首页> 外文期刊>Investigative ophthalmology & visual science >RNA-Sequencing Gene Expression Profiling of Orbital Adipose-Derived Stem Cell Population Implicate HOX Genes and WNT Signaling Dysregulation in the Pathogenesis of Thyroid-Associated Orbitopathy
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RNA-Sequencing Gene Expression Profiling of Orbital Adipose-Derived Stem Cell Population Implicate HOX Genes and WNT Signaling Dysregulation in the Pathogenesis of Thyroid-Associated Orbitopathy

机译:甲状腺相关性眼病发病机制中的轨道脂肪干细胞群体RNA测序基因表达谱牵涉HOX基因和WNT信号失调。

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Purpose: The purpose of this study was to characterize the intrinsic cellular properties of orbital adipose-derived stem cells (OASC) from patients with thyroid-associated orbitopathy (TAO) and healthy controls. Methods: Orbital adipose tissue was collected from a total of nine patients: four controls and five patients with TAO. Isolated OASC were characterized with mesenchymal stem cella??specific markers. Orbital adipose-derived stem cells were differentiated into three lineages: chondrocytes, osteocytes, and adipocytes. Reverse transcription PCR of genes involved in the adipogenesis, chondrogenesis, and osteogenesis pathways were selected to assay the differentiation capacities. RNA sequencing analysis (RNA-seq) was performed and results were compared to assess for differences in gene expression between TAO and controls. Selected top-ranked results were confirmed by RT-PCR. Results: Orbital adipose-derived stem cells isolated from orbital fat expressed high levels of mesenchymal stem cell markers, but low levels of the pluripotent stem cell markers. Orbital adipose-derived stem cells isolated from TAO patients exhibited an increase in adipogenesis, and a decrease in chondrogenesis and osteogenesis. RNA-seq disclosed 54 differentially expressed genes. In TAO OASC, expression of early neural crest progenitor marker (WNT signaling, ZIC genes and MSX2) was lost. Meanwhile, ectopic expression of HOXB2 and HOXB3 was found in the OASC from TAO. Conclusion: Our results suggest that there are intrinsic genetic and cellular differences in the OASC populations derived from TAO patients. The upregulation in adipogenesis in OASC of TAO may be is consistent with the clinical phenotype. Downregulation of early neural crest markers and ectopic expression of HOXB2 and HOXB3 in TAO OASC demonstrate dysregulation of developmental and tissue patterning pathways.
机译:目的:本研究的目的是表征甲状腺相关性眼病(TAO)和健康对照患者的眼眶脂肪衍生干细胞(OASC)的固有细胞特性。方法:从9例患者中收集眼眶脂肪组织:4例对照组和5例TAO患者。用间充质干细胞特异标记物鉴定分离的OASC。眼眶脂肪干细胞分为三个谱系:软骨细胞,骨细胞和脂肪细胞。选择与脂肪形成,软骨形成和成骨途径有关的基因进行逆转录PCR,以测定其分化能力。进行了RNA测序分析(RNA-seq),并比较了结果以评估TAO和对照之间基因表达的差异。选定的排名最高的结果通过RT-PCR确认。结果:从眼眶脂肪中分离出的眼眶脂肪干细胞表达高水平的间充质干细胞标志物,但低水平的多能干细胞标志物。从TAO患者中分离出的眼眶脂肪干细胞表现出脂肪生成的增加,以及软骨生成和成骨的减少。 RNA-seq揭示了54个差异表达的基因。在TAO OASC中,早期神经c祖细胞标记(WNT信号,ZIC基因和MSX2)的表达丢失。同时,在TAO的OASC中发现了HOXB2和HOXB3的异位表达。结论:我们的结果表明,来自TAO患者的OASC群体存在固有的遗传和细胞差异。 TAO OASC中脂肪生成的上调可能与临床表型一致。在TAO OASC中早期神经c标记的下调以及HOXB2和HOXB3的异位表达表明发育和组织模式通路的失调。

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