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NANOLAYERED FEATURES OF COLLAGEN-LIKE PEPTIDES

机译:胶原类肽的纳米制剂特征

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We have been investigating collagen-like model oligopeptides as molecular bases for complex ordered biomimetic materials. The collagen-like molecules incorporate aspects of native collagen sequence and secondary structure. Designed modifications to native primary and secondary structure have been incorporated to control the nanostructure and microstructure of the collagen-like materials produced. We find that the collagen-like molecules form a number of "lyotropic rod" liquid crystalline phases, which because of their strong temperature dependence in the liquid state can also be viewed as "solvent intercalated thermotropic" liquid crystals. The liquid crystalline phases formed by the molecules can be "captured" in the solid state by drying off solvent, resulting in solid nanopatterned (chemically and physically) thermally stable (to >100 deg C) materials. Designed sequences which stabilize smectic phases have allowed a variety of nanoscale multilayered biopolymeric materials to be developed. Preliminary investigations suggest that chemical patterns running perpendicular to the smectic layer plane can be functionalized and used to localize a variety of organic, inorganic, and organometallic moieties in very simple multilayered nanocomposites. The phase behavior of collagen-like oligopeptide materials is described, emphasizing the correlation between mesophase, molecular orientation, and chemical patterning at the microscale and nanoscale. In many cases, the textures observed for smectic and hexatic phase collagens are remarkably similar to the complex (and not fully understood) "helicoids" observed in biological collagen-based tissues. Comparisons between biological morphologies and collagen model liquid crystalline (and solidified materials) textures may help us understand the molecular features which impart order and function to the extracellular matrix and to collagen-based mineralized tissues. Initial studies have utilized synthetic collagen-like peptides while future work will also focus on similar sequences generated via genetic engineering methods.
机译:我们一直在调查胶原样模式寡肽为复杂有序的仿生材料的分子基础。胶原样分子结合天然胶原序列和二级结构的各方面。设计修改天然一级和二级结构已经被结合,以控制胶原样生产的材料的纳米结构和微观结构。我们发现,胶原蛋白样分子形成数字“溶致杆”液晶相,这是因为在液体状态下它们的强温度依赖性也可以被看作是“溶剂插层热致”液晶的。在固态下由分子形成的液晶相可以被“捕获”通过干燥除去溶剂,得到固体纳米图案(化学和物理)热稳定的(至> 100℃)的材料。其稳定的近晶相设计的序列已经允许多种纳米级多层生物聚合材料被开发。初步研究表明,运行垂直于近晶层平面化学模式可以被官能化并用于定位的各种有机,无机和有机金属部分在非常简单的多层纳米复合材料。的胶原样寡肽材料相行为描述,强调在微尺度和纳米级的中间相,分子取向和化学构图之间的相关性。在许多情况下,纹理观察到近晶型和hexatic相胶原是非常类似于在生物的基于胶原的组织中观察到的复合物(而不是完全理解)“螺旋面”。生物的形态和胶原模型液晶(和固化材料)纹理之间的比较可以帮助我们理解的分子特征赋予顺序和功能上与细胞外基质和基于胶原的矿化组织。最初的研究已利用合成的胶原蛋白样肽,而今后的工作也将集中在通过基因工程的方法产生的相似的序列。

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