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Monica Argenziano

Bio: Monica Argenziano is an academic researcher from University of Turin. The author has contributed to research in topics: Medicine & Drug delivery. The author has an hindex of 20, co-authored 62 publications receiving 1138 citations.

Papers published on a yearly basis

Papers
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Journal ArticleDOI
TL;DR: The close link between physicochemical properties and magnetic characterization is described, essential to developing innovative and powerful magnetic-driven nanocarriers for Central Nervous System disorders.
Abstract: Magnetic Nanoparticles (MNPs) are of great interest in biomedicine, due to their wide range of applications. During recent years, one of the most challenging goals is the development of new strategies to finely tune the unique properties of MNPs, in order to improve their effectiveness in the biomedical field. This review provides an up-to-date overview of the methods of synthesis and functionalization of MNPs focusing on Iron Oxide Nanoparticles (IONPs). Firstly, synthesis strategies for fabricating IONPs of different composition, sizes, shapes, and structures are outlined. We describe the close link between physicochemical properties and magnetic characterization, essential to developing innovative and powerful magnetic-driven nanocarriers. In conclusion, we provide a complete background of IONPs functionalization, safety, and applications for the treatment of Central Nervous System disorders.

149 citations

Journal ArticleDOI
TL;DR: The physico-chemical properties of nanobubbles, the formulation parameters and the drug loading approaches, besides potential applications as a therapeutic tool, are described.
Abstract: In recent decades ultrasound-guided delivery of drugs loaded on nanocarriers has been the focus of increasing attention to improve therapeutic treatments. Ultrasound has often been used in combination with microbubbles, micron-sized spherical gas-filled structures stabilized by a shell, to amplify the biophysical effects of the ultrasonic field. Nanometer size bubbles are defined nanobubbles. They were designed to obtain more efficient drug delivery systems. Indeed, their small sizes allow extravasation from blood vessels into surrounding tissues and ultrasound-targeted site-specific release with minimal invasiveness. Additionally, nanobubbles might be endowed with improved stability and longer residence time in systemic circulation. This review will describe the physico-chemical properties of nanobubbles, the formulation parameters and the drug loading approaches, besides potential applications as a therapeutic tool.

114 citations

Journal ArticleDOI
TL;DR: This review focuses on the state of the art of organic-based nanoparticles for the delivery of approved antivirals and the most promising research addressing the treatment of most important viral infections.
Abstract: Introduction: Viral infections represent a public health problem and one of the leading causes of global mortality. Nanomedicine strategies can be considered a powerful tool to enhance the effectiveness of antiviral drugs, often associated with solubility and bioavailability issues. Consequently, high doses and frequent administrations are required, resulting in adverse side effects. To overcome these limitations, various nanomedicine platforms have been designed.Areas covered: This review focuses on the state of the art of organic-based nanoparticles for the delivery of approved antivirals. A brief description of the main characteristics of nanocarriers is followed by an overview of the most promising research addressing the treatment of most important viral infections.Expert opinion: The activity of antiviral drugs could be improved with nanomedicine formulations. Indeed, nanoparticles can affect the fate of the encapsulated drugs, allowing controlled release kinetics, enhanced bioavailability, ...

110 citations

Journal ArticleDOI
TL;DR: Chitosan nanobubbles have the potential to be promising tools for ultrasound-mediated DNA delivery and cell viability experiments demonstrated that neither ultrasound nor the nanobUBbles affected cell viability under these experimental conditions.
Abstract: Background The development of nonviral gene delivery systems is one of the most intriguing topics in nanomedicine. However, despite the advances made in recent years, several key issues remain unsettled. One of the main problems relates to the difficulty in designing nanodevices for targeted delivery of genes and other drugs to specific anatomic sites. In this study, we describe the development of a novel chitosan nanobubble-based gene delivery system for ultrasound-triggered release. Methods and results Chitosan was selected for the nanobubble shell because of its low toxicity, low immunogenicity, and excellent biocompatibility, while the core consisted of perfluoropentane. DNA-loaded chitosan nanobubbles were formed with a mean diameter of less than 300 nm and a positive surface charge. Transmission electron microscopic analysis confirmed composition of the core-shell structure. The ability of the chitosan nanobubbles to complex with and protect DNA was confirmed by agarose gel assay. Chitosan nanobubbles were found to be stable following insonation (2.5 MHz) for up to 3 minutes at 37°C. DNA release was evaluated in vitro in both the presence and absence of ultrasound. The release of chitosan nanobubble-bound plasmid DNA occurred after just one minute of insonation. In vitro transfection experiments were performed by exposing adherent COS7 cells to ultrasound in the presence of different concentrations of plasmid DNA-loaded nanobubbles. In the absence of ultrasound, nanobubbles failed to trigger transfection at all concentrations tested. In contrast, 30 seconds of ultrasound promoted a moderate degree of transfection. Cell viability experiments demonstrated that neither ultrasound nor the nanobubbles affected cell viability under these experimental conditions. Conclusion Based on these results, chitosan nanobubbles have the potential to be promising tools for ultrasound-mediated DNA delivery.

