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基质金属蛋白酶-13 可控降解自组装 β-发夹肽水凝胶

Controlled biodegradation of self-assembling β-hairpin peptide hydrogels by proteolysis with matrix metalloproteinase-13.

机构信息

National Cancer Institute, Center for Cancer Research, Frederick, MD 21701, USA.

出版信息

Biomaterials. 2011 Sep;32(27):6471-7. doi: 10.1016/j.biomaterials.2011.05.052. Epub 2011 Jun 16.

Abstract

Controlled biodegradation specific to matrix metalloproteinase-13 was incorporated into the design of self-assembling β-hairpin peptide hydrogels. Degrading Peptides (DP peptides) are a series of five peptides that have varying proteolytic susceptibilities toward MMP-13. These peptides undergo environmentally triggered folding and self-assembly under physiologically relevant conditions (150 mm NaCl, pH 7.6) to form self-supporting hydrogels. In the presence of enzyme, gels prepared from distinct peptides are degraded at rates that differ according to the primary sequence of the single peptide comprising the gel. Material degradation was monitored by oscillatory shear rheology over the course of 14 days, where overall degradation of the gels vary from 5% to 70%. Degradation products were analyzed by HPLC and identified by electrospray-ionization mass spectrometry. This data shows that proteolysis of the parent peptides constituting each gel occurs at the intended sequence location. DP hydrogels show specificity to MMP-13 and are only minimally cleaved by matrix metalloproteinase-3 (MMP-3), another common enzyme present during tissue injury. In vitro migration assays performed with SW1353 cells show that migration rates through each gel differs according to peptide sequence, which is consistent with the proteolysis studies using exogenous MMP-13.

摘要

基质金属蛋白酶-13 特异性控制的生物降解被纳入自组装β发夹肽水凝胶的设计中。降解肽(DP 肽)是一系列对 MMP-13 具有不同蛋白水解敏感性的五种肽。这些肽在生理相关条件下(150 mM NaCl,pH7.6)经历环境触发的折叠和自组装,形成自支撑水凝胶。在酶的存在下,由不同肽制备的凝胶以根据构成凝胶的单个肽的一级序列而不同的速率降解。通过在 14 天的过程中进行振荡剪切流变学监测材料降解,凝胶的总降解率从 5%到 70%不等。通过 HPLC 分析和电喷雾电离质谱鉴定降解产物。该数据表明,构成每个凝胶的母体肽的蛋白水解发生在预期的序列位置。DP 水凝胶对 MMP-13 具有特异性,并且仅被基质金属蛋白酶-3(MMP-3)轻微切割,MMP-3 是组织损伤过程中另一种常见的酶。用 SW1353 细胞进行的体外迁移实验表明,通过每种凝胶的迁移率根据肽序列而不同,这与使用外源性 MMP-13 的蛋白水解研究一致。

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