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1型登革病毒非结构糖蛋白NS1以糖基化依赖的方式作为可溶性六聚体从哺乳动物细胞中分泌出来。

Dengue virus type 1 nonstructural glycoprotein NS1 is secreted from mammalian cells as a soluble hexamer in a glycosylation-dependent fashion.

作者信息

Flamand M, Megret F, Mathieu M, Lepault J, Rey F A, Deubel V

机构信息

Unité des Arbovirus et Virus des Fièvres Hémorragiques, Institut Pasteur, 75724 Paris Cedex 15, 91198 Gif-sur-Yvette Cedex, France.

出版信息

J Virol. 1999 Jul;73(7):6104-10. doi: 10.1128/JVI.73.7.6104-6110.1999.

Abstract

Nonstructural glycoprotein NS1, specified by dengue virus type 1 (Den-1), is secreted from infected green monkey kidney (Vero) cells in a major soluble form characterized by biochemical and biophysical means as a unique hexameric species. This noncovalently bound oligomer is formed by three dimeric subunits and has a molecular mass of 310 kDa and a Stokes radius of 64.4 A. During protein export, one of the two oligosaccharides of NS1 is processed into an endo-beta-N-acetylglucosaminidase F-resistant complex-type sugar while the other remains of the polymannose type, protected in the dimeric subunit from the action of maturation enzymes. Complete processing of the complex-type sugar appears to be required for efficient release of soluble NS1 into the culture fluid of infected cells, as suggested by the repressive effects of the N-glycan processing inhibitors swainsonine and deoxymannojyrimicin. These results, together with observations related to the absence of secretion of NS1 from Den-infected insect cells, suggest that maturation and secretion of hexameric NS1 depend on the glycosylation status of the host cell.

摘要

由1型登革病毒(Den-1)指定的非结构糖蛋白NS1,以主要可溶形式从感染的绿猴肾(Vero)细胞中分泌出来,通过生化和生物物理方法表征为一种独特的六聚体。这种非共价结合的寡聚体由三个二聚体亚基组成,分子量为310 kDa,斯托克斯半径为64.4 Å。在蛋白质输出过程中,NS1的两个寡糖之一被加工成耐内切β-N-乙酰葡糖胺酶F的复合型糖,而另一个仍然是多聚甘露糖型,在二聚体亚基中受到保护,免受成熟酶的作用。如N-聚糖加工抑制剂swainsonine和脱氧甘露糖霉素的抑制作用所表明的,复合型糖的完全加工似乎是可溶性NS1有效释放到感染细胞培养液中的必要条件。这些结果,连同与Den感染的昆虫细胞中NS1不分泌相关的观察结果,表明六聚体NS1的成熟和分泌取决于宿主细胞的糖基化状态。

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Lectins as chaperones in glycoprotein folding.凝集素作为糖蛋白折叠中的伴侣蛋白。
Curr Opin Struct Biol. 1998 Oct;8(5):587-92. doi: 10.1016/s0959-440x(98)80148-6.
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