微RNA 29通过miR-29-OXPHOS复合通路调节β细胞线粒体代谢和胰岛素分泌。

IF 5.6 2区医学 Q1 PHYSIOLOGY

Acta Physiologica Pub Date : 2024-05-27 DOI:10.1111/apha.14180

E. Cowan, J. Sun, A. Hamilton, S. Ruhrmann, A. Karagiannopoulos, E. Westholm, J. K. Ofori, C. Luan, E. Zhang, H. Mulder, L. Eliasson

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引用次数: 0

摘要

目的：微RNA（miRNA）调控β细胞功能，而β细胞线粒体和胰岛素分泌在糖尿病中受到干扰。我们的目的是鉴定调控β细胞线粒体代谢的关键miRNAs和新型β细胞miRNA-线粒体通路：利用 TargetScan (http://www.targetscan.org/) 预测与β细胞功能有关的 16 个 miRNA 是否以与线粒体活性有关的 27 个顺式基因为靶标。在克隆 INS-1 832/13 β 细胞中测定了候选 miRNAs 的表达以及在 2.8、11.1 和 16.7 毫摩尔葡萄糖中预孵育 24 小时和 1 小时后的胰岛素分泌。对沉默了 MiR-29 的 INS-1 832/13 细胞进行了胰岛素分泌（葡萄糖、丙酮酸和 K+）、目标顺式基因表达（线粒体复合体 I（CI）的 Ndufv3 和 Ndufa10 成分）、OXPHOS（CI-V）蛋白表达和线粒体 OXPHOS 呼吸/活性的评估。研究评估了在后藤柿崎（GK）大鼠、db/db小鼠和2型糖尿病（T2D）人胰岛以及在葡萄糖脂毒性条件下培养的NMRI小鼠胰岛中不同表达的miR-29 miRNAs的表达情况：结果：在大鼠和人类物种中，MiR-29、miR-15和miR-124被预测能调控约20个顺式基因，而单独的miR-29被预测能调控≥12个顺式基因。在葡萄糖升高 24 小时后，INS-1 832/13 细胞中 MiR-29 的表达和胰岛素分泌减少。MiR-29的敲除增加了所有测试的胰岛素分泌反应、Nudfv3、Ndufa10、复合体I和II的表达以及细胞线粒体的OXPHOS。MiR-29在db/db胰岛中表达减少，但在GK大鼠和T2D人类胰岛中表达增加：我们得出结论：miR-29 是通过 miR-29-OXPHOS 复合通路调节β细胞线粒体代谢和胰岛素分泌的关键 miRNA。此外，我们还推断，在葡萄糖毒性条件下，miR-29 的表达减少可补偿性地增强胰岛素分泌。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

MicroRNA 29 modulates β-cell mitochondrial metabolism and insulin secretion via underlying miR-29-OXPHOS complex pathways

查看原文本刊更多论文

MicroRNA 29 modulates β-cell mitochondrial metabolism and insulin secretion via underlying miR-29-OXPHOS complex pathways

Aim

MicroRNAs (miRNAs) regulate β-cell function, and β-cell mitochondria and insulin secretion are perturbed in diabetes. We aimed to identify key miRNAs regulating β-cell mitochondrial metabolism and novel β-cell miRNA-mitochondrial pathways.

Methods

TargetScan (http://www.targetscan.org/) was used to predict if 16 miRNAs implicated in β-cell function target 27 cis-eGenes implicated in mitochondrial activity. The expression of candidate miRNAs and insulin secretion after 24 and 1 h pre-incubation in 2.8, 11.1- and 16.7-mM glucose was measured in clonal INS-1 832/13 β-cells. MiR-29 silenced INS-1 832/13 cells were assessed for insulin secretion (glucose, pyruvate, and K⁺), target cis-eGene expression (Ndufv3 and Ndufa10 components of mitochondrial complex I (CI)), OXPHOS (CI-V) protein expression, and mitochondrial OXPHOS respiration/activity. The expression of differentially expressed miR-29 miRNAs was evaluated in Goto-Kakizaki (GK) rat, db/db mouse and type 2 diabetic (T2D) human islets, as well as NMRI mouse islets cultured under glucolipotoxic conditions.

Results

MiR-29, miR-15 and miR-124 were predicted to regulate ~20 cis-eGenes, while miR-29 alone was predicted to regulate ≥12 of these in rat and human species. MiR-29 expression and insulin secretion were reduced in INS-1 832/13 cells after 24 h in elevated glucose. MiR-29 knockdown increased all tested insulin secretory responses, Nudfv3, Ndufa10, complex I and II expression, and cellular mitochondrial OXPHOS. MiR-29 expression was reduced in db/db islets but increased in GK rat and T2D human islets.

Conclusion

We conclude miR-29 is a key miRNA in regulating β-cell mitochondrial metabolism and insulin secretion via underlying miR-29-OXPHOS complex pathways. Furthermore, we infer reduced miR-29 expression compensatorily enhances insulin secretion under glucotoxicity.

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来源期刊

Acta Physiologica 医学-生理学

CiteScore

11.80

自引率

15.90%

发文量

182

审稿时长

4-8 weeks

期刊介绍： Acta Physiologica is an important forum for the publication of high quality original research in physiology and related areas by authors from all over the world. Acta Physiologica is a leading journal in human/translational physiology while promoting all aspects of the science of physiology. The journal publishes full length original articles on important new observations as well as reviews and commentaries.