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Publication : Temporal increase in thymocyte negative selection parallels enhanced thymic SIRPα<sup>+</sup> DC function.

First Author  Kroger CJ Year  2016
Journal  Eur J Immunol Volume  46
Issue  10 Pages  2352-2362
PubMed ID  27501268 Mgi Jnum  J:250480
Mgi Id  MGI:5924174 Doi  10.1002/eji.201646354
Citation  Kroger CJ, et al. (2016) Temporal increase in thymocyte negative selection parallels enhanced thymic SIRPalpha+ DC function. Eur J Immunol 46(10):2352-2362
abstractText  Dysregulation of negative selection contributes to T-cell-mediated autoimmunity, such as type 1 diabetes. The events regulating thymic negative selection, however, are ill defined. Work by our group and others suggest that negative selection is inefficient early in ontogeny and increases with age. This study examines temporal changes in negative selection and the thymic DC compartment. Peptide-induced thymocyte deletion in vivo was reduced in newborn versus 4-week-old NOD mice, despite a similar sensitivity of the respective thymocytes to apoptosis induction. The temporal increase in negative selection corresponded with an elevated capacity of thymic antigen-presenting cells to stimulate T cells, along with altered subset composition and function of resident DC. The frequency of signal regulatory protein alpha+ (SIRPalpha+ ) and plasmacytoid DCs was increased concomitant with a decrease in CD8alpha+ DC in 4-week-old NOD thymi. Importantly, 4-week-old versus newborn thymic SIRPalpha+ DC exhibited increased antigen processing and presentation via the MHC class II but not class I pathway, coupled with an enhanced T-cell stimulatory capacity not seen in thymic plasmacytoid DC and CD8alpha+ DC. These findings indicate that the efficiency of thymic DC-mediated negative selection is limited early after birth, and increases with age paralleling expansion of functionally superior thymic SIRPalpha+ DC.
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