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通过工程化TiC MXene纳米片表面实现高稳定性和多模态抗癌治疗

Engineering the Surface of TiC MXene Nanosheets for High Stability and Multimodal Anticancer Therapy.

作者信息

Korupalli Chiranjeevi, You Kai-Long, Getachew Girum, Rasal Akash S, Dirersa Worku Batu, Zakki Fahmi Mochamad, Chang Jia-Yaw

机构信息

Department of Chemical Engineering, National Taiwan University of Science and Technology, Taipei 10607, Taiwan.

Department of Chemistry, Universitas Airlangga, Surabaya 60115, Indonesia.

出版信息

Pharmaceutics. 2022 Jan 27;14(2):304. doi: 10.3390/pharmaceutics14020304.

Abstract

The surface of TiC MXene nanosheets (TC NSs) was first modified with the antioxidants sodium ascorbate (SA) and dopamine (DA) (DSTC NS) to improve their stability in oxidative and hydration environments and thereby improve their bioapplications. This novel approach not only improved MXene stability by arresting oxidation but also increased the available functional groups for further functionalization with various biomolecules. The DSTC NSs were then sequentially conjugated with enzyme glucose oxidase (GOx) and photosensitizer Ce6 to render the obtained CGDSTC NSs with glucose starvation and photodynamic therapeutic properties and thus attain high efficiency in killing cancer cells through the cooperative effect. The as-synthesized CGDSTC NSs demonstrated tremendous photothermal effect with conversion efficiency of 45.1% and photodynamic (ROS generation) properties upon irradiation with 808 and 671 nm lasers. Furthermore, it was observed that the enzymatic activity of CGDSTC NSs increased upon laser irradiation due to enhanced solution temperature. During in vitro studies, the CGDSTC NSs exhibited cytocompatability to HePG2 and HeLa cells under nonstimulus conditions. However, they elicited more than 90% cell-killing efficiency in the presence of glucose and laser irradiation via the cooperative effect between starvation therapy and phototherapy. These results indicate that CGDSTC NSs could be used as potential therapeutic agents to eradicate cancers with no or few adverse effects. This surface modification approach is also simple and facile to adopt in MXene-based research.

摘要

首先用抗氧化剂抗坏血酸钠(SA)和多巴胺(DA)对TiC MXene纳米片(TC NSs)的表面进行修饰(DSTC NS),以提高其在氧化和水合环境中的稳定性,从而改善其生物应用。这种新方法不仅通过阻止氧化提高了MXene的稳定性,还增加了可用于与各种生物分子进一步功能化的官能团。然后将DSTC NSs依次与酶葡萄糖氧化酶(GOx)和光敏剂Ce6共轭,使所得的CGDSTC NSs具有葡萄糖饥饿和光动力治疗特性,从而通过协同作用高效杀死癌细胞。合成的CGDSTC NSs在808和671 nm激光照射下表现出巨大的光热效应,转换效率为45.1%,并具有光动力(产生活性氧)特性。此外,观察到由于溶液温度升高,激光照射后CGDSTC NSs的酶活性增加。在体外研究中,CGDSTC NSs在非刺激条件下对HePG2和HeLa细胞表现出细胞相容性。然而,在葡萄糖存在和激光照射下,通过饥饿疗法和光疗之间的协同作用,它们引发了超过90%的细胞杀伤效率。这些结果表明,CGDSTC NSs可作为潜在的治疗剂来根除癌症,且副作用很少或没有。这种表面修饰方法在基于MXene的研究中也简单易行。

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