A T-cell dormant state in the autoimmune process of nonobese diabetic mice treated with complete Freund's adjuvant.

Abstract: lymphocytes from diabetic mice into male NOD mice transferred the diabetic state, but this transfer was markedly suppressed when the recipients were treated with CFA. In all three cases the spleen cells from the normoglycemic mice treated with CFA induced diabetes when transferred into NOD male mice. CFA, therefore, induces a state of T-cell dormancy, in which the islets are no longer subject to an immune attack.The autoimmune diabetic process of the nonobese diabetic (NOD) strain of mice is easily suppressed … Show more

“…Three aspects of this treatment regimen appear to operate in parallel and in a synergistic manner: (a) Injection of CFA, and the consequent induction of TNF-α, results in the elimination of TNF-α-sensitive cells, which have been shown previously to transfer existing disease (28)(29)(30)(31); (b) the introduction of functional MHC class I peptide complexes expressed on the surface of either normal islet cells or normal lymphocytes results in partial but stable reselection of the T cell population of the NOD host, leading to an increase in the abundance of long-term memory T cells (6,12,23); and (c) suppression of hyperglycemia, although not obligatory, promotes the functional restoration of endogenous β cells or their precursors.…”

“…Adoptive transfer was performed as described (29). Recipient male NOD mice, 4-8 weeks of age, were irradiated (790 rads) with a 137 Cs source and injected intravenously within 2 hours of irradiation with donor splenocytes (2 × 10 7 viable cells) suspended in 0.25 ml of serum-free medium.…”

“…Successful therapy generated a subpopulation of nonpathologic but TNF-α-resistant T cells that exhibited an increased tendency to undergo cell death in culture (Figure 7a). Disease reversal, even 210 days after cessation of treatment, was thus associated with the persistent elimination of TNF-α-sensitive T cells, a population of cells with a demonstrated ability to play a role in disease (29,30). The permanent elimination of these formerly abundant TNF-α-sensitive lymphoid cells, presumably in response to TNF-α (and, perhaps, to other CFA-induced cytokines), was observed uniformly in successfully treated diabetic NOD mice.…”

“…The increased susceptibility to apoptosis of misselected T cells that result from improper education by MHC class I peptide complexes suggested that the production of TNF-α in vivo might promote the selective death of such poorly educated lineages (10,26,27). Furthermore, treatment of diabetic NOD mice or BB rats with CFA, an inducer of TNF-α production, both impairs the transfer of disease by T cells from these animals to naive hosts (28)(29)(30)(31) as well as prolongs the survival of syngeneic islet grafts in spontaneously diabetic hosts (2,32). We therefore hypothesized that CFA treatment might eliminate, at least temporarily, the autoreactive lymphoid cells of NOD mice by promoting their apoptosis, in part through the induction of TNF-α.…”

Reversal of established autoimmune diabetes by restoration of endogenous β cell function

“…Three aspects of this treatment regimen appear to operate in parallel and in a synergistic manner: (a) Injection of CFA, and the consequent induction of TNF-α, results in the elimination of TNF-α-sensitive cells, which have been shown previously to transfer existing disease (28)(29)(30)(31); (b) the introduction of functional MHC class I peptide complexes expressed on the surface of either normal islet cells or normal lymphocytes results in partial but stable reselection of the T cell population of the NOD host, leading to an increase in the abundance of long-term memory T cells (6,12,23); and (c) suppression of hyperglycemia, although not obligatory, promotes the functional restoration of endogenous β cells or their precursors.…”

“…Adoptive transfer was performed as described (29). Recipient male NOD mice, 4-8 weeks of age, were irradiated (790 rads) with a 137 Cs source and injected intravenously within 2 hours of irradiation with donor splenocytes (2 × 10 7 viable cells) suspended in 0.25 ml of serum-free medium.…”

“…Successful therapy generated a subpopulation of nonpathologic but TNF-α-resistant T cells that exhibited an increased tendency to undergo cell death in culture (Figure 7a). Disease reversal, even 210 days after cessation of treatment, was thus associated with the persistent elimination of TNF-α-sensitive T cells, a population of cells with a demonstrated ability to play a role in disease (29,30). The permanent elimination of these formerly abundant TNF-α-sensitive lymphoid cells, presumably in response to TNF-α (and, perhaps, to other CFA-induced cytokines), was observed uniformly in successfully treated diabetic NOD mice.…”

“…The increased susceptibility to apoptosis of misselected T cells that result from improper education by MHC class I peptide complexes suggested that the production of TNF-α in vivo might promote the selective death of such poorly educated lineages (10,26,27). Furthermore, treatment of diabetic NOD mice or BB rats with CFA, an inducer of TNF-α production, both impairs the transfer of disease by T cells from these animals to naive hosts (28)(29)(30)(31) as well as prolongs the survival of syngeneic islet grafts in spontaneously diabetic hosts (2,32). We therefore hypothesized that CFA treatment might eliminate, at least temporarily, the autoreactive lymphoid cells of NOD mice by promoting their apoptosis, in part through the induction of TNF-α.…”

Reversal of established autoimmune diabetes by restoration of endogenous β cell function

“…Transfer of diabetes by spleen cells was conducted by the method described previously (18). In brief, spleen cells (2 ϫ 10 7 ) from diabetic mice were injected i.v.…”

Thymic and Postthymic Regulation of Diabetogenic CD8 T Cell Development in TCR Transgenic Nonobese Diabetic (NOD) Mice

Type 1 diabetes: the facts fit a deficient inhibitory signal given by MHC Class II