QuantiFERON-TB gold in-tube implementation for latent tuberculosis diagnosis in a public health clinic: a cost-effectiveness analysis

The incidence of active TB disease in Baltimore City in 2010 was 5.2/100,000 (population 620,961) [24]. Base-case analysis parameters were based on data from BCHD, which annually evaluates approximately 500 individuals, 64% foreign-born, referred by community providers for a positive TST [4]. Per routine care, all individuals referred for suspected LTBI are interviewed by clinical staff for demographics, medical history, and signs and symptoms of active TB disease, and also receive a chest x-ray and liver function tests. Patients with signs or symptoms of active TB disease are evaluated by sputum smear microscopy, culture, and other testing.

For the base-case analysis, 100% uptake of QFT-GIT testing and implementation was assumed with 3% of tests requiring repeat due to processing failure or an indeterminate result [4]. Without a true reference standard LTBI diagnostic test, it is impossible to ascertain the true proportion of LTBI among individuals referred to the BCHD with a positive TST; we assumed only patients with LTBI are at risk for progression to active TB disease. Among individuals referred to BCHD with a positive TST, only 58% of those who were foreign-born and 36% of those who were US-born had a positive QFT-GIT [4]. It is unknown if this test discordance represents false-positive TST results or false-negative QFT-GIT results, or some combination. Given these observed rates of QFT-GIT positivity, true LTBI prevalence among referrals was calculated based on estimated QFT-GIT sensitivity and specificity: true LTBI Prevalence = (% test positive + specificity −1)/(sensitivity + specificity −1). For the base-case, QFT-GIT sensitivity of 81% and specificity of 99% were assumed based on published literature [8, 9, 14]. Reported QFT-GIT sensitivity for LTBI may be underestimated since test performance has largely been assessed in people with active TB disease as a surrogate for LTBI. Longitudinal studies have shown that less than 1% of individuals with a negative QFT-GIT progress to active TB disease even in high-risk groups, suggesting higher QFT-GIT sensitivity for identifying LTBI [6, 25, 26]. Given parameter uncertainties, a wide range of QFT-GIT test characteristics and LTBI prevalence were explored in sensitivity-analysis.

At BCHD, individuals diagnosed with LTBI are treated with a 9-month regimen of Isoniazid (9INH) or a 4-month regimen of Rifampin (4Rif), as per CDC guidelines [3]. Treatment completion rates were incorporated into the model. For the base-case, lifetime risk of progression to active TB disease among those with untreated LTBI was assumed to be 5% at an average of 5 years from time of referral [6, 12, 21, 25, 27]. LTBI treatment regimens were assumed to have 90% treatment efficacy if completed [3, 22]; given variability in timing of drug discontinuation and efficacy of partial treatment, incomplete treatment was assumed to offer on average 25% of complete treatment protection [17, 21, 22]. Individuals experiencing hepatotoxicity were assumed to complete only partial treatment. Mean age at time of referral to BCHD was 36 years (SD 16 years).

The primary outcomes were the expected costs per referral, Quality-Adjusted Life Years (QALYs) accrued per referral, and expected active TB disease cases per referral comparing the Intervention to Standard algorithms. Cost-effectiveness was represented using Incremental Cost-Effectiveness Ratios (ICERs), expressed as $US Dollars/QALY-gained [28]; a probabilistic sensitivity analysis was additionally performed using monte-carlo simulation methods to generate 95% confidence intervals and explore varying willingness to pay thresholds. QALYs accrued based on years of remaining life experienced with utility weights shown in Table 1 [29]. Mortality for individuals developing active TB disease was assumed to be 5% in the base-case [21, 30]. Future QALYs were discounted at 3%.

Costs associated with LTBI evaluation and treatment were collected at BCHD. QFT-GIT test costs were collected from the time of specimen collection through reporting of completed test results. QFT-GIT is currently performed at an off-site local BCHD laboratory at a location separate from the BCHD TB clinic, with samples transported daily. An “ingredients” approach was used, which involved multiplying input quantities used by unit prices. Staff time, consumable supplies, and equipment quantities utilized for performing the QFT-GIT test were determined through direct observation of testing procedures and time-motion studies. QFT-GIT tests were assumed to be performed in batches of 24 based on current laboratory practice and batch size was varied in sensitivity-analysis. Capitol item costs were estimated from manufacturer quotations and/or laboratory invoices and were annualized over their useful lifespans as estimated by the laboratory manager. Overhead laboratory costs were determined, including those for quality assurance, specimen transport, supply delivery, and estimates for rent and utilities attributable to QFT-GIT testing based on building space and volume of testing. Costs of LTBI treatment included drug costs based on invoices. Labor costs were determined based on clerical and clinician staff time spent during an average office visit. One office visit was included for initial evaluation and monthly office visits were included for patients on LTBI treatment. Translation service costs were added for non-English speaking patients. Costs associated with drug toxicity were based on BCHD estimates of additional diagnostic testing and clinic visits. There is little recent published literature on the downstream costs associated with developing active TB disease [21, 23]. As such, base-case estimates for BCHD costs per patient were based on current staff, drug, and diagnostic expenditures for an average active TB case; uncomplicated active TB cases were assumed to require only outpatient treatment with no hospital days. Each individual was assumed to receive standard drug treatment, directly observed, with routine monitoring for treatment response and toxicity [31]. Potential inpatient hospitalization costs associated with active TB disease were incorporated into the sensitivity-analysis. All key costs were explored in sensitivity-analysis; when published estimates of cost ranges were unavailable, potential price variations of 75% were explored. Costs are presented in $US 2012 and future costs were discounted at 3%.