Pro- and anti-oxidant properties of near-infrared (NIR) light responsive carbon nanoparticles

Elemental carbon nanomaterials (ECNMs) are redox active agents that can be exploited to purposely modify the redox balance of cells. Both pro- or antioxidant properties have been reported. However, to the best of our knowledge, there are not comprehensive studies exploring both properties on the same material in view of a potential application in medicine. At the same time, the effect of the bulk structure on the pro/antioxidant properties is poorly known. Here, carbon nanoparticles (CNPs) derived by glucose with definite size and shape have been prepared, and their redox properties evaluated in cell free systems in the dark or following activation with a Near Infrared (NIR) laser beam (945 nm, 1.3 W/cm2). We found that, when irradiated with NIR, CNPs efficiently generate heat and singlet oxygen (1O2), a property that can be exploited for dual photo-thermal (PT)/photodynamic (PD) therapy in cancer. On the other hand, in the absence of photo-activation, CNPs react with both oxidant (hydroxyl radicals) and antioxidant (glutathione) species. When tested on a murine macrophages cell line (RAW 264.7) CNPs were clearly antioxidant. Furthermore, albeit efficiently internalized, CNPs do not exert cytotoxic effect up to 80 µg/ml and do not exacerbate TNF-α-mediated inflammation. Overall, the results reported herein suggest that CNPs may represent a new class of safe nanomaterials with potential applications in medicine

Molecular Aspects of the Interaction with Gram-Negative and Gram-Positive Bacteria of Hydrothermal Carbon Nanoparticles Associated with Bac8c2,5Leu Antimicrobial Peptide

Molecular Aspects of the Interaction with Gram-Negative and Gram- Positive Bacteria of Hydrothermal Carbon Nanoparticles Associated with Bac8c2,5Leu Antimicrobial Peptide Giulia Barzan,⊥ Ida Kokalari,⊥ Giacomo Gariglio, Elena Ghibaudi, Marc Devocelle, Marco P. Monopoli, Alessio Sacco, Angelo Greco, Andrea M. Giovannozzi, Andrea M. Rossi, and Ivana Fenoglio* Cite This: https://doi.org/10.1021/acsomega.2c00305 Read Online ACCESS Metrics & More Article Recommendations *sı Supporting Information ABSTRACT: Antimicrobial peptides (AMPs) are widely studied as therapeutic agents due to their broad-spectrum efficacy against infections. However, their clinical use is hampered by the low in vivo bioavailability and systemic toxicity. Such limitations might be overcome by using appropriate drug delivery systems. Here, the preparation of a drug delivery system (DDS) by physical conjugation of an arginine-rich peptide and hydrothermal carbon nanoparticles (CNPs) has been explored, and its antimicrobial efficacy against Eschericia coli (E. coli) and Staphylococcus aureus investigated in comparison with the unloaded carrier and the free peptide. The mechanism of interaction between CNPs and the bacteria was investigated by scanning electron microscopy and a combined dielectrophoresis−Raman spectroscopy method for real- time analysis. In view of a possible systemic administration, the effect of proteins on the stability of the DDS was investigated by using albumin as a model protein. The peptide was bounded electrostatically to the CNPs surface, establishing an equilibrium modulated by pH and albumin. The DDS exhibited antimicrobial activity toward the two bacterial strains, albeit lower as compared to the free peptide. The decrease in effectiveness toward E. coli was likely due to the rapid formation of a particle-induced extracellular matrix. The present results are relevant for the future development of hydrothermal CNPs as drug delivery agents of AMP

A compact diode laser based all-fiber delivery system for PDT+PTT with integrated temperature sensing capabilities

The paper first reviews the main laser based cancer therapies and then presents a new 9xx nm high power laser diode system specifically devised to irradiate carbon graphitic nanoparticles that have shown photodynamic and photo-thermal behavior when exposed to near-IR laser light. The peculiarity of the laser system is that its delivery is through a fiber probe that integrates Bragg gratings to allow monitoring the induced temperature increase without introducing artifacts due to the interaction with the laser beam. Experimental validations through EPR spectrum and temperature measurements on hydroxylated fullerene and carbon nanoparticle samples are provided to assess the effectiveness of the developed system

Identification of the physical-chemical properties that modulate the nanoparticles aggregation in blood

Inorganic materials are receiving significant interest in medicine given their usefulness for therapeutic applications such as targeted drug delivery, carriers of active pharmaceutical and medical imaging. However, the poor knowledge of the side effects related to their use is an obstacle to their clinical translation. For the molecular drug development, safe-by-design has become as a novel pharmaceutical strategy that allows a reduction of the costs and an acceleration of the translation of research to market. In the case of materials, the application of such approaches is hampered by a poor knowledge of how the physical and chemical properties of the material trigger biological response. Hemocompatibility is a crucial factor for those materials that are intended for medical applications. In particular, the formation of agglomerates is a serious side effect that may induce occlusion of blood vessels and thrombotic events. Additionally, nanoparticles can interfere with the coagulation cascades where they have been reported to induce both pro- and anti-coagulant properties where their properties like size, shape and surface charge have been see to be critical parameters.   Here, we developed two sets of tailored carbon and silica nano/submicron-particles with three different sizes (100-500 nm) with the purpose of investigating the role of surface curvature and chemistry on platelet aggregation, activation and adhesion. We show that that large carbon nanoparticles, but not small carbon nanoparticles or silica nanoparticles, have a strong tendency to form aggregates both in plasma and blood, as a consequence of the formation of a protein corona and not of platelets activation. Substantial differences were found in the composition of the protein corona depending upon the chemical nature of the nanoparticles, while the surface curvature plays a minor role. On the other hand, coagulation proteins were abundant in the corona of both silica and carbon nanoparticles.  The results presented herein suggest that vessel occlusion and formation of thrombi in vivo may occur through independent mode of action (MoA), differently affected by the physico-chemical properties of the materials

Identification of physicochemical properties that modulate nanoparticle aggregation in blood

Inorganic materials are receiving significant interest in medicine given their usefulness for therapeutic applications such as targeted drug delivery, active pharmaceutical carriers and medical imaging. However, poor knowledge of the side effects related to their use is an obstacle to clinical translation. For the development of molecular drugs, the concept of safe-by-design has become an efficient pharmaceutical strategy with the aim of reducing costs, which can also accelerate the translation into the market. In the case of materials, the application these approaches is hampered by poor knowledge of how the physical and chemical properties of the material trigger the biological response. Hemocompatibility is a crucial aspect to take into consideration for those materials that are intended for medical applications. The formation of nanoparticle agglomerates can cause severe side effects that may induce occlusion of blood vessels and thrombotic events. Additionally, nanoparticles can interfere with the coagulation cascade causing both pro-and anti-coagulant properties. There is contrasting evidence on how the physicochemical properties of the material modulate these effects. In this work, we developed two sets of tailored carbon and silica nanoparticles with three different diameters in the 100-500 nm range with the purpose of investigating the role of surface curvature and chemistry on platelet aggregation, activation and adhesion. Substantial differences were found in the composition of the protein corona depending on the chemical nature of the nanoparticles, while the surface curvature was found to play a minor role. On the other hand, large carbon nanoparticles (but not small carbon nanoparticles or silica nanoparticles) have a clear tendency to form aggregates both in plasma and blood. This effect was observed both in the presence or absence of platelets and was independent of platelet activation. Overall, the results presented herein suggest the existence of independent modes of action that are differently affected by the physicochemical properties of the materials, potentially leading to vessel occlusion and/or formation of thrombi in vivo