結晶中と溶液状態での耐熱性エンテロトキシンアナログの比較研究
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概要
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Comparative study of heat-stable enterotoxin analogs from Escherichia coli porcine strain (STp) in crystal and solution states was performed. Structures of 3-mercaptopropionic acid (Mpr) analogs, [Mpr^5]STp(5-17) and [Mpr^5, Leu^<13>]STp(5-17) were determined in crystal state. Structures of STp(5-17) and [Leu^<13>]STp(5-17) were those in solution state. In the crystalline state, the replacement of Ala^<13> with Leu^<13> resulted in the change of torsion angles (φ) at amino acid residues included in the second β-turn (Asn^<11>-Cys^<14>), except for a change of the side chain. While in the solution state, the replacement at 13 th position did not cause notable changes in the chemical shift of protons and the distribution of NOEs. Almost all inter-residual NOEs observed for NH, C_αH, and C_βH of STp(5-17) were also detected in the proton pairs of [Leu^<13>]STp(5-17). ^3J_<αN> values for residues included in the second β-turn were similar to each other between these analogs. These results strongly suggest that the backbone structure of ST is not affected by the replacement of Ala^<13> with Leu^<13> in the solution state. Above results demonstrated that the change of torsion angles, observed in the crystalline state by the replacement of Ala^<13> with Leu^<13>, might be caused by the change of the molecular packing in crystal. Results in this study also confirmed that the ST molecule possesses the flexibility at the region of the second β-turn. Taking into account that ST loses its toxicity by the replacement of Ala^<13> with Leu^<13>, the second β-turn region is the important part of ST to generate its toxicity. Therefore, the flexibility at this region is expected to play an important role in the recognition of ST by its receptor protein.
- 明治大学の論文
- 2002-03-25
著者
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河合 充
明治大学農学部生命科学科タンパク質工学研究室
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尾崎 宏
明治大学農学部生命科学科タンパク質工学研究室
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宮本 貴文
明治大学農学部生命科学科タンパク質工学研究室
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新井 恵理子
明治大学農学部生命科学科タンパク質工学研究室
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網代 卓祐
明治大学農学部生命科学科タンパク質工学研究室
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網代 卓祐
明治大学農学部
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宮本 貴史
明治大学農学部
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新井 恵理子
明治大学農学部
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