Structural differences between the putative carbohydrate-recognition domains of human IL-1 alpha, IL-1 beta and IL-1 receptor antagonist obtained by in silico modeling
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作者:
Vergoten, Gerard
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Univ Sci & Tech Lille Flandres Artois, Unite Glycobiol Struct & Fonctionnelle, CNRS, UMR 8576, F-59655 Villeneuve Dascq, FranceUniv Sci & Tech Lille Flandres Artois, Unite Glycobiol Struct & Fonctionnelle, CNRS, UMR 8576, F-59655 Villeneuve Dascq, France
Vergoten, Gerard
[1
]
Zanetta, Jean-Pierre
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Univ Sci & Tech Lille Flandres Artois, Unite Glycobiol Struct & Fonctionnelle, CNRS, UMR 8576, F-59655 Villeneuve Dascq, FranceUniv Sci & Tech Lille Flandres Artois, Unite Glycobiol Struct & Fonctionnelle, CNRS, UMR 8576, F-59655 Villeneuve Dascq, France
Zanetta, Jean-Pierre
[1
]
机构:
[1] Univ Sci & Tech Lille Flandres Artois, Unite Glycobiol Struct & Fonctionnelle, CNRS, UMR 8576, F-59655 Villeneuve Dascq, France
In a previous report (Cebo et al. J Biol Chem 276 (2001) 5685-5691), it was established that biologically active recombinant human IL-1 alpha and IL-1 beta had different carbohydrate-binding properties. IL-1 alpha recognized a di-antennary N-glycan with two alpha 2-3-linked sialic acid residues, whereas IL-1 beta recognized the GM(4), a alpha 2-3-linked sialylated glycosphingolipid. These different carbohydrate-binding properties of two interleukins binding to the same receptor (IL-1R) could explain why these molecules had different biological effects and cell specificities. Molecular modeling of the ligands and in silico docking experiments defined putative carbohydrate-recognition domains localized in the same area of the two molecules, a domain different from that defined as the type I IL-1R binding domain. The calculated pattern of hydrogen bonding and of van der Waals interactions fulfilled the essential features observed for calcium-independent lectins (mammalian, viral or bacterial). The analysis of the same domain of the third members of this family of molecules, the IL-1R-antagonist, indicated it did not fulfill the criteria for carbohydrate-recognition domains. It is proposed that its role as a pure antagonist is due to the absence of lectin activity and consequently explained its inability to associate IL-1R with other surface molecular complexes necessary for signaling.
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UNIV EDINBURGH,VET FIELD STN,DEPT VET PATHOL,ROSLIN EH25 9RG,MIDLOTHIAN,SCOTLANDUNIV EDINBURGH,VET FIELD STN,DEPT VET PATHOL,ROSLIN EH25 9RG,MIDLOTHIAN,SCOTLAND
Alzuherri, HM
Woodall, CJ
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UNIV EDINBURGH,VET FIELD STN,DEPT VET PATHOL,ROSLIN EH25 9RG,MIDLOTHIAN,SCOTLANDUNIV EDINBURGH,VET FIELD STN,DEPT VET PATHOL,ROSLIN EH25 9RG,MIDLOTHIAN,SCOTLAND
Woodall, CJ
Clarke, CJ
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UNIV EDINBURGH,VET FIELD STN,DEPT VET PATHOL,ROSLIN EH25 9RG,MIDLOTHIAN,SCOTLANDUNIV EDINBURGH,VET FIELD STN,DEPT VET PATHOL,ROSLIN EH25 9RG,MIDLOTHIAN,SCOTLAND
机构:
Chugai Pharmaceut Co Ltd, Prod Res Dept, Fuji Gotemba Res Labs, Shizuoka 4128513, JapanChugai Pharmaceut Co Ltd, Prod Res Dept, Fuji Gotemba Res Labs, Shizuoka 4128513, Japan
Suzuki, Miho
Hashizume, Misato
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Chugai Pharmaceut Co Ltd, Prod Res Dept, Fuji Gotemba Res Labs, Shizuoka 4128513, JapanChugai Pharmaceut Co Ltd, Prod Res Dept, Fuji Gotemba Res Labs, Shizuoka 4128513, Japan
Hashizume, Misato
Yoshida, Hiroto
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Chugai Pharmaceut Co Ltd, Prod Res Dept, Fuji Gotemba Res Labs, Shizuoka 4128513, JapanChugai Pharmaceut Co Ltd, Prod Res Dept, Fuji Gotemba Res Labs, Shizuoka 4128513, Japan
Yoshida, Hiroto
Shiina, Masashi
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Chugai Pharmaceut Co Ltd, Prod Res Dept, Fuji Gotemba Res Labs, Shizuoka 4128513, JapanChugai Pharmaceut Co Ltd, Prod Res Dept, Fuji Gotemba Res Labs, Shizuoka 4128513, Japan
Shiina, Masashi
Mihara, Masahiko
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Chugai Pharmaceut Co Ltd, Prod Res Dept, Fuji Gotemba Res Labs, Shizuoka 4128513, JapanChugai Pharmaceut Co Ltd, Prod Res Dept, Fuji Gotemba Res Labs, Shizuoka 4128513, Japan