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NFATC1、NADSYN1 和 JAK3 基因在单层培养扩增的马软骨细胞中的差异表达和甲基化模式。

Differential expression and methylation patterns of NFATC1, NADSYN1 and JAK3 gene in equine chondrocytes expanded in monolayer culture.

机构信息

Department of Animal Molecular Biology, National Research Institute of Animal Production, Krakowska 1 Street, 32-083 Balice, Poland.

Department of Animal Molecular Biology, National Research Institute of Animal Production, Krakowska 1 Street, 32-083 Balice, Poland.

出版信息

Res Vet Sci. 2022 Dec 20;152:48-52. doi: 10.1016/j.rvsc.2022.07.017. Epub 2022 Jul 26.

Abstract

Ex vivo expansion of chondrocytes in monolayer (ML) culture for therapeutic purposes is burdened with difficulties related to the loss of cartilaginous phenotype. Epigenetic mechanisms responsible for regulation of gene expression are believed to underlie chondrocyte dedifferentiation. We have inspected the relevance of DNA methylation alterations for passage-related differential expression of NFATC1 gene involved in hard connective tissue turnover and development, NADSYN1 influencing redox metabolism, and JAK3 - an important driver of inflammation. We have assessed relative amount of transcript abundance and performed DNA bisulfite sequencing of upstream located elements. It seems that anabolic-like effects of chondrogenic differentiation were observed in form of NFATC1 and NADSYN1 upregulation in chondrocytes at the earlier stages of passaging whereas JAK3 upregulation at the 11th passage was the sign of chondrocytes dedifferentiation. Summarizing the inversely correlated DNA methylation and expression patterns in NFATC1 and JAK3 locus might be relevant for cellular dedifferentiation during chondrocyte expansion in monolayer. Obtained results are supportive for further studies on the role of encoded proteins in regenerative biology of articular cartilage using in vitro expanded chondrocytes.

摘要

为了治疗目的,在单层(ML)培养物中扩增软骨细胞会遇到与软骨表型丧失相关的困难。负责调节基因表达的表观遗传机制被认为是软骨细胞去分化的基础。我们已经检查了 DNA 甲基化改变与 NFATC1 基因表达相关的相关性,该基因参与硬结缔组织的转化和发育、影响氧化还原代谢的 NADSYN1 以及炎症的重要驱动因素 JAK3。我们评估了转录物丰度的相对量,并对位于上游的元件进行了 DNA 亚硫酸氢盐测序。似乎在传代的早期阶段,软骨细胞中 NFATC1 和 NADSYN1 的上调表现出合成代谢样作用,而在第 11 代时 JAK3 的上调则是软骨细胞去分化的标志。NFATC1 和 JAK3 基因座中 DNA 甲基化和表达模式的反向相关可能与单层软骨细胞扩增过程中的细胞去分化有关。这些结果支持使用体外扩增的软骨细胞进一步研究编码蛋白在关节软骨再生生物学中的作用。

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