Enzyme-Assisted Metabolically Coated Bimetallic Thalassiosira pseudonana Nanosilica as a Surface-Enhanced Raman Scattering Substrate for Specific Screening of Prostate Cancer Individuals

材料科学 拉曼散射 截锥 表面等离子共振 等离子体子 纳米技术 肌氨酸 拉曼光谱 纳米颗粒 光电子学 化学 硅藻 光学 物理 生物 植物 氨基酸 甘氨酸 生物化学
作者
Muhammad Ibrar,Tao Wang,Yanqing Luo,Yajun Ruan,Shiqinq Zhu,Yue Wu,Shuangfei Li,Ming Ying,Xuewei Yang
出处
期刊:ACS applied nano materials [American Chemical Society]
卷期号:6 (20): 18790-18802 被引量:2
标识
DOI:10.1021/acsanm.3c02876
摘要

Multicomponent heteronanostructures offering catalytic and optical properties have applications across various fields. Photonic crystals (diatom frustules) coated with Au and copper chalcogenide domains represent a unique nanosystem that integrates multiple plasmon resonances from guided-mode resonance, conduction electrons, and valence holes in a single nanoscale system. In this work, we fabricate an enzyme-assisted photonic crystal-enhanced plasmonic nanosystem using a live diatom (Thalassiosira pseudonana) for surface-enhanced Raman scattering (SERS) quantification of sarcosine, an early stage prostate cancer (PCa) biomarker. The biosynthesized heteronanostructure was constructed by coating bimetallic nanoparticles (Au/CuX) on the diatom frustule via a two-stage cultivation process. A silaffin peptide-tagged sarcosine oxidase (SoX) was designed for specific substrate recognition and oriented conjunction. The components were coupled into a single entity (SoX-immobilized Au/CuX-coated frustule, BioNPS) to overcome the interenzyme distance and analyte trade-offs between mass transport. The sarcosine detection by BioNPS outperforms suspended bimetallic nanoparticles and single NP-coated diatom frustules. The improvement is attributed to the coupling of photonic frustule guided-mode resonance to the localized surface plasmonic resonance of bimetallic NPs via both electromagnetic and CT mechanisms. The cascade reaction in close proximity greatly enhances the catalytic efficiency by 5.47-fold compared to the solution-phase assay. The biochem nanosystem precisely detects tiny sarcosine concentration changes in the urine samples of PCa patients and healthy individuals. As a proof of concept, the in vivo fabrication of photonic/plasmonic heterostructures with tunable properties holds great promise for noninvasive biomarker screening.
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