88 citations

Journal ArticleDOI
TL;DR: It is suggested that siNrf2-GCD is a promising drug delivery system for gene therapy to be used in vivo; and it may represent an important tool in the therapy of CDDP-resistant cancer.
Abstract: The transcription factor nuclear factor erythroid 2-related factor 2 (Nrf2) is considered as the master regulator of antioxidant and cytoprotective gene expressions. Moreover, it plays a pivotal role in cancer progression. Nrf2 mediates the adaptive response which contributes to the resistance to chemotherapeutic pro-oxidant drugs, such as cisplatin (CDDP), in various tumors, including bladder cancers. For this reason, Nrf2 could be a promising target to overcome chemoresistance. There are several known Nrf2 pharmacological inhibitors; however, most of them are not specific. The use of a specific small interfering RNA (siRNA) targeting the Nrf2 gene (siNrf2) loaded into nanovehicles is an attractive alternative, since it can increase specificity. This study aimed to evaluate the biological activity of siNrf2 loaded on guanidine-terminated carbosilane dendrimers (GCDs) in overcoming CDDP resistance in bladder cancer cells with a high level of Nrf2. Parameters such as viability, proliferation, apoptosis, migration, and oxidative stress level were taken into account. Results demonstrated that siNrf2-GCD treatment sensitized CDDP-resistant cells to CDDP treatment. Moreover, data obtained by treating the non-cancerous human kidney HK-2 cell line strongly suggest a good safety profile of the carbosilane dendrimers loaded with siNrf2. In conclusion, we suggest that siNrf2-GCD is a promising drug delivery system for gene therapy to be used in vivo; and it may represent an important tool in the therapy of CDDP-resistant cancer.

87 citations


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01 Aug 1953
TL;DR: In this paper, a solution for the radius of the vapor bubble as a function of time is obtained which is valid for sufficiently large radius, since the radius at which it becomes valid is near the lower limit of experimental observation.
Abstract: The growth of a vapor bubble in a superheated liquid is controlled by three factors: the inertia of the liquid, the surface tension, and the vapor pressure. As the bubble grows, evaporation takes place at the bubble boundary, and the temperature and vapor pressure in the bubble are thereby decreased. The heat inflow requirement of evaporation, however, depends on the rate of bubble growth, so that the dynamic problem is linked with a heat diffusion problem. Since the heat diffusion problem has been solved, a quantitative formulation of the dynamic problem can be given. A solution for the radius of the vapor bubble as a function of time is obtained which is valid for sufficiently large radius. This asymptotic solution covers the range of physical interest since the radius at which it becomes valid is near the lower limit of experimental observation. It shows the strong effect of heat diffusion on the rate of bubble growth. Comparison of the predicted radius‐time behavior is made with experimental observations in superheated water, and very good agreement is found.

729 citations

Journal ArticleDOI
TL;DR: An overview of the different types and characteristics of nanoparticles used to deliver drugs to the target, followed by a review of current research and clinical trials addressing the use of nanoparticle systems within the field of infectious diseases.

292 citations

Journal ArticleDOI
22 Jun 2020-ACS Nano
TL;DR: Recent as well as ongoing nanotechnology-based therapeutic and prophylactic strategies to fight against this pandemic are discussed, outlining the key areas for nanoscientists to step in.
Abstract: The current global health threat by the novel coronavirus disease 2019 (COVID-19) requires an urgent deployment of advanced therapeutic options available The role of nanotechnology is highly relevant to counter this "virus" nano enemy Nano intervention is discussed in terms of designing effective nanocarriers to counter the conventional limitations of antiviral and biological therapeutics This strategy directs the safe and effective delivery of available therapeutic options using engineered nanocarriers, blocking the initial interactions of viral spike glycoprotein with host cell surface receptors, and disruption of virion construction Controlling and eliminating the spread and reoccurrence of this pandemic demands a safe and effective vaccine strategy Nanocarriers have potential to design risk-free and effective immunization strategies for severe acute respiratory syndrome coronavirus 2 vaccine candidates such as protein constructs and nucleic acids We discuss recent as well as ongoing nanotechnology-based therapeutic and prophylactic strategies to fight against this pandemic, outlining the key areas for nanoscientists to step in

265 citations

Journal ArticleDOI
TL;DR: This review article focuses on therapeutically-active nanoparticles (NPs) when stimulated by ultrasound and the possible working mechanisms under debate of NPs-assisted sonodynamic treatments, showing that this very innovative and promising approach is however still at its infancy in the clinical cancer treatment.

244 citations

Journal ArticleDOI
11 Aug 2020
TL;DR: This review focuses on the most recent developments in the field of hydrogel-based skin substitutes for skin replacement, and discusses the synthesis, fabrication, and biomedical application of novel “smart” hydrogels.
Abstract: Skin is the largest organ of the human body, protecting it against the external environment. Despite high self-regeneration potential, severe skin defects will not heal spontaneously and need to be covered by skin substitutes. Tremendous progress has been made in the field of skin tissue engineering, in recent years, to develop new skin substitutes. Among them, hydrogels are one of the candidates with most potential to mimic the native skin microenvironment, due to their porous and hydrated molecular structure. They can be applied as a permanent or temporary dressing for different wounds to support the regeneration and healing of the injured epidermis, dermis, or both. Based on the material used for their fabrication, hydrogels can be subdivided into two main groups—natural and synthetic. Moreover, hydrogels can be reinforced by incorporating nanoparticles to obtain “in situ” hybrid hydrogels, showing superior properties and tailored functionality. In addition, different sensors can be embedded in hydrogel wound dressings to provide real-time information about the wound environment. This review focuses on the most recent developments in the field of hydrogel-based skin substitutes for skin replacement. In particular, we discuss the synthesis, fabrication, and biomedical application of novel “smart” hydrogels.

233 citations