Weems Andrew C, Wacker Kevin T, Carrow James K, Boyle Anthony J, Maitland Duncan J
Department of Biomedical Engineering, Texas A&M University, College Station, TX 77843-3120, USA.
Department of Chemistry, Texas A&M University, College Station, TX 77843-3120, USA.
Acta Biomater. 2017 Sep 1;59:33-44. doi: 10.1016/j.actbio.2017.06.030. Epub 2017 Jun 21.
The synthesis of thermoset shape memory polymer (SMP) polyurethanes from symmetric, aliphatic alcohols and diisocyanates has previously demonstrated excellent biocompatibility in short term in vitro and in vivo studies, although long term stability has not been investigated. Here we demonstrate that while rapid oxidation occurs in these thermoset SMPs, facilitated by the incorporation of multi-functional, branching amino groups, byproduct analysis does not indicate toxicological concern for these materials. Through complex multi-step chemical reactions, chain scission begins from the amines in the monomeric repeat units, and results, ultimately, in the formation of carboxylic acids, secondary and primary amines; the degradation rate and product concentrations were confirmed using liquid chromatography mass spectrometry, in model compound studies, yielding a previously unexamined degradation mechanism for these biomaterials. The rate of degradation is dependent on the hydrogen peroxide concentration, and comparison of explanted samples reveals a much slower rate in vivo compared to the widely accepted literature in vitro real-time equivalent of 3% HO. Cytotoxicity studies of the material surface, and examination of the degradation product accumulations, indicate that degradation has negligible impact on cytotoxicity of these materials.
This paper presents an in-depth analysis on the degradation of porous, shape memory polyurethanes (SMPs), including traditional surface characterization as well as model degradation compounds with absolute quantification. This combination of techniques allows for determination of rates of degradation as well as accumulation of individual degradation products. These behaviors are used for in vivo-in vitro comparisons for determination of real time degradation rates. Previous studies have primarily been limited to surface characterization without examination of degradation products and accumulation rates. To our knowledge, our work presents a unique example where a range of material scales (atomistic-scale model compounds along with macroscopic porous SMPs) are used in conjunction with ex planted samples for calculation of degradation rates and toxicological risk.
先前已证明,由对称脂肪族醇和二异氰酸酯合成的热固性形状记忆聚合物(SMP)聚氨酯在短期体外和体内研究中具有出色的生物相容性,尽管尚未研究其长期稳定性。在此我们证明,虽然这些热固性SMP中会发生快速氧化,这是由多功能支链氨基的引入所促进的,但副产物分析并未表明这些材料存在毒理学问题。通过复杂的多步化学反应,链断裂从单体重复单元中的胺开始,最终导致羧酸、仲胺和伯胺的形成;在模型化合物研究中,使用液相色谱质谱法确认了降解速率和产物浓度,从而得出了这些生物材料此前未被研究过的降解机制。降解速率取决于过氧化氢浓度,对取出样本的比较显示,与广泛接受的体外实时等效3%过氧化氢的文献相比,体内降解速率要慢得多。对材料表面的细胞毒性研究以及对降解产物积累的检查表明,降解对这些材料的细胞毒性影响可忽略不计。
本文对多孔形状记忆聚氨酯(SMP)的降解进行了深入分析,包括传统的表面表征以及具有绝对定量的模型降解化合物。这些技术的结合能够确定降解速率以及各个降解产物的积累情况。这些行为被用于体内 - 体外比较,以确定实时降解速率。先前的研究主要局限于表面表征,而未检查降解产物和积累速率。据我们所知,我们的工作提供了一个独特的例子,即一系列材料尺度(原子尺度的模型化合物以及宏观多孔SMP)与取出样本结合使用,以计算降解速率和毒理学风险。
