Mycobacterial heat shock protein‐induced blood T lymphocytes subsets and cytokine pattern: Comparison of sarcoidosis with tuberculosis and healthy controls

Dubaniewicz, Anna; Trzonkowski, Piotr; Dubaniewicz-Wybieralska, Mirosława; Dubaniewicz, Andrzej; Singh, Mahavir; Myśliwski, Andrzej

doi:10.1111/j.1440-1843.2007.01076.x

Cited by 52 publications

(74 citation statements)

References 37 publications

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“…Two studies demonstrate the presence of circulating antibodies against mycobacterial cell culture extracts in subsets of patients with sarcoidosis [96,97]. More recently, Drake and colleagues demonstrated sarcoidosis patients have immune responses to mycobacteria-derived antigens to ESAT-6, CFP-10, antigen-85A, and superoxide dismutase while Dubaniewicz and colleagues report immune responses to mycobacterial heat shock proteins in sarcoidosis [98][99][100][101][102][103][104]. There may be a genetic basis for responses to mycobacterial antigens in sarcoidosis (Table 2).…”

Section: Role Of Mycobacterial Organisms In Sarcoidosismentioning

confidence: 96%

Etiologies of Sarcoidosis

Chen

Möller

2015

Clinic Rev Allerg Immunol

117

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Since sarcoidosis was first described more than a century ago, the etiologic determinants causing this disease remain uncertain. Studies suggest that genetic, host immunologic, and environmental factors interact together to cause sarcoidosis. Immunologic characteristics of sarcoidosis include non-caseating granulomas, enhanced local expression of T helper-1 (and often Th17) cytokines and chemokines, dysfunctional regulatory T-cell responses, dysregulated Toll-like receptor signaling, and oligoclonal expansion of CD4+ T cells consistent with chronic antigenic stimulation. Multiple environmental agents have been suggested to cause sarcoidosis. Studies from several groups implicate mycobacterial or propionibacterial organisms in the etiology of sarcoidosis based on tissue analyses and immunologic responses in sarcoidosis patients. Despite these studies, there is no consensus on the nature of a microbial pathogenesis of sarcoidosis. Some groups postulate sarcoidosis is caused by an active viable replicating infection while other groups contend there is no clinical, pathologic, or microbiologic evidence for such a pathogenic mechanism. The authors posit a novel hypothesis that proposes that sarcoidosis is triggered by a hyperimmune Th1 response to pathogenic microbial and tissue antigens associated with the aberrant aggregation of serum amyloid A within granulomas, which promotes progressive chronic granulomatous inflammation in the absence of ongoing infection.

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Section: Role Of Mycobacterial Organisms In Sarcoidosismentioning

confidence: 96%

Etiologies of Sarcoidosis

Chen

Möller

2015

Clinic Rev Allerg Immunol

117

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“…If the remaining parenchymal cells cannot re-establish the normal architecture, T H 2 type cytokines (e.g. IL-4, IL-5, IL-10, IL-13) and macrophage-derived factors including fibronectin, platelet-derived growth factor, insulin-like Immunological markers of sarcoidosis 57 (Saboor et al 1992;Grosser et al 1999;Li et al 1999;Klemen et al 2000;Drake et al 2002;Eishi et al 2002;Gazouli et al 2002;Gupta et al 2007), which could suggest cell-wall deficient mycobacterial infection (Kon and du Bois 1997;Brown et al 2003), however, others have not found PCR evidence of mycobacterial DNA or RNA (Lisby et al 1993;Cannone et al 1997;Vokurka et al 1997) Elevated circulating IgG directed against mycobacterial catalase-peroxidase (KatG) peptides in sarcoidosis patients and other circulating antibodies against mycobacterial antigens (Song et al 2005), and other evidence of BAL and peripheral blood mononuclear cell responses to Mycobacterium tuberculosis heat shock proteins, mycolyl transferase antigen 85A, superoxide dismutase A, ESAT-6 and KatG peptides Drake et al 2007;Dubaniewicz et al 2007;Hajizadeh et al 2007;Allen et al 2008;Oswald-Richter et al 2009;Dubaniewicz 2010). A large worldwide study confirmed T H 1 responses to Mycobacterium tuberculosis KatG despite differences in patient phenotype, genetic and prognostic characteristics and showed that mKatG reactive CD4?…”

Section: Immunopathogenesis Of Sarcoidosismentioning

confidence: 96%

The potential of the immunological markers of sarcoidosis in exhaled breath and peripheral blood as future diagnostic and monitoring techniques

2011

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Sarcoidosis is characterised by non-caseating granulomatous inflammation, with exaggerated immune responses at sites of disease and derangements of normal tissue architecture. The lungs are most commonly involved and progressive inflammation may result in pulmonary fibrosis. The immunopathogenesis and aetiology remain uncertain, which has made it difficult to identify a single sufficiently sensitive or specific diagnostic marker. Further investigation is needed to identify sensitive and specific markers of disease, such as in peripheral blood and exhaled breath condensate (EBC). Identification of disease markers may also be useful for investigating disease activity and predicting progression to fibrosis. This review explores the literature on the cytokine profiles of blood and bronchoalveolar lavage lymphocytes following ex vivo stimulation, as well as disease markers measured using the medium of EBC.

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“…An aliquot of PBMCs was analysed by flow cytometry (reviewed in [31,32]). The population of PBMCs, that is, lymphocytes and monocytes together, was chosen to mimic in vivo occurring conditions, including possible cell-tocell interactions of different PBMC subpopulations.…”

Section: Isolation Of Pbmcsmentioning

confidence: 99%

Changed phagocytic activity and pattern of Fcγ and complement receptors on blood monocytes in sarcoidosis

et al. 2012

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Mycobacterial heat shock protein‐induced blood T lymphocytes subsets and cytokine pattern: Comparison of sarcoidosis with tuberculosis and healthy controls

Abstract: After Mtb-hsp stimulation, increased levels of pro-inflammatory cytokines, TNF-alpha and IL-6 were found in sera from SA and TB patients in comparison with healthy controls; SA patients demonstrated the lowest levels of IL-4 and the highest levels of IL-10.

Cited by 52 publications

References 37 publications

Etiologies of Sarcoidosis

Etiologies of Sarcoidosis

The potential of the immunological markers of sarcoidosis in exhaled breath and peripheral blood as future diagnostic and monitoring techniques

Changed phagocytic activity and pattern of Fcγ and complement receptors on blood monocytes in sarcoidosis

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