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活细胞中腺相关病毒核输入的超分辨率成像。

Super-resolution imaging of nuclear import of adeno-associated virus in live cells.

机构信息

Department of Biology, Temple University , Philadelphia, Pennsylvania, USA.

Department of Microbiology and Immunology, School of Medicine, Temple University , Philadelphia, Pennsylvania, USA.

出版信息

Mol Ther Methods Clin Dev. 2015 Dec 2;2:15047. doi: 10.1038/mtm.2015.47. eCollection 2015.

Abstract

Adeno-associated virus (AAV) has been developed as a promising human gene therapy vector. Particularly, recombinant AAV vector (rAAV) achieves its transduction of host cells by crossing at least three physiological barriers including plasma membrane, endosomal membrane, and nuclear envelope (NE). So far, the AAV transduction mechanism has not been explored thoroughly at the single viral particle level. In this study, we employed high-speed super-resolution single-point edge-excitation sub-diffraction (SPEED) microscopy to map the events of single rAAV2 particles infecting live human cells with an unprecedented spatiotemporal resolution of 9-12 nm and 2-20 ms. Data reveal that rAAV2 particles are imported through nuclear pore complexes (NPCs) rather than nuclear membrane budding into the nucleus. Moreover, approximately 17% of the rAAV2 molecules starting from the cytoplasm successfully transverse the NPCs to reach the nucleoplasm, revealing that the NPCs act as a strict selective step for AAV delivery. This study lastly suggests a new pathway to improve AAV vectors for human gene therapy.

摘要

腺相关病毒(AAV)已被开发为一种很有前途的人类基因治疗载体。特别是,重组 AAV 载体(rAAV)通过穿过至少三个生理屏障,包括质膜、内体膜和核膜(NE),来实现对宿主细胞的转导。到目前为止,AAV 转导机制尚未在单个病毒颗粒水平上得到充分探索。在这项研究中,我们采用高速超分辨率单点边缘激发亚衍射(SPEED)显微镜,以空前的 9-12nm 和 2-20ms 的时空分辨率来绘制单个 rAAV2 颗粒感染活人体细胞的事件。数据显示,rAAV2 颗粒通过核孔复合体(NPC)而不是核膜出芽进入细胞核。此外,大约 17%的起始于细胞质的 rAAV2 分子成功地穿过 NPC 到达核质,这表明 NPC 是 AAV 传递的严格选择性步骤。这项研究最后提出了一种新的途径来改进 AAV 载体用于人类基因治疗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3808/4667716/f28c913340d5/mtm201547-f1.jpg

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