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胰岛素样生长因子-1(IGF-1)c.258 A > G同义突变改善老年性骨质疏松症。

IGF-1 c.258 A > G synonymous mutation ameliorates senile osteoporosis.

作者信息

Wang Zhaoguo, Dai Dayou, Wang Siyao, Zhang Libo, Li Yi, Zhang Xunming, Cheng Yunyun, Hao Linlin

机构信息

College of Animal Science, Jilin University, Changchun, Jilin, China.

State Key Laboratory of Systems Medicine for Cancer, Shanghai Cancer Institute, Ren Ji Hospital, School of medicine, Shanghai Jiao Tong University, Shanghai, China.

出版信息

Commun Biol. 2024 Dec 19;7(1):1675. doi: 10.1038/s42003-024-07369-x.

Abstract

Senile osteoporosis (SOP) is a multifactorial, age-related progressive phenomenon with a considerable morbidity and mortality. IGF-1 is an important regulator of bone reconstruction and metabolism throughout life. Nevertheless, our previous study unexpectedly found there is no change in the peak bone mass with a altered IGF-1 gene expression leaded by IGF-1 c.258 A > G synonymous mutation. Considering its involvement in the cellular senescence, we suspected c.258 A > G may participate in SOP. Therefore, the effect of IGF-1 c.258 A > G on SOP was firstly detected, the changes of bone formation and bone resorption index in SOP mice with two genotypes indicated it improved SOP. Then, the in vitro study confirmed the mutation ameliorates SOP by promoting the growth and development of senescent osteoblasts. At last, co-culture of osteoblast and osteoclast further verified the mutation prevents SOP by increasing the bone formation capacity of senescent osteoblasts. Collectively, this study illuminated the role of IGF-1 c.258 A > G in ameliorating SOP.

摘要

老年性骨质疏松症(SOP)是一种多因素、与年龄相关的进行性现象,具有相当高的发病率和死亡率。胰岛素样生长因子-1(IGF-1)是一生中骨重建和代谢的重要调节因子。然而,我们之前的研究意外发现,由IGF-1 c.258 A > G同义突变导致的IGF-1基因表达改变并未使骨峰值发生变化。考虑到其与细胞衰老有关,我们怀疑c.258 A > G可能参与了老年性骨质疏松症的发生。因此,我们首先检测了IGF-1 c.258 A > G对老年性骨质疏松症的影响,具有两种基因型的老年性骨质疏松症小鼠的骨形成和骨吸收指标变化表明该突变改善了老年性骨质疏松症。随后,体外研究证实该突变通过促进衰老成骨细胞的生长和发育来改善老年性骨质疏松症。最后,成骨细胞与破骨细胞的共培养进一步证实该突变通过提高衰老成骨细胞的骨形成能力来预防老年性骨质疏松症。总的来说,本研究阐明了IGF-1 c.258 A > G在改善老年性骨质疏松症中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cd8d/11659520/1ec53b874eba/42003_2024_7369_Fig1_HTML.jpg

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