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肽导向的聚集诱导发光增强型金纳米簇的合成及其用于溶酶体和表达的 αβ 整合素受体的单光子和双光子成像。

Peptide-Directed Synthesis of Aggregation-Induced Emission Enhancement-Active Gold Nanoclusters for Single- and Two-Photon Imaging of Lysosome and Expressed αβ Integrin Receptors.

机构信息

Department of Chemistry, National Sun Yat-sen University, No. 70 Lienhai Rd., Kaohsiung 80424, Taiwan.

Department of Environmental Engineering, Da-Yeh University. No. 168, University Road, Dacun, Changhua 515006, Taiwan.

出版信息

Anal Chem. 2024 Jun 4;96(22):9007-9015. doi: 10.1021/acs.analchem.4c00321. Epub 2024 May 23.

Abstract

This study explores the synthesis and characterization of aggregation-induced emission enhancement (AIEE)-active gold nanoclusters (AuNCs), focusing on their near-infrared luminescence properties and potential applications in biological imaging. These AIEE-active AuNCs were synthesized via the NaBH-mediated reduction of HAuCl in the presence of peptides. We systematically investigated the influence of the peptide sequence on the optical features of the AuNCs, highlighting the role of glutamic acid in enhancing their quantum yield (QY). Among the synthesized peptide-stabilized AuNCs, EECEE-stabilized AuNCs exhibited the maximum QY and a pronounced AIEE effect at pH 5.0, making them suitable for the luminescence imaging of intracellular lysosomes. The AIEE characteristic of the EECEE-stabilized AuNCs was demonstrated through examinations using transmission electron microscopy, dynamic light scattering, zeta potential analysis, and single-particle imaging. The formation of the EECEE-stabilized AuNCs was confirmed by size-exclusion chromatography and mass spectrometry. Spectroscopic and electrochemical examinations uncover the formation process of EECEE-stabilized AuNCs, comprising EECEE-mediated reduction, NaBH-induced nucleation, complex aggregation, and subsequent cluster growth. Furthermore, we demonstrated the utility of these AuNCs as luminescent probes for intracellular lysosomal imaging, leveraging their pH-responsive AIEE behavior. Additionally, cyclic arginylglycylaspartic acid (RGD)-modified AIEE dots, derived from cyclic RGD-linked peptide-induced aggregation of EECEE-stabilized AuNCs, were developed for single- and two-photon luminescence imaging of αβ integrin receptor-positive cancer cells.

摘要

本研究探索了聚集诱导发射增强(AIEE)活性金纳米团簇(AuNCs)的合成与表征,重点关注其近红外发光特性及其在生物成像中的潜在应用。这些 AIEE 活性 AuNCs 是通过 NaBH 在肽存在下介导 HAuCl 的还原合成的。我们系统研究了肽序列对 AuNCs 光学特性的影响,强调了谷氨酸在提高其量子产率(QY)方面的作用。在所合成的肽稳定的 AuNCs 中,EECEE 稳定的 AuNCs 在 pH 5.0 时表现出最大的 QY 和明显的 AIEE 效应,使其适合用于细胞内溶酶体的荧光成像。通过透射电子显微镜、动态光散射、Zeta 电位分析和单粒子成像对 EECEE 稳定的 AuNCs 的 AIEE 特性进行了验证。通过尺寸排阻色谱和质谱对 EECEE 稳定的 AuNCs 的形成进行了确认。光谱和电化学研究揭示了 EECEE 稳定的 AuNCs 的形成过程,包括 EECEE 介导的还原、NaBH 诱导的成核、复杂聚集以及随后的团簇生长。此外,我们证明了这些 AuNCs 作为细胞内溶酶体成像的荧光探针的实用性,利用其对 pH 响应的 AIEE 行为。此外,还开发了基于循环精氨酸-甘氨酰-天冬氨酸(RGD)修饰的 AIEE 点,这些点源自循环 RGD 连接肽诱导 EECEE 稳定的 AuNCs 的聚集,用于 αβ 整合素受体阳性癌细胞的单光子和双光子荧光成像。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9c3f/11154667/6e099be82594/ac4c00321_0001.jpg

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