Evaluation of Quantitative Interferon-{gamma} Response for Risk Stratification of Active Tuberculosis Suspects

doi:10.1164/rccm.200906-0981OC

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Evaluation of Quantitative Interferon- ${gamma}$ Response for Risk Stratification of Active Tuberculosis Suspects

John Z Metcalfe¹^*, Adithya Cattamanchi², Eric Vittinghoff³, Christine Ho⁴, Jennifer Grinsdale⁵, Philip C Hopewell⁶, L. Masae Kawamura⁵, and Payam Nahid⁶

¹ Division of Pulmonary and Critical Care Medicine, University of California, San Francisco at San Francisco General Hospital, San Francisco, California, United States, ² Division of Pulmonary and Critical Care Medicine, University of California, San Francisco at San Francisco General Hospital, California, United States, ³ Department of Epidemiology and Biostatistics, University of California, San Francisco, San Francisco, California, United States, ⁴ Tuberculosis Control Section, Department of Public Health and, Centers for Disease Control and Prevention, San Francisco, California, United States, ⁵ Tuberculosis Control Section, Department of Public Health, San Francisco, California, United States, ⁶ Division of Pulmonary and Critical Care Medicine, University of California, San Francisco at San Francisco General Hospital and, Tuberculosis Control Section, Department of Public Health, San Francisco, CA, United States

^* To whom correspondence should be addressed. E-mail: john.metcalfe{at}ucsf.edu.

Rationale: The contribution of interferon- ${gamma}$ release assays (IGRAs)to appropriate risk stratification of active tuberculosis suspectshas not been studied. Objective: To determine whether additionof quantitative IGRA results to a prediction model incorporatingclinical criteria improves risk stratification of smear-negativetuberculosis suspects. Methods: Clinical data from tuberculosissuspects evaluated by the San Francisco Department of PublicHealth Tuberculosis Control Clinic from March 2005 to February2008 were reviewed. We excluded tuberculosis suspects who wereacid fast bacilli smear-positive, HIV-infected, or under 10years of age. We developed a clinical prediction model for culture-positivedisease and examined the benefit of adding quantitative interferon- ${gamma}$ results measured by QuantiFERON®-TB Gold. Main Results:Of 660 patients meeting eligibility criteria, 65 (10%) had culture-proventuberculosis. The odds of active tuberculosis increased by 7%(95% CI 3-11%) for each doubling of interferon- ${gamma}$ level. The additionof quantitative interferon- ${gamma}$ results to objective clinical datasignificantly improved model performance (c-statistic 0.71 vs.0.78, p<0.001) and correctly reclassified 32% of tuberculosissuspects (95% CI 11-52%, p<0.001) into higher or lower riskcategories. However, quantitative interferon- ${gamma}$ results did notsignificantly improve appropriate risk reclassification beyondthat provided by clinician assessment of risk (5%, 95% CI -7to +22%, p=0.14). Conclusion: Higher quantitative interferon- ${gamma}$ results were associated with active tuberculosis, and addedclinical value to a prediction model incorporating conventionalrisk factors. While this benefit may be attenuated within highlyexperienced centers, the predictive accuracy of quantitativeinterferon- ${gamma}$ levels should be evaluated in other settings.

Key words: Interferon-gamma release assay • Quantiferon • risk prediction • risk reclassification

Evaluation of Quantitative Interferon- Response for Risk Stratification of Active Tuberculosis Suspects

Evaluation of Quantitative Interferon- ${gamma}$ Response for Risk Stratification of Active Tuberculosis Suspects