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体外培养的具有增强体内成骨能力的人成骨祖细胞的单细胞特征分析和代谢特征分析。

Single-cell characterization and metabolic profiling of in vitro cultured human skeletal progenitors with enhanced in vivo bone forming capacity.

机构信息

Tissue Engineering Laboratory, Skeletal Biology and Engineering Research Center, KU Leuven, Leuven, Belgium.

Prometheus, Division of Skeletal Tissue Engineering, KU Leuven, Leuven, Belgium.

出版信息

Stem Cells Transl Med. 2020 Mar;9(3):389-402. doi: 10.1002/sctm.19-0151. Epub 2019 Nov 18.

Abstract

Cell populations and their interplay provide the basis of a cell-based regenerative construct. Serum-free preconditioning can overcome the less predictable behavior of serum expanded progenitor cells, but the underlying mechanism and how this is reflected in vivo remains unknown. Herein, the cellular and molecular changes associated with a cellular phenotype shift induced by serum-free preconditioning of human periosteum-derived cells were investigated. Following BMP-2 stimulation, preconditioned cells displayed enhanced in vivo bone forming capacity, associated with an adapted cellular metabolism together with an elevated expression of BMPR2. Single-cell RNA sequencing confirmed the activation of pathways and transcriptional regulators involved in bone development and fracture healing, providing support for the augmentation of specified skeletal progenitor cell populations. The reported findings illustrate the importance of appropriate in vitro conditions for the in vivo outcome. In addition, BMPR2 represents a promising biomarker for the enrichment of skeletal progenitor cells for in vivo bone regeneration.

摘要

细胞群体及其相互作用为基于细胞的再生构建提供了基础。无血清预处理可以克服血清扩展祖细胞不太可预测的行为,但潜在的机制以及这在体内是如何反映的仍然未知。在此,研究了无血清预处理诱导人骨膜来源细胞表型转变相关的细胞和分子变化。在 BMP-2 刺激后,预处理细胞显示出增强的体内成骨能力,与适应的细胞代谢以及 BMPR2 的高表达相关。单细胞 RNA 测序证实了参与骨发育和骨折愈合的途径和转录调节剂的激活,为特定骨骼祖细胞群体的扩增提供了支持。所报道的发现说明了适当的体外条件对于体内结果的重要性。此外,BMPR2 是用于体内骨再生的骨骼祖细胞富集的有前途的生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/44ef/7031650/788846ef7862/SCT3-9-389-g001.jpg

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