<i>In Situ</i>Expression of Regulatory Cytokines by Heart Inflammatory Cells in Chagas' Disease Patients with Heart Failure

Rodrigues, Denise Bertulucci Rocha; Reis, Marlene Antônia dos; Romano, Audrey; Pereira, Sanívia Aparecida de Lima; Teixeira, Vicente de Paula Antunes; Tostes, Sebastião; Rodrigues, Virmondés

doi:10.1155/2012/361730

Cited by 69 publications

(84 citation statements)

References 28 publications

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“…TNF-α has been pointed out as a key molecule in the generation of ectopic TLO which might facilitate the perpetuation of inflammation in the heart. Cells expressing TNF-α and IFN-γ have been identified in heart tissues from patients with chronic chagasic cardiomyopathy [9], [50]. Our findings showing T-bet expression in areas of high inflammation and proliferation further confirmed a type 1 T cell response in patients with severe heart disease.…”

Section: Discussionsupporting

confidence: 77%

“…Lymphocytes in these lesions express lymphocyte function antigen-a (LFA-1), CD44, very late antigen-4 (VLA-4) [7] and cytotoxic lymphocyte antigen 4 (CTLA-4) [8]. A Th1 cytokine pattern predominated in the cardiac inflammatory cell infiltrate of Chagas disease patients with heart failure [9].Whereas some authors have shown increased peripheral levels of IFN-γ in patients with severe heart disease [10]–[12], other studies have demonstrated an inverse association between disease severity and IFN-γ production [8], [13], [14].We have previously shown that most IFN-γ-secreting T cells in response to T. cruzi display a low grade of differentiation but high expression of the inhibitory receptor CTLA-4 in the circulation of subjects with chronic T. cruzi infection [8], [15], [16]. Conversely, the total T cell compartment in Chagas disease patients is enriched in highly differentiated T cells compared to uninfected controls [15]–[17].…”

Section: Introductionmentioning

confidence: 99%

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Presence of Antigen-Experienced T Cells with Low Grade of Differentiation and Proliferative Potential in Chronic Chagas Disease Myocarditis

et al. 2014

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BackgroundThe main consequence of chronic Trypanosoma cruzi infection is the development of myocarditis in approximately 20–30% of infected individuals but not until 10–20 years after the initial infection. We have previously shown that circulating interferon-γ-secreting T cells responsive to Trypanosoma cruzi antigens in chronic Chagas disease patients display a low grade of differentiation and the frequency of these T lymphocytes decreases along with the severity of heart disease. This study thought to explore the expression of inhibitory receptors, transcription factors of type 1 or regulatory T cells, and markers of T cell differentiation, immunosenescence or active cell cycle in cardiac explants from patients with advanced Chagas disease myocarditis.Methodology/Principal FindingsThe expression of different markers for T and B cells as well as for macrophages was evaluated by immunohistochemistry and immunofluorescence techniques in cardiac explants from patients with advanced chronic Chagas disease submitted to heart transplantation. Most infiltrating cells displayed markers of antigen-experienced T cells (CD3+, CD4+, CD8+, CD45RO+) with a low grade of differentiation (CD27+, CD57−, CD45RA−, PD-1−). A skewed T helper1/T cytotoxic 1 profile was supported by the expression of T-bet; whereas FOXP3+ cells were scarce and located only in areas of severe myocarditis. In addition, a significant proliferative capacity of CD3+ T cells, assessed by Ki67 staining, was found.Conclusions/SignificanceThe quality of T cell responses and immunoregulatory mechanisms might determine the pattern of the cellular response and the severity of disease in chronic Trypanosoma cruzi infection.

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Section: Discussionsupporting

confidence: 77%

Section: Introductionmentioning

confidence: 99%

Presence of Antigen-Experienced T Cells with Low Grade of Differentiation and Proliferative Potential in Chronic Chagas Disease Myocarditis

et al. 2014

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“…The etiology of Chagas disease is multifaceted, and may involve an autoimmune component in addition to protracted damage to myocytes and cardiac neuronal and vascular networks caused by parasites persisting in host tissues (Bonney et al 2011; Cummings and Tarleton 2003; Davila et al 1989; Girones et al 2007; Leon et al 2004; Ribeiro dos Santos et al 1992; Rossi 1990; Teixeira et al 2011; Zhang and Tarleton 1999). Both cytotoxic CD8+ effector T lymphocytes and IFN-γ-producing CD4+ T cells (Th1 cells), are important for controlling T. cruzi parasitosis (Hoft et al 2000; Hunter et al 1997; Kumar and Tarleton 2001; Rodrigues et al 2000; Tzelepis et al 2007), yet these T cells may also contribute to the development of pathogenic inflammation during T. cruzi infection (Bonney et al 2011; Gomes et al 2003; Laucella et al 2004; Minoprio 2001; Ribeiro dos Santos et al 1992; Rizzo et al 1989; Rocha Rodrigues et al 2012; Soares et al 2001; Tarleton et al 1996; Tarleton et al 1994). IL-17, which is produced by Th17 cells and other cell types, has been associated with both pro- and anti-inflammatory functions in other disease models, and may play an anti-inflammatory role during T. cruzi infection by indirectly down-regulating the functions of pro-inflammatory Th1 cells, without interfering with parasite clearance (Guedes et al 2012; Soares et al 2012; Tosello Boari et al 2012).…”

