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“An integral component of tuberculosis (TB) control in

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“An integral component of tuberculosis (TB) control in the United States is the identification and treatment of persons with latent tuberculosis infection (LTBI) [1]. Approximately 10% of persons infected with Mycobacterium

tuberculosis (M. tuberculosis) develop TB disease. However, the risk of developing TB varies, and recently infected persons have an increased risk for TB disease [2] and [3]. One group for whom screening is recommended is persons recently arrived from areas of the world with a high incidence of TB, many of whom have been vaccinated with Bacillus Calmette-Guérin (BCG) [4]. LTBI has historically been diagnosed using the tuberculin skin test (TST). The interpretation of the TST requires knowledge of a person’s medical and

Erastin chemical structure epidemiologic factors to determine the threshold at which the reaction is considered positive. Because the purified protein derivative used in the TST is a poorly defined mixture of antigens shared by the M. tuberculosis complex, including wild type Mycobacterium bovis, M. bovis var. BCG, and several other species of mycobacteria, it results in a specificity of approximately 60% in BCG-vaccinated populations [5]. Bleomycin datasheet The lack of specificity of the TST for M. tuberculosis has led to the inappropriate diagnosis of some patients with LTBI and to the development of alternative tests. Interferon-γ release assays (IGRAs), including QuantiFERON-TB-Gold (QFT-G), represent a new class of tests that has been approved by the Federal Drug Administration for the diagnosis of LTBI. The QFT-G test uses an enzyme-linked immunosorbent assay to measure the concentration of interferon-γ

Histone demethylase released by activated T-lymphocytes after stimulation by antigens that are specific to the M. tuberculosis complex, are widely absent in nontuberculous mycobacteria, and more importantly, are not expressed in BCG [6]. Thus, IGRAs, such as QFT-G, might be particularly useful to test for LTBI in persons who have been vaccinated with BCG [7]. The higher specificity of QFT-G and other IGRAs compared with the TST can be used to eliminate the unnecessary treatment of persons with false-positive TSTs. The aims of this study were (1) to determine the percentage of QFT-G positivity in persons with a history of BCG vaccination who had a positive TST result and (2) to identify patient characteristics that might predict a positive QFT test result. Patients with a positive TST result were referred by local providers to the pulmonary clinic that serves as a referral center for the greater Hartford metropolitan area for medical evaluations to exclude TB disease. Patients aged ≥18 years with a documented positive TST result (≥10 mm induration or ≥5 mm with a chest radiograph consistent with pulmonary TB) who presented to the clinic from June 2008 to December 2009 were included in this study.

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