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低氧环境下人脐带华通氏胶间充质基质细胞的增殖和差异基因表达分析。

Increased proliferation and analysis of differential gene expression in human Wharton's jelly-derived mesenchymal stromal cells under hypoxia.

机构信息

Stempeutics Research Pvt Ltd, Manipal Hospital, Bangalore, India.

出版信息

Int J Biol Sci. 2010 Sep 9;6(5):499-512. doi: 10.7150/ijbs.6.499.

Abstract

Multipotent mesenchymal stromal cells (MSCs) from Wharton's jelly (WJ) of umbilical cord bear higher proliferation rate and self-renewal capacity than adult tissue-derived MSCs and are a primitive stromal cell population. Stem cell niche or physiological microenvironment plays a crucial role in maintenance of stem cell properties and oxygen concentration is an important component of the stem cell niche. Low oxygen tension or hypoxia is prevalent in the microenvironment of embryonic stem cells and many adult stem cells at early stages of development. Again, in vivo, MSCs are known to home specifically to hypoxic events following tissue injuries. Here we examined the effect of hypoxia on proliferation and in vitro differentiation potential of WJ-MSCs. Under hypoxia, WJ-MSCs exhibited improved proliferative potential while maintaining multi-lineage differentiation potential and surface marker expression. Hypoxic WJ-MSCs expressed higher mRNA levels of hypoxia inducible factors, notch receptors and notch downstream gene HES1. Gene expression profile of WJ-MSCs exposed to hypoxia and normoxia was compared and we identified a differential gene expression pattern where several stem cells markers and early mesodermal/endothelial genes such as DESMIN, CD34, ACTC were upregulated under hypoxia, suggesting that in vitro culturing of WJ-MSCs under hypoxic conditions leads to adoption of a mesodermal/endothelial fate. Thus, we demonstrate for the first time the effect of hypoxia on gene expression and growth kinetics of WJ-MSCs. Finally, although WJ-MSCs do not induce teratomas, under stressful and long-term culture conditions, MSCs can occasionally undergo transformation. Though there were no chromosomal abnormalities, certain transformation markers were upregulated in a few of the samples of WJ-MSCs under hypoxia.

摘要

脐带华通氏胶来源的多能间充质基质细胞(MSCs)比成人组织来源的 MSCs 具有更高的增殖率和自我更新能力,是原始的基质细胞群体。干细胞龛或生理微环境在维持干细胞特性方面起着至关重要的作用,而氧浓度是干细胞龛的重要组成部分。低氧张力或缺氧普遍存在于胚胎干细胞和许多处于发育早期的成体干细胞的微环境中。同样,在体内,已知间充质干细胞专门归巢到组织损伤后的缺氧事件。在这里,我们研究了缺氧对 WJ-MSCs 增殖和体外分化潜能的影响。在缺氧条件下,WJ-MSCs 表现出改善的增殖潜能,同时保持多能分化潜能和表面标志物表达。缺氧 WJ-MSCs 表达更高水平的缺氧诱导因子、Notch 受体和 Notch 下游基因 HES1 的 mRNA。比较了在缺氧和常氧条件下暴露的 WJ-MSCs 的基因表达谱,我们发现了一个差异基因表达模式,其中几个干细胞标志物和早期中胚层/内皮基因,如 DESMIN、CD34、ACTC,在缺氧下上调,表明在缺氧条件下体外培养 WJ-MSCs 会导致中胚层/内皮命运的形成。因此,我们首次证明了缺氧对 WJ-MSCs 基因表达和生长动力学的影响。最后,尽管 WJ-MSCs 不会诱导畸胎瘤,但在应激和长期培养条件下,间充质干细胞偶尔会发生转化。虽然没有染色体异常,但在缺氧下的少数 WJ-MSCs 样本中,某些转化标志物上调。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f214/2945278/8e6ba1810c4a/ijbsv06p0499g01.jpg

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