Regeneration of Dendritic Cells in Aged Mice

Overview

Journal Cell Mol Immunol

Date 2010 Feb 2

PMID 20118970

Citations 9

Authors

Serani L H van Dommelen

Alexandra Rizzitelli

Ann Chidgey

Richard Boyd

Ken Shortman

Li Wu

Affiliations

Soon will be listed here.

Abstract

Age-related thymic involution causes a decreased output of thymocytes from the thymus, thereby resulting in impairment of T cell-mediated immunity. While alterations in the T cell and non-haematopoietic stromal compartments have been described, the effects of thymic involution on thymic dendritic cells (DC) are not clearly known. Thymic DC play an essential role in shaping T cell-mediated immune responses by deleting self-reactive thymocytes to establish central tolerance and by inducing regulatory T-cell (Treg) development. It is therefore important to assess the prevalence of and alterations to thymic DC with age, as this may impact on their function. We assessed the numbers and proportions of the three distinct subsets of thymic DC in ageing mice, and showed that these subsets are differentially regulated. This is expected as thymic DC subsets have different origins of development. We further assessed the responses of thymic DC in a regenerative environment, such as that induced by sex-steroid ablation (SSA), and clearly showed that, consistent with global thymus regrowth, all three DC populations increased in numbers and regained their relative proportions to thymocytes after an initial lag period. These findings are important for the clinical translation of thymic regenerative approaches, and indicate that SSA facilitates the maintenance of critical processes such as negative selection and Treg induction through promoting thymic DC regeneration.

Citing Articles

Age-Related Thymic Involution.

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Aging of lymphoid stromal architecture impacts immune responses.

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Central tolerance is impaired in the middle-aged thymic environment.

Lancaster J, Keatinge-Clay D, Srinivasan J, Li Y, Selden H, Nam S Aging Cell. 2022; 21(6):e13624.

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