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Isolation of murine bone marrow derived mesenchymal stem cells using Twist2 Cre transgenic mice.

机译:使用Twist2 Cre转基因小鼠分离鼠骨髓来源的间充质干细胞。

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While human bone marrow derived mesenchymal stem cells (BMSCs) are of great interest for their potential therapeutic value, their murine equivalent remains an important basic research model that can provide critical insights into the biology of this progenitor cell population. Here we present a novel transgenic strategy that allowed for the selective identification and isolation of murine BMSCs at the early stages of stromal cell culture. This strategy involved crossing Twist2 -Cre mice with Cre reporter mice such as Z/EG or Ai9, which express EGFP or Tomato fluorescent protein, respectively, upon Cre mediated excision of a stop sequence. Using this approach, we identified an adherent fluorescent protein+cell population (T2C+) that is present during the earliest stages of colony formation and by day 5 of culture represents ~20% of the total cell population. Cell surface profiling by flow cytometry showed that T2C+cells are highly positive for SCA1 and CD29 and negative for CD45, CD117, TIE2, and TER119. Isolation of T2C+cells by FACS selected for a cell population with skeletal potential that can be directed to differentiate into osteoblasts, adipocytes, or chondrocytes. We also demonstrated in a calvarial bone defect model that T2C+cells retain a strong efficacy for osteogenic repair and can support a hematopoietic environment. Collectively, these studies provide evidence that the Twist2-Cre x Cre reporter breeding strategy can be used to positively identify and isolate multipotent murine BMSCs.
机译:尽管人骨髓来源的间充质干细胞(BMSC)具有潜在的治疗价值,但它们的鼠等效物仍然是重要的基础研究模型,可以为该祖细胞群的生物学提供重要的见识。在这里,我们提出了一种新颖的转基因策略,允许在基质细胞培养的早期阶段选择性鉴定和分离鼠骨髓间充质干细胞。该策略涉及在Cre介导的终止序列切除后,将Twist2-Cre小鼠与Cre报告基因小鼠(例如Z / EG或Ai9)杂交,它们分别表达EGFP或Tomato荧光蛋白。使用这种方法,我们确定了在集落形成的最早阶段存在的粘附荧光蛋白+细胞群(T2C +),到培养的第5天,约占总细胞群的20%。通过流式细胞仪进行细胞表面分析表明,T2C +细胞对SCA1和CD29高度阳性,而对CD45,CD117,TIE2和TER119呈阴性。通过FACS分离T2C +细胞,选择的是具有骨骼潜能的细胞群,可以定向分化为成骨细胞,脂肪细胞或软骨细胞。我们还在颅骨缺损模型中证明,T2C +细胞保留了强大的成骨修复功效并可以支持造血环境。这些研究共同提供了证据,证明Twist2-Cre x Cre报告基因育种策略可用于阳性鉴定和分离多能小鼠BMSC。

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