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Enhanced Nitrite Reductase Activity and Its Correlation with Oxygen Affinity in Hemoglobin Bis-Tetramers
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  • 作者:Aizhou Wang ; Ronald Kluger
  • 刊名:Biochemistry
  • 出版年:2016
  • 出版时间:August 23, 2016
  • 年:2016
  • 卷:55
  • 期:33
  • 页码:4688-4696
  • 全文大小:499K
  • 年卷期:0
  • ISSN:1520-4995
文摘
The vasoactivity of circulating cross-linked hemoglobin is consistent with the acellular protein penetrating the endothelial lining of blood vessels where hemoglobin can bind nitric oxide, the signal for relaxation of the muscles that surround blood vessels. In an important contrast, derivatives of bis-tetramers that are produced from hemoglobin by chemical coupling do not cause vasoconstriction in animal models. Presumably, they are unable to enter the endothelia where hemoglobin tetramers bind to nitric oxide. In addition, hemoglobin bis-tetramers can produce nitric oxide in circulation through their intrinsic nitrite reductase activity. Examination of this activity for hemoglobin-derived bis-tetramers that are acetylated at lysyl amino groups in their α subunits reveals enhanced activity (k = 2.21 M–1 s–1) compared to that of nonacetylated bis-tetramers (k = 0.70 M–1 s–1). Plots of nitrite reductase activities as a function of the corresponding oxygen affinities of certain allosteric-state-stabilized derivatives reveal a significant correlation, providing a basis for interpretation of the correlated functions.

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