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皮肤间充质干细胞向施万细胞表型的分化:σ1 受体激活的影响。

The Differentiation of Skin Mesenchymal Stem Cells Towards a Schwann Cell Phenotype: Impact of Sigma-1 Receptor Activation.

机构信息

Faculty of Medicine, University of Latvia, Raina blvd. 19, Riga, LV-1586, Latvia.

Latvian Institute of Organic Synthesis, Laboratory of Pharmaceutical Pharmacology, Aizkraukles Street 21, Riga, Latvia.

出版信息

Mol Neurobiol. 2018 Apr;55(4):2840-2850. doi: 10.1007/s12035-017-0511-9. Epub 2017 Apr 28.

Abstract

Neural crest stem cells (NCSCs) are the source of mature Schwann cells in the peripheral nervous system (PNS). The NCSC population resides in the bulge of hair follicles and in the dermis. Recently, it was shown that 2-3% of the human dermis mesenchymal stem cell (MSC) population expresses the NCSC marker CD271, thus enabling the use of skin MSCs for studying Schwann cell differentiation in vitro. The aims of this study were to establish a protocol for human skin MSC differentiation towards Schwann cell-like cells (SC-lcs) and to analyse the expression of sigma-1 receptor (S1R) in SC-lcs. The impact of S1R ligands, namely the selective agonist PRE-084, the positive allosteric modulator E1R and the selective antagonist NE-100, on Schwann cell differentiation was assessed. The expression of the neuron-specific genes Tubulin-βIII and Integrin-6α, the Schwann cell-specific gene S100b, MBP and the NCSC-specific genes p75NTR, Sox10, Notch1, Integrin-4α, Ap2α and Pax6 was analysed in MSCs and SC-lcs by real-time RT-PCR. BDNF secretion was evaluated by ELISA. The effect of S1R ligands on SC-lc differentiation was measured using BDNF ELISA and MBP flow cytometry. After MSC differentiation, NCSC markers p75NTR and Integrin-4α were downregulated 3.5-fold and 2-fold, respectively. To the contrary, MBP and S100b were significantly upregulated in SC-lcs. S1R ligands showed a tendency to increase the secretion of BDNF by the SC-lc population. PRE-084 and E1R increased MBP expression in the SC-lc population, whereas 3 μM NE-100 inhibited MBP expression in SC-lcs. In conclusion, our data demonstrate that S1R plays an important role in skin MSC differentiation towards myelinating Schwann cells.

摘要

神经嵴干细胞 (NCSC) 是周围神经系统 (PNS) 中成熟雪旺细胞的来源。NCSC 群体存在于毛囊隆起处和真皮中。最近,研究表明,人类真皮间充质干细胞 (MSC) 群体中有 2-3%表达 NCSC 标志物 CD271,从而使皮肤 MSC 能够用于体外研究雪旺细胞分化。本研究的目的是建立一个人类皮肤 MSC 向雪旺细胞样细胞 (SC-lc) 分化的方案,并分析 SC-lc 中 sigma-1 受体 (S1R) 的表达。评估了 S1R 配体,即选择性激动剂 PRE-084、正变构调节剂 E1R 和选择性拮抗剂 NE-100,对 Schwann 细胞分化的影响。通过实时 RT-PCR 分析 MSC 和 SC-lc 中神经元特异性基因 Tubulin-βIII 和 Integrin-6α、雪旺细胞特异性基因 S100b、MBP 和 NCSC 特异性基因 p75NTR、Sox10、Notch1、Integrin-4α、Ap2α 和 Pax6 的表达。通过 ELISA 评估 BDNF 的分泌。通过 BDNF ELISA 和 MBP 流式细胞术测量 S1R 配体对 SC-lc 分化的影响。在 MSC 分化后,NCSC 标志物 p75NTR 和 Integrin-4α 分别下调 3.5 倍和 2 倍。相反,SC-lc 中 MBP 和 S100b 的表达显著上调。S1R 配体显示出增加 SC-lc 群体中 BDNF 分泌的趋势。PRE-084 和 E1R 增加了 SC-lc 群体中 MBP 的表达,而 3μM NE-100 抑制了 SC-lcs 中的 MBP 表达。总之,我们的数据表明,S1R 在皮肤 MSC 向髓鞘形成 Schwann 细胞分化中起重要作用。

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