Treatment with anti-CD86 costimulatory molecule prevents the autoimmune lesions in murine Sjögren’s syndrome (SS) through up-regulated Th2 response

Saegusa, Kaoru; Ishimaru, Naozumi; Yanagi, Kumiko; Haneji, Norio; Nishino, Mizuho; Azuma, Masayuki; Saito, Ichiro; Hayashi, Yoshio

doi:10.1046/j.1365-2249.2000.01121.x

Cited by 39 publications

(25 citation statements)

References 45 publications

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“…In contrast, once activated ex vivo, BDC2.5 cells could efficiently transfer diabetes in B7-2KO mice. These observations provide further credence to the notion that B7-2 plays a significant role during the initiation of autoreactive T cell responses (18,38,39) and is dispensable during the later (effector) phase of the immune response. Accordingly, late B7-2 blockade in NOD (10 wk of age or older) is ineffective in controlling diabetes (13).…”

Section: Discussionsupporting

confidence: 71%

“…It is likely that local cellular interactions and the cytokine/chemokine microenvironment may play a role in this tissue specific up-regulation of B7-1. Moreover, B7-1 has been shown to play an important role in the effector phase of immune response (9,45), whereas B7-2 regulates the initiation phase (5,38,46,47). Furthermore, despite the presence of enhanced B7-1 signals in the spleen, there is an absence of pathogenic islet reactive T cells.…”

Section: Discussionmentioning

confidence: 99%

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B7-2 (CD86) Controls the Priming of Autoreactive CD4 T Cell Response against Pancreatic Islets

Yadav

Judkowski

Flodström‐Tullberg

et al. 2004

The Journal of Immunology

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The B7-1/2-CD28 system provides the critical signal for the generation of an efficient T cell response. We investigated the role played by B7-2 in influencing pathogenic autoimmunity from islet-reactive CD4 T cells in B7-2 knockout (KO) NOD mice which are protected from type 1 diabetes. B7-2 deficiency caused a profound diminishment in the generation of spontaneously activated CD4 T cells and islet-specific CD4 T cell expansion. B7-2 does not impact the effector phase of the autoimmune response as adoptive transfer of islet Ag-specific BDC2.5 splenocytes stimulated in vitro could easily induce disease in B7-2KO mice. CD4 T cells showed some hallmarks of hyporesponsiveness because TCR/CD28-mediated stimulation led to defective activation and failure to induce disease in NODscid recipients. Furthermore, CD4 T cells exhibited enhanced death in the absence of B7-2. Interestingly, we found that B7-2 is required to achieve normal levels of CD4+CD25+CD62L+ T regulatory cells because a significant reduction of these T regulatory cells was observed in the thymus but not in the peripheral compartments of B7-2KO mice. In addition, our adoptive transfer experiments did not reveal either pathogenic or regulatory potential associated with the B7-2KO splenocytes. Finally, we found that the lack of B7-2 did not induce a compensatory increase in the B7-1 signal on APC in the PLN compartment. Taken together these results clearly indicate that B7-2 plays a critical role in priming islet-reactive CD4 T cells, suggesting a simplified, two-cell model for the impact of this costimulatory molecule in autoimmunity against islets.

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Section: Discussionsupporting

confidence: 71%

Section: Discussionmentioning

confidence: 99%

B7-2 (CD86) Controls the Priming of Autoreactive CD4 T Cell Response against Pancreatic Islets

Yadav

Judkowski

Flodström‐Tullberg

et al. 2004

The Journal of Immunology

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“…In this study, we evaluated whether ED administration of CD4 effectively inhibits autoimmune pathology in the lacrimal glands of a mouse model of SS (12). We have previously reported that anti-CD86 mAb treatment improved the autoimmune pathology in both the lacrimal and the salivary glands of mice with SS (30). We used an antibody because the specific binding ability of a mAb against the target molecule allows the establishment of a molecule-specific therapeutic strategy with fewer side effects.…”

Section: Discussionmentioning

confidence: 99%

Effective treatment of a mouse model of Sjögren's syndrome with eyedrop administration of anti‐CD4 monoclonal antibody

