探索异烟肼负载铜基金属有机框架作为有效杀死结核分枝杆菌的新策略的抗菌潜力。

IF 6.1 3区 医学 Q1 MATERIALS SCIENCE, BIOMATERIALS
Pawan Kumar, Ananyaashree Behera, Pranav Tiwari, Sibi Karthik, Mainak Biswas, Avinash Sonawane and Shaikh M. Mobin
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引用次数: 0

摘要

结核病仍然是最具传染性的病原体之一,人类死亡率和发病率最高。结核分枝杆菌(Mtb)感染期间的生物膜形成负责细菌的生长、交流,最重要的是,增加对抗生素的耐药性/耐受性,导致细菌更高的持久性。因此,生物膜生长目前被认为是慢性病的一个关键毒力因素。金属有机框架(MOFs)最近成为一种高效的系统,可以提高现有抗生素的治疗效果并减少不良反应。在这方面,我们使用溶剂热方法合成了Cu-MOF(IITI-3)。通过各种光谱技术对IITI-3进行了很好的表征。在此,IITI-3首先用异烟肼(INH)包封形成INH@IITI-3在1小时内负载10wt%。INH@IITI-3通过PXRD、TGA、FTIR和BET表面积分析对其进行了良好的表征。此外INH@IITI-3分别在pH 5.8和7.4下进行以模拟小肠和血液pH。结果表明,药物释放遵循一级动力学。此外INH@IITI-3显示出显著的细菌杀伤作用并改变了细菌的结构形态。此外INH@IITI-3在处理时能够抑制分枝杆菌生物膜的形成,并且对小鼠RAW264.7巨噬细胞表现出较小的细胞毒性。因此,这项工作为INH@IITI-3在结核分枝杆菌的生物膜感染中,并进一步有助于结核病治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Exploring the antimicrobial potential of isoniazid loaded Cu-based metal–organic frameworks as a novel strategy for effective killing of Mycobacterium tuberculosis†

Exploring the antimicrobial potential of isoniazid loaded Cu-based metal–organic frameworks as a novel strategy for effective killing of Mycobacterium tuberculosis†

Tuberculosis (TB) remains one of the most infectious pathogens with the highest human mortality and morbidity. Biofilm formation during Mycobacterium tuberculosis (Mtb) infection is responsible for bacterial growth, communication, and, most essentially, increased resistance/tolerance to antibiotics leading to higher bacterial persistence. Thus, biofilm growth is presently considered a key virulence factor in the case of chronic disease. Metal–Organic Frameworks (MOFs) have recently emerged as a highly efficient system to improve existing antibiotics' therapeutic efficacy and reduce adverse effects. In this regard, we have synthesized Cu-MOF (IITI-3) using a solvothermal approach. IITI-3 was well characterized by various spectroscopic techniques. Herein, IITI-3 was first encapsulated with isoniazid (INH) to form INH@IITI-3 with 10 wt% loading within 1 hour. INH@IITI-3 was well characterized by PXRD, TGA, FTIR, and BET surface area analysis. Furthermore, the drug release kinetics studies of INH@IITI-3 have been performed at pH 5.8 and 7.4 to mimic the small intestine and blood pH, respectively. The results show that drug release follows first-order kinetics. Furthermore, the antimycobacterial activity of INH@IITI-3 demonstrated significant bacterial killing and altered the structural morphology of the bacteria. Moreover, INH@IITI-3 was able to inhibit the mycobacterial biofilm formation upon treatment and showed less cytotoxicity toward the murine RAW264.7 macrophages. Thus, this work significantly opens up new possibilities for the applications of INH@IITI-3 in biofilm infections in Mtb and further contributes to TB therapeutics.

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来源期刊
Journal of Materials Chemistry B
Journal of Materials Chemistry B MATERIALS SCIENCE, BIOMATERIALS-
CiteScore
11.50
自引率
4.30%
发文量
866
期刊介绍: Journal of Materials Chemistry A, B & C cover high quality studies across all fields of materials chemistry. The journals focus on those theoretical or experimental studies that report new understanding, applications, properties and synthesis of materials. Journal of Materials Chemistry A, B & C are separated by the intended application of the material studied. Broadly, applications in energy and sustainability are of interest to Journal of Materials Chemistry A, applications in biology and medicine are of interest to Journal of Materials Chemistry B, and applications in optical, magnetic and electronic devices are of interest to Journal of Materials Chemistry C.Journal of Materials Chemistry B is a Transformative Journal and Plan S compliant. Example topic areas within the scope of Journal of Materials Chemistry B are listed below. This list is neither exhaustive nor exclusive: Antifouling coatings Biocompatible materials Bioelectronics Bioimaging Biomimetics Biomineralisation Bionics Biosensors Diagnostics Drug delivery Gene delivery Immunobiology Nanomedicine Regenerative medicine & Tissue engineering Scaffolds Soft robotics Stem cells Therapeutic devices
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