impact of the whole "Xpert package" on
all-cause mortality during the first 6 months of ART, among adult patients.
Design: Stepped-wedge cluster randomized trial. Sample Size: 6,136 patients were
prospectively enrolled to meet the first primary objective. A retrospective cohort of 10,131
persons was also enrolled to meet the second objective. Projected power to meet both
objectives is >80%.
Time line: Prospective cohort enrollment started in July 2012 and was complete by March 2014.
Retrospective cohort enrollment was complete by March 2015. Patient follow-up and data entry
will be complete in March 2016 at which time analysis to answer the first two primary study
questions will be possible.
Status | Completed |
Enrollment | 18696 |
Est. completion date | July 1, 2017 |
Est. primary completion date | July 1, 2017 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | N/A and older |
Eligibility |
Prospective cohorts: Inclusion Criteria: - All new HIV clinic enrollees who meet consent requirements. Exclusion Criteria: - Prisoners Retrospective cohort: Inclusion Criteria: - All patients starting antiretroviral therapy at a study clinic in the 24 months before study start. Exclusion Criteria: - Prisoners |
Country | Name | City | State |
---|---|---|---|
Botswana | 22 HIV care and Treatment clinics in Botswana | Multiple Locations | Multiple |
Lead Sponsor | Collaborator |
---|---|
Centers for Disease Control and Prevention | Botswana Ministry of Health, University of Pennsylvania |
Botswana,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | TB diagnostic sensitivity among adults (>12 years old). Sensitivity proportions will be estimated using laboratory data on TB diagnoses (see "Description" below). | TB diagnostic algorithm sensitivity will be estimated in the pre-Xpert and post-Xpert time periods of this stepped wedge design, among adults (>12 years old). Sensitivity is the proportion of culture-positive TB cases correctly diagnosed with TB using the relevant diagnostic algorithm. The denominator is all culture-confirmed TB cases and the numerator the number of culture-confirmed TB cases that were correctly identified as positive by the relevant TB diagnostic algorithm. | Patients will be followed for an average of about 6 months each, and TB diagnostic sensitivity will be estimated at each clinical visit where the patient tests culture-positive for TB, with clinic visits occuring every one to 3 months. | |
Primary | All-cause mortality | All-cause 6-month mortality among adult antiretroviral therapy enrollees will be compared between the pre-Xpert retrospective cohort and the post-Xpert package cohorts. | Patients will be followed for an average of about 6 months each, with vital status assessed across the 6 month follow-up period. | |
Secondary | Clinician TB screening compliance. Compliance proportions will be estimated using data from study questionnaires (see "Description" below). | Clinician TB screening compliance will be compared between the pre-Xpert and post-Xpert cohorts. This is the proportion of clinic visits that the TB screening algorithm for adults was correctly administered by the attending clinician. The denominator is the number of clinic visits and the numerator is the number of occasions that the TB screening algorithm was completely and correctly administered. | Patients will be followed for an average of about 6 months each, with clinician TB screening compliance assessed at each clinic visit, which should occur every one to 3 months. | |
Secondary | The proportion of patients screening positive for TB at the HIV clinic enrollment visit. Proportions screening positive will be estimated using data from study questionnaires (see "Description" below). | The proportion of HIV clinic enrollees, who screen positive for TB, will be compared between the pre-Xpert and post-Xpert cohorts. The denominator of the proportion will be the number of patients screened for TB at the HIV clinic enrollment visit, and the numerator will be the number of patients screening positive for TB at the HIV clinic enrollment visit. | Patients will be followed for an average of about 6 months each, and the proportion screening positive for TB will be estimated at each clinical visit, including the first clinic visit, with clinic visits occuring every one to 3 months. | |
Secondary | The proportion of patients diagnosed with TB at HIV clinic enrollment. Proportions diagnosed with TB will be estimated using data from study questionnaires and laboratory tests. | The proportion of HIV clinic enrollees, who are diagnosed with TB following tests conducted at the enrollment visit, will be compared between the pre-Xpert and post-Xpert cohorts. The denominator will be the number of patients attending the HIV clinic enrollment visit, and the numerator will be the number of patients diagnosed with TB at the HIV clinic enrollment visit. | Patients will be followed for an average of about 6 months each, and the proportion diagnosed with TB will be estimated at each clinical visit, with clinic visits occuring every one to 3 months. | |
Secondary | TB diagnostic sensitivity among children (<=12 years old). Sensitivity proportions will be estimated using laboratory data on TB diagnoses (see "Description" below). | TB diagnostic algorithm sensitivity will be estimated in the pre-Xpert and post-Xpert time periods of this stepped wedge design, among children (<=12 years old). Sensitivity is the proportion of culture-positive TB cases among children correctly diagnosed with TB using the relevant diagnostic algorithm. The denominator is all culture-confirmed TB cases among children and the numerator the number of culture-confirmed TB cases that were correctly identified as positive by the relevant TB diagnostic algorithm. | Patients will be followed for an average of about 6 months each, and TB diagnostic sensitivity will be estimated at each clinical visit where the patient tests culture-positive for TB, with clinic visits occuring every one to 3 months. | |
