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Mapping Glycans onto Specific N-Linked Glycosylation Sites of Pyrus Communis PGIP Redefines the Interface for EPG:PGIP Interactions

机译:将糖类映射到Pyrus Communis的特定N-连接糖基化位点PGIP重新定义了EPG:PGIP相互作用的界面

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摘要

Polygalacturonase inhibiting proteins (PGIPs) are members of the leucine rich repeat family of proteins, involved in plant defense against fungal pathogens. PGIPs exhibit a remarkable degree of specificity in terms of their ability to bind and inhibit their target molecules, the endopolygalacturonases (EPGs). This specificity has been attributed for certain EPG/PGIP combinations to differences in primary sequence, but this explanation is unable to account for the full range of binding and inhibitory activities observed. In this paper we have fully characterized the glycosylation on the PGIP derived from Pyrus communis and demonstrated, using a combination of PNGaseF and PNGaseA in 18O-water, that the Pyrus communis PGIP utilizes all seven potential sites of N-linked glycosylation. Further, we demonstrate that certain sites appear to be modified only by glycans bearing α3-linked core fucosylation, while others are occupied by a mixture of fucosylated and non-fucosylated glycans. Modeling of the carbohydrates onto a homologous structure of PGIP indicates potential roles for glycosylation in mediating the interactions of PGIPs with EPGs.
机译:聚半乳糖醛酸酶抑制蛋白(PGIP)是富含亮氨酸的重复蛋白家族的成员,参与植物对真菌病原体的防御。 PGIP在结合和抑制其靶分子即内聚半乳糖苷酶(EPG)的能力方面表现出显着的特异性。这种特异性已经归因于某些EPG / PGIP组合的一级序列差异,但是这种解释无法解释观察到的全部结合和抑制活性。在本文中,我们充分表征了梨属植物PGIP上的糖基化,并结合了PNGaseF和PNGaseA在 18 O水中的使用,证明梨属植物PGIP利用了Pyrus communis的所有七个潜在位点N-联糖基化。此外,我们证明某些位点似乎仅被带有α3连接的核心岩藻糖基化的聚糖修饰,而其他位点则由岩藻糖基化和非岩藻糖基化的聚糖混合物占据。碳水化合物在PGIP同源结构上的建模表明糖基化在介导PGIP与EPG相互作用中的潜在作用。

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