Hayashi¹,

Ishimaru²,

Arakaki³

et al. 2004

Arthritis & Rheumatism

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Objective. To determine whether eyedrop administration of an anti-CD4 monoclonal antibody (mAb) is effective in the treatment of Sjögren's syndrome (SS) using a mouse model of the disease.Methods. The anti-CD4 mAb was administered daily into the eyes of mice with SS from ages 4 to 8 weeks or ages 10 to 12 weeks. During treatment, tear volume was monitored and after final treatment, histologic features of the lacrimal and salivary glands, the phenotypes and function of T cells, and serum titers of anti-␣-fodrin antibody were examined.Results. Eyedrop administration of anti-CD4 mAb before the onset of SS prevented the autoimmune pathology seen in the lacrimal glands but not that in the salivary glands. Furthermore, eyedrop administration of anti-CD4 mAb after the development of SS inhibited mononuclear cell infiltration and the destruction of parenchyma only in the lacrimal glands. Eyedrop administration of anti-CD4 mAb suppressed the local activation of CD4؉ T cells rather than deleting CD4؉ T cells, which reduced the expansion of pathologic CD4؉ T cells against ␣-fodrin.Conclusion. These results demonstrate the remarkable efficacy of anti-CD4 mAb eyedrops in the treatment of SS eye symptoms, which illustrates a new antibody-based therapeutic strategy for patients with eye problems caused by SS as well as other diseases.

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“…For instance, blocking B7.1 activity in SJL mice inhibited the induction of pathogenic Th1 response and abrogated susceptibility to experimental autoimmune encephalomyelitis, while blocking B7.2 functions inhibited Th2 responses and led to disease exacerbation (17,18). In other models of murine autoimmune disease, such as diabetes in NOD mice (19) and Sjogren's syndrome in NFS/sld mice (20), blocking B7.2, in contrast, prevented disease development. In the murine model of mercury-induced autoimmunity where both Th1 and Th2 responses are involved, B7.1 and B7.2 were found to regulate different manifestations of the autoimmune syndrome, and absence of either one did not completely protect from disease (21).…”

mentioning

confidence: 99%

B7 Costimulation Is Critical for Host Control of Chronic Mycobacterium tuberculosis Infection

Bhatt

Uzelac

Mathur

et al. 2009

The Journal of Immunology

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Although much is understood regarding the role of B7/CD28 family of costimulatory molecules in regulating host resistance in the context of several pathogens, analogous information with Mycobacterium tuberculosis is lacking. To address the requirements of B7-mediated costimulation in host resistance against tuberculosis, mice deficient in both B7.1 and B7.2 (B7DKO) were aerosol infected with M. tuberculosis Erdman and disease progression was monitored. We report herein that B7DKO mice are initially able to contain the bacterial load in the lung, but exhibit enhanced susceptibility during chronic infection. Despite the early control of bacterial replication, B7DKO mice essentially start off with compromised Th1 immunity and slower granulomatous response in the lung, characterized by markedly reduced lymphocytic infiltration. As the infection progresses from acute phase to the chronic phase, the nascent granulomas in the B7DKO lungs never fully achieve the architecture of granulomas developing in wild-type mice. Instead, lesions spread progressively to involve much of the lung in the B7DKO mice, ultimately leading to necrosis. Thus, early control of M. tuberculosis growth in the lung can occur in the absence of B7 costimulation and is less dependent on Th1 immunity and formation of a granulomatous structure. However, B7 costimulation is critical for long-term containment of infection within lung granulomas. These findings suggest that the use of costimulation-based immunomodulators may have significant repercussions on the induction of host protective immunity against tuberculosis.

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Treatment with anti-CD86 costimulatory molecule prevents the autoimmune lesions in murine Sjögren’s syndrome (SS) through up-regulated Th2 response

Cited by 39 publications

References 45 publications

B7-2 (CD86) Controls the Priming of Autoreactive CD4 T Cell Response against Pancreatic Islets

B7-2 (CD86) Controls the Priming of Autoreactive CD4 T Cell Response against Pancreatic Islets

Effective treatment of a mouse model of Sjögren's syndrome with eyedrop administration of anti‐CD4 monoclonal antibody

B7 Costimulation Is Critical for Host Control of Chronic Mycobacterium tuberculosis Infection

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