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Conserved and divergent aspects of human T-cell development and migration in humanized mice.

Authors :
Halkias J
Yen B
Taylor KT
Reinhartz O
Winoto A
Robey EA
Melichar HJ
Source :
Immunology and cell biology [Immunol Cell Biol] 2015 Sep; Vol. 93 (8), pp. 716-26. Date of Electronic Publication: 2015 Mar 06.
Publication Year :
2015

Abstract

Humanized mice represent an important model to study the development and function of the human immune system. While it is known that mouse thymic stromal cells can support human T-cell development, the extent of interspecies cross-talk and the degree to which these systems recapitulate normal human T-cell development remain unclear. To address these questions, we compared conventional and non-conventional T-cell development in a neonatal chimera humanized mouse model with that seen in human fetal and neonatal thymus samples, and also examined the impact of a human HLA-A2 transgene expressed by the mouse stroma. Given that dynamic migration and cell-cell interactions are essential for T-cell differentiation, we also studied the intrathymic migration pattern of human thymocytes developing in a murine thymic environment. We found that both conventional T-cell development and intra-thymic migration patterns in humanized mice closely resemble human thymopoiesis. Additionally, we show that developing human thymocytes engage in short, serial interactions with other human hematopoietic-derived cells. However, non-conventional T-cell differentiation in humanized mice differed from both fetal and neonatal human thymopoiesis, including a marked deficiency of Foxp3(+) T-cell development. These data suggest that although the murine thymic microenvironment can support a number of aspects of human T-cell development, important differences remain, and additional human-specific factors may be required.

Details

Language :
English
ISSN :
1440-1711
Volume :
93
Issue :
8
Database :
MEDLINE
Journal :
Immunology and cell biology
Publication Type :
Academic Journal
Accession number :
25744551
Full Text :
https://doi.org/10.1038/icb.2015.38