Details

Autor(en) / Beteiligte

• Hwang, SuJin
• Tatsi, Christina
• Kuehn, Hye Sun
• Niemela, Julie E.
• Stoddard, Jennifer
• Su, Yan
• Lodish, Maya
• Uzel, Gulbu
• Spolski, Rosanne
• Leonard, Warren J.
• Holland, Steven M.
• Fleisher, Thomas A.
• Stratakis, Constantine A.
• Rosenzweig, Sergio D.

Titel

Cushing syndrome and glucocorticoids: T-cell lymphopenia, apoptosis, and rescue by IL-21

Ist Teil von

• Journal of allergy and clinical immunology, 2022-01, Vol.149 (1), p.302-314

Ort / Verlag

United States: Elsevier Inc

Erscheinungsjahr

2022

Quelle

MEDLINE

Beschreibungen/Notizen

• Pediatric endogenous Cushing syndrome (eCs) is mainly caused by pituitary corticotropin–producing adenomas, and most glucocorticoid-dependent effects progressively regress upon tumor removal. eCs reproduces long-term, high-dose glucocorticoid therapy, representing a clean, natural, and unbiased model in which to study glucocorticoid bona fide effects on immunity. We performed extensive immunologic studies in otherwise healthy pediatric patients with eCs before and 6 to 13 months after tumor resection, as well as in in vitro glucocorticoid-treated control cells. Flow cytometry, immunoblotting, enzyme-linked immunosorbent assay, real-time quantitative PCR, and RNA-Seq techniques were used to characterize patients’ and in vitro glucocorticoid treated cells. Reduced thymic output, decreased naive T cells, diminished proliferation, and increased T-cell apoptosis were detected before surgery; all these defects eventually normalized after tumor removal in patients. In vitro studies also showed increased T-cell apoptosis, with correspondingly diminished NF-κB signaling and IL-21 levels. In this setting, IL-21 addition upregulated antiapoptotic BCL2 expression and rescued T-cell apoptosis in a PI3K pathway–dependent manner. Similar and reproducible findings were confirmed in eCs patient cells as well. We identified decreased thymic output and lymphocyte proliferation, together with increased apoptosis, as the underlying causes to T-cell lymphopenia in eCs patients. IL-21 was decreased in both natural and in vitro long-term, high-dose glucocorticoid environments, and in vitro addition of IL-21 counteracted the proapoptotic effects of glucocorticoid therapy. Thus, our results suggest that administration of IL-21 in patients receiving long-term, high-dose glucocorticoid therapy may contribute to ameliorate lymphopenia and the complications associated to it. [Display omitted]