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天然纤维蛋白凝胶网络及其在健康和疾病中影响其形成的因素。

Native fibrin gel networks and factors influencing their formation in health and disease.

作者信息

Blombäck B, Banerjee D, Carlsson K, Hamsten A, Hessel B, Procyk R, Silveira A, Zacharski L

机构信息

Karolinska Institutet, Stockholm, Sweden.

出版信息

Adv Exp Med Biol. 1990;281:1-23. doi: 10.1007/978-1-4615-3806-6_1.

Abstract

Hydrated fibrin gels were studied by confocal laser 3D microscopy, liquid permeation and turbidity. The gels from normal fibrinogen were found to be composed of straight rod-like fiber elements which sometimes originated from denser nodes. In gels formed at increasing thrombin or fibrinogen concentrations, the gel networks became tighter and the porosity decreased. The fiber strands also became shorter. Gel porosity of the network decreased dramatically in gels formed at increasing ionic strengths. Shortening of the fibers were observed and fiber swelling occurred at ionic strength above 0.24. Albumin and dextran, when present in the gel forming system, affected the formation of more porous structures with strands of larger mass-length ratio and fiber thickness. This type of gels were also formed in plasma. Albumin and lipoproteins may be among the determinants for the formation of this type of gel structure in plasma. Gels formed when factor XIIIa instead of thrombin was used as catalyst for gelation showed a completely different structure in which lumps of polymeric material were held together by a network of fine fiber strands. Our studies have also shown that the methodologies employed may be useful in studies of gel structures in certain dysfibrinogenemias as well as in other diseases. We give examples of two patients with abnormal fibrinogen and of patients with ischaemic heart disease.

摘要

通过共聚焦激光三维显微镜、液体渗透和浊度研究了水合纤维蛋白凝胶。发现来自正常纤维蛋白原的凝胶由直的棒状纤维元件组成,这些元件有时起源于较致密的节点。在凝血酶或纤维蛋白原浓度增加时形成的凝胶中,凝胶网络变得更紧密,孔隙率降低。纤维束也变得更短。在离子强度增加时形成的凝胶中,网络的凝胶孔隙率急剧下降。在离子强度高于0.24时观察到纤维缩短且纤维发生肿胀。白蛋白和右旋糖酐存在于凝胶形成系统中时,会影响形成具有更大质量-长度比的链和纤维厚度的更多孔结构。这种类型的凝胶也在血浆中形成。白蛋白和脂蛋白可能是血浆中这种类型凝胶结构形成的决定因素之一。当使用因子XIIIa而不是凝血酶作为凝胶化催化剂时形成的凝胶显示出完全不同的结构,其中聚合物材料块由细纤维束网络连接在一起。我们的研究还表明,所采用的方法可能有助于研究某些异常纤维蛋白原血症以及其他疾病中的凝胶结构。我们给出了两名纤维蛋白原异常患者和缺血性心脏病患者的例子。

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