IL-6预处理可增强促炎细胞因子诱导的β细胞死亡。

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
V R Oliveira, C C Paula, S Taniguchi, F Ortis
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引用次数: 1

摘要

背景:1型糖尿病(T1D)以免疫系统特异性破坏β细胞为特征。在此过程中,促炎细胞因子在胰岛中释放,并促进β细胞的死亡。细胞因子诱导的iNOS活化,通过NF-κB,参与β细胞死亡的诱导,包括内质网应激激活。体育锻炼已被用作T1D患者更好地控制血糖的辅助手段,因为它能够独立于胰岛素增加葡萄糖摄取。最近有研究发现,运动过程中骨骼肌释放IL-6可预防促炎细胞因子诱导的β细胞死亡。然而,这种对β细胞有益作用的分子机制尚未完全阐明。我们的目的是评估IL-6对暴露于促炎细胞因子的β细胞的影响。结果:IL-6预处理使INS-1E细胞致敏,细胞因子诱导的细胞死亡增加,细胞因子诱导的iNOS和Caspase-3表达增加。然而,在这些条件下,细胞因子诱导的p-eIF2-α表达下降,但与内质网应激相关的蛋白p- ire1表达没有下降。为了确定IL-6预处理诱导的β-细胞死亡标志物的增加是否与UPR反应的预防有关,我们使用了一种化学伴侣(TUDCA),它可以提高内质网折叠能力。在IL-6预处理的情况下,使用TUDCA增加了细胞因子诱导的Caspase-3表达和Bax/Bcl-2比值。然而,在这种情况下,TUDCA对p-eIF2-α的表达没有调节作用,而CHOP的表达增加。结论:单独使用IL-6治疗对β细胞无益处,可导致细胞死亡标志物增加和UPR激活受损。此外,在这种情况下,TUDCA不能恢复内质网稳态或提高β细胞活力,这表明可能涉及其他机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Pre-treatment with IL-6 potentiates β-cell death induced by pro-inflammatory cytokines.

Pre-treatment with IL-6 potentiates β-cell death induced by pro-inflammatory cytokines.

Pre-treatment with IL-6 potentiates β-cell death induced by pro-inflammatory cytokines.

Pre-treatment with IL-6 potentiates β-cell death induced by pro-inflammatory cytokines.

Background: Type I Diabetes mellitus (T1D) is characterized by a specific destruction of β-cells by the immune system. During this process pro-inflammatory cytokines are released in the pancreatic islets and contribute for β-cells demise. Cytokine-induced iNOS activation, via NF-κB, is implicated in induction of β-cells death, which includes ER stress activation. Physical exercise has been used as an adjunct for better glycemic control in patients with T1D, since it is able to increase glucose uptake independent of insulin. Recently, it was observed that the release of IL-6 by skeletal muscle, during physical exercise, could prevent β-cells death induced by pro-inflammatory cytokines. However, the molecular mechanisms involved in this beneficial effect on β-cells are not yet completely elucidated. Our aim was to evaluate the effect of IL-6 on β-cells exposed to pro-inflammatory cytokines.

Results: Pre-treatment with IL-6 sensitized INS-1E cells to cytokine-induced cell death, increasing cytokine-induced iNOS and Caspase-3 expression. Under these conditions, however, there was a decrease in cytokines-induced p-eIF2-α but not p-IRE1expression, proteins related to ER stress. To address if this prevention of adequate UPR response is involved in the increase in β-cells death markers induced by IL-6 pre-treatment, we used a chemical chaperone (TUDCA), which improves ER folding capacity. Use of TUDCA increased cytokines-induced Caspase-3 expression and Bax/Bcl-2 ratio in the presence of IL-6 pre-treatment. However, there is no modulation of p-eIF2-α expression by TUDCA in this condition, with increase of CHOP expression.

Conclusion: Treatment with IL-6 alone is not beneficial for β-cells, leading to increased cell death markers and impaired UPR activation. In addition, TUDCA has not been able to restore ER homeostasis or improve β-cells viability under this condition, suggesting that other mechanisms may be involved.

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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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