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冠蛋白7在人类、小鼠和果蝇体重调节中的作用。

Implication of coronin 7 in body weight regulation in humans, mice and flies.

作者信息

Eriksson Anders, Williams Michael J, Voisin Sarah, Hansson Ida, Krishnan Arunkumar, Philippot Gaetan, Yamskova Olga, Herisson Florence M, Dnyansagar Rohit, Moschonis George, Manios Yannis, Chrousos George P, Olszewski Pawel K, Frediksson Robert, Schiöth Helgi B

机构信息

Department of Neuroscience, Functional Pharmacology, Uppsala University, Husargatan 3, Box 593, Uppsala, 75 124, Sweden.

Department of Biological Sciences, University of Waikato, Hamilton, New Zealand.

出版信息

BMC Neurosci. 2015 Mar 14;16:13. doi: 10.1186/s12868-015-0151-9.

Abstract

BACKGROUND

Obesity is a growing global concern with strong associations with cardiovascular disease, cancer and type-2 diabetes. Although various genome-wide association studies have identified more than 40 genes associated with obesity, these genes cannot fully explain the heritability of obesity, suggesting there may be other contributing factors, including epigenetic effects.

RESULTS

We performed genome wide DNA methylation profiling comparing normal-weight and obese 9-13 year old children to investigate possible epigenetic changes correlated with obesity. Of note, obese children had significantly lower methylation levels at a CpG site located near coronin 7 (CORO7), which encodes a tryptophan-aspartic acid dipeptide (WD)-repeat containing protein most likely involved in Golgi complex morphology and function. Anatomical profiling of coronin 7 (Coro7) mRNA expression in mice revealed that it is highly expressed in appetite and energy balance regulating regions, including the hypothalamus, striatum and locus coeruleus, the main noradrenergic brain site. Interestingly, we found that food deprivation in mice downregulates hypothalamic Coro7 mRNA levels, and injecting ethanol, an appetite stimulant, increased the number of Coro7 expressing cells in the locus coeruleus. Finally, by employing the genetically-tractable Drosophila melanogaster model we were able to demonstrate an evolutionarily conserved metabolic function for the CORO7 homologue pod1. Knocking down the pod1 in the Drosophila adult nervous system increased their resistance to starvation. Furthermore, feeding flies a high-calorie diet significantly increased pod1 expression.

CONCLUSION

We conclude that coronin 7 is involved in the regulation of energy homeostasis and this role stems, to some degree, from the effect on feeding for calories and reward.

摘要

背景

肥胖是一个日益引起全球关注的问题,与心血管疾病、癌症和2型糖尿病密切相关。尽管各种全基因组关联研究已经确定了40多个与肥胖相关的基因,但这些基因并不能完全解释肥胖的遗传性,这表明可能存在其他促成因素,包括表观遗传效应。

结果

我们对9至13岁体重正常和肥胖儿童进行了全基因组DNA甲基化分析,以研究与肥胖相关的可能表观遗传变化。值得注意的是,肥胖儿童在coronin 7(CORO7)附近的一个CpG位点的甲基化水平显著降低,CORO7编码一种最有可能参与高尔基体形态和功能的含色氨酸-天冬氨酸二肽(WD)重复序列的蛋白质。对小鼠中coronin 7(Coro7)mRNA表达的解剖学分析表明,它在食欲和能量平衡调节区域高度表达,包括下丘脑、纹状体和蓝斑,蓝斑是大脑主要的去甲肾上腺素能位点。有趣 的是,我们发现小鼠禁食会下调下丘脑Coro7 mRNA水平,而注射食欲刺激剂乙醇会增加蓝斑中表达Coro7的细胞数量。最后,通过使用遗传上易于处理的果蝇模型,我们能够证明CORO7同源物pod1具有进化上保守的代谢功能。在果蝇成虫神经系统中敲低pod1会增加它们对饥饿的抵抗力。此外,给果蝇喂食高热量饮食会显著增加pod1的表达。

结论

我们得出结论,coronin 7参与能量稳态的调节,并且这一作用在一定程度上源于对热量摄入和奖赏性进食的影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/66eb/4364644/1ec4988af2d0/12868_2015_151_Fig1_HTML.jpg

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