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首页> 外文期刊>Stem cells and development >Human amniotic fluid-derived mesenchymal cells from fetuses with a neural tube defect do not deposit collagen type i protein after TGF-β1 stimulation in vitro
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Human amniotic fluid-derived mesenchymal cells from fetuses with a neural tube defect do not deposit collagen type i protein after TGF-β1 stimulation in vitro

机译:TGF-β1体外刺激后,来自人羊水的具有神经管缺陷的胎儿间充质细胞未沉积i型胶原蛋白

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摘要

In spina bifida, the neural tube fails to close during the embryonic period. Exposure of the neural tube to the amniotic fluid during pregnancy causes additional neural damage. Intrauterine tissue engineering using a biomaterial seeded with stem cells might prevent this additional damage. For this purpose, autologous cells from the amniotic fluid are an attractive source. To close the defect, it is important that these cells deposit an extracellular matrix. However, it is not known if amniotic fluid mesenchymal cells (AFMCs) from a fetus with a neural tube defect (NTD) share the same characteristics as AFMCs from a healthy fetus. We found that cells derived from fetuses with a NTD, in contrast to healthy human amniotic fluid cells, did not deposit collagen type I. Furthermore, the NTD cells showed, compared with both healthy amniotic fluid cells and fetal fibroblasts, much lower mRNA expression levels of genes that are involved in collagen biosynthesis [procollagen C-endopeptidase enhancer proteins (PCOLCE), PCOLCE2, ADAM metallopeptidase with thrombospondin type 1 motif, 2 (ADAMTS2), ADAMTS14]. This indicates that NTD-AFMCs have different characteristics compared with healthy AFMCs and might not be suitable for fetal therapy to close the defect in spina bifida patients.
机译:在脊柱裂中,神经管在胚胎期无法关闭。怀孕期间神经管暴露于羊水会引起额外的神经损伤。使用植入干细胞的生物材料进行宫内组织工程可能会防止这种额外的损害。为此,来自羊水的自体细胞是有吸引力的来源。为了弥补缺陷,重要的是这些细胞应沉积细胞外基质。但是,尚不清楚来自具有神经管缺陷(NTD)的胎儿的羊水间充质细胞(AFMC)是否具有与来自健康胎儿的AFMC相同的特征。我们发现,与健康人羊水细胞相比,具有NTD的胎儿细胞未沉积I型胶原。此外,与健康羊水细胞和胎儿成纤维细胞相比,NTD细胞显示出低得多的mRNA表达水平胶原生物合成中涉及的基因[原胶原C-肽酶增强蛋白(PCOLCE),PCOLCE2,具有血小板反应蛋白1型基序的ADAM金属肽酶,2(ADAMTS2),ADAMTS14]。这表明NTD-AFMC与健康的AFMC具有不同的特征,可能不适合用于闭合脊柱裂患者的胎儿治疗。

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