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Molecular basis for RGD-containing peptides supporting adhesion and self-renewal of human pluripotent stem cells on synthetic surface

机译:用于含RGD的肽的分子基础支持合成表面对人多能干细胞的粘附和自我更新

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摘要

The ability to obtain a large number of human pluripotent stem cells (hPSCs) under chemically defined conditions plays a key role in clinical application of hPSCs. Chemically defined, economical and effective synthetic peptide displaying surfaces should be the optimal choice for clinical applications involving hPSCs. However, synthetic peptide displaying surfaces are worse than Matrigel surface in supporting cell adhesion and self-renewal. Moreover, the correlations between peptide amino acid sequences and the ability of peptides to support cell survival has never been investigated in hPSCs. In this study, we focused on the Arg-Gly-Asp (RGD) sequence and integrin receptors, which constitute the major recognition system for cell adhesion. Several new ROD containing peptides were designed by altering the amino acids surrounding the RGD sequence. We investigated the ability of these peptides to sustain hPSC survival, and identified the Ac-KGGPQVIRGDTYRAY sequence, which was capable of supporting cell reprogramming, long-term self-renewal and lineage differentiation. In addition, this report demonstrates that the introduction of mutations in the amino acids surrounding the RGD sequence is a good strategy to design peptides that display excellent adhesion properties and promote hPSC self renewal. Our results will help improve the current understanding of the mechanisms by which RGD-containing peptides exhibit different abilities in sustaining hPSC culture, and will promote clinical application of both peptide displaying surfaces and hPSCs.
机译:在化学定义的条件下获得大量人多能干细胞(HPSC)的能力在HPSCS的临床应用中起着关键作用。化学定义的,经济和有效的合成肽显示表面应该是涉及HPSCS的临床应用的最佳选择。然而,合成肽显示表面比基质胶表面更差,用于支撑细胞粘附和自我更新。此外,从未在HPSC中研究了肽氨基酸序列与肽以支持细胞存活的能力之间的相关性。在本研究中,我们专注于arg-gly-Asp(RGD)序列和整联受体,其构成细胞粘附的主要识别系统。通过改变RGD序列周围的氨基酸来设计几种含有的肽的肽。我们研究了这些肽维持HPSC存活的能力,并确定了能够支持细胞重编程,长期自我更新和谱系分化的AC-KGGPQvirgdryray序列。此外,本报告表明,在RGD序列周围的氨基酸中引入突变是设计肽的良好策略,其设计出优异的粘附性能并促进HPSC自我更新。我们的结果将有助于改善目前对含RGD肽在维持HPSC培养方面表现出不同能力的机制的理解,并将促进肽显示表面和HPSC的临床应用。

著录项

  • 来源
    《Colloids and Surfaces, B. Biointerfaces》 |2018年第2018期|共10页
  • 作者单位

    Lanzhou Univ Sch &

    Hosp Stomatol Lanzhou 730000 Peoples R China;

    Natl Univ Singapore Suzhou Res Inst Suzhou Ind Pk Suzhou 215123 Peoples R China;

    Lanzhou Univ Sch &

    Hosp Stomatol Lanzhou 730000 Peoples R China;

    Lanzhou Univ Sch Pharm Lanzhou 730000 Peoples R China;

    Shenzhen Cell Inspire Biotechnol CO Ltd Tao Huayuan Sci &

    Technol Innovat Pk Shenzhen 518102 Peoples R China;

    Shenzhen Cell Inspire Biotechnol CO Ltd Tao Huayuan Sci &

    Technol Innovat Pk Shenzhen 518102 Peoples R China;

    Peking Univ Acad Adv Interdisciplinary Studies Ctr Biomed Mat &

    Tissue Engn Beijing 100871 Peoples R China;

    Peking Univ Acad Adv Interdisciplinary Studies Ctr Biomed Mat &

    Tissue Engn Beijing 100871 Peoples R China;

    Peking Univ Sch &

    Hosp Stomatol Natl Engn Lab Digital &

    Mat Technol Stomatol Cent Lab Beijing Key Lab Digital Stomatol Beijing 100081 Peoples R China;

    Lanzhou Univ Sch Pharm Lanzhou 730000 Peoples R China;

    Natl Univ Singapore Suzhou Res Inst Suzhou Ind Pk Suzhou 215123 Peoples R China;

    Peking Univ Acad Adv Interdisciplinary Studies Ctr Biomed Mat &

    Tissue Engn Beijing 100871 Peoples R China;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 胶体化学(分散体系的物理化学);
  • 关键词

    Human pluripotent stem cells; Peptides; RGD sequences; Synthetic surface;

    机译:人多能干细胞;肽;RGD序列;合成表面;

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