A Comprehensive Review of Interventions in the NOD Mouse and Implications for Translation

Shoda, Lisl K. M.; Young, David; Ramanujan, Saroja; Whiting, Chan C.; Atkinson, Mark A.; Bluestone, Jeffrey A.; Eisenbarth, George S.; Mathis, Diane; Rossini, Aldo A.; Campbell, Scott E.; Kahn, Richard; Kreuwel, Huub T. C.

doi:10.1016/j.immuni.2005.08.002

Cited by 281 publications

(257 citation statements)

References 106 publications

(1 reference statement)

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“…present in the lymphoid organs or recently emigrated from the thymus. Our results add IL-7Rα blockade to the list of only a handful of treatments capable of reversing the disease (12) and is unique as a cytokine receptor blockade therapy for the treatment of autoimmune diabetes. Surprisingly, histological analysis showed only a limited reduction of the islet infiltrates ( Fig.…”

Section: Il-7rαmentioning

confidence: 84%

“…IL-7 is a critical cytokine for the generation and maintenance of virusspecific memory T cells, but its role in autoimmune disease is poorly defined. One of the challenges in treating autoimmune type 1 diabetes is that it is a slowly developing chronic disease, and the efficacy of most treatments highly depends on the stage of the disease at which the treatment is given (12). To assess whether blocking IL-7 signals in NOD mice would interfere with disease development, we administered anti-IL-7Rα mAbs to block IL-7 cytokine activity.…”

Section: Il-7rαmentioning

confidence: 99%

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IL-7 receptor blockade reverses autoimmune diabetes by promoting inhibition of effector/memory T cells

Peñaranda

Kuswanto

Hofmann

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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To protect the organism against autoimmunity, self-reactive effector/memory T cells (T E/M ) are controlled by cell-intrinsic and -extrinsic regulatory mechanisms. However, how some T E/M cells escape regulation and cause autoimmune disease is currently not understood. Here we show that blocking IL-7 receptor-α (IL-7Rα) with monoclonal antibodies in nonobese diabetic (NOD) mice prevented autoimmune diabetes and, importantly, reversed disease in new-onset diabetic mice. Surprisingly, IL-7-deprived diabetogenic T E/M cells remained present in the treated animals but showed increased expression of the inhibitory receptor Programmed Death 1 (PD-1) and reduced IFN-γ production. Conversely, IL-7 suppressed PD-1 expression on activated T cells in vitro. Adoptive transfer experiments revealed that T E/M cells from anti-IL-7Rα-treated mice had lost their pathogenic potential, indicating that absence of IL-7 signals induces cell-intrinsic tolerance. In addition to this mechanism, IL-7Rα blockade altered the balance of regulatory T cells and T E/M cells, hence promoting cell-extrinsic regulation and further increasing the threshold for diabetogenic T-cell activation. Our data demonstrate that IL-7 contributes to the pathogenesis of autoimmune diabetes by enabling T E/M cells to remain in a functionally competent state and suggest IL-7Rα blockade as a therapy for established T-cell-dependent autoimmune diseases.type 1 diabetes | cytokines | immune regulation

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Section: Il-7rαmentioning

confidence: 84%

Section: Il-7rαmentioning

confidence: 99%

IL-7 receptor blockade reverses autoimmune diabetes by promoting inhibition of effector/memory T cells

Peñaranda

Kuswanto

Hofmann

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

120

127

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“…The NOD model has been widely used to test many therapeutic regimens, the majority of which have been reviewed [1]. Although many of these treatments had a successful outcome in young NOD mice (treated before 8 wks of age), fewer were tested or found to demonstrate efficacy in older NOD mice with advanced insulitis or hyperglycemia.…”

Section: Introductionmentioning

confidence: 99%

Tissue-targeted therapy of autoimmune diabetes using dendritic cells transduced to express IL-4 in NOD mice

Creusot

Yaghoubi²,

Kodama

et al. 2008

Clinical Immunology

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A deficit in IL-4 production has been previously reported in both diabetic human patients and nonobese diabetic (NOD) mice. In addition, re-introducing IL-4 into NOD mice systemically, or as a transgene, led to a beneficial outcome in most studies. Here, we show that prediabetic, 12-wk old female NOD mice have a deficit in IL-4 expression in the pancreatic lymph nodes (PLN) compared to age-matched diabetes-resistant NOD.B10 mice. By bioluminescence imaging, we demonstrated that the PLN was preferentially targeted by bone marrow-derived dendritic cells (DCs) following intravenous (IV) administration. Following IV injection of DCs transduced to express IL-4 (DC/ IL-4) into 12-wk old NOD mice, it was possible to significantly delay or prevent the onset of hyperglycemia. We then focused on the PLN to monitor, by microarray analysis, changes in gene expression induced by DC/IL-4 and observed a rapid normalization of the expression of many genes, that were otherwise under-expressed compared to NOD.B10 PLN. The protective effect of DC/IL-4 required both MHC and IL-4 expression by the DCs. Thus, adoptive cellular therapy, using DCs modified to express IL-4, offers an effective, tissue-targeted cellular therapy to prevent diabetes in NOD mice at an advanced stage of pre-diabetes, and may offer a safe approach to consider for treatment of high risk human pre-diabetic patients.

