功能失调的β细胞自噬诱导β细胞应激，增强胰岛免疫原性。

IF 5.9 2区医学 Q1 IMMUNOLOGY Frontiers in Immunology Pub Date : 2025-01-29 eCollection Date: 2025-01-01 DOI:10.3389/fimmu.2025.1504583

Matthew C Austin, Charanya Muralidharan, Saptarshi Roy, Justin J Crowder, Jon D Piganelli, Amelia K Linnemann

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引用次数: 0

摘要

背景：1型糖尿病（T1D）是由遗传和环境因素共同引起的，触发自身免疫介导的胰腺β细胞破坏。β细胞应激反应途径的缺陷，如自噬，可能在疾病发展中激活和/或加剧免疫反应中发挥重要作用。先前，我们发现β细胞自噬在T1D发病前受损，暗示该途径在T1D发病中起作用。目的：探讨自噬在β细胞健康和存活中的作用，以及自噬缺陷是否使胰岛细胞更具免疫原性。方法：我们敲除小鼠β细胞中的关键自噬酶ATG7 (ATG7Δβ-cell)，然后监测血糖，进行糖耐量试验，并评估大量胰岛mRNA和蛋白质。我们还评估了ATG7Δβ-cell胰岛中MHC-I的表达和CD45+免疫细胞的存在，并评估了在基础和IFNα刺激条件下自噬受损如何影响EndoC-βH1 HLA-I的表达。最后，我们将ATG7Δβ-cell胰岛细胞与糖尿病源性BDC2.5辅助性T细胞共培养，并评估T细胞的活化情况。结果：我们发现所有ATG7Δβ-cell小鼠在11-15周龄之间发生糖尿病。基因本体论分析显示，参与炎症过程、内质网应激反应和内质网相关降解途径的通路显著上调。有趣的是，我们还观察到参与mhc - 1呈递的蛋白上调，这表明有缺陷的β细胞自噬可能改变免疫肽丘或抗原库，并增强β细胞的免疫可见性。为了支持这一假设，我们观察到ATG7Δβ-cell胰岛中MHC-I表达和CD45+免疫细胞增加。我们还证明，当自噬降解被抑制时，hla - 1在内皮细胞β-细胞中上调。在基础条件和IFNα刺激条件下均观察到这种效应。相反，溶酶体酸化/功能刺激剂C381降低hla - 1表达。最后，我们发现在存在自噬缺陷的胰岛细胞时，BDC2.5 T细胞的激活增强。结论：我们的研究结果表明β细胞自噬对细胞存活/功能至关重要。有缺陷的β细胞自噬诱导内质网应激，改变抗原产生途径，并增强MHC-I/HLA-I的递呈以监视免疫细胞。总的来说，我们的结果表明，自噬缺陷使β细胞更容易受到免疫攻击和破坏。

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Dysfunctional β-cell autophagy induces β-cell stress and enhances islet immunogenicity.

Background: Type 1 Diabetes (T1D) is caused by a combination of genetic and environmental factors that trigger autoimmune-mediated destruction of pancreatic β-cells. Defects in β-cell stress response pathways such as autophagy may play an important role in activating and/or exacerbating the immune response in disease development. Previously, we discovered that β-cell autophagy is impaired prior to the onset of T1D, implicating this pathway in T1D pathogenesis.

Aims: To assess the role of autophagy in β-cell health and survival, and whether defects in autophagy render islets more immunogenic.

Methods: We knocked out the critical autophagy enzyme, ATG7, in the β-cells of mice (ATG7^Δβ-cell) then monitored blood glucose, performed glucose tolerance tests, and evaluated bulk islet mRNA and protein. We also assessed MHC-I expression and presence of CD45+ immune cells in ATG7^Δβ-cell islets and evaluated how impaired autophagy affects EndoC-βH1 HLA-I expression under basal and IFNα stimulated conditions. Lastly, we co-cultured ATG7^Δβ-cell islet cells with diabetogenic BDC2.5 helper T cells and evaluated T cell activation.

Results: We found that all ATG7^Δβ-cell mice developed diabetes between 11-15 weeks of age. Gene ontology analysis revealed a significant upregulation of pathways involved in inflammatory processes, response to ER stress, and the ER-associated degradation pathway. Interestingly, we also observed upregulation of proteins involved in MHC-I presentation, suggesting that defective β-cell autophagy may alter the immunopeptidome, or antigen repertoire, and enhance β-cell immune visibility. In support of this hypothesis, we observed increased MHC-I expression and CD45+ immune cells in ATG7^Δβ-cell islets. We also demonstrate that HLA-I is upregulated in EndoC β-cells when autophagic degradation is inhibited. This effect was observed under both basal and IFNα stimulated conditions. Conversely, a stimulator of lysosome acidification/function, C381, decreased HLA-I expression. Lastly, we showed that in the presence of islet cells with defective autophagy, there is enhanced BDC2.5 T cell activation.

Conclusions: Our findings demonstrate that β-cell autophagy is critical to cell survival/function. Defective β-cell autophagy induces ER stress, alters pathways of antigen production, and enhances MHC-I/HLA-I presentation to surveilling immune cells. Overall, our results suggest that defects in autophagy make β-cells more susceptible to immune attack and destruction.

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来源期刊

Frontiers in Immunology IMMUNOLOGY-

CiteScore

9.80

自引率

11.00%

发文量

7153

审稿时长

14 weeks

期刊介绍： Frontiers in Immunology is a leading journal in its field, publishing rigorously peer-reviewed research across basic, translational and clinical immunology. This multidisciplinary open-access journal is at the forefront of disseminating and communicating scientific knowledge and impactful discoveries to researchers, academics, clinicians and the public worldwide. Frontiers in Immunology is the official Journal of the International Union of Immunological Societies (IUIS). Encompassing the entire field of Immunology, this journal welcomes papers that investigate basic mechanisms of immune system development and function, with a particular emphasis given to the description of the clinical and immunological phenotype of human immune disorders, and on the definition of their molecular basis.