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Layer-by-layer assembled fluorescent probes in the second near-infrared window for systemic delivery and detection of ovarian cancer

机译:在第二个近红外窗口中逐层组装的荧光探针用于系统递送和检测卵巢癌

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摘要

Fluorescence imaging in the second near-infrared window (NIR-II, 1,000–1,700 nm) features deep tissue penetration, reduced tissue scattering, and diminishing tissue autofluorescence. Here, NIR-II fluorescent probes, including down-conversion nanoparticles, quantum dots, single-walled carbon nanotubes, and organic dyes, are constructed into biocompatible nanoparticles using the layer-by-layer (LbL) platform due to its modular and versatile nature. The LbL platform has previously been demonstrated to enable incorporation of diagnostic agents, drugs, and nucleic acids such as siRNA while providing enhanced blood plasma half-life and tumor targeting. This work carries out head-to-head comparisons of currently available NIR-II probes with identical LbL coatings with regard to their biodistribution, pharmacokinetics, and toxicities. Overall, rare-earth-based down-conversion nanoparticles demonstrate optimal biological and optical performance and are evaluated as a diagnostic probe for high-grade serous ovarian cancer, typically diagnosed at late stage. Successful detection of orthotopic ovarian tumors is achieved by in vivo NIR-II imaging and confirmed by ex vivo microscopic imaging. Collectively, these results indicate that LbL-based NIR-II probes can serve as a promising theranostic platform to effectively and noninvasively monitor the progression and treatment of serous ovarian cancer.
机译:在第二个近红外窗口(NIR-II,1,000-1,700 nm)中的荧光成像具有深层组织穿透,减少组织散射和减少组织自发荧光的特征。在这里,NIR-II荧光探针(包括下转换纳米颗粒,量子点,单壁碳纳米管和有机染料)由于具有模块化和通用性,因此使用逐层(LbL)平台构建为生物相容性纳米颗粒。先前已证明LbL平台可整合诊断剂,药物和核酸(如siRNA),同时提供增强的血浆半衰期和肿瘤靶向性。这项工作对具有相同LbL涂层的当前可用NIR-II探针进行了生物分布,药代动力学和毒性方面的面对面比较。总体而言,基于稀土的向下转换纳米粒子表现出最佳的生物学和光学性能,并被评估为高级浆液性卵巢癌(通常在晚期诊断)的诊断探针。通过体内NI​​R-II成像可成功检测到原位卵巢肿瘤,并通过离体显微镜成像得到证实。总体而言,这些结果表明,基于LbL的NIR-II探针可以作为有希望的治疗学平台,有效且无创地监测浆液性卵巢癌的进展和治疗。

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