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Open AccessJournal ArticleDOI

Identification of a human recent thymic emigrant phenotype

TLDR
It is demonstrated that alphaE integrin (CD103) expression is up-regulated very late in thymic development on a subset of CD8(+)/CD4(-) thymocytes and also defines a distinct subset of naiveCD8(+) T cells in the periphery, which suggest that these cells are a population of RTE and that quantification of their frequency in peripheral blood provides an estimate of the level of ongoing thymopoiesis.
Abstract
The ability to measure human thymic output would be an invaluable tool for the study of the development of the naive T cell repertoire, as well as naive T cell regeneration after intensive cytotoxic chemotherapy or effective antiretroviral therapy of progressive HIV infection. We and others have demonstrated previously that quantification of T cell receptor rearrangement excision circles (TREC) within peripheral T cell populations provides insight into the frequency of recent thymic emigrants (RTE) and, therefore, into thymic function. However, measurement of RTE by this approach is complicated by the fact that TREC levels also are determined by turnover within the naive T cell compartment. Here, we report a phenotypic approach to RTE measurement. We demonstrate that αE integrin (CD103) expression is up-regulated very late in thymic development on a subset of CD8+/CD4− thymocytes and also defines a distinct subset of naive CD8+ T cells in the periphery. The latter subset is differentiated from circulating CD103+ mucosa-associated memory T cells by its naive T cell phenotype (CD45RO−, CD62Lbright, CD27bright, CD11adim, CD95dim) and its high concentration of TREC. Indeed, sorted CD103+ naive CD8+ cells display higher levels of TREC than their CD103− naive counterparts, and these cells demonstrate an age-related decline in frequency that is enhanced significantly by thymectomy. The thymic dependence of this subset and the cells' relatively evanescent presence in the periphery suggest that these cells are a population of RTE and that quantification of their frequency in peripheral blood provides an estimate of the level of ongoing thymopoiesis.

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Citations
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Journal ArticleDOI

Maintaining the norm: T-cell homeostasis.

TL;DR: The persistence of naive and memory T cells has long been of interest to immunologists, but the factors that influence the survival and homeostasis of these subsets have remained obscure.
Journal ArticleDOI

Development and Homeostasis of T Cell Memory in Rhesus Macaque

TL;DR: A phenotypic paradigm allowing definitive characterization of these subsets and their comprehensive functional analysis is reported, revealing the RM “effector memory” subset within the overall memory population and demonstrating similar in vivo proliferative activity and survival as CD28+ “central memory’ T cells, consistent with independent homeostatic regulation.
Journal ArticleDOI

MHC Class II Expression Identifies Functionally Distinct Human Regulatory T Cells

TL;DR: It is demonstrated that MHC-II expression on human CD4+CD25high T cells identifies a functionally distinct population of Treg that induces early contact-dependent suppression that is associated with high Foxp3 expression.
Journal ArticleDOI

T cell receptor excision circles as markers for recent thymic emigrants: basic aspects, technical approach, and guidelines for interpretation.

TL;DR: In this paper, the authors proposed a method for quantifying the T cell receptor excision circles (TREC) in the thymus using the δRec-ψJα TREC marker, which is a new and elegant tool for identification of recent thymic emigrants.
Journal ArticleDOI

Life after the thymus: CD31+ and CD31− human naive CD4+ T-cell subsets

Siegfried Kohler, +1 more
- 22 Jan 2009 - 
TL;DR: This work reviews studies that have characterized TREC(hi) CD31(+ thymic)naive CD4(+) T cells and has accordingly used the assessment of this distinct subset of naive CD4-naive T cells as a correlate ofThymic activity and discusses further potential clinical applications.
References
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Journal ArticleDOI

Age, thymopoiesis, and CD4+ t-lymphocyte regeneration after intensive chemotherapy

TL;DR: Thymus-dependent regeneration of CD4+ T lymphocytes occurs primarily in children, whereas even young adults have deficiencies in this pathway, and the results suggest that rapid T-cell regeneration requires residual thymic function in patients receiving high-dose chemotherapy.
Journal ArticleDOI

Thymus cell migration. Quantitative aspects of cellular traffic from the thymus to the periphery in mice.

TL;DR: Intathymic injection of fluorescein isothiocyanate is used to label thymocytes in situ and so can be used to quantitate the extent of migration of cells from the thymus to the periphery.
Journal ArticleDOI

A monoclonal antibody (HML-1) defining a novel membrane molecule present on human intestinal lymphocytes

TL;DR: A monoclonal antibody, HML‐1, was produced by fusion of NSI myeloma cells with spleen cells of a mouse immunized with isolated human intestinal intraepithelial lymphocytes and defined a novel human membrane antigen present on a subpopulation of lymphocytes preferentially associated with epithelia, and particularly with the intestinal epithelium.
Journal ArticleDOI

The involution of the ageing human thymic epithelium is independent of puberty. A morphometric study.

TL;DR: The velocity and nature of involution of the thymic epithelium do not change under the influence of the changing hormonal balance due to puberty, and when defined by the silver impregnation technique, the volumes show a continuous involution from the first year to the end of life.
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