Differentially expressed plasma microRNAs in premature ovarian failure patients and the potential regulatory function of mir-23a in granulosa cell apoptosis

Yang, Xiaokui; Zhou, Ying; Peng, Sha; Wu, Liang; Lin, Haiyan; Wang, Shuyu; Wang, Hongmei

doi:10.1530/rep-11-0371

Cited by 151 publications

(136 citation statements)

References 48 publications

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“…In addition, the clinical relevance of miRNAs has steadily grown over the past few years particularly in relation to their significant potential as biomarkers of tissue function (Laterza et al 2009, Schwarzenbach et al 2011. Also, the possibility that miRNAs associated with certain clinical diseases, including ovarian diseases (Yang et al 2012), could be therapeutically targeted has generated enormous interest within medical communities (Pfeifer & Lehmann 2010). An increased understanding of ovarian miRNAs over the coming years will facilitate the application of this potential in clinical reproduction.…”

Section: Discussionmentioning

confidence: 99%

“…Yan et al (2012) reported attenuation of activininduced proliferation of mouse granulosa cells by miR-145 targeting of both activin receptor 1B and cyclin D2. In another study, Yang et al (2012) showed that miR-23a was pro-apoptotic in cultured human luteinised granulosa cells presumably by decreasing the levels of X-linked inhibitor of apoptosis protein (XIAP) and increasing caspase-3 cleavage, although it was not clarified whether these were actually direct targets of miR-23a in granulosa cells. Finally, using a microarray approach in porcine ovarian follicles, Lin et al (2012) found that miR-26b expression increased during follicular atresia and further showed that this miRNA could induce granulosa cell death by directly targeting ataxia telangiectasia mutated (ATM), a gene involved in DNA repair.…”

Section: Involvement Of Mirnas During Follicular Growth and Steroidogmentioning

confidence: 99%

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Involvement of miRNAs in ovarian follicular and luteal development

Donadeu¹,

Schauer²,

Sontakke³

2012

Journal of Endocrinology

156

106

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Although much progress has been made in the genetic dissection of biological networks involved in follicular/luteal development in the mammalian ovary, the gene regulation mechanisms involved are still poorly understood. Over the last 10 years, miRNAs have emerged as master regulators of tissue growth and differentiation in animals. However, compared with other body tissues, little is still known about the functional involvement of miRNAs in the ovary. Several studies have identified miRNA populations specifically associated with the development of follicles and corpora lutea, particularly in relation to the follicular-luteal transition, and the functional involvement of some of these miRNAs has been characterised in vitro and/or in vivo. Specifically, three different miRNAs, miR-224, miR-378 and miR-383, have shown to be involved in regulating aromatase expression during follicle development. In addition, miR-21 has been identified as promoting follicular cell survival during ovulation, and pro-angiogenic miR-17-5p and let-7b were shown to be necessary for normal development of the corpus luteum. Experimental evidence for the involvement of several other miRNAs in different aspects of follicle/luteal development has also been obtained. In addition, many of these studies exemplify the challenges associated with identifying physiologically relevant targets of ovarian miRNAs. Continuous advances in this field will be considerably facilitated by progress in understanding miRNA physiology in other body systems and will eventually lead to a much better understanding of the control of follicular/luteal development. In turn, through the potential offered by miRNA diagnostics and miRNA therapeutics, this new knowledge should bring considerable benefits to reproductive medicine.

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Section: Discussionmentioning

confidence: 99%

Section: Involvement Of Mirnas During Follicular Growth and Steroidogmentioning

confidence: 99%

Involvement of miRNAs in ovarian follicular and luteal development

Donadeu¹,

Schauer²,

Sontakke³

2012

Journal of Endocrinology

156

106

View full text Add to dashboard Cite

show abstract

“…Several studies have already reported effects of specific miRNAs on different aspects of granulosa cell function , including steroidogenesis (Yao et al 2010, Xu et al 2011, Yin et al 2012, Dai et al 2013, proliferation (Yao et al 2010, Yan et al 2012, Dai et al 2013, survival (Carletti et al 2010, Yang et al 2012, terminal differentiation (Kitahara et al 2013), and cumulus expansion (Yao et al 2014). With a few exceptions (Carletti et al 2010, Kitahara et al 2013, most evidence on follicular roles of miRNAs has been obtained using cultured cells, particularly rodent cells, and in some cases actual changes in the expression of these miRNAs during follicle development have not been demonstrated.…”

