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大规模平行测序技术鉴定新生期小鼠卵巢中的 microRNA 转录组

MicroRNA transcriptome in the newborn mouse ovaries determined by massive parallel sequencing.

机构信息

Department of Obstetrics, Gynecology and Reproductive Sciences, Magee-Womens Research Institute, University of Pittsburgh, Pittsburgh, PA, USA.

出版信息

Mol Hum Reprod. 2010 Jul;16(7):463-71. doi: 10.1093/molehr/gaq017. Epub 2010 Mar 9.

Abstract

Small non-coding RNAs, such as microRNAs (miRNAs), are involved in diverse biological processes including organ development and tissue differentiation. Global disruption of miRNA biogenesis in Dicer knockout mice disrupts early embryogenesis and primordial germ cell formation. However, the role of miRNAs in early folliculogenesis is poorly understood. In order to identify a full transcriptome set of small RNAs expressed in the newborn (NB) ovary, we extracted small RNA fraction from mouse NB ovary tissues and subjected it to massive parallel sequencing using the Genome Analyzer from Illumina. Massive sequencing produced 4 655 992 reads of 33 bp each representing a total of 154 Mbp of sequence data. The Pash alignment algorithm mapped 50.13% of the reads to the mouse genome. Sequence reads were clustered based on overlapping mapping coordinates and intersected with known miRNAs, small nucleolar RNAs (snoRNAs), piwi-interacting RNA (piRNA) clusters and repetitive genomic regions; 25.2% of the reads mapped to known miRNAs, 25.5% to genomic repeats, 3.5% to piRNAs and 0.18% to snoRNAs. Three hundred and ninety-eight known miRNA species were among the sequenced small RNAs, and 118 isomiR sequences that are not in the miRBase database. Let-7 family was the most abundantly expressed miRNA, and mmu-mir-672, mmu-mir-322, mmu-mir-503 and mmu-mir-465 families are the most abundant X-linked miRNA detected. X-linked mmu-mir-503, mmu-mir-672 and mmu-mir-465 family showed preferential expression in testes and ovaries. We also identified four novel miRNAs that are preferentially expressed in gonads. Gonadal selective miRNAs may play important roles in ovarian development, folliculogenesis and female fertility.

摘要

小非编码 RNA,如 microRNAs (miRNAs),参与多种生物过程,包括器官发育和组织分化。Dicer 敲除小鼠中 miRNA 生物发生的全局破坏会破坏早期胚胎发生和原始生殖细胞形成。然而,miRNAs 在早期卵泡发生中的作用知之甚少。为了鉴定在新生(NB)卵巢中表达的小 RNA 完整转录组集,我们从小鼠 NB 卵巢组织中提取小 RNA 馏分,并使用 Illumina 的 Genome Analyzer 进行大规模平行测序。大规模测序产生了 4655992 个 33bp 的读取,总共代表了 154 Mbp 的序列数据。Pash 比对算法将 50.13%的读取映射到了小鼠基因组。根据重叠映射坐标对序列读取进行聚类,并与已知的 miRNA、小核仁 RNA (snoRNA)、piwi 相互作用 RNA (piRNA) 簇和重复基因组区域进行交叉;25.2%的读取映射到已知的 miRNA,25.5%映射到基因组重复序列,3.5%映射到 piRNA,0.18%映射到 snoRNA。在测序的小 RNA 中,有 398 种已知的 miRNA 物种,有 118 种 miRNA 是不在 miRBase 数据库中的 miRNA 同型。Let-7 家族是表达最丰富的 miRNA,而 mmu-mir-672、mmu-mir-322、mmu-mir-503 和 mmu-mir-465 家族是检测到的最丰富的 X 连锁 miRNA。X 连锁的 mmu-mir-503、mmu-mir-672 和 mmu-mir-465 家族在睾丸和卵巢中表现出优先表达。我们还鉴定了四个在性腺中优先表达的新 miRNA。性腺特异性 miRNA 可能在卵巢发育、卵泡发生和女性生育力中发挥重要作用。

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