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腺病毒的成熟使蛋白纳米壳能够成功地逃离内体。

Maturation of adenovirus primes the protein nano-shell for successful endosomal escape.

机构信息

Moleculaire Biofysica, Zernike Instituut, Rijksuniversiteit Groningen, The Netherlands and Natuur- en Sterrenkunde and LaserLaB, Vrije Universiteit Amsterdam, The Netherlands.

Department of Immunology and Microbiology, the Scripps Research Institute, La Jolla, CA 92037, USA.

出版信息

Nanoscale. 2019 Mar 7;11(9):4015-4024. doi: 10.1039/c8nr10182e. Epub 2019 Feb 15.

Abstract

The ability of adenoviruses to infect a broad range of species has spurred a growing interest in nanomedicine to use adenovirus as a cargo delivery vehicle. While successful maturation of adenovirus and controlled disassembly are critical for efficient infection, the underlying mechanisms regulating these processes are not well understood. Here, we present Atomic Force Microscopy nanoindentation and fatigue studies of adenovirus capsids at different maturation stages to scrutinize their dynamic uncoating properties. Surprisingly, we find that the early intermediate immature (lacking DNA) capsid is mechanically indistinguishable in both break force and spring constant from the mature (containing DNA) capsid. However, mature and immature capsids do display distinct disassembly pathways, as revealed by our mechanically-induced fatigue analysis. The mature capsid first loses the pentons, followed by either long-term capsid stability or abrupt and complete disassembly. However, the immature capsid has a stable penton region and undergoes a stochastic disassembly mechanism, thought to be due to the absence of genomic pressure. Strikingly, the addition of the genome alone is not sufficient to achieve penton destabilization as indicated by the penton stability of the maturation-intermediate mutant, G33A. Full penton destabilization was achieved only when the genome was present in addition to the successful maturation-linked proteolytic cleavage of preprotein VI. Therefore these findings strongly indicate that maturation of adenovirus in concert with genomic pressure induces penton destabilization and thus, primes the capsid for controlled disassembly. This latter aspect is critical for efficient infection and successful cargo delivery.

摘要

腺病毒能够感染广泛的物种,这促使人们越来越关注纳米医学,将腺病毒作为一种货物输送载体。虽然腺病毒的成功成熟和受控解体对于有效感染至关重要,但调节这些过程的潜在机制尚未得到很好的理解。在这里,我们通过原子力显微镜纳米压痕和疲劳研究了不同成熟阶段的腺病毒衣壳,以仔细研究它们的动态脱壳特性。令人惊讶的是,我们发现早期中间不成熟(缺乏 DNA)衣壳在断裂力和弹性常数方面与成熟(含有 DNA)衣壳机械上无法区分。然而,成熟和不成熟的衣壳确实显示出不同的解体途径,这是我们通过机械诱导的疲劳分析揭示的。成熟的衣壳首先失去五聚体,然后是长期的衣壳稳定性或突然和完全的解体。然而,不成熟的衣壳具有稳定的五聚体区域,并经历随机的解体机制,据认为这是由于缺乏基因组压力。引人注目的是,仅仅添加基因组不足以实现五聚体失稳,正如成熟中间体突变体 G33A 的五聚体稳定性所表明的那样。只有当基因组存在并且前蛋白 VI 的成功成熟相关蛋白水解切割时,才会实现完全的五聚体失稳。因此,这些发现强烈表明,腺病毒的成熟与基因组压力协同作用诱导五聚体失稳,从而为受控解体做好准备。后一方面对于有效感染和成功的货物输送至关重要。

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