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用于高效渗透和靶向递送溶栓剂的细菌驱动微管马达

Bacteria-propelled microtubular motors for efficient penetration and targeting delivery of thrombolytic agents.

作者信息

Xie Songzhi, Mo Chuanfei, Cao Wenxiong, Xie Shuang, Li Shang, Zhang Zhanlin, Li Xiaohong

机构信息

Key Laboratory of Advanced Technologies of Materials, Ministry of Education, School of Materials Science and Engineering, Southwest Jiaotong University, Chengdu 610031, PR China; Key Laboratory for Meat Processing of Sichuan Province, School of Food and Biological Engineering, Chengdu University, Chengdu 610106, PR China.

Key Laboratory of Advanced Technologies of Materials, Ministry of Education, School of Materials Science and Engineering, Southwest Jiaotong University, Chengdu 610031, PR China.

出版信息

Acta Biomater. 2022 Apr 1;142:49-59. doi: 10.1016/j.actbio.2022.02.008. Epub 2022 Feb 11.

DOI:10.1016/j.actbio.2022.02.008
PMID:35158079
Abstract

Effective thrombolysis is critical to rapidly rebuild blood flow for thrombosis patients. Drug delivery systems have been developed to address inadequate pharmacokinetics of thrombolytic agents, but challenges still remain in the timely removal of blood clots regarding the dense fibrin networks. Herein, rod-shaped tubular micromotors were developed to achieve efficient penetration and thorough destruction of thrombi. By using electrospun fiber fragments as the template, urokinase (uPA)-loaded polydopamine (PDA) microtubes with surface decorated fucoidan (PDA) were prepared at the aspect ratio of around 2. One E. coli Nissle 1917 (EcN) was assembled into one microtube to construct a PDA@EcN hybrid micromotor through PDA adhesion and L-aspartate induction. The pharmacokinetic analysis indicates that the encapsulation of uPA into micromotors extends the half-life from 0.4 to 5.6 h and increases the bioavailability over 10 times. EcN-propelled motion elevates adsorption capacities of PDA@EcN for more than four times compared with that of PDA. The fucoidan-mediated targeting causes 2-fold higher thrombolysis capacity in vitro and over 10-fold higher uPA accumulation in thrombi in vivo. In the treatment of venous thrombi at mouse hindlimbs, intravenous administration of PDA@EcN completely removed blood clots with almost full recovery of blood flows and apparently alleviated tail bleeding. It should be noted that PDA@EcN treatment at a reduced uPA dose caused no significant difference in the blood flow rate compared with those of PDA. The synergistic action of fucoidan-induced targeting and EcN-driven motion provides a prerequisite for promoting thrombolytic efficacy and reducing uPA dose and bleeding side effect. STATEMENT OF SIGNIFICANCE: The standard treatment to thrombosis patient is intravenous infusion of thrombolytic agents, but the associated bleeding complications and impairment of normal haemostasis greatly offset the therapeutic benefits. Drug delivery systems have been developed to address the limitations of inadequate pharmacokinetics of thrombolytic agents, but challenges still exist in less efficient penetration into dense networks for thorough destruction of thrombi. Up to now only few attempts have been made to construct nano-/micromotors for combating thrombosis and there is no single case that antithrombosis is assisted by bacteria or cells-propelled motors. Herein, bacteria-propelled microtubes were developed to carry urokinase for efficient penetration into blood clots and effective thrombolysis. The synergistic action of bacteria-driven motion and specific ligand-induced targeting holds a promising treatment strategy for life-threatening cardiovascular diseases such as thrombosis and atherosclerosis.

摘要

有效的溶栓治疗对于迅速恢复血栓形成患者的血流至关重要。已经开发了药物递送系统来解决溶栓剂药代动力学不足的问题,但在及时清除由致密纤维蛋白网络构成的血栓方面仍然存在挑战。在此,开发了棒状管状微马达以实现对血栓的有效穿透和彻底破坏。以电纺纤维片段为模板,制备了表面修饰有岩藻依聚糖的负载尿激酶(uPA)的聚多巴胺(PDA)微管,长径比约为2。将一株大肠杆菌Nissle 1917(EcN)组装到一根微管中,通过PDA粘附和L-天冬氨酸诱导构建PDA@EcN混合微马达。药代动力学分析表明,将uPA封装到微马达中可将半衰期从0.4小时延长至5.6小时,并使生物利用度提高10倍以上。EcN驱动的运动使PDA@EcN的吸附能力比PDA提高了四倍以上。岩藻依聚糖介导的靶向作用在体外使溶栓能力提高了2倍,在体内使血栓中的uPA积累增加了10倍以上。在治疗小鼠后肢静脉血栓时,静脉注射PDA@EcN可完全清除血栓,血流几乎完全恢复,并明显减轻尾部出血。需要注意的是,在降低uPA剂量的情况下进行PDA@EcN治疗,与PDA治疗相比,血流速度没有显著差异。岩藻依聚糖诱导的靶向作用和EcN驱动的运动的协同作用为提高溶栓疗效、降低uPA剂量和出血副作用提供了前提条件。重要意义声明:对血栓形成患者的标准治疗是静脉输注溶栓剂,但相关的出血并发症和正常止血功能的损害大大抵消了治疗益处。已经开发了药物递送系统来解决溶栓剂药代动力学不足的局限性,但在有效穿透致密网络以彻底破坏血栓方面仍然存在挑战。到目前为止,只有少数尝试构建用于对抗血栓形成的纳米/微马达,并且没有单个案例表明抗血栓形成是由细菌或细胞驱动的马达辅助的。在此,开发了细菌驱动的微管来携带尿激酶,以有效穿透血栓并进行有效的溶栓治疗。细菌驱动的运动和特异性配体诱导的靶向作用的协同作用为治疗危及生命的心血管疾病(如血栓形成和动脉粥样硬化)提供了一种有前景的治疗策略。

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