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Zebrafish: A Visual Model To Evaluate the Biofate of Transferrin Receptor-Targeted 7Peptide-Decorated Coumarin 6 Micelles

机译:斑马鱼:一种评价转铁蛋白受体靶向7肽装饰香豆素6胶束的生物糖的视觉模型

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In the present study, the zebrafish was explored as an in vivo model to assess the biofate of transferrin receptor (TfR)-targeted coumarin 6 (C6) micelles across various biological barriers. Three 7peptide (7pep)-decorated poly-(ethylene glycol)-block-poly(epsilon-caprolactone) micelles loaded with fluorescence coumarin 6 (7pep-M-C6) with different ligand densities were constructed with particle sizes between 30 and 40 nm. Whole-mount immunostaining revealed that the expression level of TfR. in the retina, brain, and intestine increased along with development stage. Compared to unmodified micelles, 7pep-M-C6 demonstrated higher uptake efficiency in the larval zebrafish. Preinhibition of TfR with 7pep implicated the TfR-mediated endocytosis pathway in the uptake of 7pep-M-C6. Confocal images of the larval zebrafish eye and brain showed the efficient delivery of C6 across the retinal pigment epithelial to the ganglion cell layer and the significant accumulation of C6 in all brain tissues, respectively, which plateaued when the ligand density was 10%. To investigate the intestinal distribution of C6, micelles were administered to adult zebrafish via gavaging. Notably, 7pep-M-C6 enhanced the transport of C6 across the villi and increased its aggregation into the basolateral membrane of the intestine. After the oral administration of 7pep-M-C6, C6 accumulated in the eye and brain. Forster resonance energy transfer analysis suggested thatintact 7pep-modified micelles could enter the epithelial cells of the intestine, brain, and eye after oral administration in adult zebrafish. In conclusion, zebrafish could be used as a model for in vivo visual assessment of the biofate of TfR-targeted drug delivery systems.
机译:在本研究中,斑马鱼被探索为体内模型,以评估在各种生物屏障上的转铁蛋白受体(TFR)的生物素 - 细胞胶质蛋白6(C6)胶束。用不同配体密度的荧光香豆素6(7Pep-M-C6)的三种7肽(7Pep)的聚 - (乙二醇)-Block-poly(epsilon-己内酯)胶束,其颗粒尺寸在30至40nm之间构建。全山免疫抑制揭示了TFR的表达水平。在视网膜,脑和肠中随着发展阶段而增加。与未修饰的胶束相比,7PEP-M-C6在幼虫斑马鱼中表现出更高的摄取效率。在7PPEP中,TFR的预抑制意味着TFR介导的内吞作用途径在7PEP-M-C6的摄取中。幼虫斑马鱼眼和大脑的共聚焦图像显示,在整个脑组织中,C6在整个脑组织上的显着积累的高效递送C6,并且当配体密度为10%时,该脑组织中的C6的显着积累。为了研究C6的肠道分布,通过饲养给成年斑马鱼施用胶束。值得注意的是,7PEP-M-C6增强了绒毛的C6的运输,并将其聚集在肠道的基底外侧。在口服7PEP-M-C6,C6累积在眼睛和脑中。福尔斯特共振能量转移分析表明,由于在成人斑马鱼口服施用后,该胶质胶质细胞可以进入肠道,脑和眼的上皮细胞。总之,斑马鱼可以用作体内视觉评估TFR靶向药物递送系统的型号的模型。

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