Section: Introductionmentioning

confidence: 99%

Depletion of regulatory T cells decreases cardiac parasitosis and inflammation in experimental Chagas disease

et al. 2015

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Infection with the protozoan parasite Trypanosoma cruzi may lead to a potentially fatal cardiomyopathy known as Chagas heart disease. This disease is characterized by infiltration of the myocardium by mononuclear cells, including CD4+ T cells, together with edema, myofibrillary destruction and fibrosis. A multifaceted systemic immune response develops that ultimately keeps parasitemia and tissue parasitosis low. T helper 1 and other pro-inflammatory T cell responses are effective at keeping levels of T. cruzi low in tissues and blood, but they may also lead to tissue inflammation when present chronically. The mechanism by which the inflammatory response is regulated in T. cruzi infected individuals is complex, and the specific roles that Th17 and T regulatory (Treg) cells may play in that regulation are beginning to be elucidated. In this study, we found that depletion of Treg cells in T. cruzi-infected mice leads to reduced cardiac parasitosis and inflammation, accompanied by an augmented Th1 response early in the course of infection. This is followed by a down-regulation of the Th1 response and increased Th17 response late in infection. The effect of Treg cell depletion on the Th1 and Th17 cells is not observed in mice immunized with T. cruzi in adjuvant. This suggests that Treg cells specifically regulate Th1 and Th17 cell responses during T. cruzi infection, and may also be important for modulating parasite clearance and inflammation in the myocardium of T. cruzi-infected individuals.

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“…Durante a fase crônica da infecção, o miocárdio de pacientes com CCC apresenta um infiltrado inflamatório com predominância de células correspondentes a uma resposta do tipo Th1, sendo composto principalmente por células T CD8 + , CD4 + e macrófagos (Abel et al, 2001;Higuchi et al, 1993;Milei et al, 1992;Morato et al, 1998;Reis et al, 1993;Rocha Rodrigues et al, 2012). Além disso, ocorre a produção de grandes quantidades de IFN-e TNF , por outro lado IL-4, IL-6, IL-7, e IL-15 são encontradas em pequenas quantidades no miocárdio (Abel et al, 2001;Cunha-Neto et al, 2005;Fonseca et al, 2007;Higuchi et al, 1993;Reis et al, 1993Reis et al, ,1997Rocha Rodrigues et al, 2012 (Kierszenbaum, 1980;Krettli, Brener, 1976).…”

Section: A Resposta Imuneunclassified

“…Além disso, ocorre a produção de grandes quantidades de IFN-e TNF , por outro lado IL-4, IL-6, IL-7, e IL-15 são encontradas em pequenas quantidades no miocárdio (Abel et al, 2001;Cunha-Neto et al, 2005;Fonseca et al, 2007;Higuchi et al, 1993;Reis et al, 1993Reis et al, ,1997Rocha Rodrigues et al, 2012 (Kierszenbaum, 1980;Krettli, Brener, 1976). A resposta celular é importante para o controle inicial da infecção, no entanto, uma resposta efetiva mediada por anticorpos é crítica para o aumento da sobrevivência.…”

Section: A Resposta Imuneunclassified

A prolinemia como um fator de severidade na infecção causada pelo <i>Trypanosoma cruzi</i>.

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In SituExpression of Regulatory Cytokines by Heart Inflammatory Cells in Chagas' Disease Patients with Heart Failure

Cited by 69 publications

References 28 publications

Presence of Antigen-Experienced T Cells with Low Grade of Differentiation and Proliferative Potential in Chronic Chagas Disease Myocarditis

Presence of Antigen-Experienced T Cells with Low Grade of Differentiation and Proliferative Potential in Chronic Chagas Disease Myocarditis

Depletion of regulatory T cells decreases cardiac parasitosis and inflammation in experimental Chagas disease

A prolinemia como um fator de severidade na infecção causada pelo <i>Trypanosoma cruzi</i>.

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