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人免疫球蛋白G与无毒、近红外发射水性硅量子点胶束之间的纳米生物相互作用。

Nano-bio interaction between human immunoglobulin G and nontoxic, near-infrared emitting water-borne silicon quantum dot micelles.

作者信息

Chinnathambi Shanmugavel, Shirahata Naoto, Kumar Mahima, Karthikeyan Subramani, Abe Katsuhiko, Thangavel Vaijayanthi, Pandian Ganesh N

机构信息

Institute for Integrated Cell-Material Sciences (WPI-iCeMS), Institute for Advanced Study, Kyoto University Kyoto 606-8501 Japan

International Center for Young Scientists, National Institute for Materials Science (NIMS) 1-2-1 Sengen Tsukuba 305-0047 Ibaraki Japan.

出版信息

RSC Adv. 2023 Feb 20;13(9):6051-6064. doi: 10.1039/d3ra00552f. eCollection 2023 Feb 14.

Abstract

In recent years, the field of nanomaterials has exponentially expanded with versatile biological applications. However, one of the roadblocks to their clinical translation is the critical knowledge gap about how the nanomaterials interact with the biological microenvironment (nano-bio interactions). When nanomaterials are used as drug carriers or contrast agents for biological imaging, the nano-bio interaction-mediated protein conformational changes and misfolding could lead to disease-related molecular alterations and/or cell death. Here, we studied the conformation changes of human immunoglobulin G (IgG) upon interaction with silicon quantum dots functionalized with 1-decene, Pluronic-F127 (SiQD-De/F127 micelles) using UV-visible, fluorescence steady state and excited state kinetics, circular dichroism, and molecular modeling. Decene monolayer terminated SiQDs are accumulated inside the Pluronic F127 shells to form SiQD-De/F127 micelles and were shown to bind strongly with IgG. In addition, biological evaluation studies in cell lines (HeLa, Fibroblast) and medaka fish (eggs and larvae) showed enhanced uptake and minimal cytotoxicity. Our results substantiate that engineered QDs obviating the protein conformational changes could have adept bioefficacy.

摘要

近年来,纳米材料领域凭借其多样的生物学应用呈指数级扩展。然而,其临床转化的障碍之一是关于纳米材料如何与生物微环境相互作用(纳米-生物相互作用)的关键知识空白。当纳米材料用作生物成像的药物载体或造影剂时,纳米-生物相互作用介导的蛋白质构象变化和错误折叠可能导致与疾病相关的分子改变和/或细胞死亡。在此,我们使用紫外-可见光谱、荧光稳态和激发态动力学、圆二色光谱以及分子建模,研究了人免疫球蛋白G(IgG)与用1-癸烯、普朗尼克-F127(SiQD-De/F127胶束)功能化的硅量子点相互作用时的构象变化。癸烯单层封端的硅量子点聚集在普朗尼克F127壳层内形成SiQD-De/F127胶束,并显示出与IgG强烈结合。此外,在细胞系(HeLa、成纤维细胞)和青鳉鱼(卵和幼虫)中的生物学评估研究表明摄取增强且细胞毒性最小。我们的结果证实,避免蛋白质构象变化的工程化量子点可能具有良好的生物功效。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4056/9939978/71dee47970e3/d3ra00552f-f1.jpg

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