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髓鞘碱性蛋白肽段的质子核磁共振研究:组氨酸谱线展宽揭示的Lys74-His77相互作用的证据

Proton NMR study of peptides from myelin basic protein: evidence for Lys74-His77 interaction revealed from histidine line broadening.

作者信息

Koshy K M, Hashim G A, Boggs J M

机构信息

Biochemistry Department, Research Institute, Hospital for Sick Children, Toronto, Ont., Canada.

出版信息

Biochim Biophys Acta. 1996 Mar 7;1293(1):23-30. doi: 10.1016/0167-4838(95)00229-4.

Abstract

Residues 69-84 of guinea pig myelin basic protein contain the encephalitogenic determinant for the Lewis rat. Insertion of histidine and glycine at positions 77 and 78 in bovine MBP greatly reduces the encephalitogenicity of the protein. Synthetic peptides analogous to this region of MBP containing glycine and histidine are encephalitogenic if they lack the N-terminal half, residues 69-74. However, if they contain both histidine plus the N-terminal half, encephalitogenicity is abolished, suggesting that an interaction of histidine with an amino acid in the N-terminal half changes the conformation or the properties of the peptide. This was investigated by measuring the 1H-NMR spectra of synthetic peptides analogous to this region of MBP, both containing histidine but with and without the N-terminal half. The major difference in the spectra of the two peptides was the pH dependence of line broadening of the histidine resonances. The histidine C2H and C4H resonances were broadened at intermediate pH values in both peptides. However, sharpening of the lines at high pH showed a different pH dependence in the two peptides. For the longer peptide containing the N-terminal half, the lines did not sharpen until the pH was increased above 10.2, coinciding with the pKa of Lys-74. Acetylation of this peptide caused the pH at which the lines began to sharpen to drop to 8.8. In the shorter peptide, lacking the N-terminal half and Lys-74, the lines also sharpened at pH 8.8. The greater broadening which persisted up above pH 10 for the longer peptide suggests slow exchange between two different conformations or environments of the histidine. One of these could be a conformation in which the deprotonated histidine hydrogen bonds with Lys-74. The Lys side-chain resonances indicated a decrease in rotational freedom above the pKa of histidine, consistent with this conclusion. Although this putative interaction between His and Lys-74 did not appear to have a significant effect on the overall conformation of the peptide, it could result in a reduction in encephalitogenicity by altering the properties of the peptide. This could affect processing and presentation of this determinant by antigen presenting cells.

摘要

豚鼠髓鞘碱性蛋白的69 - 84位残基包含针对Lewis大鼠的致脑炎决定簇。在牛髓鞘碱性蛋白的77和78位插入组氨酸和甘氨酸会大大降低该蛋白的致脑炎能力。与髓鞘碱性蛋白这一区域类似的含甘氨酸和组氨酸的合成肽,如果缺少N端的一半(69 - 74位残基)则具有致脑炎作用。然而,如果它们同时含有组氨酸和N端的一半,则致脑炎能力消失,这表明组氨酸与N端一半中的一个氨基酸相互作用会改变肽的构象或性质。通过测量与髓鞘碱性蛋白这一区域类似的合成肽的1H - NMR光谱对此进行了研究,这些肽都含有组氨酸,但分别有和没有N端的一半。两种肽光谱的主要差异在于组氨酸共振峰线宽的pH依赖性。两种肽中组氨酸的C2H和C4H共振峰在中等pH值时都变宽。然而,在高pH值时谱线变锐在两种肽中表现出不同的pH依赖性。对于含有N端一半的较长肽,直到pH值升高到10.2以上谱线才变锐,这与74位赖氨酸的pKa值相符。该肽的乙酰化导致谱线开始变锐的pH值降至8.8。在缺少N端一半和74位赖氨酸的较短肽中,谱线在pH 8.8时也变锐。较长肽在pH高于10时持续存在的更大程度的谱线展宽表明组氨酸在两种不同构象或环境之间的交换缓慢。其中一种可能是去质子化的组氨酸与74位赖氨酸形成氢键的构象。赖氨酸侧链共振峰表明在组氨酸的pKa值以上旋转自由度降低,这与该结论一致。尽管组氨酸与74位赖氨酸之间的这种假定相互作用似乎对肽的整体构象没有显著影响,但它可能通过改变肽的性质导致致脑炎能力降低。这可能会影响抗原呈递细胞对该决定簇的加工和呈递。

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