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构建基于月桂酸的纳米药物递送系统,用于恢复 5-FU 和 OxPt 对结直肠肿瘤的化疗敏感性并提高其生物相容性。

Engineering lauric acid-based nanodrug delivery systems for restoring chemosensitivity and improving biocompatibility of 5-FU and OxPt against -associated colorectal tumor.

机构信息

State Key Laboratory of Separation Membranes and Membrane Processes, School of Materials Science and Engineering, Tiangong University, Tianjin 300387, China.

Hebei Key Laboratory of Functional Polymers, School of Chemical Engineering and Technology, Hebei University of Technology, Tianjin 300130, China.

出版信息

J Mater Chem B. 2024 Apr 24;12(16):3947-3958. doi: 10.1039/d4tb00103f.


DOI:10.1039/d4tb00103f
PMID:38586917
Abstract

Colorectal cancer (CRC) occurs in the colorectum and ranks second in the global incidence of all cancers, accounting for one of the highest mortalities. Although the combination chemotherapy regimen of 5-fluorouracil (5-FU) and platinum(IV) oxaliplatin prodrug (OxPt) is an effective strategy for CRC treatment in clinical practice, chemotherapy resistance caused by tumor-resided () could result in treatment failure. To enhance the efficacy and improve the biocompatibility of combination chemotherapy, we developed an antibacterial-based nanodrug delivery system for -associated CRC treatment. A tumor microenvironment-activated nanomedicine 5-FU-LA@PPL was constructed by the self-assembly of chemotherapeutic drug derivatives 5-FU-LA and polymeric drug carrier PPL. PPL is prepared by conjugating lauric acid (LA) and OxPt to hyperbranched polyglycidyl ether. In principle, LA is used to selectively combat , inhibit autophagy in CRC cells, restore chemosensitivity of 5-FU as well as OxPt, and consequently enhance the combination chemotherapy effects for -associated drug-resistant colorectal tumor. Both and studies exhibited that the tailored nanomedicine possessed efficient antibacterial and anti-tumor activities with improved biocompatibility and reduced non-specific toxicity. Hence, this novel anti-tumor strategy has great potential in the combination chemotherapy of CRC, which suggests a clinically relevant valuable option for bacteria-associated drug-resistant cancers.

摘要

结直肠癌(CRC)发生在结肠直肠部位,其全球癌症发病率居第二位,死亡率也位居前列。虽然氟尿嘧啶(5-FU)联合铂(IV)奥沙利铂前药(OxPt)的联合化疗方案是临床治疗 CRC 的有效策略,但肿瘤内的 ()引起的化疗耐药会导致治疗失败。为了提高联合化疗的疗效和生物相容性,我们开发了一种基于抗菌的纳米药物递送系统,用于治疗与 相关的 CRC。通过化疗药物衍生物 5-FU-LA 和聚合物药物载体 PPL 的自组装,构建了一种肿瘤微环境激活的纳米药物 5-FU-LA@PPL。PPL 通过将月桂酸(LA)和 OxPt 接枝到超支化聚缩水甘油醚上制备而成。原则上,LA 用于选择性对抗 ,抑制 CRC 细胞中的自噬,恢复 5-FU 和 OxPt 的化疗敏感性,从而增强与 相关的耐药结直肠肿瘤的联合化疗效果。体内外研究表明,定制的纳米药物具有高效的抗菌和抗肿瘤活性,同时提高了生物相容性,降低了非特异性毒性。因此,这种新型抗肿瘤策略在 CRC 的联合化疗中具有巨大潜力,为与细菌相关的耐药性癌症提供了一种有临床价值的选择。

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