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Characterization of Cellular and Molecular Heterogeneity of Bone Marrow Stromal Cells

机译:骨髓基质细胞细胞和分子异质性的表征

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摘要

Human bone marrow-derived stromal stem cells (hBMSC) exhibit multiple functions, including differentiation into skeletal cells (progenitor function), hematopoiesis support, and immune regulation (nonprogenitor function). We have previously demonstrated the presence of morphological and functional heterogeneity of hBMSC cultures. In the present study, we characterized in detail two hTERT-BMSC clonal cell populations termed here CL1 and CL2 that represent an opposing phenotype with respect to morphology, markers expression: alkaline phosphatase (ALP) and CD146, and ex vivo differentiation potential. CL1 differentiated readily to osteoblasts, adipocytes, and chondrocytes as shown by expression of lineage specific genes and proteins. Whole genome transcriptome profiling of CL1 versus CL2 revealed enrichment in CL1 of bone-, mineralization-, and skeletal muscle-related genes, for example, ALP, POSTN, IGFBP5 BMP4, and CXCL12. On the other hand, CL2 transcriptome was enriched in immune modulatory genes, for example, CD14, CD99, NOTCH3, CXCL6, CFB, and CFI. Furthermore, gene expression microarray analysis of osteoblast differentiated CL1 versus CL2 showed significant upregulation in CL1 of bone development and osteoblast differentiation genes which included several homeobox genes: TBX15, HOXA2 and HOXA10, and IGF1, FGFR3, BMP6, MCAM, ITGA10, IGFBP5, and ALP. siRNA-based downregulation of the ALP gene in CL1 impaired osteoblastic and adipocytic differentiation. Our studies demonstrate the existence of molecular and functional heterogeneity in cultured hBMSC. ALP can be employed to identify osteoblastic and adipocytic progenitor cells in the heterogeneous hBMSC cultures.
机译:人骨髓来源的基质干细胞(hBMSC)具有多种功能,包括分化为骨骼细胞(祖细胞功能),造血支持和免疫调节(非祖细胞功能)。我们以前已经证明了hBMSC培养物的形态和功能异质性的存在。在本研究中,我们详细表征了两个hTERT-BMSC克隆细胞群(此处称为CL1和CL2),它们在形态,标记物表达方面代表相反的表型:碱性磷酸酶(ALP)和CD146,以及离体分化潜能。如谱系特异性基因和蛋白的表达所示,CL1易于分化为成骨细胞,脂肪细胞和软骨细胞。 CL1和CL2的全基因组转录组分析显示,与骨骼,矿化和骨骼肌相关的基因(例如ALP,POSTN,IGFBP5 BMP4和CXCL12)的CL1富集。另一方面,CL2转录组富含免疫调节基因,例如CD14,CD99,NOTCH3,CXCL6,CFB和CFI。此外,成骨细胞分化的CL1和CL2的基因表达微阵列分析显示,骨骼发育和成骨细胞分化基因的CL1明显上调,其中包括几个同源盒基因:TBX15,HOXA2和HOXA10,IGF1,FGFR3,BMP6,MCAM,ITGA10,IGFBP5和ALP。基于siRNA的CL1中ALP基因的下调会损害成骨细胞和脂肪细胞的分化。我们的研究表明在培养的hBMSC中存在分子和功能异质性。 ALP可用于鉴定异质hBMSC培养物中的成骨细胞和脂肪细胞祖细胞。

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