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Tunable geometry of bacterial inclusion bodies as substrate materials for tissue engineering

机译:细菌包涵体作为组织工程基质材料的可调几何形状

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摘要

A spectrum of materials for biomedical applications is produced in bacteria, and some of them, such as metals or polyhydroxyalkanoates, are straightforwardly obtained as particulate entities. We have explored the biofabrication process of bacterial inclusion bodies, particulate proteinaceous materials (ranging from 50 to 500nm in diameter) recently recognized as suitable for surface topographical modification and tissue engineering. Inclusion bodies have been widely described as spherical or pseudo-spherical particles with only minor morphological variability, mostly restricted to their size. Here we have identified a cellular gene in Escherichia coli (clpP) that controls the in vivo fabrication process of inclusion bodies. In the absence of the encoded protease, the dynamics of protein deposition is perturbed, resulting in unusual tear-shaped particles with enhanced surface-volume ratios. This fact modifies the ability of inclusion bodies to promote mammalian cell attachment and differentiation upon surface decoration. The implications of the genetic control of inclusion body geometry are discussed in the context of their biological fabrication and regarding the biomedical potential of these protein clusters in regenerative medicine.
机译:在细菌中产生了用于生物医学应用的多种材料,其中一些诸如金属或聚羟基链烷酸酯可直接作为颗粒实体获得。我们已经探索了细菌包涵体,最近被认为适用于表面形貌修饰和组织工程的颗粒状蛋白质材料(直径从50到500nm)的生物制造过程。包涵体已被广泛描述为球形或伪球形颗粒,仅具有很小的形态变异性,主要限于其大小。在这里,我们已经确定了大肠杆菌(clpP)中的一种细胞基因,该基因控制包涵体的体内制备过程。在不存在编码的蛋白酶的情况下,蛋白质沉积的动力学受到干扰,导致表面容积比增加的不寻常的泪状颗粒。这一事实改变了包涵体在表面装饰时促进哺乳动物细胞附着和分化的能力。包涵体几何结构的遗传控制的意义在它们的生物制造和有关这些蛋白质簇在再生医学中的生物医学潜力的背景下进行了讨论。

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