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首页> 外文期刊>Pharmaceutics >Rapid Target Binding and Cargo Release of Activatable Liposomes Bearing HER2 and FAP Single-Chain Antibody Fragments Reveal Potentials for Image-Guided Delivery to Tumors
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Rapid Target Binding and Cargo Release of Activatable Liposomes Bearing HER2 and FAP Single-Chain Antibody Fragments Reveal Potentials for Image-Guided Delivery to Tumors

机译:轴承HER2和FAP单链抗体片段的可活化脂质体的快速靶结合和货物释放揭示了图像引导递送给肿瘤的潜力

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Liposomes represent suitable tools for the diagnosis and treatment of a variety of diseases, including cancers. To study the role of the human epidermal growth factor receptor 2 (HER2) as target in cancer imaging and image-guided deliveries, liposomes were encapsulated with an intrinsically quenched concentration of a near-infrared fluorescent dye in their aqueous interior. This resulted in quenched liposomes (termed LipQ), that were fluorescent exclusively upon degradation, dye release, and activation. The liposomes carried an always-on green fluorescent phospholipid in the lipid layer to enable tracking of intact liposomes. Additionally, they were functionalized with single-chain antibody fragments directed to fibroblast activation protein (FAP), a marker of stromal fibroblasts of most epithelial cancers, and to HER2, whose overexpression in 20–30% of all breast cancers and many other cancer types is associated with a poor treatment outcome and relapse. We show that both monospecific (HER2-IL) and bispecific (Bi-FAP/HER2-IL) formulations are quenched and undergo HER2-dependent rapid uptake and cargo release in cultured target cells and tumor models in mice. Thereby, tumor fluorescence was retained in whole-body NIRF imaging for 32–48 h post-injection. Opposed to cell culture studies, Bi-FAP/HER2-IL-based live confocal microscopy of a high HER2-expressing tumor revealed nuclear delivery of the encapsulated dye. Thus, the liposomes have potentials for image-guided nuclear delivery of therapeutics, and also for intraoperative delineation of tumors, metastasis, and tumor margins.
机译:脂质体代表合适的工具,用于诊断和治疗各种疾病,包括癌症。为了研究人表皮生长因子受体2(HER2)作为癌症成像和图像引导递送的靶标的作用,脂质体被包封在其含水内部的近红外荧光染料的内在猝灭浓度。这导致淬火脂质体(称为LiPQ),其专门在降解,染料释放和活化时荧光。脂质体在脂质层中载有一体的绿色荧光磷脂,以便能够跟踪完整的脂质体。另外,它们用指向成纤维细胞活化蛋白(FAP)的单链抗体片段官能化,是大多数上皮癌的基质成纤维细胞的标志物,以及HER2,其过表达在所有乳腺癌的20-30%和许多其他癌症类型中与差的治疗结果和复发有关。我们表明,单特异性(HER2-IL)和双特异性(BI-FAP / HER2-IL)配方淬火并在小鼠中培养的靶细胞和肿瘤模型进行HER2依赖的快速摄取和货物释放。由此,肿瘤荧光保留在注射后32-48小时的全体NIRF成像中。反对细胞培养研究,Bi-FAP / HER2-IL的活共聚焦显微镜高HER2表达肿瘤揭示了包封染料的核递送。因此,脂质体具有用于治疗剂的图像引导的核递送的潜力,并且还用于术中描绘肿瘤,转移和肿瘤余量。

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