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纤维蛋白凝块的流变学。III. 细结扎和粗未结扎凝块的剪切蠕变和蠕变恢复

Rheology of fibrin clots. III. Shear creep and creep recovery of fine ligated and coarse unligated closts.

作者信息

Nelb G W, Gerth C, Ferry J D

出版信息

Biophys Chem. 1976 Sep;5(3):377-87. doi: 10.1016/0301-4622(76)80050-6.

Abstract

Creep and creep recovery of human fibrin clots in small shearing deformations have been investigated over a time scale from 24 to 10(4) s. Coarse, unligated clots and fine clots ligated by fibrinoligase in the presence of calcium ions were studied to suppliement previous data on coarse ligated and fine unligated clots. Stress was found to be proportional to strain up to at least a maximum shear strain (in torsion geometry) of 6.2%. The initial modulus (25 s after imposition of stress) is proportional to approximately the 1.5 power of concentration for fine ligated and coarse unligated clots. For fine unligated closts there is comparatively little creep subsequent to the initial deformation; ligation (in this case involving mostly the gamma chains) reduces the creep to nearly zero. For coarse unligated clots, there is substantially more creep under constant stress, and creep recovery is not complete. Ligation (in this case involving both camma and alpha chains) alrgely supresses the creep and causes the recovery to be complete. If the structure if fully formed before creep begins, tests of creep recovery by the Boltzmann superposition principle show adherence to linear visoelastic behavior for all four clot types. Otherwise, the Boltzmann test fails and the recovery is much less than calculated. For fine ligated clots, the observed recovery agrees well with that calculated on the basis of a dual structure model in which an additional independent structure is built up in the deformed state, so that the state of ease after removal of stress is a balance between two structures deformed in opposite senses. It is postulated that the coherence and elastic modulus of the fine ligated clot are largely due to steric blocking of long protofibrils with a high flexural stiffness. In the coarse clot, it is proposed that the structure involves extensive branching of thick bundles of protofibrils, which become permanently secured by the ligation of the alpha chains of the fibrin.

摘要

在24秒至10⁴秒的时间尺度上,研究了人体纤维蛋白凝块在小剪切变形下的蠕变和蠕变恢复情况。研究了粗的、未结扎的凝块以及在钙离子存在下由纤维蛋白连接酶结扎的细凝块,以补充先前关于粗结扎和细未结扎凝块的数据。发现在至少高达6.2%的最大剪切应变(在扭转几何形状中)时,应力与应变成正比。对于细结扎和粗未结扎凝块,初始模量(施加应力后25秒)与浓度的约1.5次方成正比。对于细未结扎凝块,初始变形后蠕变相对较小;结扎(在这种情况下主要涉及γ链)将蠕变降低到几乎为零。对于粗未结扎凝块,在恒定应力下蠕变要大得多,并且蠕变恢复不完全。结扎(在这种情况下涉及γ链和α链)基本上抑制了蠕变并使恢复完全。如果在蠕变开始前结构已完全形成,通过玻尔兹曼叠加原理进行的蠕变恢复测试表明,所有四种凝块类型均符合线性粘弹性行为。否则,玻尔兹曼测试失败,恢复远小于计算值。对于细结扎凝块,观察到的恢复与基于双结构模型计算的结果非常吻合,在该模型中,在变形状态下形成了额外的独立结构,因此去除应力后的松弛状态是两种相反方向变形的结构之间的平衡。据推测,细结扎凝块的凝聚性和弹性模量很大程度上归因于具有高弯曲刚度的长原纤维的空间位阻。在粗凝块中,提出其结构涉及原纤维粗束的广泛分支,这些分支通过纤维蛋白α链的结扎而永久固定。

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