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Neural stem cell neural differentiation in 3D extracellular matrix and endoplasmic reticulum stress microenvironment

机译:3D细胞外基质中神经干细胞神经分化和内质网胁迫微环境

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摘要

Successful neural stem cell (NSC) transplantation for treating neurological disorders is dependent on the effective differentiation of NSCs towards neurons especially in a pathological microenvironment. The purpose of this study was to evaluate NSC differentiation in an in vivo-like three-dimensional (3D) pathological microenvironment. We investigated use of a nano-scale electrospinning scaffold called nanomatrix incorporated into extracellular matrix proteins (ECM) for improvement of NSC differentiation capacity even under the endoplasmic reticulum (ER) stress condition, which generally occurred in various neurological disorders. ECM proteins used here included collagen, collagen + laminin, Matrigel, and Matrigel + laminin groups. NSCs cultured in Matrigel + laminin group were more potent for neural differentiation in comparison with other ECM groups. Addition of nanomatrix to the Matrigel + laminin group resulted in the enhancement of neuron marker TUJ1 expression and an increase in the length of neurite outgrowth even though the culture was treated with a toxic dose of tunicamycin, a commonly used ER stress inducer. Similarly, the downregulated expression levels of hippocampal granule neuron markers of PROX1 and FOXG1 in response to tunicamycin were reversed by addition of nanomatrix to the Matrigel + laminin group. The protective mechanism of nanomatrix combined with Matrigel and laminin was found to regulate unfolded protein response (UPR) signaling molecules, including Bip, ATF4 and CHOP. Taken together, these results implicated that combination of nanomatrix with Matrigel and laminin contributed to neural differentiation from NSCs even under an ER stress condition. It should be useful for researching the control of transplanted or endogenous NSC differentiation, especially in ER stress-related neurological diseases.
机译:用于治疗神经系统疾病的成功神经干细胞(NSC)移植依赖于NSCs对神经元的有效分化,尤其是在病理微环境中。本研究的目的是评估体内三维(3D)病理微环境中的NSC分化。我们研究了使用称为Nanomatrix的纳米级静电纺丝支架(ECM)中的纳米级电纺花支架,即使在内质网(ER)应激条件下,通常也发生在各种神经系统疾病中的NSC分化能力。这里使用的ECM蛋白包括胶原蛋白,胶原蛋白+层粘连蛋白,基质蛋白和基质蛋白+层蛋白组。与其他ECM组相比,在Matrigel + Laminin组中培养的NSCs更有效地进行神经分化。向Matrigel +层蛋白组添加Nanomatrix导致神经元标记TUJ1表达的增强,即使用毒性剂量的杂霉素处理培养物,常用的ER应激诱导剂也增加了神经突上几出的长度。类似地,通过加入纳米氨酰键对基质蛋白+层粘蛋白基团,反相持续蛋白霉素的海马颗粒神经元标记的下调表达水平。发现Nanomatrix与Matrigel和层粘蛋白联合的保护机制调节展开的蛋白质响应(UPR)信号分子,包括BIP,ATF4和Chec。总之,这些结果涉及与Matrigel和Laminin的Nanomatrix与Matrigel和Laminin的组合甚至在ER应力条件下导致来自NSC的神经分化。它应该有助于研究移植或内源性NSC分化的控制,尤其是在ER应激相关的神经疾病中。

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  • 来源
    《RSC Advances》 |2016年第41期|共11页
  • 作者单位

    Dalian Med Univ Acad Integrat Med Dalian 116044 Peoples R China;

    Nanjing Univ Chinese Med Sch Basic Med Sci Nanjing 210023 Jiangsu Peoples R China;

    Dalian Med Univ Acad Integrat Med Dalian 116044 Peoples R China;

    Dalian Med Univ Acad Integrat Med Dalian 116044 Peoples R China;

    Dalian Med Univ Acad Integrat Med Dalian 116044 Peoples R China;

    Dalian Med Univ Acad Integrat Med Dalian 116044 Peoples R China;

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  • 正文语种 eng
  • 中图分类 化学;
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