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人呼吸道上皮细胞的rAAV-2感染不需要膜相关硫酸乙酰肝素。

Membrane-associated heparan sulfate is not required for rAAV-2 infection of human respiratory epithelia.

作者信息

Boyle Michael P, Enke Raymond A, Reynolds Jeffrey B, Mogayzel Peter J, Guggino William B, Zeitlin Pamela L

机构信息

Department of Medicine, The Johns Hopkins University School of Medicine, Baltimore MD 21205, USA.

出版信息

Virol J. 2006 Apr 22;3:29. doi: 10.1186/1743-422X-3-29.

Abstract

BACKGROUND

Adeno-associated virus type 2 (AAV-2) attachment and internalization is thought to be mediated by host cell membrane-associated heparan sulfate proteoglycans (HSPG). Lack of HSPG on the apical membrane of respiratory epithelial cells has been identified as a reason for inefficient rAAV-2 infection in pulmonary applications in-vivo. The aim of this investigation was to determine the necessity of cell membrane HSPG for efficient infection by rAAV-2.

RESULTS

Rates of transduction with rAAV2-CMV-EGFP3 in several different immortalized airway epithelial cell lines were determined at different multiplicities of infection (MOI) before and after removal of membrane HSPG by heparinase III. Removal of HSPG decreased the efficacy of infection with rAAV2 by only 30-35% at MOI < or = 100 for all of respiratory cell lines tested, and had even less effect at an MOI of 1000. Studies in mutant Chinese Hamster Ovary cell lines known to be completely deficient in surface HSPG also demonstrated only moderate effect of absence of HSPG on rAAV-2 infection efficacy. However, mutant CHO cells lacking all membrane proteoglycans demonstrated dramatic reduction in susceptibility to rAAV-2 infection, suggesting a role of membrane glycosaminoglycans other than HSPG in mediating rAAV-2 infection.

CONCLUSION

Lack of cell membrane HSPG in pulmonary epithelia and other cell lines results in only moderate decrease in susceptibility to rAAV-2 infection, and this decrease may be less important at high MOIs. Other cell membrane glycosaminoglycans can play a role in permitting attachment and subsequent rAAV-2 internalization. Targeting alternative membrane glycosaminoglycans may aid in improving the efficacy of rAAV-2 for pulmonary applications.

摘要

背景

2型腺相关病毒(AAV-2)的附着和内化被认为是由宿主细胞膜相关的硫酸乙酰肝素蛋白聚糖(HSPG)介导的。呼吸道上皮细胞顶膜上缺乏HSPG已被确定为体内肺部应用中重组AAV-2感染效率低下的一个原因。本研究的目的是确定细胞膜HSPG对重组AAV-2有效感染的必要性。

结果

在通过肝素酶III去除膜HSPG之前和之后,在几种不同的永生化气道上皮细胞系中,以不同的感染复数(MOI)测定了rAAV2-CMV-EGFP3的转导率。对于所有测试的呼吸道细胞系,在MOI≤100时,去除HSPG仅使rAAV2的感染效率降低30%-35%,而在MOI为1000时影响更小。在已知表面HSPG完全缺乏的突变中国仓鼠卵巢细胞系中的研究也表明,缺乏HSPG对rAAV-2感染效率的影响仅为中等程度。然而,缺乏所有膜蛋白聚糖的突变CHO细胞对rAAV-2感染的敏感性显著降低,这表明除HSPG外的膜糖胺聚糖在介导rAAV-2感染中起作用。

结论

肺上皮细胞和其他细胞系中细胞膜HSPG的缺乏仅导致对rAAV-2感染的敏感性适度降低,并且这种降低在高MOI时可能不太重要。其他细胞膜糖胺聚糖可以在允许附着和随后的rAAV-2内化中发挥作用。靶向替代的膜糖胺聚糖可能有助于提高rAAV-2在肺部应用中的疗效。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5829/1459113/c265a1aae916/1743-422X-3-29-1.jpg

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