αvβ3 Integrin and Folate-Targeted pH-Sensitive Liposomes with Dual Ligand Modification for Metastatic Breast Cancer Treatment.

IF 3.8 3区医学 Q2 ENGINEERING, BIOMEDICAL

Bioengineering Pub Date : 2024-08-07 DOI:10.3390/bioengineering11080800

Prashant Pandey, Dilip Kumar Arya, Payal Deepak, Daoud Ali, Saud Alarifi, Saurabh Srivastava, Afsaneh Lavasanifar, Paruvathanahalli Siddalingam Rajinikanth

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引用次数: 0

Abstract

The advent of pH-sensitive liposomes (pHLips) has opened new opportunities for the improved and targeted delivery of antitumor drugs as well as gene therapeutics. Comprising fusogenic dioleylphosphatidylethanolamine (DOPE) and cholesteryl hemisuccinate (CHEMS), these nanosystems harness the acidification in the tumor microenvironment and endosomes to deliver drugs effectively. pH-responsive liposomes that are internalized through endocytosis encounter mildly acidic pH in the endosomes and thereafter fuse or destabilize the endosomal membrane, leading to subsequent cargo release into the cytoplasm. The extracellular tumor matrix also presents a slightly acidic environment that can lead to the enhanced drug release and improved targeting capabilities of the nano-delivery system. Recent studies have shown that folic acid (FA) and iRGD-coated nanocarriers, including pH-sensitive liposomes, can preferentially accumulate and deliver drugs to breast tumors that overexpress folate receptors and αvβ3 and αvβ5 integrins. This study focuses on the development and characterization of 5-Fluorouracil (5-FU)-loaded FA and iRGD surface-modified pHLips (FA-iRGD-5-FU-pHLips). The novelty of this research lies in the dual targeting mechanism utilizing FA and iRGD peptides, combined with the pH-sensitive properties of the liposomes, to enhance selective targeting and uptake by cancer cells and effective drug release in the acidic tumor environment. The prepared liposomes were small, with an average diameter of 152 ± 3.27 nm, uniform, and unilamellar, demonstrating efficient 5-FU encapsulation (93.1 ± 2.58%). Despite surface functionalization, the liposomes maintained their pH sensitivity and a neutral zeta potential, which also conferred stability and reduced aggregation. Effective pH responsiveness was demonstrated by the observation of enhanced drug release at pH 5.5 compared to physiological pH 7.4. (84.47% versus 46.41% release at pH 5.5 versus pH 7.4, respectively, in 72 h). The formulations exhibited stability for six months and were stable when subjected to simulated biological settings. Blood compatibility and cytotoxicity studies on MDA-MB-231 and SK-BR3 breast cancer cell lines revealed an enhanced cytotoxicity of the liposomal formulation that was modified with FA and iRGD compared to free 5-FU and minimal hemolysis. Collectively, these findings support the potential of FA and iRGD surface-camouflaged, pH-sensitive liposomes as a promising drug delivery strategy for breast cancer treatment.

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双配体修饰的αvβ3整合素和叶酸靶向pH敏感脂质体用于转移性乳腺癌治疗

对 pH 值敏感的脂质体（pHLips）的出现为改善抗肿瘤药物和基因疗法的靶向递送提供了新的机遇。pH敏感脂质体通过内吞作用内化，在内质体中遇到微酸性pH值，然后融合或破坏内质体膜的稳定性，导致随后的货物释放到细胞质中。细胞外的肿瘤基质也呈现微酸性环境，这也会导致纳米递送系统的药物释放和靶向能力增强。最近的研究表明，叶酸（FA）和 iRGD 包被的纳米载体（包括 pH 敏感脂质体）可优先积聚药物并将药物输送到叶酸受体、αvβ3 和 αvβ5 整合素过度表达的乳腺肿瘤。本研究的重点是5-氟尿嘧啶（5-FU）负载的FA和iRGD表面修饰的pHLips（FA-iRGD-5-FU-pHLips）的开发和表征。这项研究的创新之处在于利用FA和iRGD肽的双重靶向机制，结合脂质体的pH敏感特性，增强了癌细胞的选择性靶向和吸收，并在酸性肿瘤环境中有效释放药物。制备的脂质体体积小，平均直径为 152 ± 3.27 nm，均匀且为单线粒体，能有效包封 5-FU (93.1 ± 2.58%)。尽管进行了表面官能化，但脂质体仍保持了对 pH 值的敏感性和中性 ZETA 电位，这也赋予了脂质体稳定性并减少了聚集。与生理 pH 值 7.4 相比，pH 值为 5.5 时的药物释放量增加（72 小时内，pH 值为 5.5 时的释放量为 84.47%，pH 值为 7.4 时的释放量为 46.41%）。制剂的稳定性可维持 6 个月，在模拟生物环境下也很稳定。对 MDA-MB-231 和 SK-BR3 乳腺癌细胞系进行的血液相容性和细胞毒性研究表明，与游离 5-FU 相比，用 FA 和 iRGD 修饰的脂质体制剂的细胞毒性更强，溶血现象极少。总之，这些研究结果支持了 FA 和 iRGD 表面掩蔽、pH 值敏感的脂质体作为乳腺癌治疗药物递送策略的潜力。

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来源期刊

Bioengineering Chemical Engineering-Bioengineering

CiteScore

4.00

自引率

8.70%

发文量

661

期刊介绍： Aims Bioengineering (ISSN 2306-5354) provides an advanced forum for the science and technology of bioengineering. It publishes original research papers, comprehensive reviews, communications and case reports. Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. All aspects of bioengineering are welcomed from theoretical concepts to education and applications. There is no restriction on the length of the papers. The full experimental details must be provided so that the results can be reproduced. There are, in addition, four key features of this Journal: ● We are introducing a new concept in scientific and technical publications “The Translational Case Report in Bioengineering”. It is a descriptive explanatory analysis of a transformative or translational event. Understanding that the goal of bioengineering scholarship is to advance towards a transformative or clinical solution to an identified transformative/clinical need, the translational case report is used to explore causation in order to find underlying principles that may guide other similar transformative/translational undertakings. ● Manuscripts regarding research proposals and research ideas will be particularly welcomed. ● Electronic files and software regarding the full details of the calculation and experimental procedure, if unable to be published in a normal way, can be deposited as supplementary material. ● We also accept manuscripts communicating to a broader audience with regard to research projects financed with public funds. Scope ● Bionics and biological cybernetics: implantology; bio–abio interfaces ● Bioelectronics: wearable electronics; implantable electronics; “more than Moore” electronics; bioelectronics devices ● Bioprocess and biosystems engineering and applications: bioprocess design; biocatalysis; bioseparation and bioreactors; bioinformatics; bioenergy; etc. ● Biomolecular, cellular and tissue engineering and applications: tissue engineering; chromosome engineering; embryo engineering; cellular, molecular and synthetic biology; metabolic engineering; bio-nanotechnology; micro/nano technologies; genetic engineering; transgenic technology ● Biomedical engineering and applications: biomechatronics; biomedical electronics; biomechanics; biomaterials; biomimetics; biomedical diagnostics; biomedical therapy; biomedical devices; sensors and circuits; biomedical imaging and medical information systems; implants and regenerative medicine; neurotechnology; clinical engineering; rehabilitation engineering ● Biochemical engineering and applications: metabolic pathway engineering; modeling and simulation ● Translational bioengineering

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