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Preclinical Evaluation and Monitoring of the Therapeutic Response of a Dual Targeted Hyaluronic Acid Nanodrug

机译:双靶透明质酸纳米药物的治疗反应的临床前评估和监测

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摘要

Chemotherapy is a powerful cancer treatment but suffers from poor biocompatibility and a lack of tumor targeting. Here, we developed a CD44-targeted polymeric nanocomplex by encapsulating 10-hydroxycamptothecin (HCPT) into hyaluronic acid nanoparticles (HANP) for targeted cancer therapy. In vitro, the HANP/HCPT showed improved cytotoxicity to five cancer cell lines including HT29, A549, MDA-MB-231, HepG2, and MDA-MB-435 versus free HCPT. After systemic administration into MDA-MB-231 breast cancer xenograft, tumor growth was significantly inhibited 5.25 ± 0.21 times in the HANP/HCPT treated group relative to the nontreated group. In addition, the treatment response was also accessed and confirmed by 18F-fluoro-2-deoxy-D-glucose ([18F] FDG) positron emission tomography (PET). The MDA-MB-231 tumors responded to HANP/HCPT 7 days after the first treatment, which benefits treatment strategy adjustment and personalization. No apparent systemic toxic effects were seen in mice treated with HANP/HCPT. In summary, the HANPs have great promise as a targeted drug carrier for cancer chemotherapy. Our HANP platform can also deliver other hydrophobic chemotherapy agents.
机译:化学疗法是一种强有力的癌症治疗方法,但其生物相容性差且缺乏靶向肿瘤的能力。在这里,我们通过将10-羟基喜树碱(HCPT)封装到透明质酸纳米颗粒(HANP)中用于靶向癌症治疗,开发了靶向CD44的聚合物纳米复合物。在体外,与游离HCPT相比,HAMP / HCPT对包括HT29,A549,MDA-MB-231,HepG2和MDA-MB-435在内的五种癌细胞系表现出改善的细胞毒性。全身性施用于MDA-MB-231乳腺癌异种移植后,相对于未治疗组,在HANP / HCPT治疗组中,肿瘤生长被显着抑制了5.25±0.21倍。此外,还可以通过18F-氟-2-脱氧-D-葡萄糖([18F] FDG)正电子发射断层显像(PET)获得并确认治疗反应。首次治疗后7天,MDA-MB-231肿瘤对HANP / HCPT有反应,这有利于治疗策略的调整和个性化。在用HANP / HCPT处理的小鼠中未观察到明显的全身毒性作用。总之,HANP作为癌症化学疗法的靶向药物载体具有广阔的前景。我们的HANP平台还可以提供其他疏水化学治疗剂。

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