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TiO2 纳米生物图案化揭示了细胞-基质黏附形成的最佳配体呈现。

TiO Nano-Biopatterning Reveals Optimal Ligand Presentation for Cell-Matrix Adhesion Formation.

机构信息

Mechanobiology Institute, National University of Singapore (NUS), Singapore, 117411, Singapore.

Tech4Health Institute and Department of Radiology, NYU Langone Health, New York, NY, 10016, USA.

出版信息

Adv Mater. 2024 May;36(21):e2309284. doi: 10.1002/adma.202309284. Epub 2024 Feb 19.

DOI:10.1002/adma.202309284
PMID:38340044
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11126362/
Abstract

Nanoscale organization of transmembrane receptors is critical for cellular functions, enabled by the nanoscale engineering of bioligand presentation. Previously, a spatial threshold of ≤60 nm for integrin binding ligands in cell-matrix adhesion is demonstrated using monoliganded gold nanoparticles. However, the ligand geometric arrangement is limited to hexagonal arrays of monoligands, while plasmonic quenching limits further investigation by fluorescence-based high-resolution imaging. Here, these limitations are overcome with dielectric TiO nanopatterns, eliminating fluorescence quenching, thus enabling super-resolution fluorescence microscopy on nanopatterns. By dual-color super-resolution imaging, high precision and consistency among nanopatterns, bioligands, and integrin nanoclusters are observed, validating the high quality and integrity of both nanopattern functionalization and passivation. By screening TiO nanodiscs with various diameters, an increase in fibroblast cell adhesion, spreading area, and Yes-associated protein (YAP) nuclear localization on 100 nm diameter compared with smaller diameters was observed. Focal adhesion kinase is identified as the regulatory signal. These findings explore the optimal ligand presentation when the minimal requirements are sufficiently fulfilled in the heterogenous extracellular matrix network of isolated binding regions with abundant ligands. Integration of high-fidelity nano-biopatterning with super-resolution imaging allows precise quantitative studies to address early signaling events in response to receptor clustering and their nanoscale organization.

摘要

纳米尺度的跨膜受体组织对于细胞功能至关重要,这得益于生物配体呈现的纳米尺度工程。此前,使用单配体金纳米粒子证明了细胞-基质黏附中整合素结合配体的空间阈值≤60nm。然而,配体的几何排列仅限于单配体的六边形阵列,而等离子体淬灭限制了基于荧光的高分辨率成像的进一步研究。在这里,这些限制被介电 TiO 纳米图案克服,消除了荧光淬灭,从而能够在纳米图案上进行超分辨率荧光显微镜。通过双色超分辨率成像,观察到纳米图案、生物配体和整合素纳米簇之间具有高精度和一致性,验证了纳米图案功能化和钝化的高质量和完整性。通过筛选具有不同直径的 TiO 纳米盘,与较小直径相比,观察到在 100nm 直径的纳米盘上,成纤维细胞黏附、扩展面积和 Yes 相关蛋白 (YAP) 核定位增加。发现粘着斑激酶是调节信号。这些发现探索了在异质细胞外基质网络中,当最小要求在具有丰富配体的隔离结合区域中得到充分满足时,最佳的配体呈现。高保真纳米生物图案与超分辨率成像的集成允许进行精确的定量研究,以解决受体聚类及其纳米尺度组织的早期信号事件。

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Dielectric metasurfaces for next-generation optical biosensing: a comparison with plasmonic sensing.用于下一代光学生物传感的介电超表面:与等离子体传感的比较。
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