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Transcriptional landscape of mouse-aged ovaries reveals a unique set of non-coding RNAs associated with physiological and environmental ovarian dysfunctions

生物 卵巢储备 卵巢 卵泡闭锁 转录组 毒物 卵泡期 抗苗勒氏激素 小RNA 生理学 激素 卵泡 内科学 内分泌学 生物信息学 遗传学 基因 医学 基因表达 怀孕 不育 毒性
作者
Danila Cuomo,Immacolata Porreca,Michele Ceccarelli,David W. Threadgill,William Barrington,Annacristina Petriella,Fulvio D’Angelo,Gilda Cobellis,Francesca De Stefano,Massimo D’Agostino,Mario De Felice,Massimo Mallardo,Concetta Ambrosino
出处
期刊:Cell death discovery [Springer Nature]
卷期号:4 (1) 被引量:23
标识
DOI:10.1038/s41420-018-0121-y
摘要

The progressive and physiological decline in ovarian function depends on the rate of follicular loss by atresia, contributing to the reduction in ovarian reserve. Genetics and environmental factors play important roles in ovarian senescence and in the onset of ovarian dysfunctions such as diminished ovarian reserve. A better understanding of the mechanisms underlying ovarian aging and their regulation by genetic and environmental factors is needed to evaluate ovarian reserve and to predict fertility potential by identification of more accurate and less invasive markers. We report transcriptomic data (i) implicating novel (e.g. EIF2 signalling) and well-known pathways (e.g. TGFβ signalling), and (ii) defining a unique set of non-coding RNA (ncRNA), both associated with ovarian function. The latter includes miRNAs (e.g. Mir143 and Mir145), snoRNAs (e.g. Snord16a and Snora34), and one lncRNA (Gas5), which are differentially expressed in middle-aged ovaries (12 months) vs young-aged (3 months) from CD1 mice. Experimental analysis confirms that ovary lifespan varies across genetic backgrounds in mice and, genetics influences the response to environmental perturbations such as diet. Moreover, the identified ncRNAs were verified in a model of reproductive dysfunction promoted by the environmental toxicant ethylenthiourea. We also report the increase of miRNA143 and miRNA145 in follicular fluid of women with diminished ovarian reserve. Their levels inversely correlate with the hormonal profile and with the number of the oocytes recruited upon hormonal stimulation. Overall, we report a transcriptomic signature for ovarian dysfunction in vivo that provides a valuable resource for translational research in human reproductive aging.

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