Repetitive Antigen Responses of LDL-Reactive CD4+ T Cells Induce Tr1 Cell-Mediated Immune Tolerance.

Reiner K Mailer Sandra Konrath Lydia Zhan Hanna Thode Manu Beerens Maike Frye Daniel F J Ketelhuth Thomas Renné Göran K Hansson

Arterioscler Thromb Vasc Biol

Cardiovascular Medicine Unit, Department of Medicine, Karolinska Institutet, Karolinska University Hospital, Stockholm, Sweden (R.K.M., D.F.J.K., G.K.H.).

Published: August 2023

The study investigates how LDL (low-density lipoprotein) contributes to atherosclerosis and the role of Treg (regulatory T) cells in managing inflammation caused by LDL deposition in arteries.
Researchers found that while LDL-specific T cells express the anti-inflammatory cytokine IL-10 as mice age, their population doesn't increase; however, transferring specific naïve T cells can promote immune tolerance and enhance Treg cell activity.
The findings suggest that repeated stimulation of LDL-specific T cells can help generate Treg type 1 cells that effectively suppress LDL-related immune responses, highlighting a potential therapeutic approach for managing atherosclerosis.

Background: Inflammation triggered by the deposition of LDL (low-density lipoprotein) in the arterial wall leads to the development of atherosclerosis. Regulatory T (Treg) cells inhibit vascular inflammation through the induction of immune tolerance toward LDL-related antigens. However, tolerogenic mechanisms that promote the generation of LDL-specific Treg cells in vivo remain unclear.

Methods: We identified LDL-specific T cells by activation-induced marker expression and analyzed expression profiles and suppressive functions of TCR (T-cell antigen receptor)-transgenic T cells upon repetitive transfer into antigen-transgenic mice via flow cytometry.

Results: We investigated the naturally occurring Treg-cell response against human LDL in standard chow diet-fed mice that are transgenic for human ApoB100 (apolipoprotein B100). We found that IL (interleukin)-10 expression in LDL-specific T cells from spleen increases with age, albeit LDL-specific populations do not enlarge in older mice. To investigate the generation of IL-10-producing LDL-specific T cells, we transferred naive CD4+ T cells recognizing human ApoB100 from TCR-transgenic mice into human ApoB100-transgenic mice. Adoptive transfer of human ApoB100-specific T cells induced immune tolerance in recipient mice and effectively inhibited activation of subsequently transferred naive T cells of the same specificity in vivo. Moreover, repetitive transfers increased the population of Treg type 1 cells that suppress ApoB100-specific responses via IL-10. In a translational approach, LDL-specific Treg type 1 cells from blood of healthy donors suppressed the activation of monocytic THP-1 cells in an IL-10-dependent manner.

Conclusions: We show that repetitive transfer of naive ApoB100-specific T cells and recurrent LDL-specific T-cell stimulation induces Treg type 1 cell-mediated immune tolerance against LDL in vivo. Our results provide insight into the generation of autoantigen-specific anti-inflammatory T cells under tolerogenic conditions.

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http://dx.doi.org/10.1161/ATVBAHA.123.319135	DOI Listing

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