1型糖尿病器官供体胰岛细胞肠病毒VP1蛋白与HLA I类高表达

IF 8.4 1区医学 Q1 ENDOCRINOLOGY & METABOLISM

Diabetologia Pub Date : 2025-03-17 DOI:10.1007/s00125-025-06384-9

Teresa Rodriguez-Calvo, Jutta E. Laiho, Maarit Oikarinen, Pouria Akhbari, Christine Flaxman, Thomas Worthington, Paola Apaolaza, John S. Kaddis, Irina Kusmartseva, Sisko Tauriainen, Martha Campbell-Thompson, Mark A. Atkinson, Matthias von Herrath, Heikki Hyöty, Noel G. Morgan, Alberto Pugliese, Sarah J. Richardson

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引用次数: 0

摘要

目的/假设早期对1型糖尿病供体胰腺的研究表明，β细胞中存在肠病毒衣壳蛋白VP1。在npod病毒组开展的多学科方法的背景下，我们评估了来自188个器官供体的胰腺和其他组织（脾脏、十二指肠和胰淋巴结）的VP1阳性，包括1型糖尿病供体和表达自身抗体风险标记的供体。我们还研究了VP1阳性是否与胰岛细胞中HLA I类（HLA- 1）分子的高表达有关。方法通过糖尿病胰腺器官供体网络（nPOD）收集非糖尿病供体（ND, n=76）、表达单一或多种糖尿病相关自身抗体(AAb+, n=20；AAb++, n=9)和伴有残留含胰岛素胰岛（T1D-ICIs, n=41）或仅有胰岛素缺乏胰岛（T1D-IDIs, n=42）的1型糖尿病供体。VP1在两个独立的实验室采用免疫组化（IHC）和hla - 1 （IHC和免疫荧光）进行评估。我们在个案基础上和供体组之间确定了实验室间的检测一致性和阳性检测的总体发生率。结果大多数T1D-ICI供者（77.5%）检测到胰岛细胞VP1阳性，而ND供者仅为38.2% （p<0.001）。VP1阳性与hla - 1高表达相关。在接受hla - 1和VP1评估的献血者中，73.7%既有VP1免疫阳性，又有hla - 1高表达（p<0.001 vs ND）。此外，VP1+细胞在hla - 1高表达的供者中检测到的频率更高（p<；0.001与正常hla - 1相比）。在VP1+供者中，AAb++组和T1D-ICI组hla - 1高表达比例显著高于对照组（94.9%,p<0.001 vs ND）；这并不局限于新近发病的糖尿病患者。关键的是，在所有供体组中，VP1+组与VP1 -组相比，hla - 1高表达在VP1+组中更常见（45.8% vs 16%, p<0.001）。结论/解释：我们报道了迄今为止对临床前和诊断为1型糖尿病的供体胰腺中VP1和hla - 1的最广泛分析。我们发现VP1与诊断后残留的β细胞有关，并在自身抗体阳性的临床前阶段证明VP1阳性。我们首次发现胰岛细胞中VP1阳性和hla - 1高表达均存在于临床前阶段。虽然对组织的研究不允许我们证明因果关系，但我们的数据支持肠道病毒感染可能发生在1型糖尿病的整个自然史中，并且可能是驱动胰岛细胞hla - 1高表达的多种机制之一的假设。图形抽象

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Enterovirus VP1 protein and HLA class I hyperexpression in pancreatic islet cells of organ donors with type 1 diabetes

Aims/hypothesis

Earlier studies of pancreases from donors with type 1 diabetes demonstrated enteroviral capsid protein VP1 in beta cells. In the context of a multidisciplinary approach undertaken by the nPOD-Virus group, we assessed VP1 positivity in pancreas and other tissues (spleen, duodenum and pancreatic lymph nodes) from 188 organ donors, including donors with type 1 diabetes and donors expressing autoantibody risk markers. We also investigated whether VP1 positivity is linked to the hyperexpression of HLA class I (HLA-I) molecules in islet cells.

Methods

Organ donor tissues were collected by the Network for Pancreatic Organ Donors with Diabetes (nPOD) from donors without diabetes (ND, n=76), donors expressing a single or multiple diabetes-associated autoantibodies (AAb⁺, n=20; AAb⁺⁺, n=9) and donors with type 1 diabetes with residual insulin-containing islets (T1D-ICIs, n=41) or only insulin-deficient islets (T1D-IDIs, n=42). VP1 was assessed using immunohistochemistry (IHC) and HLA-I using IHC and immunofluorescence, in two independent laboratories. We determined assay concordance across laboratories and overall occurrence of positive assays, on a case-by-case basis and between donor groups.

Results

Islet cell VP1 positivity was detected in most T1D-ICI donors (77.5%) vs only 38.2% of ND donors (p<0.001). VP1 positivity was associated with HLA-I hyperexpression. Of those donors assessed for HLA-I and VP1, 73.7% had both VP1 immunopositivity and HLA-I hyperexpression (p<0.001 vs ND). Moreover, VP1⁺ cells were detected at higher frequency in donors with HLA-I hyperexpression (p<0.001 vs normal HLA-I). Among VP1⁺ donors, the proportion with HLA-I hyperexpression was significantly higher in the AAb⁺⁺ and T1D-ICI groups (94.9%, p<0.001 vs ND); this was not restricted to individuals with recent-onset diabetes. Critically, for all donor groups combined, HLA-I hyperexpression occurred more frequently in VP1⁺ compared with VP1⁻ donors (45.8% vs 16%, p<0.001).

Conclusions/interpretation

We report the most extensive analysis to date of VP1 and HLA-I in pancreases from donors with preclinical and diagnosed type 1 diabetes. We find an association of VP1 with residual beta cells after diagnosis and demonstrate VP1 positivity during the autoantibody-positive preclinical stage. For the first time, we show that VP1 positivity and HLA-I hyperexpression in islet cells are both present during the preclinical stage. While the study of tissues does not allow us to demonstrate causality, our data support the hypothesis that enterovirus infections may occur throughout the natural history of type 1 diabetes and may be one of multiple mechanisms driving islet cell HLA-I hyperexpression.

Graphical Abstract

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来源期刊

Diabetologia 医学-内分泌学与代谢

CiteScore

18.10

自引率

2.40%

发文量

193

审稿时长

1 months

期刊介绍： Diabetologia, the authoritative journal dedicated to diabetes research, holds high visibility through society membership, libraries, and social media. As the official journal of the European Association for the Study of Diabetes, it is ranked in the top quartile of the 2019 JCR Impact Factors in the Endocrinology & Metabolism category. The journal boasts dedicated and expert editorial teams committed to supporting authors throughout the peer review process.