利用茜草植物制造生物相容性氧化锌纳米粒子及其对人类乳腺癌细胞(MDA-MB-231)的体外抗菌、抗生物膜和细胞毒性作用。

IF 3.5 3区 生物学 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Bioprocess and Biosystems Engineering Pub Date : 2024-08-01 Epub Date: 2024-05-31 DOI:10.1007/s00449-024-03035-y
R Kavipriya, R Ramasubburayan
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引用次数: 0

摘要

乳腺癌和医疗器械中细菌生物膜的发病率不断上升,大大提高了全球死亡率和发病率,对合成药物提出了挑战。因此,绿色合成纳米材料已成为各种生物医学应用的多功能替代品,提供了新的治疗途径。本研究探讨了利用爵床科植物合成生物相容性氧化锌(ZnONPs)纳米颗粒及其抗菌、抗生物膜和细胞毒性特性。对 ZnONPs 的表征推断出,紫外可见光谱在 370 纳米处显示出尖锐的峰值。傅立叶变换红外光谱分析显示了活性官能团的存在,如醛、炔、环烯、硫酸盐、烷基芳基醚和 Zn-O 键。X 射线衍射分析结果证实了纳米粒子的结晶性质。扫描电子显微镜分析表明其形态为六角形,能量色散 X 射线分析证实了锌的含量。高分辨率透射电子显微镜分析显示 ZnONPs 呈六角形和棒状,尺寸为 5 纳米。Zeta 电位结果证实了纳米颗粒的稳定性。ZnONPs 可有效抑制革兰氏阳性(18-20 毫米)细菌病原体,抑菌值低于革兰氏阴性(12-18 毫米)细菌病原体,杀菌值高于革兰氏阳性细菌病原体。根据生物膜抑制特性推断,ZnONPs 对革兰氏阳性菌(38-94%)的抑制率高于对革兰氏阴性菌(27-86%)的抑制率。ZnONPs 对革兰氏阳性菌(179.26-203.95 μg/mL)产生 50%生物膜抑制作用的浓度低于革兰氏阴性菌(201.46-236.19 μg/mL)。显微镜观察推断,在 250 μg/mL 的浓度下,ZnONPs 能强烈破坏生物膜的形成,生物膜密度的降低和结构的改变就是证明。ZnONPs 对乳腺癌细胞的细胞毒性显示,细胞存活率的降低呈剂量依赖性,IC50 值为 19.4 µg/mL。在荧光显微镜下,AO/EB 染色显示了乳腺癌细胞的早期和晚期凋亡。溶血活性结果验证了 ZnONPs 的生物相容性。因此,绿色合成的 ZnONPs 的独特性质表明,它们有望成为有效的药物载体,用于癌症治疗和生物膜相关感染的靶向递送。
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Phytofabrication of biocompatible zinc oxide nanoparticle using Gymnema sylvestre and its potent in vitro antibacterial, antibiofilm, and cytotoxicity against human breast cancer cells (MDA-MB-231).

The increasing incidence of breast cancer and bacterial biofilm in medical devices significantly heightens global mortality and morbidity, challenging synthetic drugs. Consequently, greener-synthesized nanomaterials have emerged as a versatile alternative for various biomedical applications, offering new therapeutic avenues. This study explores the synthesis of biocompatible zinc oxide (ZnONPs) nanoparticles using Gymnema sylvestre and its antibacterial, antibiofilm, and cytotoxic properties. Characterization of ZnONPs inferred that UV-Vis spectra exhibited a sharp peak at 370 nm. Fourier transform infrared spectroscopical analysis revealed the presence of active functional groups such as aldehyde, alkyne, cyclic alkene, sulfate, alkyl aryl ether, and Zn-O bonds. X-ray diffraction analysis results confirmed the crystalline nature of the nanoparticle. Scanning electron microscope analysis evidenced hexagonal morphology, and energy-dispersive X-ray analysis confirmed zinc content. High-resolution transmission electron microscope analysis showed hexagonal and rod-shaped ZnONPs with a size of 5 nm. Zeta potential results affirmed the stability of nanoparticles. The ZnONPs effectively inhibited gram-positive (18-20 mm) than gram-negative (12-18 mm) bacterial pathogens with lower bacteriostatic and higher bactericidal values. Biofilm inhibitory property inferred ZnONPs were more effective against gram-positive (38-94%) than gram-negative bacteria (27-86%). The concentration of ZnONPs to exert 50% biofilm-inhibitory is lower against gram-positive bacteria (179.26-203.95 μg/mL) than gram-negative bacteria (201.46-236.19 μg/mL). Microscopic visualization inferred that at 250 μg/mL, ZnONPs strongly disrupted biofilm formation, as evidenced by decreased biofilm density and altered architecture. The cytotoxicity of ZnONPs against breast cancer cells showed a dose-dependent reduction in cell viability with an IC50 value of 19.4 µg/mL. AO/EB staining indicated early and late apoptotic cell death of breast cancer cells under fluorescence microscopy. The results of hemolytic activity validated the biocompatibility of the ZnONPs. Thus, the unique properties of the green-synthesized ZnONPs suggest their potential as effective drug carriers for targeted delivery in cancer therapy and the treatment of biofilm-related infections.

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来源期刊
Bioprocess and Biosystems Engineering
Bioprocess and Biosystems Engineering 工程技术-工程:化工
CiteScore
7.90
自引率
2.60%
发文量
147
审稿时长
2.6 months
期刊介绍: Bioprocess and Biosystems Engineering provides an international peer-reviewed forum to facilitate the discussion between engineering and biological science to find efficient solutions in the development and improvement of bioprocesses. The aim of the journal is to focus more attention on the multidisciplinary approaches for integrative bioprocess design. Of special interest are the rational manipulation of biosystems through metabolic engineering techniques to provide new biocatalysts as well as the model based design of bioprocesses (up-stream processing, bioreactor operation and downstream processing) that will lead to new and sustainable production processes. Contributions are targeted at new approaches for rational and evolutive design of cellular systems by taking into account the environment and constraints of technical production processes, integration of recombinant technology and process design, as well as new hybrid intersections such as bioinformatics and process systems engineering. Manuscripts concerning the design, simulation, experimental validation, control, and economic as well as ecological evaluation of novel processes using biosystems or parts thereof (e.g., enzymes, microorganisms, mammalian cells, plant cells, or tissue), their related products, or technical devices are also encouraged. The Editors will consider papers for publication based on novelty, their impact on biotechnological production and their contribution to the advancement of bioprocess and biosystems engineering science. Submission of papers dealing with routine aspects of bioprocess engineering (e.g., routine application of established methodologies, and description of established equipment) are discouraged.
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