Advances in the diagnosis of tuberculosis

Lange, Christoph; Mori, Toru

doi:10.1111/j.1440-1843.2009.01692.x

Cited by 135 publications

(120 citation statements)

References 248 publications

(315 reference statements)

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“…sarcoidosis or NTM infections except for the demonstration of stained tubercle bacilli [6]. Culture test has variable sensitivities of 3-80% in various clinical EPTB samples and it takes 4-8 weeks to get those results and also requires trained technicians [7]. The Mantoux test is widely employed world-wide but the false-positive results are observed due to the previous bacillus Calmette-Guérin (BCG) immunization or exposure to atypical mycobacteria and false-negative results also occur in aged individuals or immuno-suppressed individuals [7].…”

Section: Present Scenario Of Tb Diagnosismentioning

confidence: 99%

Gene Xpert MTB/RIF Assay: A New Hope for Extrapulmonary Tuberculosis

Raj¹

2012

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The diagnostic efforts for extrapulmonary tuberculosis (TB) have been severely hampered by the lack of diagnostic tests that are accurate, simple to use and can be applied at the point of clinical care. This has been further enhanced by the widespread inability to test for drug resistance. Gene Xpert® MTB/RIF test is a novel test for the diagnosis of extrapulmonary TB and rifampicin resistance. This unique test can be used almost everywhere with minimal technical expertise, enabling diagnosis of extrapulmonary TB and simultaneous assessment of rifampicin resistance to be completed within 2 h. In low-income countries, however, its cost, environmental limitations and difficulties involved in supply and maintenance are major obstacles. While it may be suitable for major reference hospitals, operational research is needed to evaluate the test and its additional yield above high-quality smear microscopy. In high TB burden countries like India, WHO in 2010 endorsed some guidelines for implantation of Gene Xpert® MTB/RIF test for diagnosis of TB and drug resistance.

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Section: Present Scenario Of Tb Diagnosismentioning

confidence: 99%

Gene Xpert MTB/RIF Assay: A New Hope for Extrapulmonary Tuberculosis

Raj¹

2012

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“…Preference is given to sensitivity at the cost of specificity if the expected risk is particularly high, such as in the case of immunodeficiency of an individual [39], but whether this trade-off is as efficient as postulated has been called into question, at least in HIV-associated immunodeficiency [40]. More recently, bloodbased IGRAs have been developed and evaluated for the risk estimation of TB in clinical routine [41]. As with TST, IGRAs rely on specific stimulation of effector T-cells that are activated to produce cytokines within hours after stimulation, and IFN-c is most commonly used as readout for specific activation of T-cells [42].…”

Section: Risk Of Tb In Sot Recipientsmentioning

confidence: 99%

The risk of tuberculosis in transplant candidates and recipients: a TBNET consensus statement

Bumbăcea

Arend

Eyüboğlu³

et al. 2012

Eur Respir J

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Tuberculosis (TB) is a possible complication of solid organ and hematopoietic stem cell transplantation. The identification of candidates for preventive chemotherapy is an effective intervention to protect transplant recipients with latent infection with Mycobacterium tuberculosis from progressing to active disease. The best available proxy for diagnosing latent infection with M. tuberculosis is the identification of an adaptive immune response by the tuberculin skin test or an interferon-c based ex vivo assay. Risk assessment in transplant recipients for the development of TB depends on, among other factors, the locally expected underlying prevalence of infection with M. tuberculosis in the target population. In areas of high prevalence, preventive chemotherapy for all transplant recipients may be justified without immunodiagnostic testing while in areas of medium and low prevalence, preventive chemotherapy should only be offered to candidates with positive M. tuberculosis-specific immune responses. The diagnosis of TB in transplant recipients can be challenging. Treatment of TB is often difficult due to substantial interactions between anti-TB drugs and immunosuppressive medications. This management guideline summarises current knowledge on the prevention, diagnosis and treatment of TB related to solid organ and hematopoietic stem cell transplantation and provides an expert consensus on questions where scientific evidence is still lacking. KEYWORDS: Guideline, management, Mycobacterium tuberculosis, transplantation, tuberculosis T uberculosis (TB) is caused by the pathogenic species of the Mycobacterium tuberculosis complex. Only a minority of individuals who develop an adaptive immune response following infection with M. tuberculosis will ever develop TB, with the actual risk depending on the extent to which the host immune system provides a successful or inadequate response [1,2]. Therefore, individuals with impaired immune response, such as solid organ transplant (SOT) and hematopoietic stem cell transplant (HSCT) recipients, are more prone to develop TB than immunocompetent persons. TB in transplant recipients is more frequent compared to the general population (estimates from the last decades state 20-74 times as frequent in SOT [3,4] and twice as frequent in HSCT [5]), and more often fatal (up to 31% in SOT [6] and up to 50% in HSCT recipients [7]), thus adding effectiveness to interventions for its prevention, even in the face of difficulties, with treatment related to adverse drug events and drug-drug interactions. Active TB in transplant recipients can result from latent infection with M. tuberculosis (LTBI) in the transplant candidate or in the donor tissue, or from de novo post-transplant infection. These various scenarios prompt for targeted pre-transplant screening of both recipient and, if possible, donors to allow focused management of recipients selected for preventive intervention in the pre-and/or posttransplant period. The term ''preventive chemotherapy'' is used to denote treatmen...

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“…Further evidence has since substantiated this discovery and >40 additional biomarkers have been screened for diagnostic potential. Of all investigated markers, it appears that IP-10 is the most consistently expressed in response to antigen challenge, rendering it the most promising alternative marker to IFN-g [18][19][20][21][22][23][24][25][26][27] and a promising means of improving IGRAs [28][29][30][31][32][33][34].…”

Section: Discovery Of Ip-10 As a Biomarker For Tb Infectionmentioning

confidence: 99%