Mycobacterium tuberculosis Infection in Health Care Workers in Rural India

Pai, Madhukar; Gokhale, Kaustubh; Joshi, Rajnish; Dogra, Sandeep; Kalantri, Shriprakash; Mendiratta, DK; Narang, P; Daley, Charles L.; Granich, Reuben; Mazurek, Gerald H.; Reingold, Arthur; Riley, Lee W.; Colford, John M.

doi:10.1001/jama.293.22.2746

Cited by 292 publications

(129 citation statements)

References 26 publications

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“…Our results with an overall high percent agreement between TST and IFN-␥ assay with low are consistent with and support the findings by other studies that have reported overall agreements of 81.4 to 95.0% with values of 0.08 to 0.87 (8,23,29,30). Kappa statistics have been accepted and widely used as a test of interobserver agreement (16).…”

Section: Discussionsupporting

confidence: 92%

“…Consequently, IFN-␥ assays utilizing ESAT-6 and CFP-10 either as recombinant antigens (5,7,38) or mixtures of overlapping peptides (8,27,37) have been shown to be significantly more specific than TST. In addition, these assays offer several advantages over TST, including the need for only a single patient contact, simultaneous measurement of a subject's immune reactivity to mitogen (phytohemagglutinin) and nil control (normal saline) antigens, elimination of subjectivity in administering the test or reading the result, and the availability of test results within 24 h. IFN-␥ assays utilizing ESAT-6 and CFP-10 antigens have been studied in the general population in several countries including India, Korea, Italy, Denmark, The Netherlands, and Japan (5,7,8,15,23,27,29,30,38). To date, there are no published reports on comparison of TST to the newly approved IFN-␥ assay in studies within the United States.…”

mentioning

confidence: 99%

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Comparison of a New ESAT-6/CFP-10 Peptide-Based Gamma Interferon Assay and a Tuberculin Skin Test for Tuberculosis Screening in a Moderate-Risk Population

Porsa

Liu

Seale

et al. 2006

Clin Vaccine Immunol

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Section: Discussionsupporting

confidence: 92%

mentioning

confidence: 99%

Comparison of a New ESAT-6/CFP-10 Peptide-Based Gamma Interferon Assay and a Tuberculin Skin Test for Tuberculosis Screening in a Moderate-Risk Population

Porsa

Liu

Seale

et al. 2006

Clin Vaccine Immunol

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“…Perhaps most intriguing was our finding that in the blood, ESAT-6-specific IFN-␥ production could not distinguish M. tuberculosis-infected susceptible CBA/J mice from noninfected mice. The same pattern can also be observed in humans, for whom peripheral-blood IGRAs failed to detect small proportions of M. tuberculosisinfected individuals (18,37) and TB patients (45) bovis BCG vaccination of calves (59) and relatively resistant C57BL/6 mice (17) showed decreased ESAT-6-specific IFN-␥ blood responses, likely reflecting antigenic loads lower than those of nonvaccinated control animals. Because CBA/J, DBA/2, and C3H/HeJ mice had low circulating ESAT-6 responses during primary M. tuberculosis infection, we predict minimal changes due to BCG vaccination, antibiotic treatment, or immunosuppression.…”

supporting

confidence: 57%

Peripheral Blood Gamma Interferon Release Assays Predict Lung Responses andMycobacterium tuberculosisDisease Outcome in Mice

Beamer

Flaherty

Vesosky

et al. 2008

Clin Vaccine Immunol

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Current diagnostic tests for tuberculosis (TB) are not able to distinguish active disease from latent Mycobacterium tuberculosis infection, nor are they able to quantify the risk of a latently infected person progressing to active TB. There is interest, however, in adapting antigen-specific gamma interferon (IFN-␥) release assays (IGRAs) to predict disease outcome. In this study, we used the differential susceptibilities of inbred mouse strains to M. tuberculosis infection to evaluate the prognostic capabilities of IGRAs. Using lung and blood cultures, we determined that CBA/J, DBA/2, and C3H/HeJ mice (models of heightened risk of progression to active TB) produced less antigen-specific IFN-␥ in response to M. tuberculosis culture filtrate proteins and early secreted antigenic target-6 than the relatively resistant C57BL/6 mouse strain. Additionally, reduced IFN-␥ secretion in supernatants reflected a reduced frequency of IFN-␥-responding cells in the lung and blood and not a specific defect in IFN-␥ secretion at the single-cell level. Importantly, detection of antigen-specific IFN-␥ from blood cultures accurately reflected lung responses, indicating that blood can be an appropriate test tissue in humans. Furthermore, reduced antigen-specific IFN-␥ production and low frequencies of IFN-␥-responding cells from peripheral blood predicted increased risk of TB disease progression across genetically diverse TB disease-susceptible mouse strains, suggesting that similar results may occur in humans. The development of efficacious predictive diagnostic tests for humans would lead to targeted therapy prior to progression to active TB, reducing transmission, incidence, and prevalence rates while maximizing the use of public health resources.Mycobacterium tuberculosis, the causative agent of tuberculosis (TB), infects up to one-third of the world's population (60). The majority (90%) of infected adults control M. tuberculosis in a latent state that is clinically silent and is not considered contagious. In contrast, the remaining 10% of M. tuberculosis-infected individuals progress to contagious, active TB and may transmit bacilli to others, resulting in significant global morbidity and mortality each year (61). The mechanisms that contribute to M. tuberculosis susceptibility and TB disease progression in humans are multifactorial and reflect altered pulmonary immunity due to polygenic interactions, immune status, age, and environmental factors (6, 50). These interactions contribute to the common outcome of active TB, associated with increased growth of M. tuberculosis in the lung and detrimental pulmonary inflammation, for which similar disease characteristics have been described in animal models (4,12,54).Although the predisposing mechanisms underlying progression to active TB are not fully understood, we and others (1,36,41) propose that the transition from latency to active TB can be detected, quantified, and predicted by peripheral immune responses prior to disease onset. The identification of such biomarkers could then...

