Regulatory and effector T-cells are differentially modulated by Dexamethasone

Pandolfi, Julieta Belen; Baz, Placida; Fernandez, Pablo Mariano; Discianni Lupi, Ailen; Payaslián, Florencia; Billordo, Luis Ariel; Fainboim, Leonardo; Arruvito, Maria Lourdes

Artículos de revistas

Fecha

2013-12

Registro en:

Pandolfi, Julieta Belen; Baz, Placida; Fernandez, Pablo Mariano; Discianni Lupi, Ailen; Payaslián, Florencia; et al.; Regulatory and effector T-cells are differentially modulated by Dexamethasone; Elsevier; Clinical Immunology; 149; 3B; 12-2013; 400-410

1521-6616

http://hdl.handle.net/11336/1901

http://repositorioslatinoamericanos.uchile.cl/handle/2250/1883755

Autor

Pandolfi, Julieta Belen

Baz, Placida

Fernandez, Pablo Mariano

Discianni Lupi, Ailen

Payaslián, Florencia

Billordo, Luis Ariel

Fainboim, Leonardo

Arruvito, Maria Lourdes

Institución

Consejo Nacional de Investigaciones Científicas y Tecnológicas (Argentina)

Resumen

It is assumed that the ratio between effector T cells (Teff) and regulatory T cells (Tregs) controls the immune reactivity within the T-cell compartment. The purpose of this study was to investigate if Dexamethasone (Dex) affects Teff and Tregs subsets. Dex induced on Tregs a dose and time-dependent apoptosis which resulted in a relative increase of Teff. After TCR activation, Dex induced a strong proliferative inhibition of Teff, but a weaker proliferative inhibition on Tregs. These effects were modulated by IL-2, which not only restored the proliferative response, but also prevented Dex-induced apoptosis. The highest dose of IL-2 prevented apoptosis on all FOXP3 + CD4+ T cells. Meanwhile, the lowest dose only rescued activated Tregs (aTregs), probably related to their CD25 higher expression. Because Dex did not affect the suppressor capacity of aTregs either, our results support the notion that under Dex treatment, the regulatory T-cell compartmentmaintains its homeostasis.

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