Class I-restricted cross-presentation of exogenous self-antigens leads to deletion of autoreactive CD8(+) T cells

Kurts, C; Kosaka, H; Carbone, FR; Miller, JFAP; Heath, WR

Author(s): Kurts, C; Kosaka, H; Carbone, FR; Miller, JFAP; Heath, WR;
Details: Publication Year 1997-07-21,Volume 186,Issue #2,Page 239-245
Journal Title: JOURNAL OF EXPERIMENTAL MEDICINE
Publication Type: Journal Article
Abstract: In this report, we show that cross-presentation of self-antigens can lead to the peripheral deletion of autoreactive CD8(+) T cells. We had previously shown that transfer of ovalbumin (OVA)-specific CD8(+) T cells (OT-I cells) into rat insulin promoter-membrane-bound form of OVA transgenic mice, which express the model autoantigen OVA in the proximal tubular cells of the kidneys, the beta cells of the pancreas, the thymus, and the testis of male mice, led to the activation of OT-I cells in the draining lymph nodes. This was due to class I-restricted cross-presentation of exogenous OVA on a bone marrow-derived antigen presenting cell (APC) population. Here, we show that adoptively transferred or thymically derived OT-I cells activated by cross-presentation are deleted from the peripheral pool of recirculating lymphocytes. Such deletion only required antigen recognition on a bone marrow-derived population, suggesting that cells of the professional APC class may be tolerogenic under these circumstances. Our results provide a mechanism by which the immune system can induce CD8(+) T cell tolerance to autoantigens that are expressed outside the recirculation pathway of naive T cells.
Publisher: ROCKEFELLER UNIV PRESS
Keywords: TRANSGENIC MICE; EXTRATHYMIC TOLERANCE; CLONAL ELIMINATION; VIRUS-INFECTION; LYMPHOCYTE-T; INDUCTION; PEPTIDES; ENCEPHALOMYELITIS; AUTOIMMUNITY; CONSEQUENCE
Publisher's Version: https://doi.org/10.1084/jem.186.2.239
Terms of Use/Rights Notice: Refer to copyright notice on published article.

Creation Date: 1997-07-21 12:00:00