Differentially expressed genes and gene networks involved in pig ovarian follicular atresia

生物 卵泡闭锁 闭锁 卵泡期 卵泡 转录组 微阵列分析技术 基因 卵泡发生 男科 细胞生物学 基因表达 遗传学 解剖 胚胎发生 医学
作者
Elena Terenina,Stéphane Fabre,Agnès Bonnet,Danielle Monniaux,Christèle Robert-Granié,Magali SanCristobal,Julien Sarry,Florence Vignoles,Florence Gondret,Philippe Monget,Gwenola Tosser‐Klopp
出处
期刊:Physiological Genomics [American Physical Society]
卷期号:49 (2): 67-80 被引量:56
标识
DOI:10.1152/physiolgenomics.00069.2016
摘要

Ovarian folliculogenesis corresponds to the development of follicles leading to either ovulation or degeneration, this latter process being called atresia. Even if atresia involves apoptosis, its mechanism is not well understood. The objective of this study was to analyze global gene expression in pig granulosa cells of ovarian follicles during atresia. The transcriptome analysis was performed on a 9,216 cDNA microarray to identify gene networks and candidate genes involved in pig ovarian follicular atresia. We found 1,684 significantly regulated genes to be differentially regulated between small healthy follicles and small atretic follicles. Among them, 287 genes had a fold-change higher than two between the two follicle groups. Eleven genes ( DKK3, GADD45A, CAMTA2, CCDC80, DAPK2, ECSIT, MSMB, NUPR1, RUNX2, SAMD4A, and ZNF628) having a fold-change higher than five between groups could likely serve as markers of follicular atresia. Moreover, automatic confrontation of deregulated genes with literature data highlighted 93 genes as regulatory candidates of pig granulosa cell atresia. Among these genes known to be inhibitors of apoptosis, stimulators of apoptosis, or tumor suppressors INHBB, HNF4, CLU, different interleukins ( IL5, IL24), TNF-associated receptor ( TNFR1), and cytochrome-c oxidase ( COX) were suggested as playing an important role in porcine atresia. The present study also enlists key upstream regulators in follicle atresia based on our results and on a literature review. The novel gene candidates and gene networks identified in the current study lead to a better understanding of the molecular regulation of ovarian follicular atresia.
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