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Use of proteolytic sequences with different cleavage kinetics as a way to generate hydrogels with preprogrammed cell-infiltration patterns imparted over their given 3D spatial structure

机译:用不同的裂解动力学的使用蛋白水解序列作为在给定的3D空间结构上赋予预编程的细胞渗透图案的水凝胶的一种方法

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摘要

Control over biodegradation processes is crucial to generate advanced functional structures with a more interactive and efficient role for biomedical applications. Herein, a simple, high-throughput approach is developed based on a three-dimensional (3D)-structured system that allows a preprogramed spatial-temporal control over cell infiltration and biodegradation. The 3D-structured system is based on elastin-like recombinamers (ELRs) characterized by differences in the kinetics of their peptide cleavage and consists of a three-layer hydrogel disk comprising an internal layer containing a rapidly degrading component, with the external layers containing a slow-degrading ELR. This structure is intended to invert the conventional pattern of cell infiltration, which goes from the outside to the inside of the implant, to allow an anti-natural process in which infiltration takes place first in the internal layer and later progresses to the outer layers. Time-course in vivo studies proved this hypothesis, i.e. that it is possible to drive the infiltration of cells over time in a given 3D-structured implant in a controlled and predesigned way that is able to overcome the natural tendency of conventional cell infiltration. The results obtained herein open up the possibility of applying this concept to more complex systems with multiple biological functions.
机译:对生物降解过程的控制对于为生物医学应用具有更具交互和有效的作用来生成高级功能结构至关重要。这里,基于三维(3D)结构的结构进行简单,高通量的方法,其允许预编程的空间 - 时间控制细胞渗透和生物降解。 3D结构系统基于弹性蛋白的重组蛋白(ELR),其特征在于它们的肽切割的动力学的差异,并且由三层水凝胶盘组成,包括含有快速降解组分的内层,其中含有a的外层缓慢降级的elr。该结构旨在倒置传统的细胞渗透模式,该细胞渗透的图案从外部到植入物的内部,以允许抗自然过程,其中首先在内层中进行渗透,并且后来进入外层。体内研究中的时间课程证明了这一假设,即,在给定的3D结构植入物中可以以控制和预先的方式在给定的3D结构植入物中驱动细胞的渗透,这能够克服常规细胞浸润的自然趋势。本文获得的结果开辟了将该概念应用于具有多种生物学功能的更复杂的系统的可能性。

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