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A Carbon Nanotube Optical Sensor Reports Nuclear Entry via a Noncanonical Pathway

机译:碳纳米管光学传感器通过非共同途径报告核进入

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Single-walled carbon nanotubes are of interest in biomedicine for imaging and molecular sensing applications and as shuttles for various cargos such as chemotherapeutic drugs, peptides, proteins, and oligonucleotides. Carbon nanotube surface chemistry can be modulated for subcellular targeting while preserving photoluminescence for label-free visualization in complex biological environments, making them attractive materials for such studies. The cell nucleus is a potential target for many pathologies including cancer and infectious diseases. Understanding mechanisms of nanomaterial delivery to the nucleus may facilitate diagnostics, drug development, and gene-editing tools. Currently, there are no systematic studies to understand how these nanomaterials gain access to the nucleus. Herein, we developed a carbon nanotube based hybrid material that elucidate a distinct mechanism of nuclear translocation of a nanomaterial in cultured cells. We developed a nuclear-targeted probe via cloaking photoluminescent single-walled carbon nanotubes in a guanidinium-functionalized helical polycarbodiimide. We found that the nuclear entry of the nanotubes was mediated by the import receptor importin beta without the aid of importin alpha and not by the more common importin alpha/beta pathway. Additionally, the nanotube photoluminescence exhibited distinct red-shifting upon entry to the nucleus, potentially functioning as a reporter of the importin beta-mediated nuclear transport process. This work delineates a noncanonical mechanism for nanomaterial delivery to the nucleus and provides a reporter for the study of nucleus-related pathologies.
机译:单壁碳纳米管对生物医生感兴趣,用于成像和分子传感应用以及用于各种尸体的梭,例如化学治疗药物,肽,蛋白质和寡核苷酸。可以调节碳纳米管表面化学,用于亚细胞靶向,同时保留在复杂的生物环境中无标记可视化的光致发光,使它们为这些研究的吸引力。细胞核是许多病态的潜在目标,包括癌症和传染病。理解纳米材料传递给核的机制可以促进诊断,药物开发和基因编辑工具。目前,没有系统研究可以了解这些纳米材料如何进入核。在此,我们开发了一种基于碳纳米管的杂化材料,其阐明培养细胞中纳米材料的核易位的不同机制。我们通过粘附的光致发光单壁碳纳米管在胍酰胺型螺旋聚碳二亚胺酰亚胺中开发了一种核目标探针。我们发现纳米管的核进入由进口受体Importinβ介导,而不是衍生α的辅助,而不是更常见的Importinα/β途径。另外,纳米管光致发光在进入细胞核时表现出明显的红移,潜在的作用作为进一步β介导的核运输过程的报告。这项工作描绘了纳米材料向核的非甘露解机制,为核心相关病理学提供了报告。

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