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Isolation and characterization of lung resident mesenchymal stem cells capable of differentiating into alveolar epithelial type II cells.

机译:肺常驻间充质干细胞的分离与表征能够区分肺泡上皮型II细胞。

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摘要

Controversies and risks continue to be reported about exogenous mesenchymal stem cell-based therapies. In contrast with employing exogenous stem cells, making use of lung resident mesenchymal stem cells (LR-MSCs) could be advantageous. Our study sought to isolate the LR-MSCs and explore their potential to differentiate into alveolar epithelial type II cells (ATII cells). Total lung cells were first precultured, from which the Sca-1(+) CD45(-) CD31(-) population was purified using fluorescence activated cell sorting (FACS). By these methods, it would seem that the Sca-1(+) CD45(-) CD31(-) cells were LR-MSCs. Similar to bone marrow derived mesenchymal stem cells (BM-MSCs), these cells express Sca-1, CD29, CD90, CD44 and CD106, but not CD31 or CD45. They share the same gene expression file with the BM-MSCs and have a similar DNA content during long-term culturing. Furthermore, they could be serially passaged with all these properties being sustained. Above all, LR-MSCs could differentiate into ATII cells when co-cultured with ATII cells in a trans-well system. These findings demonstrated that the Sca-1(+) CD45(-) CD31(-) cells appear to be LR-MSCs that can differentiate into ATII cells. This approach may hold promise for their use in the treatment of lung disease.
机译:关于外源间充质干细胞的疗法,仍然报告了争议和风险。与采用外源干细胞的相反,利用肺部驻地间充质干细胞(LR-MSCs)可能是有利的。我们的研究寻求分离LR-MSCs并探讨它们分化为肺泡上皮II型细胞(ATII细胞)的可能性。首先使用肺细胞的总肺细胞,使用荧光活性细胞分选(FACS)纯化SCA-1(+)CD45( - )CD31( - )群。通过这些方法,似乎SCA-1(+)CD45( - )CD31( - )细胞是LR-MSCs。类似于骨髓衍生的间充质干细胞(BM-MSCs),这些细胞表达SCA-1,CD29,CD90,CD44和CD106,但不是CD31或CD45。它们与BM-MSCs共享相同的基因表达文件,并且在长期培养期间具有类似的DNA含量。此外,它们可以串联传代,所有这些属性都是持续的。最重要的是,当在反式井系统中与ATII细胞共培养时,LR-MSCs可以分化为ATII细胞。这些发现证明了SCA-1(+)CD45( - )CD31( - )CD31( - )细胞似乎是可以分化为ATII细胞的LR-MSC。这种方法可能会持希望他们在治疗肺病中的使用。

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