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pH响应性泡囊去铁胺的制备:来自、和评估的证据。

Preparation of pH-Responsive Vesicular Deferasirox: Evidence from , , and Evaluations.

作者信息

Barani Mahmood, Sargazi Saman, Hajinezhad Mohammad Reza, Rahdar Abbas, Sabir Fakhara, Pardakhty Abbas, Zargari Farshid, Anwer Md Khalid, Aboudzadeh M Ali

机构信息

Medical Mycology and Bacteriology Research Center, Kerman University of Medical Sciences, Kerman 7616913555, Iran.

Cellular and Molecular Research Center, Resistant Tuberculosis Institute, Zahedan University of Medical Sciences, Zahedan 9816743463, Iran.

出版信息

ACS Omega. 2021 Sep 13;6(37):24218-24232. doi: 10.1021/acsomega.1c03816. eCollection 2021 Sep 21.

Abstract

pH-sensitive nanocarriers can effectively deliver anticancer drugs to tumors and reduce the adverse effects of conventional chemotherapy. In this light, we prepared a novel pH-responsive deferasirox (DFX)-loaded vesicle and comprehensively performed , , and studies to examine the properties of the newly synthesized formulation. Physiochemical assessment of the developed formulations showed that they have an average size (107 ± 2 nm), negative zeta potential (-29.1 ± 1.5 mV), high encapsulation efficiency (84.2 ± 2.6%), and a pH-responsive release. Using the molecular dynamics simulation, the structural and dynamic properties of ergosterol-containing niosomes (ST60/Ergo) in the presence of DFX molecules were analyzed and showed a good interaction between DFX and vesicle components. Cytotoxic assessment showed that niosomal DFX exhibited a greater cytotoxic effect than free DFX in both human cancer cells (MCF-breast cancer and Hela cervical cancer) and induced evident morphological features of apoptotic cell death. No marked difference between the ability of free and niosomal DFX was found in activating caspase-3 in Hela cells. Eight weeks of intraperitoneal administrations of free DFX at three doses caused a significant increase in serum biochemical parameters and liver lipid peroxidation. Treatment with 5 mg/kg dose of niosomal DFX caused a significant increase in serum creatinine ( < 0.05); however, other parameters remained unchanged. On the other hand, administration of niosomal DFX at the highest dose (10 mg/kg) significantly increased serum creatinine ( < 0.05), BUN, and serum liver enzymes compared to the control rats ( < 0.001). Based on the results, the application of pH-responsive DFX-loaded niosomes, as a novel drug delivery platform, may yield promising results in cancer treatment.

摘要

pH敏感纳米载体能够有效地将抗癌药物递送至肿瘤部位,并减少传统化疗的副作用。鉴于此,我们制备了一种新型的负载去铁胺(DFX)的pH响应囊泡,并全面开展了 、 和 研究,以考察新合成制剂的性质。对所开发制剂的理化评估表明,它们具有平均粒径(107±2 nm)、负的zeta电位(-29.1±1.5 mV)、高包封率(84.2±2.6%)以及pH响应释放特性。利用分子动力学模拟,分析了存在DFX分子时含麦角固醇的非离子型表面活性剂囊泡(ST60/Ergo)的结构和动力学性质,结果显示DFX与囊泡成分之间存在良好的相互作用。细胞毒性评估表明,在人癌细胞(MCF-乳腺癌和Hela宫颈癌)中,纳米粒载DFX比游离DFX表现出更强的细胞毒性作用,并诱导了明显的凋亡细胞死亡形态特征。在Hela细胞中,游离DFX和纳米粒载DFX激活caspase-3的能力未发现显著差异。以三种剂量腹腔注射游离DFX八周导致血清生化参数和肝脏脂质过氧化显著增加。用5 mg/kg剂量的纳米粒载DFX处理导致血清肌酐显著升高(<0.05);然而,其他参数保持不变。另一方面,与对照大鼠相比,以最高剂量(10 mg/kg)给予纳米粒载DFX显著增加了血清肌酐(<0.05)、血尿素氮和血清肝酶(<0.001)。基于这些结果,作为一种新型药物递送平台,应用pH响应性载DFX纳米粒在癌症治疗中可能会产生有前景的结果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/406b/8459436/2896dae7fbc8/ao1c03816_0002.jpg

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