Lymphopenia-induced Proliferation is a Potent Activator for CD4+ T Cell-mediated Autoimmune Disease in the Retina

Overview

Journal J Immunol

Specialty Allergy & Immunology

Date 2009 Jan 7

PMID 19124740

Citations 16

Authors

Scott W McPherson

Neal D Heuss

Dale S Gregerson

Affiliations

Soon will be listed here.

Abstract

To study retinal immunity in a defined system, a CD4+ TCR transgenic mouse line (betagalTCR) specific for beta-galactosidase (betagal) was created and used with transgenic mice that expressed betagal in retinal photoreceptor cells (arrbetagal mice). Adoptive transfer of resting betagalTCR T cells, whether naive or Ag-experienced, into arrbetagal mice did not induce retinal autoimmune disease (experimental autoimmune uveoretinitis, EAU) and gave no evidence of Ag recognition. Generation of betagalTCR T cells in arrbetagal mice by use of bone marrow grafts, or double-transgenic mice, also gave no retinal disease or signs of Ag recognition. Arrbetagal mice were also resistant to EAU induction by adoptive transfer of in vitro-activated betagalTCR T cells, even though the T cells were pathogenic if the betagal was expressed elsewhere. In vitro manipulations to increase T cell pathogenicity before transfer did not result in EAU. The only strategy that induced a high frequency of severe EAU was transfer of naive, CD25-depleted, betagalTCR T cells into lymphopenic arrbetagal recipients, implicating regulatory T cells in the T cell inoculum, as well as in the recipients, in the resistance to EAU. Surprisingly, activation of the CD25-depleted betagalTCR T cells before transfer into the lymphopenic recipients reduced EAU. Taken together, the results suggest that endogenous regulatory mechanisms, as well as peripheral induction of regulatory T cells, play a role in the protection from EAU.

Citing Articles

Parabiosis reveals the correlation between the recruitment of circulating antigen presenting cells to the retina and the induction of spontaneous autoimmune uveoretinitis.

McPherson S, Heuss N, Abedin M, Roehrich H, Pierson M, Gregerson D J Neuroinflammation. 2022; 19(1):295.

PMID: 36494807 PMC: 9733026. DOI: 10.1186/s12974-022-02660-2.

Lymphopenia, Lymphopenia-Induced Proliferation, and Autoimmunity.

Sheu T, Chiang B Int J Mol Sci. 2021; 22(8).

PMID: 33923792 PMC: 8073364. DOI: 10.3390/ijms22084152.

Treatment With FoxP3+ Antigen-Experienced T Regulatory Cells Arrests Progressive Retinal Damage in a Spontaneous Model of Uveitis.

Liu Y, Molzer C, Makinen K, Kamoi K, Corbett C, Klaska I Front Immunol. 2020; 11:2071.

PMID: 33013877 PMC: 7498671. DOI: 10.3389/fimmu.2020.02071.

Prior to Peripheral Tolerance, Newly Generated CD4 T Cells Maintain Dangerous Autoimmune Potential: Fas- and Perforin-Independent Autoimmunity Controlled by Programmed Death-1.

Ellestad K, Thangavelu G, Haile Y, Lin J, Boon L, Anderson C Front Immunol. 2018; 9:12.

PMID: 29416537 PMC: 5787554. DOI: 10.3389/fimmu.2018.00012.

Ocular antigen does not cause disease unless presented in the context of inflammation.

Voigt V, Wikstrom M, Kezic J, Schuster I, Fleming P, Makinen K Sci Rep. 2017; 7(1):14226.

PMID: 29079770 PMC: 5660195. DOI: 10.1038/s41598-017-14618-z.

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