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“…The specificity of the ELISPOT-MTP assay was confirmed by the fact that 100% of the ELISPOT-MTP positive subjects were ELISPOT-BCG positive and 97% were ELISPOT-PPD positive. Conversely, the fact that 76% of the ELISPOT-MTP negative subjects were ELISPOT-BCG positive and 59% were ELISPOT-PPD positive supports the idea that most contacts may be vaccinated (Table 1) or NTM infected, thus underlining the greater sensitivity of the ELISPOT assay over the TST, as has also been reported by others (20,28,32,34). Of note, 44 of the 67 individuals with a documented BCG scar were ELISPOT-MTP negative but ELISPOT-BCG positive.…”

Section: Discussionsupporting

confidence: 71%

An In-House RD1-Based Enzyme-Linked Immunospot-Gamma Interferon Assay Instead of the Tuberculin Skin Test for Diagnosis of LatentMycobacterium tuberculosisInfection

et al. 2006

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Identification of individuals infected with Mycobacterium tuberculosis is essential for the control of tuberculosis (TB). The specificity of the currently used tuberculin skin test (TST) is poor because of the broad antigenic cross-reactivity of purified protein derivative (PPD) with BCG vaccine strains and environmental mycobacteria. Both ESAT-6 and CFP-10, two secretory proteins that are highly specific for M. tuberculosis complex, elicit strong T-cell responses in subjects with TB. Using an enzyme-linked immunospot (ELISPOT)-IFN-␥ assay and a restricted pool of peptides derived from ESAT-6 and CFP-10, we have previously demonstrated a high degree of specificity and sensitivity of the test for the diagnosis of TB. Here, 119 contacts of individuals with contagious TB who underwent TST and the ELISPOT-IFN-␥ assay were consecutively recruited. We compared the efficacy of the two tests in detecting latent TB infection and defined a more appropriate TST cutoff point. There was little agreement between the tests (k ‫؍‬ 0.33, P < 0.0001): 53% of the contacts with a positive TST were ELISPOT negative, and 7% with a negative TST were ELISPOT positive. Furthermore, respectively 76 and 59% of the ELISPOT-negative contacts responded in vitro to BCG and PPD, suggesting that most of them were BCG vaccinated or infected with nontuberculous mycobacteria. The number of spot-forming cells significantly correlated with TST induration (P < 0.0001). Our in-house ELISPOT assay based on a restricted pool of highly selected peptides is more accurate than TST for identifying individuals with latent TB infection and could improve chemoprophylaxis for the control of TB.One-third of the world's population is believed to be latently infected with Mycobacterium tuberculosis, the etiological agent of tuberculosis (TB), whose global resurgence, supported by the human immunodeficiency virus type 1 (HIV-1) pandemic and emerging multidrug resistance, underlines the need for new control measures and strategies to make a specific diagnosis and prevent transmission (19). Moreover, continued vigilance against active and latent TB is essential in industrialized countries because of the increased immigration from areas with endemic infection.The compulsory screening of immigrant populations for TB has been proposed as a means of controlling this communicable disease (14, 15) but, although the tuberculin skin test (TST) is the method of choice for detecting latent M. tuberculosis infection (LTBI), it cannot be considered a gold standard because of the number of false-positive and negative reactions, and the variability of their interpretation (1, 2). In particular, the purified protein derivative (PPD) antigen used for the test has broad cross-reactivity with antigens derived from various mycobacterial species, including the vaccine strains of Bacillus Calmette-Guérin (BCG) (1, 2), and false-negative results occur in patients with advanced TB or severe immunodeficiency (10,25). Another operational drawback of TST is the need for a return visit to allo...

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Mycobacterium tuberculosis Infection in Health Care Workers in Rural India

Cited by 292 publications

References 26 publications

Comparison of a New ESAT-6/CFP-10 Peptide-Based Gamma Interferon Assay and a Tuberculin Skin Test for Tuberculosis Screening in a Moderate-Risk Population

Comparison of a New ESAT-6/CFP-10 Peptide-Based Gamma Interferon Assay and a Tuberculin Skin Test for Tuberculosis Screening in a Moderate-Risk Population

Peripheral Blood Gamma Interferon Release Assays Predict Lung Responses andMycobacterium tuberculosisDisease Outcome in Mice

An In-House RD1-Based Enzyme-Linked Immunospot-Gamma Interferon Assay Instead of the Tuberculin Skin Test for Diagnosis of LatentMycobacterium tuberculosisInfection

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