Abstract
Hassall's corpuscles (HCs) are composed of cornifying, terminally differentiated medullary thymic epithelial cells (mTECs) that are developed under the control of Aire. Here, we demonstrated that HC-mTECs show features of cellular senescence and produce inflammatory cytokines and chemokines including CXCL5, thereby recruiting and activating neutrophils to produce IL-23 in the thymic medulla. We further indicated that thymic plasmacytoid dendritic cells (pDCs) expressing IL-23 receptors constitutively produced Ifna, which plays a role in single positive (SP) cell maturation, in an Il23a-dependent manner. Neutrophil depletion with anti-Ly6G antibody injection resulted in a significant decrease of Ifna expression in the thymic pDCs, suggesting that thymic neutrophil activation underlies the Ifna expression in thymic pDCs in steady state conditions. A New Zealand White mouse strain showing HC hyperplasia exhibited greater numbers and activation of thymic neutrophils and pDCs than B6 mice, whereas Aire-deficient B6 mice with defective HC development and SP thymocyte maturation showed significantly compromised numbers and activation of these cells. These results collectively suggested that HC-mTECs with cell-senescence features initiate a unique cell activation cascade including neutrophils and pDCs leading to the constitutive IFNα expression required for SP T-cell maturation in the thymic medulla.
Highlights
Hassall’s corpuscles (HCs) were first described as cornifying thymic epithelial cells in the medulla of the human thymus by A
Recent studies have revealed that the medullary thymic epithelial cells constituting HC (HC-mTECs) can be identified in mice by the expression of molecules related to keratinocyte cornification such as keratin 10 (K10) and involucrin
It was demonstrated that HC development depends on autoimmune regulator (Aire), the gene responsible for causing the monogenic human autoimmune disease autoimmune polyendocrinopathy-candidiasis- ectodermal dystrophy, suggesting a role of HCs in T
Summary
Hassall’s corpuscles (HCs) were first described as cornifying thymic epithelial cells in the medulla of the human thymus by A. IFNα production through neutrophils and pDC activation in the thymus( Abstract要旨 ) Hassall’s corpuscles with cellular-senescence features maintain IFNα production through neutrophils and pDC activation in the thymus
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