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对稀释的人类胚胎血红蛋白进行凝胶过滤揭示了其氧结合增加的基础。

Gel filtration of dilute human embryonic hemoglobins reveals basis for their increased oxygen binding.

作者信息

Manning Lois R, Popowicz Anthony M, Padovan Julio C, Chait Brian T, Manning James M

机构信息

Department of Biology, Northeastern University, Boston, MA 02115, USA.

Information Technology, The Rockefeller University, New York, NY 10065, USA.

出版信息

Anal Biochem. 2017 Feb 15;519:38-41. doi: 10.1016/j.ab.2016.12.008. Epub 2016 Dec 11.

Abstract

This report establishes a correlation between two known properties of the human embryonic hemoglobins-- their weak subunit assemblies as demonstrated here by gel filtration at very dilute protein concentrations and their high oxygen affinities and reduced cooperativities reported previously by others but without a mechanistic basis. We demonstrate here that their high oxygen affinities are a consequence of their weak assemblies. Weak vs strong hemoglobin tetramers represent a regulatory mechanism to modulate oxygen binding capacity by altering the equilibrium between the various steps in the assembly process that can be described as an inverse allosteric effect.

摘要

本报告建立了人类胚胎血红蛋白两个已知特性之间的关联——在此通过在极低蛋白质浓度下的凝胶过滤所证明的其弱亚基组装,以及先前其他人报道的但无机制基础的高氧亲和力和降低的协同性。我们在此证明,它们的高氧亲和力是其弱组装的结果。弱血红蛋白四聚体与强血红蛋白四聚体代表了一种调节机制,通过改变组装过程中各个步骤之间的平衡来调节氧结合能力,这一过程可被描述为一种反向变构效应。

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本文引用的文献

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Intrinsic regulation of hemoglobin expression by variable subunit interface strengths.
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