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叶酸偶联白蛋白作为靶向纳米载体用于漆黄素递送及其生物学研究

Folate conjugated albumin as a targeted nanocarrier for the delivery of fisetin: and biological studies.

作者信息

Solanki Raghu, Srivastav Amit Kumar, Patel Sejal, Singh Sanju Kumari, Jodha Bhavana, Kumar Umesh, Patel Sunita

机构信息

School of Life Sciences, Central University of Gujarat Gandhinagar 382030 India

School of Nano Sciences, Central University of Gujarat Gandhinagar 382030 India.

出版信息

RSC Adv. 2024 Mar 1;14(11):7338-7349. doi: 10.1039/d3ra08434e. eCollection 2024 Feb 29.

Abstract

Fisetin (FST), a natural flavonoid compound derived from various fruits and vegetables, including apple, strawberry, and onion, demonstrates potential for a wide range of pharmaceutical applications, including potential anticancer properties. However, challenges such as low bioavailability, poor aqueous solubility, and limited permeability restrict the use of FST in the pharmaceutical sector. Nowadays, targeted nanomedicines have garnered attention to overcome limitations associated with phytochemicals, including FST. In the present study, we have designed and successfully prepared folate-targeted FST nanoparticles (FFNPs). Characterization through DLS and FE-SEM revealed the successful preparation of monodisperse (PDI: 0.117), nanoscale-sized (150 nm), and spherical nanoparticles. Physicochemical characterization including FTIR, XRD, DSC, and TGA analysis, confirmed the encapsulation of the FST within the Folic acid (FA) - conjugated nanoparticles (CNPs) and revealed its amorphous nature. Molecular docking analysis revealed the strong binding affinity and specific amino acid interactions involved in the BSA-FST-FA complex, suggesting the potential synergistic effect of FST and FA in enhancing the therapeutic activity of the FFANPs. Cytotoxic assessments by the MTT assay, migration assay, AO-EtBr staining assay, colony formation assay, and cellular uptake study demonstrated enhanced anticancer efficacy, apoptosis induction, and enhanced uptake of FFNPs compared to pure FST. These findings propose prepared FFNPs as a promising targeted drug delivery nanocarrier for effective FST delivery in cancer therapy.

摘要

漆黄素(FST)是一种天然黄酮类化合物,来源于包括苹果、草莓和洋葱在内的多种水果和蔬菜,具有广泛的药物应用潜力,包括潜在的抗癌特性。然而,低生物利用度、差的水溶性和有限的渗透性等挑战限制了FST在制药领域的应用。如今,靶向纳米药物已受到关注,以克服与植物化学物质(包括FST)相关的局限性。在本研究中,我们设计并成功制备了叶酸靶向的FST纳米颗粒(FFNPs)。通过动态光散射(DLS)和场发射扫描电子显微镜(FE-SEM)表征表明成功制备了单分散(多分散指数:0.117)、纳米级尺寸(150nm)的球形纳米颗粒。包括傅里叶变换红外光谱(FTIR)、X射线衍射(XRD)、差示扫描量热法(DSC)和热重分析(TGA)分析在内的物理化学表征证实了FST被包裹在叶酸(FA)共轭纳米颗粒(CNPs)中,并揭示了其无定形性质。分子对接分析揭示了牛血清白蛋白(BSA)-FST-FA复合物中存在的强结合亲和力和特定氨基酸相互作用,表明FST和FA在增强FFANPs治疗活性方面具有潜在的协同作用。通过MTT法、迁移试验、AO-EtBr染色试验、集落形成试验和细胞摄取研究进行的细胞毒性评估表明,与纯FST相比,FFNPs具有增强的抗癌疗效、诱导凋亡作用和增强的摄取。这些发现表明所制备的FFNPs是一种有前景的靶向药物递送纳米载体,可在癌症治疗中有效地递送FST。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e6b9/10906141/bf5ef7642351/d3ra08434e-f1.jpg

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