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The effects of bone growth factors and integrin-binding peptides on osteoblast function.

机译:骨生长因子和整联蛋白结合肽对成骨细胞功能的影响。

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摘要

Bone related diseases, like osteoporosis and osteoarthrosis, affect millions of people each year. The National Institutes of Health recommend basic studies focusing on increasing bone formation to better understand these diseases with the goal of developing treatments and preventative strategies. To that end, this investigation focused on the effects of engaging integrin and growth factor receptors to control clinically relevant osteoblast functions.; Adhesion strength of first and second passage osteoblasts to substrates modified with peptides that interact with integrin receptors in the presence and absence of serum was examined. In the absence of serum, all cells tested adhered more strongly to underlying substrates, and the strength of cellular adhesion was greater on modified surfaces than on plain glass surfaces. Second-passage osteoblastic cells generally adhered to substrates more strongly than first-passage osteoblastic cells.; Next, the effects of novel bioactive peptides (derived from basic fibroblast growth factor) on the proliferation, differentiation, and mineralization of osteoblasts were studied. Both bFGF peptides increased cellular differentiation. In contrast, intact bFGF inhibited osteoblast differentiation. The bound form of the bFGF peptide that most enhanced osteoblastic differentiation inhibited cell proliferation, while the intact bFGF protein increased osteoblast proliferation. The intact bFGF protein increased the amount of osteoblast produced mineral, while the peptides influenced the quality of the mineral produced. These novel bFGF peptides influence osteoblast functions in vitro in a manner distinct from that of the intact protein.; Finally, the combined effects of surface-bound integrin binding peptides and proteins and soluble bone growth factor media supplements were investigated. There was significant interaction between substrates modified with integrin-binding peptides and soluble bone growth factors with respect to osteoblast differentiation. There was also a significant interaction found between integrin and growth factor receptor engaging peptides with respect to the amount of mineral produced by osteoblasts.; Fundamental studies, such as this, increase the understanding of bone cell function on biomaterial substrates—knowledge useful in creating an optimal bone-implant interface and in the treatment of bone-related diseases such as osteoporosis.
机译:与骨相关的疾病,例如骨质疏松症和骨关节炎,每年影响数百万人。美国国立卫生研究院(National Institutes of Health)建议以增加骨骼形成为基础的基础研究,以更好地了解这些疾病,从而制定治疗和预防策略。为此,这项研究集中于使整联蛋白和生长因子受体参与控制临床相关成骨细胞功能的作用。在存在和不存在血清的情况下,检查了第一和第二代成骨细胞对用与整联蛋白受体相互作用的肽修饰的底物的粘附强度。在没有血清的情况下,所有测试的细胞都更牢固地粘附在下面的基底上,并且在改性表面上的细胞粘附强度要比在普通玻璃表面上大。通常,第二代成骨细胞比第一代成骨细胞更牢固地粘附在基质上。接下来,研究了新型生物活性肽(源自碱性成纤维细胞生长因子)对成骨细胞增殖,分化和矿化的影响。两种bFGF肽均可增加细胞分化。相反,完整的bFGF抑制成骨细胞分化。最增强成骨细胞分化的bFGF肽的结合形式抑制细胞增殖,而完整的bFGF蛋白增加成骨细胞增殖。完整的bFGF蛋白增加了成骨细胞产生矿物质的量,而肽段影响了所产生矿物质的质量。这些新颖的bFGF肽以不同于完整蛋白的方式在体外影响成骨细胞的功能。最后,研究了表面结合的整联蛋白结合肽和蛋白质以及可溶性骨生长因子培养基补充剂的联合作用。就成骨细胞分化而言,用整联蛋白结合肽修饰的底物与可溶性骨生长因子之间存在显着的相互作用。就成骨细胞产生的矿物质的量而言,在整联蛋白和生长因子受体结合肽之间也发现了显着的相互作用。诸如此类的基础研究提高了对生物材料基质上骨细胞功能的了解,该知识可用于创建最佳的骨-植入物界面并用于治疗与骨相关的疾病,例如骨质疏松症。

著录项

  • 作者

    Giliberti, Danielle C.;

  • 作者单位

    Tulane University.;

  • 授予单位 Tulane University.;
  • 学科 Engineering Biomedical.
  • 学位 Ph.D.
  • 年度 2003
  • 页码 125 p.
  • 总页数 125
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物医学工程;
  • 关键词

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