Section: Introductionmentioning

confidence: 99%

Characterization of microRNAs differentially expressed during bovine follicle development

Sontakke¹,

Mohammed²,

McNeilly³

et al. 2014

Reproduction

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Several different miRNAs have been proposed to regulate ovarian follicle function; however, very limited information exists on the spatiotemporal patterns of miRNA expression during follicle development. The objective of this study was to identify, using microarray, miRNA profiles associated with growth and regression of dominant-size follicles in the bovine monovular ovary and to characterize their spatiotemporal distribution during development. The follicles were collected from abattoir ovaries and classified as small (4-8 mm) or large (12-17 mm); the latter were further classified as healthy or atretic based on estradiol and CYP19A1 levels. Six pools of small follicles and individual large healthy (nZ6) and large atretic (nZ5) follicles were analyzed using Exiqon's miRCURY LNA microRNA Array 6th gen, followed by qPCR validation. A total of 17 and 57 sequences were differentially expressed (greater than or equal to twofold; P!0.05) between large healthy and each of small and large atretic follicles respectively. Bovine miRNAs confirmed to be upregulated in large healthy follicles relative to small follicles (bta-miR-144, bta-miR-202, bta-miR-451, bta-miR-652, and bta-miR-873) were further characterized. Three of these miRNAs (bta-miR-144, bta-miR-202, and bta-miR-873) were also downregulated in large atretic follicles relative to large healthy follicles. Within the follicle, these miRNAs were predominantly expressed in mural granulosa cells. Further, body-wide screening revealed that bta-miR-202, but not other miRNAs, was expressed exclusively in the gonads. Finally, a total of 1359 predicted targets of the five miRNAs enriched in large healthy follicles were identified, which mapped to signaling pathways involved in follicular cell proliferation, steroidogenesis, prevention of premature luteinization, and oocyte maturation.

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“…Recently, other analyses using exome sequencing, in a family with nine affected women [75], and in a consanguineous Middle-Eastern family with five affected women [76,77], have suggested new candidate genes (Table 4). Moreover, recent studies relate the regulatory function of microRNAs (miRNAs) in oocyte maturation and folliculogenesis, and different miRNA expression profiles in the plasma of POI patients and fertile women have been detected when a miRNA microarray analysis was performed [78]. Similar results have been observed in an animal model in which a different profile for differentially expressed miRNAs has been observed between normal rats and 4-vinylcyclohexene diepoxide (VCD)-induced rat POF when miRNA microarrays were used [79].…”

Section: Novel Candidate Poi Genes Identified By Genome-wide Analysismentioning

confidence: 59%

Genetics of primary ovarian insufficiency: a review

Fortuño

Labarta

2014

J Assist Reprod Genet

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Primary ovarian insufficiency is one of the main causes of female infertility owing to an abnormal ovarian reserve. Its relevance has increased in more recent years due to the fact that age of motherhood is being delayed in developed countries, with the risk of having either primary ovarian insufficiency or less chances of pregnancy when women consider the option of having their first baby. Several exogenous factors can lead to this event, such us viral infections, metabolomic dysfunction, autoimmune diseases, and environmental or iatrogenic factors, although in most cases the mechanism that leads to the disorder is unknown. Genetic factors represent the most commonly identified cause and the impact of sex chromosome abnormalities (e.g., Turner syndrome or X structural abnormalities), autosomal and X-linked mutations on the genesis of primary ovarian insufficiency has also been well described. Yet in most cases, the genetic origin remains unknown and there are multiple candidate genes. This review aims to collect all the genetic abnormalities and genes associated with syndromic and non syndromic primary ovarian insufficiency that have been published in the literature to date using the candidate-gene approach and a genome-wide analysis.

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Differentially expressed plasma microRNAs in premature ovarian failure patients and the potential regulatory function of mir-23a in granulosa cell apoptosis

Cited by 151 publications

References 48 publications

Involvement of miRNAs in ovarian follicular and luteal development

Involvement of miRNAs in ovarian follicular and luteal development

Characterization of microRNAs differentially expressed during bovine follicle development

Genetics of primary ovarian insufficiency: a review

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