Peripheral T Cell Tolerance
The most efficient way to ensure self-tolerance in the T-cell repertoire is by intrathymic deletion of self-reactive clones. Antigens not present intrathymically may, however, influence the peripheral T-cell pool in various ways. They may of course activate T cells, provided that these have the corr...
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Veröffentlicht in: | Annual review of immunology 1992, Vol.10 (1), p.51-69 |
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Sprache: | eng |
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Zusammenfassung: | The most efficient way to ensure self-tolerance in the T-cell repertoire
is by intrathymic deletion of self-reactive clones. Antigens not present
intrathymically may, however, influence the peripheral T-cell pool in various
ways. They may of course activate T cells, provided that these have
the correct specificity and affinity and that the antigens are presented in
sufficient amounts on professional antigen-presenting cells. They may be
ignored by T cells if some of these conditions are not met. In some forms,
the antigen may be toleragenic for mature T cells. If the antigens persist
in an immunogcnic form, unresponsiveness may eventually be imposed as
the end result of a powerful immune response. Extrathymic self-antigenic
components are generally encountered early in development, and the way
in which these influence peripheral T lymphocytes has been studied by
transgenic technology. They may be ignored by T cells if they are sequestered
from the immune system, or if they are present in low amounts or
on nonprofessional antigen-presenting cells which lack the appropriate
accessory molecules or signals needed to activate the relevant T-cell subset.
On the other hand, some of these self-antigens readily induce anergy in
peripheral T cells, which may or may not involve downregulation of
antigen receptors and coreceptors. Tolerance in the T-cell repertoire is
therefore achieved not only by intrathymic deletion of self-reactive clones
but also by several postthymic mechanisms |
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ISSN: | 0732-0582 1545-3278 |
DOI: | 10.1146/annurev.iy.10.040192.000411 |