CD4(+) skin resident memory T cells preferentially colocalize with dermal Folr2(hi) macrophages in contact hypersensitivity.

在接触性超敏反应中,CD4(+)皮肤驻留记忆T细胞优先与真皮Folr2(hi)巨噬细胞共定位

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作者:Murata Akihiko, Tokoyoda Koji
In contact hypersensitivity (CHS), local immune memory is established in previously affected skin through the formation of CD4(+) and CD8(+) tissue-resident memory T (T(RM)) cells. This memory contributes to disease recurrence by enhancing local antigen responsiveness and is maintained in the long term by T(RM) cells, particularly CD4(+) T(RM) cells. However, the mechanisms underlying the maintenance and reactivation of CD4(+) T(RM) cells remain unclear. We herein examined the cellular niches persistently interacting with CD4(+) T cells in naïve and CHS-healed mouse ear skin. Most CD4(+) T cells were scattered in the dermis and colocalized with Folr2(hi) macrophages, a previously unrecognized skin macrophage population, suggesting a physical interaction. In contrast, fewer than 20% of CD4(+) T cells colocalized with dendritic cells (DCs) or other cell lineages. The administration of an anti-colony stimulating factor 1 receptor (CSF1R) antibody depleted nearly all Folr2(hi) macrophages and several other myeloid cells, while the maintenance and reactivation of CD4(+) T cells as well as other αβ T cells in healed skin remained unaffected. Moreover, in macrophage-depleted healed skin, CD4(+) T cells did not establish new interactions with remaining antigen-presenting cells, and their contact rate with DCs remained unchanged. These results indicate that local immune memory in CHS-experienced skin is maintained and functions independently of CSF1R-dependent myeloid cells, including Folr2(hi) macrophages, despite their predominant colocalization with skin CD4(+) T(RM) cells.

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