Investigating preparation and characterisation of diphtheria toxoid-loaded on sodium alginate nanoparticles

IF 3.8 4区 工程技术 Q1 BIOCHEMICAL RESEARCH METHODS
Samira Aghamiri, Mojtaba Noofeli, Parvaneh Saffarian, Zahra Salehi Najafabadi, Hamid Reza Goudarzi
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引用次数: 2

Abstract

This paper aims to investigate the preparation and characterisation of the alginate nanoparticles (NPs) as antigen delivery system loaded by diphtheria toxoid (DT). For this purpose, both the loading capacity (LC) and Loading efficiency (LE) of the alginate NPs burdened by DT are evaluated. Moreover, the effects of different concentrations of sodium alginate and calcium chloride on the NPs physicochemical characteristics are surveyed in addition to other physical conditions such as homogenization time and rate. To do so, the NPs are characterised using particle size and distribution, zeta potential, scanning electron microscopy, encapsulation efficiency, in vitro release study and FT-IR spectroscopy. Subsequently, the effects of homogenization time and rate on the NPs are assessed. At the meantime, the NPs LC and efficiency in several DT concentrations are estimated. The average size of the NPs was 400.7 and 276.6 nm for unloaded and DT loaded, respectively. According to the obtained results, the zeta potential of the blank and DT loaded NPs are estimated as −23.7 mV and −21.2 mV, respectively. Whereas, the LC and LE were >80% and >90%, in that order. Furthermore, 95% of the releasing DT loaded NPs occurs at 140 h in the sustained mode without any bursting release. It can be concluded that the features of NPs such as morphology and particle size are strongly depended on the calcium chloride, sodium alginate concentrations and physicochemical conditions in the NPs formation process. In addition, appropriate concentrations of the sodium alginate and calcium ions would lead to obtaining the desirable NPs formation associated with the advantageous LE, LC (over 80%) and sustained in vitro release profile. Ultimately, the proposed NPs can be employed in vaccine formulation for the targeted delivery, controlled and slow antigen release associated with the improved antigen stability.

Abstract Image

藻酸钠纳米粒子负载白喉类毒素的制备及性质研究
摘要本文旨在研究藻酸盐纳米粒子(NPs)作为白喉类毒素(DT)抗原递送系统的制备和表征。为此,评估了DT负载的藻酸盐NP的负载能力(LC)和负载效率(LE)。此外,除了均匀化时间和速率等其他物理条件外,还考察了不同浓度的藻酸钠和氯化钙对纳米颗粒物理化学特性的影响。为此,使用粒径和分布、ζ电位、扫描电子显微镜、包封效率、体外释放研究和FT-IR光谱对NP进行了表征。随后,评估均化时间和速率对NP的影响。同时,估计了几种DT浓度下的NPs LC和效率。空载和负载DT的NP的平均尺寸分别为400.7和276.6nm。根据获得的结果,空白和DT负载的NP的ζ电位估计分别为−23.7 mV和−21.2 mV。LC和LE分别为>80%和>90%。此外,95%的释放DT负载的NP发生在140小时的持续模式下,没有任何爆裂释放。可以得出结论,纳米颗粒的形态和粒径等特征在很大程度上取决于纳米颗粒形成过程中的氯化钙、藻酸钠浓度和物理化学条件。此外,适当浓度的藻酸钠和钙离子将导致获得与有利的LE、LC(超过80%)和持续的体外释放曲线相关的所需NP形成。最终,所提出的NP可用于疫苗制剂中,用于靶向递送、控制和减缓抗原释放,并提高抗原稳定性。
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来源期刊
IET nanobiotechnology
IET nanobiotechnology 工程技术-纳米科技
CiteScore
6.20
自引率
4.30%
发文量
34
审稿时长
1 months
期刊介绍: Electrical and electronic engineers have a long and illustrious history of contributing new theories and technologies to the biomedical sciences. This includes the cable theory for understanding the transmission of electrical signals in nerve axons and muscle fibres; dielectric techniques that advanced the understanding of cell membrane structures and membrane ion channels; electron and atomic force microscopy for investigating cells at the molecular level. Other engineering disciplines, along with contributions from the biological, chemical, materials and physical sciences, continue to provide groundbreaking contributions to this subject at the molecular and submolecular level. Our subject now extends from single molecule measurements using scanning probe techniques, through to interactions between cells and microstructures, micro- and nano-fluidics, and aspects of lab-on-chip technologies. The primary aim of IET Nanobiotechnology is to provide a vital resource for academic and industrial researchers operating in this exciting cross-disciplinary activity. We can only achieve this by publishing cutting edge research papers and expert review articles from the international engineering and scientific community. To attract such contributions we will exercise a commitment to our authors by ensuring that their manuscripts receive rapid constructive peer opinions and feedback across interdisciplinary boundaries. IET Nanobiotechnology covers all aspects of research and emerging technologies including, but not limited to: Fundamental theories and concepts applied to biomedical-related devices and methods at the micro- and nano-scale (including methods that employ electrokinetic, electrohydrodynamic, and optical trapping techniques) Micromachining and microfabrication tools and techniques applied to the top-down approach to nanobiotechnology Nanomachining and nanofabrication tools and techniques directed towards biomedical and biotechnological applications (e.g. applications of atomic force microscopy, scanning probe microscopy and related tools) Colloid chemistry applied to nanobiotechnology (e.g. cosmetics, suntan lotions, bio-active nanoparticles) Biosynthesis (also known as green synthesis) of nanoparticles; to be considered for publication, research papers in this area must be directed principally towards biomedical research and especially if they encompass in vivo models or proofs of concept. We welcome papers that are application-orientated or offer new concepts of substantial biomedical importance Techniques for probing cell physiology, cell adhesion sites and cell-cell communication Molecular self-assembly, including concepts of supramolecular chemistry, molecular recognition, and DNA nanotechnology Societal issues such as health and the environment Special issues. Call for papers: Smart Nanobiosensors for Next-generation Biomedical Applications - https://digital-library.theiet.org/files/IET_NBT_CFP_SNNBA.pdf Selected extended papers from the International conference of the 19th Asian BioCeramic Symposium - https://digital-library.theiet.org/files/IET_NBT_CFP_ABS.pdf
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