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首页> 外文期刊>Journal of vascular surgery >Preparation and characterization of injectable fibrillar type I collagen and evaluation for pseudoaneurysm treatment in a pig model.
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Preparation and characterization of injectable fibrillar type I collagen and evaluation for pseudoaneurysm treatment in a pig model.

机译:注射型I型胶原纤维的制备,表征以及在猪模型中对假性动脉瘤的评价。

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OBJECTIVE: Despite the efficacy of collagen in femoral artery pseudoaneurysm treatment, as reported in one patient study, its use has not yet gained wide acceptance in clinical practice. In this particular study, the collagen was not described in detail. To further investigate the potential of collagen preparations, we prepared and characterized highly purified injectable fibrillar type I collagen and evaluated its use for femoral artery pseudoaneurysm (PSA) treatment in vivo using a pig model. METHODS: Purified fibrillar type I collagen was characterized using electron microscopy. The effect of three different sterilization procedures, ie, hydrogen peroxide gas plasma (H2O2), ethylene oxide gas (EtO), and gamma irradiation, was studied on both SDS-PAGE and platelet aggregation. Different collagen injectables were prepared (3%, 4%, and 5%) and tested using an injection force test applying a 21-gauge needle. To evaluate the network characteristics of the injectable collagen, the collagen was suspended in phosphate buffered saline (PBS) at 37 degrees C and studied both macroscopically and electron microscopically. To determine whether the collagen induced hemostasis in vivo, a pig PSA model was used applying a 4% EtO sterilized collagen injectable, and evaluation by angiography and routine histology. RESULTS: Electron microscopy of the purified type I collagen revealed intact fibrils with a distinct striated pattern and a length<300 mum. Both SDS-PAGE and platelet aggregation analysis of the sterilized collagen indicated no major differences between EtO and H2O2 sterilization, although gamma-irradiated collagen showed degradation products. Both 3% and 4% (w/v) collagen suspensions were acceptable with respect to the force used (<50 N). The 4% suspension was selected as the preferred injectable collagen, which formed a dense network under physiologic conditions. Testing the collagen in vivo (n=5), the angiograms revealed that the PSA partly or completely coagulated. Histology confirmed the network formation, which was surrounded by thrombus. CONCLUSIONS: Collagen injectables were prepared and EtO sterilized without major loss of structural integrity and platelet activity. In vivo, the injectable collagen formed a dense network and triggered (partial) local hemostasis. Although optimization is needed, an injectable collagen may be used as a therapeutic agent for femoral PSA treatment.
机译:目的:正如一项患者研究中报道的那样,尽管胶原蛋白在股动脉假性动脉瘤治疗中具有疗效,但其使用尚未在临床上得到广泛接受。在此特定研究中,没有详细描述胶原蛋白。为了进一步研究胶原蛋白制剂的潜力,我们制备并表征了高度纯化的注射型I型纤维状胶原蛋白,并使用猪模型评估了其在体内股动脉假性动脉瘤(PSA)治疗中的用途。方法:使用电子显微镜对纯化的I型原纤维胶原进行表征。在SDS-PAGE和血小板凝集上,研究了三种不同的灭菌程序,即过氧化氢气体血浆(H2O2),环氧乙烷气体(EtO)和伽马射线辐照的影响。制备了不同的胶原蛋白注射剂(3%,4%和5%),并使用21号针头通过注射力测试进行了测试。为了评估可注射胶原蛋白的网络特性,将胶原蛋白悬浮在37摄氏度的磷酸盐缓冲盐水(PBS)中,并进行肉眼和电子显微镜研究。为了确定胶原蛋白是否在体内引起止血,使用猪PSA模型,该模型应用了4%EtO无菌胶原蛋白注射剂,并通过血管造影和常规组织学评估。结果:纯化的I型胶原的电子显微镜显示完整的原纤维,具有明显的条纹图案,长度<300μm。无菌胶原蛋白的SDS-PAGE和血小板聚集分析均显示EtO和H2O2灭菌之间没有重大差异,尽管伽玛射线辐照的胶原蛋白显示降解产物。就所使用的力(<50 N)而言,3%和4%(w / v)的胶原蛋白悬浮液都是可以接受的。选择4%悬浮液作为优选的可注射胶原蛋白,其在生理条件下形成致密的网络。在体内测试胶原蛋白(n = 5)时,血管造影显示PSA部分或完全凝结。组织学证实了网络形成,其被血栓包围。结论:制备了胶原蛋白注射液并进行了EtO灭菌,而结构完整性和血小板活性没有重大损失。在体内,可注射的胶原蛋白形成密集的网络并触发(部分)局部止血。尽管需要优化,但是可注射的胶原可以用作股骨PSA治疗的治疗剂。

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