Vogler E A, Graper J C, Harper G R, Sugg H W, Lander L M, Brittain W J
Becton Dickinson Research Center, Research Triangle Park, North Carolina 27709, USA.
J Biomed Mater Res. 1995 Aug;29(8):1005-16. doi: 10.1002/jbm.820290813.
Contact activation of the intrinsic pathway of porcine blood plasma coagulation is shown to be a steep exponential-like function of procoagulant surface energy, with low activation observed for poorly water-wettable surfaces and very high activation for fully water-wettable surfaces. Test procoagulants studied were a system of oxidized polystyrene films with varying wettability (surface energy) and glass discs bearing close-packed self-assembled silane monolayers (SAMs) with well-defined chemistry consisting of 12 different terminating chemical functionalities. A monotonic trend of increasing coagulation activation with increasing water wettability was observed for the oxidized polystyrene system whereas results with SAM procoagulants suggested a level of chemical specificity over and above the surface energy trend. In particular, it was noted that coagulation activation by SAMs terminated with--CO2H was much higher than anticipated based on surface wettability whereas--NH3(+)-terminated SAMs exhibited very low procoagulant activity. SAMs terminated in--(CH2)2(CF2)7CF3 behaved as anticipated based on surface energy with very low procoagulant activity and did not exhibit special properties sometimes attributed to perfluorinated compounds. Quantitative ranking of the inherent coagulation activation properties of procoagulant surfaces was obtained by application of a straightforward phenomenological model expressed in a closed-form mathematical equation relating coagulation time to procoagulant surface area. Fit of the model with a single adjustable parameter to experimental measurements of porcine platelet-poor plasma coagulation time was very good, implying that assertions and simplifications of the model adequately simulated reality. Two important propositions of the model were that (1) the number of putative "activating sites" scaled linearly with procoagulant surface area, and (2) contact activation of the plasma coagulation cascade was catalytic in the sense that these activating sites were not consumed or "poisoned" by irreversible or slowly reversible protein adsorption during coagulation. An extension of the coagulation model proposed that procoagulant activation properties scale exponentially with the surface density of polar (acid-base) sites, which, in turn, was related to procoagulant wettability.
猪血浆凝血内源性途径的接触激活表现为促凝表面能的陡峭指数样函数,对于水可润湿性差的表面观察到低激活,而对于完全水可润湿性的表面则观察到非常高的激活。所研究的测试促凝剂是具有不同润湿性(表面能)的氧化聚苯乙烯薄膜系统以及带有紧密堆积的自组装硅烷单层(SAMs)的玻璃盘,这些SAMs具有明确的化学组成,由12种不同的末端化学官能团组成。对于氧化聚苯乙烯系统,观察到随着水润湿性增加凝血激活增加的单调趋势,而SAM促凝剂的结果表明除了表面能趋势之外还有一定程度的化学特异性。特别值得注意的是,以 - CO2H终止的SAMs的凝血激活远高于基于表面润湿性预期的值,而以 - NH3(+)终止的SAMs表现出非常低的促凝活性。以 - (CH2)2(CF2)7CF3终止的SAMs表现出基于表面能预期的非常低的促凝活性,并且没有表现出有时归因于全氟化合物的特殊性质。通过应用一个简单的现象学模型获得促凝表面固有凝血激活特性的定量排名,该模型以将凝血时间与促凝表面积相关联的封闭形式数学方程表示。用单个可调参数的模型对猪贫血小板血浆凝血时间的实验测量进行拟合非常好,这意味着模型的假设和简化充分模拟了实际情况。该模型的两个重要命题是:(1)假定的“激活位点”数量与促凝表面积成线性比例,(2)血浆凝血级联的接触激活是催化性的,即这些激活位点在凝血过程中不会被不可逆或缓慢可逆的蛋白质吸附消耗或“中毒”。所提出的凝血模型的扩展表明,促凝激活特性与极性(酸碱)位点的表面密度成指数比例,而极性位点的表面密度又与促凝润湿性相关。
