Tipping-point transition from transient to persistent inflammation in pancreatic islets

IF 3.5 2区生物学 Q1 MATHEMATICAL & COMPUTATIONAL BIOLOGY

NPJ Systems Biology and Applications Pub Date : 2024-09-12 DOI:10.1038/s41540-024-00427-4

Thomas Holst-Hansen, Pernille Yde Nielsen, Mogens H. Jensen, Thomas Mandrup-Poulsen, Ala Trusina

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Abstract

Type 2 diabetes (T2D) is associated with a systemic increase in the pro-inflammatory cytokine IL-1β. While transient exposure to low IL-1β concentrations improves insulin secretion and β-cell proliferation in pancreatic islets, prolonged exposure leads to impaired insulin secretion and collective β-cell death. IL-1 is secreted locally by islet-resident macrophages and β-cells; however, it is unknown if and how the two opposing modes may emerge at single islet level. We investigated the duality of IL-1β with a quantitative in silico model of the IL-1 regulatory network in pancreatic islets. We find that the network can produce either transient or persistent IL-1 responses when induced by pro-inflammatory and metabolic cues. This suggests that the duality of IL-1 may be regulated at the single islet level. We use two core feedbacks in the IL-1 regulation to explain both modes: First, a fast positive feedback in which IL-1 induces its own production through the IL-1R/IKK/NF-κB pathway. Second, a slow negative feedback where NF-κB upregulates inhibitors acting at different levels along the IL-1R/IKK/NF-κB pathway—IL-1 receptor antagonist and A20, among others. A transient response ensues when the two feedbacks are balanced. When the positive feedback dominates over the negative, islets transit into the persistent inflammation mode. Consistent with several observations, where the size of islets was implicated in its inflammatory state, we find that large islets and islets with high density of IL-1β amplifying cells are more prone to transit into persistent IL-1β mode. Our results are likely not limited to IL-1β but are general for the combined effect of multiple pro-inflammatory cytokines and chemokines. Generalizing complex regulations in terms of two feedback mechanisms of opposing nature and acting on different time scales provides a number of testable predictions. Taking islet architecture and cellular heterogeneity into consideration, further dynamic monitoring and experimental validation in actual islet samples will be crucial to verify the model predictions and enhance its utility in clinical applications.

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胰岛从短暂炎症到持续炎症的临界点转变

2 型糖尿病（T2D）与促炎细胞因子 IL-1β 的全身性增加有关。虽然短暂暴露于低浓度的 IL-1β 会改善胰岛的胰岛素分泌和β细胞增殖，但长期暴露会导致胰岛素分泌受损和β细胞集体死亡。驻留在胰岛的巨噬细胞和β细胞会在局部分泌IL-1；然而，在单个胰岛水平是否以及如何出现这两种相反的模式尚不清楚。我们利用胰岛中 IL-1 调控网络的定量硅学模型研究了 IL-1β 的双重性。我们发现，在促炎症和代谢线索的诱导下，该网络可产生短暂或持续的 IL-1 反应。这表明 IL-1 的双重性可能在单个胰岛水平上受到调控。我们利用 IL-1 调节中的两个核心反馈来解释这两种模式：第一，快速正反馈，即 IL-1 通过 IL-1R/IKK/NF-κB 途径诱导自身产生。第二，缓慢的负反馈，即 NF-κB 上调沿 IL-1R/IKK/NF-κB 途径作用于不同水平的抑制剂--IL-1 受体拮抗剂和 A20 等。当两种反馈平衡时，就会产生瞬时反应。当正反馈超过负反馈时，胰岛就会进入持续性炎症模式。我们发现，大的胰岛和具有高密度 IL-1β 扩增细胞的胰岛更容易转入持续性 IL-1β 模式。我们的研究结果可能并不局限于 IL-1β，而是多种促炎细胞因子和趋化因子共同作用的普遍结果。通过两种性质相反且作用于不同时间尺度的反馈机制来归纳复杂的调节机制，可以得出许多可检验的预测。考虑到胰岛结构和细胞异质性，在实际胰岛样本中进行进一步的动态监测和实验验证对于验证模型预测和提高其在临床应用中的实用性至关重要。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

NPJ Systems Biology and Applications Mathematics-Applied Mathematics

CiteScore

5.80

自引率

0.00%

发文量

审稿时长

8 weeks

期刊介绍： npj Systems Biology and Applications is an online Open Access journal dedicated to publishing the premier research that takes a systems-oriented approach. The journal aims to provide a forum for the presentation of articles that help define this nascent field, as well as those that apply the advances to wider fields. We encourage studies that integrate, or aid the integration of, data, analyses and insight from molecules to organisms and broader systems. Important areas of interest include not only fundamental biological systems and drug discovery, but also applications to health, medical practice and implementation, big data, biotechnology, food science, human behaviour, broader biological systems and industrial applications of systems biology. We encourage all approaches, including network biology, application of control theory to biological systems, computational modelling and analysis, comprehensive and/or high-content measurements, theoretical, analytical and computational studies of system-level properties of biological systems and computational/software/data platforms enabling such studies.

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