Abbasi Athena, Zahiri Mahsa, Abnous Khalil, Taghdisi Seyed Mohammad, Aliabadi Ali, Ramezani Mohammad, Alibolandi Mona
Pharmaceutical Research Center, Pharmaceutical Technology Institute, Mashhad University of Medical Sciences, Mashhad, Iran; Student Research Committee, Mahshad University of Medical Sciences, Mashhad, Iran.
Pharmaceutical Research Center, Pharmaceutical Technology Institute, Mashhad University of Medical Sciences, Mashhad, Iran.
Eur J Pharm Biopharm. 2024 Sep;202:114411. doi: 10.1016/j.ejpb.2024.114411. Epub 2024 Jul 14.
Combination therapy using chemo-photothermal therapy (chemo-PTT) shows great efficacy toward tumor ablation in preclinical studies. Besides, lipopolymersomes as a hybrid nanocarriers, integrate advantages of liposomes and polymersomes in a single platform in order to provide tremendous biocompatibility, biodegradability, noteworthy loading efficacy for both hydrophobic and hydrophilic drugs with adjustable drug release and high stability. In this study, a multipurpose lipopolymersome was fabricated for guided chemotherapy-PTT and NIR-imaging of melanoma. A lipopolymerosomal hybrid nanovesicle consisting of equal molar ratio of 1,2-dioleoyl-3-trimethylammonium propane (DOTAP) and poly (ethylene glycol)-poly (lactic acid) (PEG-PLA) diblock copolymer (molar ratio 1:1) was fabricated. The nanoparticulate system was prepared through film rehydration technique for encapsulation of doxorubicin (DOX) and indocyanine green (ICG) to form DOX-ICG-LP platform. At the next stage, AS1411 DNA aptamer was conjugated to the surface of lipopolymersome (Apt-DOX-ICG-LP) for selective delivery. The sizes of DOX-ICG-LP and Apt-DOX-ICG-LP were obtained through DLS analysis (61.0 ± 6 and 74 ± 5, respectively). Near Infrared-responsive release pattern of the prepared lipopolymersome was verified in vitro. The formulated platform showed efficient photothermal conversion, and superior stability with acceptable encapsulation efficiency. Consistent with the in vitro studies, NIR-responsive lipopolymersome exhibited significantly higher cellular toxicity for Chemo-PTT versus single anti-cancer treatment. Moreover, superlative tumor shrinkage with favorable survival profile were attained in B16F10 tumor-bearing mice received Apt-DOX-ICG-LP and irradiated with 808 nm laser compared to those treated with either DOX-ICG-LP or Apt-DOX-ICG-LP without laser irradiation. The diagnostic capability of Apt-DOX-ICG-LP was addressed using in vivo NIR imaging, 6 and 24 h post-intravenous administration. The results indicated desirable feature of an established targeted theranostic capability of Apt-DOX-ICG-LP for both diagnostics and dual chemo-PTT of melanoma.
在临床前研究中,使用化学光热疗法(chemo-PTT)的联合疗法对肿瘤消融显示出巨大疗效。此外,脂质聚合物囊泡作为一种混合纳米载体,在单一平台上整合了脂质体和聚合物囊泡的优势,以提供巨大的生物相容性、生物降解性,对疏水性和亲水性药物具有显著的负载效率,且药物释放可调节、稳定性高。在本研究中,制备了一种用于黑色素瘤导向化疗-PTT和近红外成像的多功能脂质聚合物囊泡。制备了一种由等摩尔比的1,2-二油酰基-3-三甲基铵丙烷(DOTAP)和聚(乙二醇)-聚(乳酸)(PEG-PLA)二嵌段共聚物(摩尔比1:1)组成的脂质聚合物囊泡混合纳米囊泡。通过薄膜水化技术制备纳米颗粒系统,用于封装阿霉素(DOX)和吲哚菁绿(ICG),以形成DOX-ICG-LP平台。在下一阶段,将AS1411 DNA适配体偶联到脂质聚合物囊泡表面(Apt-DOX-ICG-LP)用于选择性递送。通过动态光散射分析获得DOX-ICG-LP和Apt-DOX-ICG-LP的尺寸(分别为61.0±6和74±5)。体外验证了所制备脂质聚合物囊泡的近红外响应释放模式。所制备的平台显示出高效的光热转换、优异的稳定性和可接受的包封率。与体外研究一致,近红外响应脂质聚合物囊泡对化疗-PTT的细胞毒性明显高于单一抗癌治疗。此外,与接受DOX-ICG-LP或未进行激光照射的Apt-DOX-ICG-LP治疗的小鼠相比,接受Apt-DOX-ICG-LP并接受808 nm激光照射的B16F10荷瘤小鼠实现了极佳的肿瘤缩小和良好的生存情况。在静脉给药后6小时和24小时,使用体内近红外成像评估Apt-DOX-ICG-LP的诊断能力。结果表明,Apt-DOX-ICG-LP在黑色素瘤的诊断和双重化疗-PTT方面具有既定的靶向治疗诊断能力的理想特征。
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