Aim: Tumor cell-derived microparticles (MP) can function as a targeted delivery carrier for anti-tumor drugs. Here, we aimed to generate paclitaxel-loaded microparticles (MP-PTX) from HeLa cells and examined its therapeutic potential on human cervical carcinoma. Methods: MP-PTX was generated from HeLa cells by ultraviolet radiation and subsequent centrifugation. The particle size, drug loading rate, and stability of MP-PTX were examined in vitro. Flow cytometry and the MTT assay were performed to test the inhibitory effect of MP-PTX using different cell lines. Immunodeficient mice bearing HeLa cervical carcinoma were treated with 0.9% normal saline, MP, paclitaxel (PTX) (2.5 mg/kg), or MP-PTX (PTX content identical to PTX group) every day for 6 consecutive days. Tumor volume and animal survival were observed. Micro 18 F-FDG PET/CT was performed to monitor the therapeutic efficacy. The proliferation activity of cells and microvessel density in tumor tissues were determined by immunohistochemical staining using Ki-67 and CD31, respectively. Results: Dynamic laser scattering measurements showed that the particle size of MP-PTX was 285.58 ± 2.95 nm and the polydispersity index was 0.104 ± 0.106. And the particle size of MP-PTX was not change at 4°C for at least one week. More than 1% of PTX in the medium could be successfully encapsulated into HeLa cell-derived MP. When compared with PTX, MP-PTX treatment significantly increased apoptosis of tumor cells and reduced their proliferation. In addition, MP-PTX showed lower toxicity to normal human umbilical vein endothelial cells (HUVEC) than PTX. In vivo studies further demonstrated that MP-PTX treatment significantly inhibited the growth of cervical carcinoma, prolonged the survival of tumor-bearing mice, and reduced the toxicity of PTX. Immunohistochemical staining revealed that MP-PTX treatment led to decreased Ki-67 positive tumor cells and decreased microvessel density in tumor tissues. Conclusion: Our results demonstrated that HeLa-derived MP-PTX significantly enhanced the anti-cancer effects of PTX with reduced toxicity, which may provide a novel strategy for the treatment of cervical carcinoma.
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机译:目的:肿瘤细胞衍生的微粒(MP)可以用作抗肿瘤药物的靶向递送载体。在此,我们旨在从HeLa细胞产生紫杉醇负载的微粒(MP-PTX),并检查其对人宫颈癌的治疗潜力。方法:通过紫外线辐射和随后的离心从HeLa细胞产生MP-PTX。在体外检查MP-PTX的粒度,药物加载速率和稳定性。进行流式细胞术和MTT测定以测试使用不同细胞系的MP-PTX的抑制作用。连续6天每天用0.9%正常的盐水,MP,紫杉醇(PTX)(2.5mg / kg)或MP-PTX(PTX含量相同的PTX含量相同的PTX含量)处理免疫缺陷小鼠。观察到肿瘤体积和动物存活。进行MICR 18 F-FDG PET / CT以监测治疗效果。通过使用Ki-67和CD31分别通过免疫组织化学染色测定肿瘤组织中细胞和微血管密度的增殖活性。结果:动态激光散射测量表明,MP-PTX的粒度为285.58±2.95nm,多分散指数为0.104±0.106。 MP-PTX的粒度在4℃下不变至少一周。培养基中的超过1%的PTX可以成功封装到HeLa细胞衍生的MP中。与PTX相比,MP-PTX治疗显着增加了肿瘤细胞的凋亡并降低了它们的增殖。此外,MP-PTX对正常人脐静脉内皮细胞(HUVEC)显示出低于PTX的毒性较低。在体内研究进一步证明了MP-PTX治疗显着抑制宫颈癌的生长,延长了肿瘤小鼠的存活,并降低了PTX的毒性。免疫组织化学染色表明,MP-PTX处理导致肿瘤组织中的ki-67阳性肿瘤细胞减少,微血管密度降低。结论:我们的研究结果表明,HeLa衍生的MP-PTX显着提高了PTX的毒性降低的抗癌作用,这可能为治疗宫颈癌提供新的策略。
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