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Successful immortalization of mesenchymal progenitor cells derived from human placenta and the differentiation abilities of immortalized cells

机译:人胎盘间充质祖细胞的成功永生化和永生化细胞的分化能力

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We reported previously that mesenchymal progenitor cells derived from chorionic villi of the human placenta could differentiate into osteoblasts, adipocytes, and chondrocytes under proper induction conditions and that these cells should be useful for allogeneic regenerative medicine, including cartilage tissue engineering. However, similar to human mesenchymal stem cells (hMSCs), though these placental cells can be isolated easily, they are difficult to study in detail because of their limited life span in vitro. To overcome this problem, we attempted to prolong the life span of human placenta-derived mesenchymal cells (hPDMCs) by modifying hTERT and Bmi-1, and investigated whether these modified hPDMCs retained their differentiation capability and multipotency. Our results indicated that the combination of hTERT and Bmi-1 was highly efficient in prolonging the life span of hPDMCs with differentiation capability to osteogenic, adipogenic, and chondrogenic cells in vitro. Clonal cell lines with directional differentiation ability were established from the immortalized parental hPDMC/hTERT + Bmi-1. Interestingly, hPDMC/Bmi-1 showed extended proliferation after long-term growth arrest and telomerase was activated in the immortal hPDMC/Bmi-1 cells. However, the differentiation potential was lost in these cells. This study reports a method to extend the life span of hPDMCs with hTERT and Bmi-1 that should become a useful tool for the study of mesenchymal stem cells. (c) 2006 Elsevier Inc. All rights reserved.
机译:我们以前曾报道过,在适当的诱导条件下,源自人胎盘绒毛膜的间充质祖细胞可以分化为成骨细胞,脂肪细胞和软骨细胞,这些细胞应用于同种异体再生医学,包括软骨组织工程。然而,类似于人间充质干细胞(hMSCs),尽管这些胎盘细胞可以很容易地分离,但由于它们的体外寿命有限,因此难以进行详细研究。为了克服此问题,我们试图通过修饰hTERT和Bmi-1来延长人胎盘来源的间充质细胞(hPDMC)的寿命,并研究这些修饰的hPDMC是否保留了它们的分化能力和多能性。我们的结果表明,hTERT和Bmi-1的组合在延长hPDMC的寿命方面具有很高的效率,并且具有体外分化成骨细胞,成脂细胞和成软骨细胞的能力。从永生的亲代hPDMC / hTERT + Bmi-1建立具有方向分化能力的克隆细胞系。有趣的是,hPDMC / Bmi-1在长期生长停滞后显示出延长的增殖,并且端粒酶在永生的hPDMC / Bmi-1细胞中被激活。但是,这些细胞失去了分化潜能。这项研究报告了一种使用hTERT和Bmi-1延长hPDMC寿命的方法,该方法应成为研究间充质干细胞的有用工具。 (c)2006 Elsevier Inc.保留所有权利。

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