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胰岛中钙离子信号的出生后成熟:来自新生小鼠的研究。

Postnatal maturation of calcium signaling in islets of Langerhans from neonatal mice.

机构信息

Honors Tutorial College, Ohio University, Athens, OH, USA; Dept. of Biomedical Sciences, Heritage College of Osteopathic Medicine, Ohio University, Athens, OH, USA.

Dept. of Biomedical Sciences, Heritage College of Osteopathic Medicine, Ohio University, Athens, OH, USA; Diabetes Institute, Heritage College of Osteopathic Medicine, Ohio University, Athens, OH, USA.

出版信息

Cell Calcium. 2021 Mar;94:102339. doi: 10.1016/j.ceca.2020.102339. Epub 2020 Dec 28.

Abstract

Pancreatic islet cells develop mature physiological responses to glucose and other fuels postnatally. In this study, we used fluorescence imaging techniques to measure changes in intracellular calcium ([Ca]) to compare islets isolated from mice on postnatal days 0, 4, and 12 with islets from adult CD-1 mice. In addition, we used publicly available RNA-sequencing data to compare expression levels of key genes in β-cell physiology with [Ca] data across these ages. We show that islets isolated from mice on postnatal day 0 displayed elevated [Ca] in basal glucose (≤4 mM) but lower [Ca] responses to stimulation by 12-20 mM glucose compared to adult. Neonatal islets displayed more adult-like [Ca] in basal glucose by day 4 but continued to show lower [Ca] responses to 16 and 20 mM glucose stimulation up to at least day 12. A right shift in glucose sensing (EC) correlated with lower fragment-per-kilobase-of-transcript-per-million-reads-mapped (FPKM) of Slc2a2 (glut2) and Actn3 and increased FPKM for Galk1 and Nupr1. Differences in [Ca] responses to additional stimuli were also observed. Calcium levels in the endoplasmic reticulum were elevated on day 0 but became adult-like by day 4, which corresponded with reduced expression in Atp2a2 (SERCA2) and novel K+-channel Ktd17, increased expression of Pml, Wfs1, Thada, and Herpud1, and basal [Ca] maturing to adult levels. Ion-channel activity also matured rapidly, but RNA sequencing data mining did not yield strong leads. In conclusion, the maturation of islet [Ca] signaling is complex and multifaceted; several possible gene targets were identified that may participate in this process.

摘要

胰岛细胞在出生后会对葡萄糖和其他燃料产生成熟的生理反应。在这项研究中,我们使用荧光成像技术来测量细胞内钙离子 ([Ca]) 的变化,以比较来自出生后第 0、4 和 12 天的小鼠胰岛和成年 CD-1 小鼠胰岛。此外,我们使用公开的 RNA 测序数据,比较了这些年龄段关键基因在 β 细胞生理学中的表达水平与 [Ca] 数据。我们发现,出生后第 0 天的小鼠胰岛在基础葡萄糖(≤4mM)中显示出升高的 [Ca],但与成年相比,对 12-20mM 葡萄糖的刺激反应的 [Ca] 较低。新生胰岛在第 4 天的基础葡萄糖中显示出更接近成年的 [Ca],但直到至少第 12 天,对 16 和 20mM 葡萄糖刺激的 [Ca] 反应仍然较低。葡萄糖感应(EC)的右移与 Slc2a2(glut2)和 Actn3 的片段每千碱基转录物每百万读段映射的基因表达量(FPKM)降低以及 Galk1 和 Nupr1 的 FPKM 增加相关。对其他刺激的 [Ca] 反应也存在差异。内质网中的钙水平在第 0 天升高,但在第 4 天变得与成年相似,这与 Atp2a2(SERCA2)和新型 K+-通道 Ktd17 的表达减少、Pml、Wfs1、Thada 和 Herpud1 的表达增加以及基础 [Ca] 成熟到成年水平相对应。离子通道活性也迅速成熟,但 RNA 测序数据挖掘并未产生明确的线索。总之,胰岛 [Ca] 信号转导的成熟是复杂和多方面的;确定了几个可能参与该过程的基因靶点。

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