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纤维蛋白模型。

Models of fibrin.

作者信息

Hermans J

出版信息

Proc Natl Acad Sci U S A. 1979 Mar;76(3):1189-93. doi: 10.1073/pnas.76.3.1189.

Abstract

High-symmetry models of the fibrin fiber are proposed that reproduce the experimentally observed high specific volume of the fiber. The models meet the following criteria: fibrin monomers have the three-domain Hall and Slayter structure; the monomers are arranged lengthwise into strands (protofibrils) in which successive monomers half overlap; the monomers' alignment is nearly parallel to the fiber axis; and the monomers make adequate longitudinal and lateral contacts, as required by observed fiber properties and the high affinity of monomers for one another. All the models contain helical protofibrils related to each other by rotation axes parallel to the fiber axis; as a consequence the protofibrils are in register in the fiber direction. The protofibrils may contain two, three, or four monomers per helical turn and can be packed in four different symmetries (space groups). A large specific volume is achieved only if the D-domain (which are presumed to contain the lateral polymerization sites) are somewhat displaced from the helical axes of the protofibrils. This displacement may involve either a lateral shift of the monomers away from the helix axis or a tilt of the monomers, which swings the D-domains away from the helix axis. It is shown that the fiber containing tilted monomers is more highly interconnected; the two D-domains of each tilted monomer form lateral contacts with different adjacent protofibrils, whereas the two D-domains of each nontilted monomer contact the same adjacent protofibril(s).

摘要

提出了纤维蛋白纤维的高对称模型,该模型再现了实验观察到的纤维的高比容。这些模型满足以下标准:纤维蛋白单体具有三结构域的霍尔和斯莱特结构;单体沿长度方向排列成链(原纤维),其中连续的单体半重叠;单体的排列几乎与纤维轴平行;并且单体如观察到的纤维特性和单体之间的高亲和力所要求的那样,进行了充分的纵向和横向接触。所有模型都包含通过平行于纤维轴的旋转轴相互关联的螺旋原纤维;因此,原纤维在纤维方向上是对齐的。每个螺旋圈中原纤维可能包含两个、三个或四个单体,并且可以以四种不同的对称性(空间群)堆积。只有当D结构域(假定包含横向聚合位点)从原纤维的螺旋轴上稍有位移时,才能实现大的比容。这种位移可能涉及单体从螺旋轴的横向移动或单体的倾斜,从而使D结构域远离螺旋轴。结果表明,含有倾斜单体的纤维具有更高的相互连接性;每个倾斜单体的两个D结构域与不同的相邻原纤维形成横向接触,而每个未倾斜单体的两个D结构域与相同的相邻原纤维接触。

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本文引用的文献

1
The Mechanism of Polymerization of Fibrinogen.纤维蛋白原的聚合机制
Proc Natl Acad Sci U S A. 1952 Jul;38(7):566-9. doi: 10.1073/pnas.38.7.566.
2
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Tropomyosin crystal dynamics.原肌球蛋白晶体动力学。
Cold Spring Harb Symp Quant Biol. 1972;36:205-16. doi: 10.1101/sqb.1972.036.01.028.
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The fine structure of fibrin.
Br J Haematol. 1967 May;13(3):341-7. doi: 10.1111/j.1365-2141.1967.tb08749.x.
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Crystalline states of a modified fibrinogen.一种改性纤维蛋白原的晶体状态。
J Mol Biol. 1977 Feb 25;110(2):363-85. doi: 10.1016/s0022-2836(77)80077-6.

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