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可生物降解栓塞微球的体外和体内评估及其可调节的抗癌药物释放。

In vitro and in vivo evaluation of biodegradable embolic microspheres with tunable anticancer drug release.

机构信息

Department of Radiology, University of Minnesota, Minneapolis, MN 55455, USA.

出版信息

Acta Biomater. 2013 Jun;9(6):6823-33. doi: 10.1016/j.actbio.2013.02.017. Epub 2013 Feb 16.

DOI:10.1016/j.actbio.2013.02.017
PMID:23419554
Abstract

Natural polymer-derived materials have attracted increasing interest in the biomedical field. Polysaccharides have obvious advantages over other polymers employed for biomedical applications due to their exceptional biocompatibility and biodegradability. None of the spherical embolic agents used clinically is biodegradable. In the current study, microspheres prepared from chitosan and carboxymethyl cellulose (CMC) were investigated as a biodegradable embolic agent for arterial embolization applications. Aside from the enzymatic degradability of chitosan units, the cross-linking bonds in the matrix, Schiff bases, are susceptible to hydrolytic cleavage in aqueous conditions, which would overcome the possible shortage of enzymes inside the arteries. The size distribution, morphology, water retention capacity and degradability of the microspheres were found to be affected by the modification degree of CMC. An anticancer drug, doxorubicin, was successfully incorporated into these microspheres for local release and thus for killing cancerous cells. These microspheres demonstrated controllable degradation time, variable swelling and tunable drug release profiles. Co-culture with human umbilical vein endothelial cells revealed non-cytotoxic nature of these microspheres compared to monolayer control (P>0.95). In addition, a preliminary study on the in vivo degradation of the microspheres (100-300μm) was performed in a rabbit renal embolization model, which demonstrated that the microspheres were compatible with microcatheters for delivery, capable of occluding the arteries, and biodegradable inside arteries. These microspheres with biodegradability would be promising for embolization therapies.

摘要

天然聚合物衍生材料在生物医学领域引起了越来越多的关注。多糖由于其优异的生物相容性和可生物降解性,相对于其他用于生物医学应用的聚合物具有明显的优势。目前临床使用的球形栓塞剂中没有可生物降解的。在本研究中,研究了壳聚糖和羧甲基纤维素(CMC)制备的微球作为动脉栓塞应用的可生物降解栓塞剂。除了壳聚糖单元的酶降解性外,基质中的交联键,希夫碱,在水条件下易发生水解断裂,这将克服动脉内可能缺乏酶的问题。微球的粒径分布、形态、保水能力和降解性受 CMC 修饰程度的影响。将抗癌药物阿霉素成功地包裹在这些微球中,以实现局部释放,从而杀死癌细胞。这些微球表现出可控的降解时间、可变的溶胀和可调的药物释放特性。与人脐静脉内皮细胞共培养表明,与单层对照相比(P>0.95),这些微球具有非细胞毒性。此外,还在兔肾栓塞模型中对微球(100-300μm)的体内降解进行了初步研究,结果表明,这些微球与微导管输送相容,能够闭塞动脉,并在动脉内可生物降解。这些具有生物降解性的微球有望用于栓塞治疗。

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