首页> 外文期刊>Glycoconjugate journal >Human trachea primary epithelial cells express both sialyl(alpha 2-3)Gal receptor for human parainfluenza virus type 1 and avian influenza viruses, and sialyl(alpha 2-6)Gal receptor for human influenza viruses
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Human trachea primary epithelial cells express both sialyl(alpha 2-3)Gal receptor for human parainfluenza virus type 1 and avian influenza viruses, and sialyl(alpha 2-6)Gal receptor for human influenza viruses

机译:人气管原代上皮细胞同时表达人副流感病毒1型和禽流感病毒的唾液酸(alpha 2-3)Gal受体和人流感病毒的唾液酸(alpha 2-6)Gal受体

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摘要

We reported previously that the dominant receptors of influenza A and B viruses, and human and murine respiroviruses, were sialylglycoproteins and gangliosides containing monosialo-lactosamine type I-and II-residues, such as sialic acid-alpha 2-3(6)-Gal beta 1-3(4)-GlcNAc beta 1-. In addition, the Sia alpha 2-3Gal linkage was predominantly recognized by avian and horse influenza viruses, and human parainfluenza virus type 1 (hPIV-1), whereas the Sia alpha 2-6Gal linkage was mainly recognized by human influenza viruses (Paulson JC in "The Receptors'' [Conn M Ed] 2, 131-219 (1985); Suzuki Y, Prog Lipid Res 33, 429-57 (1994); Ito T, J Virol 73, 6743-51 (2000); Suzuki Y, J Virol 74, 11825-31 (2000); Suzuki T, J. Virol 75, 4604-4613 (2001); Suzuki Y, Biol. Pharm. Bull. 28, 399-408 (2005)). To clarify the distribution of influenza virus receptors on the human bronchial epithelium cell surface, we investigated a primary culture of normal human bronchial epithelial (NHBE) cells using two types of lectin (MAA and SNA), which recognize sialyl linkages (alpha 2-3 and alpha 2-6), using fluorescence-activated cell-sorting analysis. The results showed that both alpha 2-3- and alpha 2-6-linked Sias were expressed on the surface of primary human bronchial epithelial cells. The cells infected by hPIV-1 bound to MAA, confirming that cells targeted by hPIV-1 have alpha 2-3-linked oligosaccharides. We also compared the ability of hPIV-1 and human influenza A virus to infect primary human bronchial epithelial cells pre-treated with Sia alpha 2-3Gal-specific sialidase from Salmonella typhimurium. No difference was observed in the number of sialidase pre-treated and non-treated cells infected with human influenza A virus, which binds to Sia alpha 2-6Gal-linked oligosaccharides. By contrast, the number of cells infected with hPIV-1 decreased significantly upon sialidase treatment. Thus, cultured NHBE cells showed both alpha 2-3-linked Sias recognized by hPIV-1 and avian influenza virus receptors, and alpha 2-6-linked Sias recognized by human influenza virus receptors.
机译:我们以前曾报道甲型和乙型流感病毒以及人类和鼠类呼吸道病毒的主要受体是唾液酸糖蛋白和神经节苷脂,它们含有I-和II型单唾液酸乳糖胺残基,例如唾液酸-α2-3(6)-Gal beta 1-3(4)-GlcNAc beta 1-。此外,Sia alpha 2-3Gal连接主要被禽流感和马流感病毒以及1型人类副流感病毒(hPIV-1)识别,而Sia alpha 2-6Gal连接主要被人类流感病毒识别(Paulson JC见《 The Receptors》 [Conn M Ed] 2,131-219(1985); Suzuki Y,Prog Lipid Res 33,429-57(1994); Ito T,J Virol 73,6743-51(2000); Suzuki Y,J Virol 74,11825-31(2000); Suzuki T,J. Virol 75,4604-4613(2001); Suzuki Y,Biol。Pharm.Bull.28,399-408(2005))。流感病毒受体在人支气管上皮细胞表面的分布,我们使用两种类型的凝集素(MAA和SNA)研究了正常人支气管上皮细胞(NHBE)的原代培养,该两种凝集素可识别唾液酸键(alpha 2-3和alpha 2 -6),使用荧光激活细胞分选分析,结果显示,α2-3-和α2-6连接的Sias在原代人支气管上皮细胞表面均表达。被hPIV-1感染的细胞与MAA结合,证实hPIV-1靶向的细胞具有与α2-3-连接的寡糖。我们还比较了hPIV-1和人类甲型流感病毒感染原代人沙门氏菌Sia alpha 2-3Gal特异性唾液酸酶预处理的原代人支气管上皮细胞的能力。在与人Sia alpha 2-6Gal连接的寡糖结合的人类A型流感病毒感染的唾液酸酶预处理和未处理细胞的数量上未观察到差异。相比之下,经唾液酸酶处理后,感染了hPIV-1的细胞数量明显减少。因此,培养的NHBE细胞显示出被hPIV-1和禽流感病毒受体识别的α2-3-连接的Sias,以及被人流感病毒受体识别的α2-6连接的Sias。

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