In a bidirectional link, adrenal function may be compromised by inflammation but can also crucially affect the outcome of systemic inflammation. In the first funding period we demonstrated that endothelial Del-1, which our lab has described as the first endogenous inhibitor of leukocyte recruitment, acts as a gatekeeper of adrenal gland inflammation. In SIRS, adrenal downregulation of Del-1 promoted adrenal dysfunction. To our knowledge this was the first study demonstrating that adrenal endothelium supports adrenal homeostasis, counter-acting inflammation-related adrenal dysfunction. Interestingly, we also found the adrenal steroid DHEA, which has immune-modulatory actions, to stimulate Del-1 expression. On the contrary, the likely most prominent proinflammatory cytokine of recent years, IL-17, is strongly induced in the adrenal gland upon SIRS-related adrenal inflammation and decreases adrenal Del-1 expression. We will build upon these findings to understand further the crosstalk between adrenal steroids (such as corticosteroids or DHEA), Del-1 and IL-17 for regulating the adrenal-endothelial-immune interface in inflammation-dependent adrenal dysfunction. We will engage different tools, such as application of DHEA, as well as pharmacologic or genetic inactivation of the IL-17/IL-17R axis in mouse models of SIRS/sepsis. These experiments will improve our understanding of the factors regulating inflammation-related adrenal dysfunction and could provide the basis for new therapeutic approaches.

DFG-Verfahren Klinische Forschungsgruppen

Teilprojekt zu KFO 252:  Microenvironment of the Adrenal in Health and Disease