适应性免疫与糖尿病发病机制：α4 整合素缺陷 NOD 鼠提供的见解。

Adaptive Immunity and Pathogenesis of Diabetes: Insights Provided by the α4-Integrin Deficient NOD Mouse.

机构信息

Institute for Transfusion Medicine and Immunohematology, School of Medicine, Goethe University, Sandhofstraße 1, 60528 Frankfurt, Germany.

Institute Frankfurt, German Red Cross Blood Service BaWüHe, Sandhofstraße 1, 60528 Frankfurt, Germany.

出版信息

Cells. 2020 Dec 4;9(12):2597. doi: 10.3390/cells9122597.

DOI:10.3390/cells9122597

PMID:33291571

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7761835/

Abstract

BACKGROUND

The spontaneously diabetic "non-obese diabetic" (NOD) mouse is a faithful model of human type-1 diabetes (T1D).

METHODS

Given the pivotal role of α4 integrin (CD49d) in other autoimmune diseases, we generated NOD mice with α4-deficient hematopoiesis (NOD.α4-/-) to study the role of α4 integrin in T1D.

RESULTS

NOD.α4-/- mice developed islet-specific T-cells and antibodies, albeit quantitatively less than α4+ counterparts. Nevertheless, NOD.α4-/- mice were completely and life-long protected from diabetes and insulitis. Moreover, transplantation with isogeneic α4-/- bone marrow prevented progression to T1D of pre-diabetic NOD.α4+ mice despite significant pre-existing islet cell injury. Transfer of α4+/CD3+, but not α4+/CD4+ splenocytes from diabetic to NOD.α4-/- mice induced diabetes with short latency. Despite an only modest contribution of adoptively transferred α4+/CD3+ cells to peripheral blood, pancreas-infiltrating T-cells were exclusively graft derived, i.e., α4+. Microbiota of diabetes-resistant NOD.α4-/- and pre-diabetic NOD.α4+ mice were identical. Co- housed diabetic NOD.α4+ mice showed the characteristic diabetic dysbiosis, implying causality of diabetes for dysbiosis. Incidentally, NOD.α4-/- mice were protected from autoimmune sialitis.

CONCLUSION

α4 is a potential target for primary or secondary prevention of T1D.

摘要

背景

自发性糖尿病“非肥胖型糖尿病”（NOD）小鼠是人类 1 型糖尿病（T1D）的忠实模型。

方法

鉴于 α4 整合素（CD49d）在其他自身免疫性疾病中的关键作用，我们生成了造血细胞缺乏 α4 的 NOD 小鼠（NOD.α4-/-），以研究 α4 整合素在 T1D 中的作用。

结果

NOD.α4-/-小鼠尽管数量较少，但仍发展出胰岛特异性 T 细胞和抗体。然而，NOD.α4-/-小鼠完全且终生免受糖尿病和胰岛炎的影响。此外，尽管存在明显的胰岛细胞损伤，但同种异体 α4-/-骨髓移植可预防前驱糖尿病 NOD.α4+小鼠进展为 T1D。从糖尿病 NOD.α4-/-小鼠向 NOD.α4-/-小鼠转移 α4+/CD3+，而不是 α4+/CD4+脾细胞，可诱导潜伏期短的糖尿病。尽管来自糖尿病的转移的 α4+/CD3+细胞对外周血的贡献仅适度，但浸润胰腺的 T 细胞完全来源于移植物，即 α4+。糖尿病抵抗的 NOD.α4-/-和前驱糖尿病的 NOD.α4+小鼠的微生物群是相同的。共同饲养的糖尿病 NOD.α4+小鼠表现出典型的糖尿病菌群失调，这暗示了糖尿病对菌群失调的因果关系。顺便说一句，NOD.α4-/-小鼠还受到自身免疫性唾液腺炎的保护。

结论

α4 是 T1D 一级或二级预防的潜在靶点。

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适应性免疫与糖尿病发病机制：α4 整合素缺陷 NOD 鼠提供的见解。

Adaptive Immunity and Pathogenesis of Diabetes: Insights Provided by the α4-Integrin Deficient NOD Mouse.

机构信息

Institute for Transfusion Medicine and Immunohematology, School of Medicine, Goethe University, Sandhofstraße 1, 60528 Frankfurt, Germany.

Institute Frankfurt, German Red Cross Blood Service BaWüHe, Sandhofstraße 1, 60528 Frankfurt, Germany.

出版信息

Cells. 2020 Dec 4;9(12):2597. doi: 10.3390/cells9122597.

DOI:10.3390/cells9122597

PMID:33291571

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7761835/

Abstract

BACKGROUND

The spontaneously diabetic "non-obese diabetic" (NOD) mouse is a faithful model of human type-1 diabetes (T1D).

METHODS

Given the pivotal role of α4 integrin (CD49d) in other autoimmune diseases, we generated NOD mice with α4-deficient hematopoiesis (NOD.α4-/-) to study the role of α4 integrin in T1D.

RESULTS

CONCLUSION

α4 is a potential target for primary or secondary prevention of T1D.

摘要

背景

自发性糖尿病“非肥胖型糖尿病”（NOD）小鼠是人类 1 型糖尿病（T1D）的忠实模型。

方法

鉴于 α4 整合素（CD49d）在其他自身免疫性疾病中的关键作用，我们生成了造血细胞缺乏 α4 的 NOD 小鼠（NOD.α4-/-），以研究 α4 整合素在 T1D 中的作用。

结果

结论

α4 是 T1D 一级或二级预防的潜在靶点。

适应性免疫与糖尿病发病机制：α4 整合素缺陷 NOD 鼠提供的见解。

Adaptive Immunity and Pathogenesis of Diabetes: Insights Provided by the α4-Integrin Deficient NOD Mouse.

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出版信息

BACKGROUND

METHODS

RESULTS

CONCLUSION

背景

方法

结果

结论

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适应性免疫与糖尿病发病机制：α4 整合素缺陷 NOD 鼠提供的见解。

Adaptive Immunity and Pathogenesis of Diabetes: Insights Provided by the α4-Integrin Deficient NOD Mouse.

机构信息

出版信息

BACKGROUND

METHODS

RESULTS

CONCLUSION

背景

方法

结果

结论

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