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Study of the Adsorption Behavior of Recombinant Human Growth Hormone onto Peptide-Coated Hydrophobic Surfaces

机译:重组人生长激素在多肽包覆的疏水表面上的吸附行为研究

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摘要

Binding of a protein to a molecule involves specific interaction domains that require substrate specificity. Isolating such interaction domains and incorporating them into large polypeptide chains can provide protein-binding epitopes on the surface. These exposed epitopes can recognize their partners on the protein surface and might bind with significant strength as evidenced by a low dissociation constant. This concept allows the opportunity to design relatively small molecules to mimic the macromolecules by exhibiting the same affinity for these binding sites. Thus, developing a peptide-coated polymer surface may offer a viable system for controlled delivery of protein drugs.;The current research explores the adsorption of recombinant human growth hormone (r-hGH) to a peptide-coated colloidal system. The hypothesis is that adsorption of r-hGH to hydrophobic surfaces that have been coated with ligands that demonstrate specific binding to r-hGH will allow high loading of r-hGH without significant denaturation of the bound r-hGH. A novel rhGH-binding peptide named growth hormone binding peptide (GHBpep) allowed binding characteristics similar to that of the soluble form of growth hormone receptor known as growth hormone binding protein (GHBP). This small polypeptide encompasses most of the residues in the hot spot of GHBP that provides most of the binding energy with human growth hormone (HGH).;The project involves preparation and characterization of peptide-modified PLGA nanoparticles by covalently attaching GHBpep to the surface of these nanoparticles using various types of crosslinkers, monovalent and multivalent crosslinkers. Dynamic Light Scattering (DLS) and Laser Doppler Electrophoresis (LDE) techniques were used to characterize the size and charge of nanoparticles, respectively. The extent of surface coverage by the immobilized peptide was estimated using fluorescence spectroscopy. After characterization of the conjugated GHBpep, the interaction of r-hGH with the conjugates was studied under various microenvironmental conditions using traditional methods, such as equilibrium microdialysis and ultrafiltration. The adsorption process was found to be affected by changes in the ionic strength and the pH of the medium. A high degree of association was found at a low concentration of ions, especially at a pH of 5.3 (at the isoelectric point) and at pH of 7.2 when multivalent linkers were utilized.
机译:蛋白质与分子的结合涉及需要底物特异性的特定相互作用域。分离这样的相互作用结构域并将其掺入大的多肽链中可以在表面上提供蛋白质结合表位。这些暴露的表位可以识别它们在蛋白质表面上的伴侣,并可能以显着的强度结合,如低解离常数所证明。通过对这些结合位点表现出相同的亲和力,该概念使人们有机会设计相对较小的分子来模拟大分子。因此,开发包被肽的聚合物表面可能为控制蛋白质药物的递送提供一个可行的系统。;当前的研究探索了重组人生长激素(r-hGH)对包被肽的胶体系统的吸附。假设是,r-hGH吸附到疏水性表面上已被疏水性表面吸附,该疏水性表面已表现出与r-hGH的特异性结合,这将允许r-hGH的高负载而结合的r-hGH不会明显变性。一种名为生长激素结合肽(GHBpep)的新型rhGH结合肽具有与已知为生长激素结合蛋白(GHBP)的可溶形式的生长激素受体相似的结合特性。这种小多肽涵盖了GHBP热点中的大多数残基,可提供与人生长激素(HGH)的大部分结合能。;该项目涉及通过将GHBpep共价附于GHBpep表面上来制备和修饰肽修饰的PLGA纳米颗粒这些纳米粒子使用各种类型的交联剂,单价和多价交联剂。动态光散射(DLS)和激光多普勒电泳(LDE)技术分别用于表征纳米粒子的大小和电荷。使用荧光光谱法估计固定的肽的表面覆盖程度。在表征缀合的GHBpep后,使用传统方法,例如平衡微透析和超滤,在各种微环境条件下研究了r-hGH与缀合物的相互作用。发现吸附过程受离子强度和介质pH值变化的影响。在使用低价离子时,尤其是在使用多价连接子的pH值为5.3(等电点)和pH值为7.2时,发现高度缔合。

著录项

  • 作者

    Namazi, Nader Ibrahim.;

  • 作者单位

    University of the Sciences in Philadelphia.;

  • 授予单位 University of the Sciences in Philadelphia.;
  • 学科 Pharmaceutical sciences.
  • 学位 Ph.D.
  • 年度 2018
  • 页码 136 p.
  • 总页数 136
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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