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Hyperthermia-induced antitumor activity of thermosensitive polymer modified temperature-sensitive liposomes.

机译:热敏聚合物修饰的热敏脂质体的热疗诱导的抗肿瘤活性。

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摘要

Temperature-sensitive liposomes (TS-liposomes) have been studied for chemotherapeutic purposes to enhance the release of anticancer drugs at tumor sites. In this study, we prepared poly(N-isopropylacrylamide-co-acrylamide) (PNIPAM-AAM) and polyethylene glycol (PEG)-modified TS-liposomes (PETS-liposomes). PETS-liposomes significantly increased in vitro drug release in serum compared with PEG-fixed or PNIPAM-AAM-modified liposomes. Furthermore, incorporation of both PNIPAM-AAM and PEG into PETS-liposomes enhanced the stabilities of liposomes in serum by inhibiting protein adsorption. In addition, to investigate the therapeutic efficacy of doxorubicin (DOX)-loaded PETS-liposomes, the in vivo antitumor activity of liposomes in combination with hyperthermia was evaluated in a B16F10 melanoma tumor-bearing mouse model. PETS-liposomes showed much higher levels of tumor growth inhibition than PEG-fixed or PNIPAM-AAM-modified TS-liposomes. Moreover, the antitumor activity of PETS-liposomes was enhanced significantly when they were administered in combination with hyperthermia. PETS-liposomes were found to be highly efficacious carriers for the in vivo delivery of anticancer drugs, and to have potential anticancer applications in combination with hyperthermia.
机译:已经研究了对温度敏感的脂质体(TS-脂质体)用于化学治疗的目的,以增强抗癌药在肿瘤部位的释放。在这项研究中,我们制备了聚(N-异丙基丙烯酰胺-共丙烯酰胺)(PNIPAM-AAM)和聚乙二醇(PEG)修饰的TS-脂质体(PETS-脂质体)。与PEG固定或PNIPAM-AAM修饰的脂质体相比,PETS脂质体显着增加了血清中的体外药物释放。此外,将PNIPAM-AAM和PEG掺入PETS-脂质体中可通过抑制蛋白质吸附来增强脂质体在血清中的稳定性。此外,为了研究载有阿霉素(DOX)的PETS-脂质体的治疗功效,在B16F10黑色素瘤荷瘤小鼠模型中评估了脂质体与高热结合的体内抗肿瘤活性。 PETS脂质体显示出比PEG固定或PNIPAM-AAM修饰的TS脂质体高得多的肿瘤生长抑制水平。此外,当PETS-脂质体与热疗组合给药时,其抗肿瘤活性显着增强。发现PETS-脂质体是体内递送抗癌药的高效载体,并且与热疗结合具有潜在的抗癌应用。

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