Magnetic CuFe2O4 with intrinsic protease-like activity inhibited cancer cell proliferation and migration through mediating intracellular proteins

Q3 Biochemistry, Genetics and Molecular Biology Biomaterials and biosystems Pub Date : 2022-03-01 DOI:10.1016/j.bbiosy.2021.100038
Daomei Chen , Liang Jiang , Tao Lei , Guo Xiao , Yuanfeng Wang , Xiaoqiong Zuo , Bin Li , Lingli Li , Jiaqiang Wang
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引用次数: 3

Abstract

Protease has been widely used in biological and industrial fields. Developing efficient artificial enzyme mimics remains a major technical challenge due to the high stability of peptide bonds. Nanoenzymes with high stability, high activity and low cost, provided new opportunities to break through natural enzyme inherent limitations. However, compared with many nanomaterials with inherent peroxidase activity, the intrinsic mimic proteases properties of magnetic nanomaterials were seldom explored, let alone the interaction between magnetic nanomaterials and cellular proteins. Herein, we reported for the first time that magnetic CuFe2O4 possesses inherent protease activity to hydrolyze bovine serum albumin (BSA) and casein under physiological conditions, and the CuFe2O4 is more resistant to high temperature than the natural trypsin. It also exhibited significantly higher catalytic efficiency than other copper nanomaterials and can be recycled for many times. Protease participated in pathophysiological processes and all stages of tumor progression. Interesting, CuFe2O4 exhibited anti-proliferative effect on A549, SKOV3, HT-29, BABL-3T3 and HUVEC cells, as well as it was particularly sensitive against SKOV3 cells. CuFe2O4 was about 30 times more effective than conventional chemotherapy drugs oxaliplatin and artesunate against SKOV3 cells. In addition, CuFe2O4 also mediated the expression of intracellular proteins, such as MMP-2, MMP-9, F-actin, and NF-kB, which may be associated with global protein hydrolysis by CuFe2O4, leading to inhibition of cell migration. The merits of the high magnetic properties, good protease-mimic and antitumor activities make CuFe2O4 nanoparticles very prospective candidates for many applications such as proteomics and biotechnology.

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具有内在蛋白酶样活性的磁性CuFe2O4通过介导细胞内蛋白抑制癌细胞增殖和迁移
蛋白酶在生物和工业领域有着广泛的应用。由于肽键的高稳定性,开发高效的人工酶模拟物仍然是一个主要的技术挑战。纳米酶具有高稳定性、高活性和低成本的特点,为突破天然酶固有的局限性提供了新的机遇。然而,与许多具有固有过氧化物酶活性的纳米材料相比,磁性纳米材料的固有模拟蛋白酶性质很少被探索,更不用说磁性纳米材料与细胞蛋白质的相互作用了。本研究首次报道了磁性CuFe2O4在生理条件下具有水解牛血清白蛋白(BSA)和酪蛋白的内在蛋白酶活性,并且具有比天然胰蛋白酶更强的耐高温能力。与其他铜纳米材料相比,其催化效率显著提高,且可多次回收利用。蛋白酶参与了病理生理过程和肿瘤发展的各个阶段。有趣的是,CuFe2O4对A549、SKOV3、HT-29、BABL-3T3和HUVEC细胞均表现出抗增殖作用,其中对SKOV3细胞尤为敏感。CuFe2O4对SKOV3细胞的治疗效果是传统化疗药物奥沙利铂和青蒿琥酯的30倍左右。此外,CuFe2O4还介导了细胞内蛋白的表达,如MMP-2、MMP-9、F-actin和NF-kB,这些蛋白可能与CuFe2O4对全局蛋白的水解有关,从而抑制细胞迁移。CuFe2O4纳米粒子具有高磁性、良好的蛋白酶模拟和抗肿瘤活性等优点,在蛋白质组学和生物技术等领域具有广阔的应用前景。
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