Human T‐ and B‐Cell Reactivity to the 16 kDa α‐Crystallin Protein of <i>Mycobacterium tuberculosis</i>

Wilkinson, Robert J.; Wilkinson, Katalin A.; Smet, K. A. L. De; Hasløv, K; Pasvol, Geoffrey; Singh, Mahavir; Svarcova, Ivana; Iványi, Juraj

doi:10.1046/j.1365-3083.1998.00420.x

Cited by 75 publications

(74 citation statements)

References 31 publications

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“…It has been identified as a highly expressed protein under hypoxic conditions mimicking dormancy (38) and upon macrophage infection (26) and is considered as such as a marker for latency (6). Its species specificity and early T-cell immunodominance in the mouse and human are well documented (43,45), and our novel cattle data are in agreement with these previous reports. Since HspX is expressed primarily during the late stage of infection, it has interesting potential as a diagnostic reagent.…”

Section: Discussionsupporting

confidence: 90%

Genomic Approach to Identification of Mycobacterium bovis Diagnostic Antigens in Cattle

et al. 2003

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Differential delayed-type hypersensitivity skin testing with tuberculin purified protein derivatives from Mycobacterium bovis and M. avium is the standard for diagnosing bovine tuberculosis. However, improved tests based on defined, specific antigens are urgently needed. In the present study, a combination of bioinformatics, molecular biology, and bovine models of infection were used to screen mycobacterial proteins for their potential as diagnostic reagents which could be used in a whole-blood assay for diagnosis of tuberculosis. Initial screening of 28 proteins selected in silico and expressed as recombinants in Escherichia coli indicated that CFP-10, ESAT-6, TB27.4, TB16.2, TB15.8, and TB10.4 induced strong gamma interferon responses in experimentally infected cattle. A more thorough investigation over time in two groups of animals infected with a high (10 6 CFU) and a low (10 4 CFU) dose of M. bovis revealed that, for both groups, the strength of the in vitro response to individual antigens varied greatly over time. However, combining the results for ESAT-6, CFP-10, and TB27.4, possibly supplemented with TB10.4, gave sensitivities at different infection stages close to those obtained with M. bovis purified protein derivative. Importantly, while responsiveness to ESAT-6 and CFP-10 correlated strongly for individual samples, the same was not the case for ESAT-6 and TB27.4 responsiveness. The results suggest that combinations of specific antigens such as these have great potential in development of optimized diagnostic systems for bovine tuberculosis.

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Section: Discussionsupporting

confidence: 90%

Genomic Approach to Identification of Mycobacterium bovis Diagnostic Antigens in Cattle

et al. 2003

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“…Surprisingly, while increased IFN-␥ responses to ␣-crystallin were observed for adults with a history of past BCG vaccination (41), no significant response to this antigen was detected in BCG-immunized infants 2 months after vaccination. The expression of ␣-crystallin and the development of a primary immune response to this antigen may be slower than that of other mycobacterial antigens in vivo (15).…”

Section: Discussionmentioning

confidence: 81%

“…We endeavored to evaluate their potential value as candidates for vaccine development or for the immunodiagnosis of tuberculosis. In areas with a low incidence of tuberculosis, these antigens had been previously shown to stimulate the production of IFN-␥ in tuberculin skin test-positive but not in tuberculin skin test-negative individuals (1,4,14,16,17,34,40,41). In this study, we confirm that all antigens are able to stimulate IFN-␥ production, but important differences were observed among groups exposed to different levels and types of mycobacteria, especially in the responses to CFP-10 and ␣-crystallin.…”

Section: Discussionmentioning

confidence: 99%

Immune Responses to Mycobacterial Antigens in the Gambian Population: Implications for Vaccines and Immunodiagnostic Test Design

et al. 2004

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“…DNA vaccines have shown promise in their ability to enhance the activity of antibiotic treatment and reduce reactivation of LTBI and transmission (323)(324)(325). Adjunctive immunotherapy with a DNA vaccine containing the LTBI marker ␣-crystallin (233,(328)(329)(330) reduces the duration of antibiotic treatment in chronically infected mice (331). Similarly, RUTI, a therapeutic vaccine comprising detoxified, fragmented M. tuberculosis cells delivered in liposomes, also has been shown to enhance the effect of short-course chemotherapy in animal models (326) and is currently being evaluated in clinical trials (327).…”

Section: Reactivation Of Ltbimentioning

confidence: 99%

Latent Tuberculosis Infection: Myths, Models, and Molecular Mechanisms

Dutta

Karakousis

2014

Microbiol Mol Biol Rev

191

174

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SUMMARY The aim of this review is to present the current state of knowledge on human latent tuberculosis infection (LTBI) based on clinical studies and observations, as well as experimental in vitro and animal models. Several key terms are defined, including “latency,” “persistence,” “dormancy,” and “antibiotic tolerance.” Dogmas prevalent in the field are critically examined based on available clinical and experimental data, including the long-held beliefs that infection is either latent or active, that LTBI represents a small population of nonreplicating, “dormant” bacilli, and that caseous granulomas are the haven for LTBI. The role of host factors, such as CD4 + and CD8 + T cells, T regulatory cells, tumor necrosis factor alpha (TNF-α), and gamma interferon (IFN-γ), in controlling TB infection is discussed. We also highlight microbial regulatory and metabolic pathways implicated in bacillary growth restriction and antibiotic tolerance under various physiologically relevant conditions. Finally, we pose several clinically important questions, which remain unanswered and will serve to stimulate future research on LTBI.

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Human T‐ and B‐Cell Reactivity to the 16 kDa α‐Crystallin Protein of Mycobacterium tuberculosis

Cited by 75 publications

References 31 publications

Genomic Approach to Identification of Mycobacterium bovis Diagnostic Antigens in Cattle

Genomic Approach to Identification of Mycobacterium bovis Diagnostic Antigens in Cattle

Immune Responses to Mycobacterial Antigens in the Gambian Population: Implications for Vaccines and Immunodiagnostic Test Design

Latent Tuberculosis Infection: Myths, Models, and Molecular Mechanisms

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