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髓过氧化物酶催化的零维碳量子点分解

Myeloperoxidase enzyme-catalyzed breakdown of zero-dimension carbon quantum dots.

作者信息

Singh Pooja, Singh Lalit Kumar

机构信息

Department of Biochemical Engineering, School of Chemical Engineering, Harcourt Butler Technical University, Kanpur, India.

出版信息

Front Med Technol. 2024 Nov 28;6:1493288. doi: 10.3389/fmedt.2024.1493288. eCollection 2024.

Abstract

Carbon quantum dots (CQDs) have shown considerable interest in multiple fields including bioimaging, biosensing, photocatalysis, ion sensing, heavy metal detection, and therapy due to highly tunable photoluminescence and good photostability. Apart from having optical properties CQDs offer several advantages such as low toxicity, environmental friendliness, affordability, and simple synthesis methods. Furthermore, by modifying their surface and functionality, it's possible to precisely control their physical and chemical characteristics. Nevertheless, the growing utilization of carbon-based nanomaterials (CNMs) requires thorough examination of their potential toxicity and long-term impacts on human health and biological systems. In this study, carbon quantum dots (CQDs) were synthesized via a microwave-assisted method using citric acid and urea as precursors, resulting in an average particle diameter of 10.73 nm. The CQDs were further characterized using SEM and FTIR analysis. The CQDs exhibited an excitation wavelength of 320 nm, displaying an emission peak at 430 nm. The enzymatic biodegradation of CQDs by human myeloperoxidase enzyme has been thoroughly investigated here. It is very crucial to understand how these carbon quantum dots interact with the innate immune system that plays a vital role in recognizing and clearing foreign particles. Human myeloperoxidase (MPO), a key enzyme highly expressed in neutrophil granulocytes during inflammatory responses, has been shown to facilitate the biodegradation of carbon quantum dots and various carbon-based nanomaterials through oxidative processes. As a member of the peroxidase family, MPO produces hypochlorous acid (HOCl) and a range of reactive intermediates to eliminate pathogens. Consequently, the study of the biodegradability of CQDs within biological systems is essential for accelerating technological advancements. Here, we have assessed breakdown of CQDs through an oxidative process facilitated by a myeloperoxidase (MPO)-based peroxide system. The human MPO enzyme acted as a catalyst for the CQD degradation, and the addition of hydrogen peroxide (HO) and sodium chloride (NaCl) was found to accelerate the reaction.

摘要

碳量子点(CQDs)由于其高度可调谐的光致发光和良好的光稳定性,在生物成像、生物传感、光催化、离子传感、重金属检测和治疗等多个领域引起了广泛关注。除了具有光学性质外,碳量子点还具有低毒性、环境友好、价格低廉和合成方法简单等优点。此外,通过修饰其表面和功能,可以精确控制其物理和化学特性。然而,碳基纳米材料(CNMs)的日益广泛应用需要对其潜在毒性以及对人类健康和生物系统的长期影响进行全面研究。在本研究中,以柠檬酸和尿素为前驱体,通过微波辅助法合成了碳量子点,其平均粒径为10.73 nm。通过扫描电子显微镜(SEM)和傅里叶变换红外光谱(FTIR)分析对碳量子点进行了进一步表征。碳量子点的激发波长为320 nm,在430 nm处有发射峰。本文对人髓过氧化物酶对碳量子点的酶促生物降解进行了深入研究。了解这些碳量子点如何与在识别和清除外来颗粒中起关键作用的先天免疫系统相互作用非常重要。人髓过氧化物酶(MPO)是炎症反应期间在中性粒细胞中高度表达的一种关键酶,已被证明可通过氧化过程促进碳量子点和各种碳基纳米材料的生物降解。作为过氧化物酶家族的一员,MPO产生次氯酸(HOCl)和一系列反应中间体以消除病原体。因此,研究碳量子点在生物系统中的生物降解性对于加速技术进步至关重要。在此,我们评估了通过基于髓过氧化物酶(MPO)的过氧化物系统促进的氧化过程对碳量子点的分解。人MPO酶作为碳量子点降解的催化剂,发现添加过氧化氢(HO)和氯化钠(NaCl)可加速反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2820/11634592/987e9708b196/fmedt-06-1493288-g001.jpg

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