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整合转录组学对比了与血糖控制相关的β细胞亚群中脂肪酸代谢与低氧反应。

Integrated transcriptomics contrasts fatty acid metabolism with hypoxia response in β-cell subpopulations associated with glycemic control.

机构信息

Department of Genetics, Washington University School of Medicine, 660 South Euclid Ave, Campus Box 8232, Saint Louis, MO, 63110, USA.

出版信息

BMC Genomics. 2023 Mar 28;24(1):156. doi: 10.1186/s12864-023-09232-5.

Abstract

BACKGROUND

Understanding how heterogeneous β-cell function impacts diabetes is imperative for therapy development. Standard single-cell RNA sequencing analysis illuminates some factors driving heterogeneity, but new strategies are required to enhance information capture.

RESULTS

We integrate pancreatic islet single-cell and bulk RNA sequencing data to identify β-cell subpopulations based on gene expression and characterize genetic networks associated with β-cell function in obese SM/J mice. We identify β-cell subpopulations associated with basal insulin secretion, hypoxia response, cell polarity, and stress response. Network analysis associates fatty acid metabolism and basal insulin secretion with hyperglycemic-obesity, while expression of Pdyn and hypoxia response is associated with normoglycemic-obesity.

CONCLUSIONS

By integrating single-cell and bulk islet transcriptomes, our study explores β-cell heterogeneity and identifies novel subpopulations and genetic pathways associated with β-cell function in obesity.

摘要

背景

了解异质β细胞功能如何影响糖尿病对于治疗开发至关重要。标准的单细胞 RNA 测序分析揭示了一些驱动异质性的因素,但需要新的策略来增强信息捕获。

结果

我们整合了胰岛单细胞和批量 RNA 测序数据,根据基因表达来识别β细胞亚群,并在肥胖 SM/J 小鼠中描述与β细胞功能相关的遗传网络。我们确定了与基础胰岛素分泌、缺氧反应、细胞极性和应激反应相关的β细胞亚群。网络分析将脂肪酸代谢和基础胰岛素分泌与高血糖肥胖相关联,而 Pdyn 的表达和缺氧反应与正常血糖肥胖相关联。

结论

通过整合单细胞和批量胰岛转录组,我们的研究探讨了β细胞的异质性,并确定了与肥胖相关的β细胞功能的新亚群和遗传途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/56da/10052828/8f5a2a75277a/12864_2023_9232_Fig1_HTML.jpg

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