Significant alteration of protein profiles in a mouse model of polycystic ovary syndrome

多囊卵巢 生物 脂质代谢 内分泌系统 内分泌学 下调和上调 内科学 氧化应激 蛋白质组学 卵巢 生物信息学 胰岛素抵抗 糖尿病 激素 生物化学 医学 基因
作者
Bin Meng,Xiaoning Yang,Shiwei Luo,Chong Shen,Qiong Jia,Haifeng Zhang,Yandong Li,Yu Xue,Juan Zhao,Pengxiang Qu,Enqi Liu
出处
期刊:Molecular Reproduction and Development [Wiley]
标识
DOI:10.1002/mrd.23720
摘要

Polycystic ovary syndrome (PCOS) is an endocrine disorder, affecting women of child-bearing age, and the incidence rate is growing and assuming epidemic proportions. The etiology of PCOS remains unknown and there is no cure. Some animal models for PCOS have been established which have enhanced our understanding of the underlying mechanisms, but omics data for revealing PCOS pathogenesis and for drug discovery are still lacking. In the present study, proteomics analysis was used to construct a protein profile of the ovaries in a PCOS mouse model. The result showed a clear difference in protein profile between the PCOS and control group, with 495 upregulated proteins and 404 downregulated proteins in the PCOS group. The GO term and KEGG pathway analyses of differentially expressed proteins mainly showed involvement in lipid metabolism, oxidative stress, and immune response, which are consistent with pathological characteristics of PCOS in terms of abnormal metabolism, endocrine disorders, chronic inflammation and imbalance between oxidant and antioxidant levels. Also, we found that inflammatory responses were activated in the PCOS ovarium, while lipid biosynthetic process peroxisome, and bile secretion were inhibited. In addition, we found some alteration in unexpected pathways, such as glyoxylate and dicarboxylate metabolism, which should be investigated. The present study makes an important contribution to the current lack of PCOS ovarian proteomic data and provides an important reference for research and development of effective drugs and treatments for PCOS.
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