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Facile Attachment of TAT Peptide on Gold Monolayer Protected Clusters: Synthesis and Characterization

机译:TAT肽在金单层保护簇上的容易附着:合成和表征。

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摘要

High affinity thiolate-based polymeric capping ligands are known to impart stability onto nanosized gold nanoparticles. Due to the stable gold-sulfur bond, the ligand forms a protective layer around the gold core and subsequently controls the physicochemical properties of the resultant nanogold mononuclear protected clusters (AuMPCs). The choice of ligands to use as surfactants for AuMPCs largely depends on the desired degree of hydrophilicity and biocompatibility of the MPCs, normally dictated by the intended application. Subsequent surface modification of AuMPCs allows further conjugation of additional biomolecules yielding bilayer or multilayered clusters suitable for bioanalytical applications ranging from targeted drug delivery to diagnostics. In this study, we discuss our recent laboratory findings on a simple route for the introduction of Trans-Activator of Transcription (TAT) peptide onto the surface of biotin-derivatised gold MPCs via the biotin-strepavidin interaction. By changing the surface loading of biotin, controlled amounts of TAT could be attached. This bioconjugate system is very attractive as a carrier in intercellular delivery of various delivery cargoes such as antibodies, proteins and oligonucleotides.
机译:已知基于高亲和力硫醇盐的聚合物封端配体可赋予纳米级金纳米颗粒以稳定性。由于稳定的金硫键,配体在金核周围形成保护层,并随后控制所得纳米金单核保护簇(AuMPC)的物理化学性质。用作AuMPC的表面活性剂的配体的选择很大程度上取决于MPC的所需亲水性和生物相容性,通常由预期应用决定。 AuMPC的后续表面修饰可以进一步缀合其他生物分子,从而产生双层或多层簇,适用于从靶向药物递送到诊断的生物分析应用。在这项研究中,我们讨论了通过生物素-链霉亲和素相互作用将反式转录激活子(TAT)肽引入生物素衍生的金MPCs表面的简单途径的最新实验室发现。通过改变生物素的表面负载,可以附着受控量的TAT。这种生物缀合物系统作为细胞间递送各种递送货物如抗体,蛋白质和寡核苷酸的载体是非常有吸引力的。

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