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“…autoimmunity ͉ type 1 diabetes ͉ inflammation A destructive T cell-dependent autoimmune process directed against insulin-producing ␤ cells causes type 1 diabetes mellitus (T1DM) in humans and the nonobese diabetic (NOD) mouse model (1,2). Although many therapeutic interventions, including viral-mediated gene transfer of human ␣1-antitrypsin (AAT) (3), can prevent T1DM or resolve the T cell-rich, ␤ cell-invasive insulitis lesion in prediabetic hosts, surprisingly few therapies have succeeded in restoring long-term drug-free euglycemia and immune tolerance to ␤ cells in overtly diabetic NOD mice (4)(5)(6)(7)(8).…”

mentioning

confidence: 99%

Curative and β cell regenerative effects of α1-antitrypsin treatment in autoimmune diabetic NOD mice

Koulmanda¹,

Bhasin

Hoffman

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

153

159

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Invasive insulitis is a destructive T cell-dependent autoimmune process directed against insulin-producing ␤ cells that is central to the pathogenesis of type 1 diabetes mellitus (T1DM) in humans and the clinically relevant nonobese diabetic (NOD) mouse model. Few therapies have succeeded in restoring long-term, drug-free euglycemia and immune tolerance to ␤ cells in overtly diabetic NOD mice, and none have demonstrably enabled enlargement of the functional ␤ cell mass. Recent studies have emphasized the impact of inflammatory cytokines on the commitment of antigen-activated T cells to various effector or regulatory T cell phenotypes and insulin resistance and defective insulin signaling. Hence, we tested the hypothesis that inflammatory mechanisms trigger insulitis, insulin resistance, faulty insulin signaling, and the loss of immune tolerance to islets. We demonstrate that treatment with ␣1-antitrypsin (AAT), an agent that dampens inflammation, does not directly inhibit T cell activation, ablates invasive insulitis, and restores euglycemia, immune tolerance to ␤ cells, normal insulin signaling, and insulin responsiveness in NOD mice with recent-onset T1DM through favorable changes in the inflammation milieu. Indeed, the functional mass of ␤ cells expands in AAT-treated diabetic NOD mice.autoimmunity ͉ type 1 diabetes ͉ inflammation A destructive T cell-dependent autoimmune process directed against insulin-producing ␤ cells causes type 1 diabetes mellitus (T1DM) in humans and the nonobese diabetic (NOD) mouse model (1, 2). Although many therapeutic interventions, including viral-mediated gene transfer of human ␣1-antitrypsin (AAT) (3), can prevent T1DM or resolve the T cell-rich, ␤ cell-invasive insulitis lesion in prediabetic hosts, surprisingly few therapies have succeeded in restoring long-term drug-free euglycemia and immune tolerance to ␤ cells in overtly diabetic NOD mice (4-8). Although each of these successful therapies directly targets T cells, each bears an element that may dampen proinflammatory responses or their consequences upon target tissues.Inflammatory cytokines direct the commitment of antigenactivated CD4 ϩ T cells to specific effector or Foxp3ϩ regulatory phenotypes (9-11). In addition, islets are sensitive to proinflammatory cytokines (12-15). Adverse inflammation in muscle and fat causes faulty insulin signaling and insulin resistance (16) in type 2 diabetes mellitus (13) and, as recently shown, T1DM (7,17). Hence, we have tested the hypothesis that treatment with AAT, an acutephase reactant with known antiinflammatory and antiapoptotic effects (18-21) including effects on islets (21,22), is effective in NOD mice with overt new-onset T1DM. In short, we are probing the hypothesis that inflammatory mechanisms trigger T1DM. Results AAT Does Not Inhibit T Cell Activation.Purified carboxyfluorescein diacetate succinmidyl ester (CFSE)-labeled C57BL/6 mouse T cells were stimulated with plate-bound anti-CD3 plus soluble anti-CD28 mAbs. AAT did not impair T cell proliferation or acquisition of an ...

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A Comprehensive Review of Interventions in the NOD Mouse and Implications for Translation

Cited by 281 publications

References 106 publications

IL-7 receptor blockade reverses autoimmune diabetes by promoting inhibition of effector/memory T cells

IL-7 receptor blockade reverses autoimmune diabetes by promoting inhibition of effector/memory T cells

Tissue-targeted therapy of autoimmune diabetes using dendritic cells transduced to express IL-4 in NOD mice

Curative and β cell regenerative effects of α1-antitrypsin treatment in autoimmune diabetic NOD mice

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