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从卵巢颗粒细胞来源的表观遗传相关诱导多能干细胞高效分化生成类固醇生成细胞和类生殖细胞。

Efficient differentiation of steroidogenic and germ-like cells from epigenetically-related iPSCs derived from ovarian granulosa cells.

作者信息

Anchan Raymond, Gerami-Naini Behzad, Lindsey Jennifer S, Ho Joshua W K, Kiezun Adam, Lipskind Shane, Ng Nicholas, LiCausi Joseph A, Kim Chloe S, Brezina Paul, Tuschl Thomas, Maas Richard, Kearns William G, Williams Zev

机构信息

Division of Reproductive Endocrinology and Infertility, Department of Obstetrics, Gynecology and Reproductive Biology, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts, United States of America.

Division of Genetics, Department of Medicine, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts, United States of America.

出版信息

PLoS One. 2015 Mar 9;10(3):e0119275. doi: 10.1371/journal.pone.0119275. eCollection 2015.

Abstract

To explore restoration of ovarian function using epigenetically-related, induced pluripotent stem cells (iPSCs), we functionally evaluated the epigenetic memory of novel iPSC lines, derived from mouse and human ovarian granulosa cells (GCs) using c-Myc, Klf4, Sox2 and Oct4 retroviral vectors. The stem cell identity of the mouse and human GC-derived iPSCs (mGriPSCs, hGriPSCs) was verified by demonstrating embryonic stem cell (ESC) antigen expression using immunocytochemistry and RT-PCR analysis, as well as formation of embryoid bodies (EBs) and teratomas that are capable of differentiating into cells from all three germ layers. GriPSCs' gene expression profiles associate more closely with those of ESCs than of the originating GCs as demonstrated by genome-wide analysis of mRNA and microRNA. A comparative analysis of EBs generated from three different mouse cell lines (mGriPSCs; fibroblast-derived iPSC, mFiPSCs; G4 embryonic stem cells, G4 mESCs) revealed that differentiated mGriPSC-EBs synthesize 10-fold more estradiol (E2) than either differentiated FiPSC- or mESC-EBs under identical culture conditions. By contrast, mESC-EBs primarily synthesize progesterone (P4) and FiPSC-EBs produce neither E2 nor P4. Differentiated mGriPSC-EBs also express ovarian markers (AMHR, FSHR, Cyp19a1, ER and Inha) as well as markers of early gametogenesis (Mvh, Dazl, Gdf9, Boule and Zp1) more frequently than EBs of the other cell lines. These results provide evidence of preferential homotypic differentiation of mGriPSCs into ovarian cell types. Collectively, our data support the hypothesis that generating iPSCs from the desired tissue type may prove advantageous due to the iPSCs' epigenetic memory.

摘要

为了探索利用表观遗传相关的诱导多能干细胞(iPSC)恢复卵巢功能,我们使用c-Myc、Klf4、Sox2和Oct4逆转录病毒载体,对源自小鼠和人类卵巢颗粒细胞(GC)的新型iPSC系的表观遗传记忆进行了功能评估。通过免疫细胞化学和RT-PCR分析证明胚胎干细胞(ESC)抗原表达,以及形成能够分化为所有三个胚层细胞的胚状体(EB)和畸胎瘤,验证了小鼠和人类GC来源的iPSC(mGriPSC、hGriPSC)的干细胞特性。如通过mRNA和microRNA的全基因组分析所示,GriPSC的基因表达谱与ESC的基因表达谱比与原始GC的基因表达谱更密切相关。对由三种不同小鼠细胞系(mGriPSC;成纤维细胞来源的iPSC,mFiPSC;G4胚胎干细胞,G4 mESC)产生的EB进行的比较分析表明,在相同培养条件下,分化的mGriPSC-EB合成的雌二醇(E2)比分化的FiPSC-EB或mESC-EB多10倍。相比之下,mESC-EB主要合成孕酮(P4),而FiPSC-EB既不产生E2也不产生P4。分化的mGriPSC-EB也比其他细胞系的EB更频繁地表达卵巢标志物(AMHR、FSHR、Cyp19a1、ER和Inha)以及早期配子发生的标志物(Mvh、Dazl、Gdf9、Boule和Zp1)。这些结果提供了mGriPSC优先向卵巢细胞类型进行同型分化的证据。总体而言,我们的数据支持这样的假设,即由于iPSC的表观遗传记忆,从所需组织类型生成iPSC可能被证明是有利的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e336/4353623/0e496ef5bfd2/pone.0119275.g001.jpg

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