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牛血小板因子4的1H-NMR研究:组氨酸归属及与肝素的相互作用

1H-NMR studies of bovine platelet factor 4: histidine assignments and interactions with heparin.

作者信息

Talpas C J, Walz D A, Lee L

机构信息

Department of Chemistry and Biochemistry, University of Windsor, Canada.

出版信息

Biochim Biophys Acta. 1991 Jun 24;1078(2):208-18. doi: 10.1016/0167-4838(91)99011-g.

Abstract

1H-NMR spectroscopy has been used to assign and to characterize the two histidine C2H resonances of the heparin binding protein, bovine platelet factor 4. One histidine has a pKa value of 6.51 at 27 degrees C; the second histidine exhibits 2 pKa values of 5.52 and 5.66 at 27 degrees C. The two histidine resonances have been assigned by an analysis of their deuterium exchange kinetics. Both resonances are solvent accessible with half-times of exchange at pH 8.8 of 3.3 and 4.0 days. These two resonances have been assigned by digesting partially deuterated protein with Staphylococcus aureus V-8 proteinase, separating and purifying the resulting peptides, and determining their relative and residual hydrogen content by NMR. The results indicate that His-38 has the lower pKa value and the slower deuterium exchange rate, whereas His-50 has the higher pKa value and the faster deuterium exchange rate at pH 8.8. The 1H-NMR resonance of His-38 of bovine platelet factor 4 is preferentially perturbed by the introduction of heparin. This observation and the presence of His-38 within the belt of positively charged residues around the platelet factor 4 tetramer supports the model of the platelet factor 4-heparin complex in which the polysaccharide crosses over each of the 2 alpha-helices of the 2 dimers at right angles.

摘要

1H-核磁共振光谱已被用于确定和表征肝素结合蛋白牛血小板因子4的两个组氨酸C2H共振峰。一个组氨酸在27℃时的pKa值为6.51;第二个组氨酸在27℃时呈现出5.52和5.66两个pKa值。通过对它们的氘交换动力学进行分析,确定了这两个组氨酸共振峰。在pH 8.8时,两个共振峰都可与溶剂接触,交换半衰期分别为3.3天和4.0天。通过用金黄色葡萄球菌V-8蛋白酶消化部分氘代的蛋白质、分离和纯化所得肽段,并通过核磁共振确定它们的相对和残余氢含量,确定了这两个共振峰。结果表明,在pH 8.8时,His-38的pKa值较低,氘交换速率较慢,而His-50的pKa值较高,氘交换速率较快。牛血小板因子4的His-38的1H-核磁共振共振峰在引入肝素后优先受到干扰。这一观察结果以及His-38存在于血小板因子4四聚体周围带正电荷的残基区域内,支持了血小板因子4-肝素复合物的模型,即多糖以直角穿过2个二聚体的2个α-螺旋中的每一个。

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