Secondary | TB screening algorithm sensitivity among children (<=12 years old). Sensitivity proportions will be estimated using laboratory data on TB diagnoses and questionnaire data on the screening algorithm (see "Description" below). | MOH-recommended TB screening algorithm sensitivity will be estimated among children (<=12 years old). Sensitivity is the proportion of culture-positive TB cases correctly identified as potentially having TB using the MOH-recommended, 6-symptom, TB screening algorithm for children. The denominator is all culture-confirmed TB cases among children, and the numerator is the number of culture-confirmed TB cases that were correctly identified as potentially having TB by the 6-symptom, TB screening algorithm for children. | Patients will be followed for an average of about 6 months each, and TB diagnostic sensitivity will be estimated at each clinical visit where the patient tests culture-positive for TB, with clinic visits occuring every one to 3 months. | |
Secondary | Diagnostic sensitivity of Xpert in diagnosing culture-positive drug resistant TB. | The study will estimate the sensitivity of the Xpert-based TB diagnostic algorithm in identifying drug resistant TB. The denominator is all culture-confirmed TB cases with genotypic or phenotypic drug resistance, and the numerator is the number of culture-confirmed drug resistant TB cases that were correctly identified as rifampicin resistant by the Xpert-based diagnostic algorithm. | Patients will be followed for an average of about 6 months each, and TB diagnostic sensitivity will be estimated at each clinical visit where the patient tests culture-positive for drug resistant TB, with clinic visits occuring every one to 3 months. | |
Secondary | TB incidence | TB incidence among adult antiretroviral therapy enrollees will be compared between the pre-Xpert cohorts and the post-Xpert package cohorts. | Patients will be followed for an average of about 6 months each, and TB incidence will be estimated at each clinical visit, with clinic visits occuring every one to 3 months. | |
Secondary | TB treatment outcomes. The incidence rate will be estimated using data from study questionnaires (see "Description" below). | TB treatment outcomes among HIV clinic enrollees will be compared between the pre-Xpert cohorts and the post-Xpert package cohorts. Possible treatment outcomes include "Cured", "Completed Treatment", "Died", "Treatment failure", "Defaulted/Lost-to-follow-up/missing", "Transferred out", and "Treatment ongoing". | Patients will be followed for an average of about 6 months each, and TB treatment outcomes will be estimated at each clinical visit, with clinic visits occuring every one to 3 months. | |
Secondary | Hospitalization rates. Incidence of hospitalization rates will be estimated from study questionnaires. | Hospitalization rates among adult antiretroviral therapy enrollees in the first 6 months of ART will be compared between the pre-Xpert cohorts and the post-Xpert package cohorts. | Patients will be followed for an average of about 6 months each, and the hospitalization outcome will be measured at each clinical visit, with clinic visits occuring every one to 3 months. | |
Secondary | Xpert diagnostic sensitivity. Sensitivity proportions will be estimated using laboratory data on TB diagnoses (see "Description" below). | Variations in Xpert diagnostic accuracy by location (point of care versus lab-based), and over time, will be explored. Sensitivity is the proportion of culture-positive TB cases correctly diagnosed with TB using the relevant diagnostic algorithm. The denominator is all culture-confirmed TB cases and the numerator the number of culture-confirmed TB cases that were correctly identified as positive by the relevant TB diagnostic algorithm. | Patients will be followed for an average of about 6 months each, and TB diagnostic sensitivity will be estimated at each clinical visit where the patient tests culture-positive for TB, with clinic visits occuring every one to 3 months. | |
Secondary | The proportion of attempts to use Xpert where Xpert was considered inoperable. These data will be obtained from study questionnaires. | The study will estimate what proportion of attempts to use Xpert where Xpert was considered inoperable for any duration of time. | Patients will be followed for an average of about 6 months each, and Xpert fuctionality be estimated at each clinical visit where the patient screens positive for TB and provides a sputum sample, with clinic visits occuring every one to 3 months. | |
Secondary | Median turnaround time for sputum samples from the time of sample collection to the time the patient was initiated on TB treatment. These data will be obtained from study questionnaires. | The median time from the time of sputum sample collection to the time of TB treatment initiation will be estimated using study questionnaires. | Patients will be followed for an average of about 6 months each, and turnaround times for sputum samples will be estimated at each clinical visit where the patient provides a sputum sample, with clinic visits occuring every one to 3 months. |
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