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Design of peptides with targeted apatite and human bone marrow stromal cell adhesion for bone tissue engineering.

机译:具有靶向磷灰石和人骨髓基质细胞粘附的肽的设计,用于骨组织工程。

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摘要

The restoration and repair of orofacial and large bone defects resulting from extreme trauma, disease, or genetic inheritance is a clinical challenge in need of new solutions, as current grafting techniques can result in donor site morbidity, graft rejection, and/or inadequate bone formation and quality. Because bone is a complex organ, its hierarchical structure may only be restored in such defects if a temporary material guides tissue formation. Bone tissue engineering explores combinations of materials, biological signals, and cell sources to achieve guided tissue formation with structure-function properties matching those of native tissue.;By using nature's building blocks, or amino acids, as a design platform to synthesize multi-dimensional biomolecules in the form of peptides, biological function can be influenced. The idea is to provide specificity to induce a desired biological activity. In addition, coating a material with biomimetic bone-like mineral can provide a surface morphology and composition similar to the native hydroxyapatite in bone. While bone-like mineral can increase bone growth in vivo, the tissue formed is not uniform or spatially controlled, suggesting the need for better-designed scaffolding to spatiotemporally influence bone tissue development.;No studies have investigated the potential impact biomolecule-laden bone-like mineral has on influencing cell behavior. The work presented in this thesis is first to design dual-functioning peptides to increase in vitro cell attachment on bone-like mineral. Using a combinatorial phage library, computational modeling, and biological assays, specific peptide sequences that preferentially adsorb to bone-like mineral and attach to clonally derived human bone marrow stromal cells (hBMSCs) were identified. When combined, these sequences formed a dual-functioning peptide that exhibited an increased ability to attach hBMSCs compared to previous peptide designs. Additionally, a bioreactor was designed to coat three-dimensional porous scaffolds with uniform, continuous bone-like mineral, addressing a need for improved biomimetic coating fabrication techniques. The presented strategies can influence guided bone growth and advance the current methodologies in bone engineering. This work provides a new paradigm for peptide development linking organics to inorganics, not only for bone tissue engineered constructs, but also for any system requiring temporary or guided adhesion.
机译:由于极端的外伤,疾病或遗传遗传所造成的口腔和大骨缺损的修复和修复是需要新解决方案的临床挑战,因为当前的移植技术可能会导致供体部位发病,移植物排斥和/或骨形成不足和质量。因为骨骼是一个复杂的器官,所以只有在临时材料引导组织形成的情况下,才可以在这种缺陷中恢复骨骼的层次结构。骨组织工程探索材料,生物信号和细胞来源的组合,以实现具有与天然组织相匹配的结构功能特性的引导组织形成;通过利用自然界的构建基块或氨基酸作为设计平台来合成多维生物分子以肽的形式存在,生物学功能会受到影响。该想法是提供诱导所需生物学活性的特异性。另外,用仿生的骨样矿物质涂覆材料可以提供类似于骨中天然羟基磷灰石的表面形态和组成。虽然类骨矿物质可以增加体内骨骼的生长,但形成的组织并不均匀或不受空间控制,这表明需要设计更好的支架来时空影响骨骼组织的发育。就像矿物质对细胞行为有影响。本文提出的工作是首先设计双功能肽,以增加体外细胞在骨样矿物质上的附着。使用组合噬菌体库,计算模型和生物学分析,鉴定了优先吸附至骨样矿物质并附着于克隆来源的人骨髓基质细胞(hBMSC)的特定肽序列。当结合时,这些序列形成了双功能肽,与先前的肽设计相比,该双功能肽表现出增加的结合hBMSC的能力。此外,设计了一种生物反应器,用均匀,连续的骨样矿物质涂覆三维多孔支架,从而满足了对改进的仿生物涂层制造技术的需求。提出的策略可以影响引导的骨生长,并推进当前骨工程学中的方法。这项工作不仅为骨组织工程构造物,而且为任何需要暂时性或引导性粘附的系统提供了一种将有机物与无机物连接起来的肽开发新范式。

著录项

  • 作者

    Segvich, Sharon Janell.;

  • 作者单位

    University of Michigan.;

  • 授予单位 University of Michigan.;
  • 学科 Engineering Biomedical.
  • 学位 Ph.D.
  • 年度 2008
  • 页码 197 p.
  • 总页数 197
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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