Project description:It is a major challenge to effectively inhibit microbial pathogens in the treatment of infectious diseases. Research on the application of nanomaterials as antibacterial agents has evidenced their great potential for the remedy of infectious disease. Among these nanomaterials, carbon quantum dots (CQDs) have attracted much attention owing to their unique optical properties and high biosafety. In this work, P-doped CQDs were prepared by simple hydrothermal treatment of m-aminophenol and phosphoric acid with fluorescence emission at 501 nm when excited at 429 nm. The P-doped CQDs showed effective antibacterial activity against Escherichia coli (E. coli) and Staphylococcus aureus (S. aureus). The minimal inhibitory concentrations (MICs) of P-doped CQD were 1.23 mg/mL for E. coli and 1.44 mg/mL for S. aureus. Furthermore, the morphologies of E. coli cells were damaged and S. aureus became irregular when treated with the P-doped CQDs. The results of zeta potential analysis demonstrated that the P-doped CQDs inhibit antibacterial activity and destroy the structure of bacteria by electronic interaction. In combination, the results of this study indicate that the as-prepared P-doped CQDs can be a promising candidate for the treatment of bacterial infections.

Project description:Carbon quantum dots (CQDs), a novel fluorescent nanomaterial, have been extensively employed/explored in various applications, that is, biosensors, bioimaging, nanomedicine, therapeutics, photocatalysis, electrocatalysis, energy storage system, and so forth. In this study, we report the synthesis, characterization, and the application of phosphorus-doped CQDs (PCQDs), synthesized using trisodium citrate and phosphoric acid by the hydrothermal method. The effect of phosphorus doping on optical features and the formation of PCQDs have been explored elaborately by controlling the concentrations of precursors, reaction time, and the temperature. The fluorescent quantum yield for PCQDs was determined to be 16.1% at an excitation/emission wavelength of 310/440 nm. Also, the optical and structural properties of PCQDs were determined by using various spectroscopic and microscopic techniques. Static quenching of fluorescence was determined upon the addition of Fe3+ to PCQDs because of the formation of the fluorescent inactive complex (PCQDs-Fe3+). Hence, this chemistry leads to the development of a new fluorometric assay for the detection of Fe3+. The lower limit of Fe3+ detection is determined to be 9.5 nM (3σ/slope), with the linear fit from 20 nM to 3.0 μM (R 2 = 0.99). We have validated this new assay in the raw, ejected, and purified water samples of the RO plant by the standard addition method. These results suggest the possibility of developing a new commercial assay for Fe3+ detection in blood, urine, and various industrial waste and sewage water samples. Furthermore, recycling the pollutant water into the freshwater using filters that consist of PCQDs offers a great deal.

Project description:Carbon quantum dots (CQDs) have potential applications in many fields such as light-emitting devices, photocatalysis, and bioimaging due to their unique photoluminescence (PL) properties and environmental benignness. Here, we report the synthesis of nitrogen-doped carbon quantum dots (NCQDs) from citric acid and m-phenylenediamine using a one-pot hydrothermal approach. The environment-dependent emission changes of NCQDs were extensively investigated in various solvents, in the solid state, and in physically assembled PMMA-PnBA-PMMA copolymer gels in 2-ethyl-hexanol. NCQDs display bright emissions in various solvents as well as in the solid state. These NCQDs exhibit multicolor PL emission across the visible region upon changing the environment (solutions and polymer matrices). NCQDs also exhibit excitation-dependent PL and solvatochromism, which have not been frequently investigated in CQDs. Most CQDs are nonemissive in the aggregated or solid state due to the aggregation-caused quenching (ACQ) effect, limiting their solid-state applications. However, NCQDs synthesized here display a strong solid-state emission centered at 568 nm attributed to the presence of surface functional groups that restrict the π-π interaction between the NCQDs and assist in overcoming the ACQ effect in the solid state. NCQD-containing gels display significant fluorescence enhancement in comparison to the NCQDs in 2-ethyl hexanol, likely because of the interaction between the polar PMMA blocks and NCQDs. The application of NCQDs-Gel as a solid/gel state fluorescent display has been presented. This research facilitates the development of large-scale, low-cost multicolor phosphor for the fabrication of optoelectronic devices, sensing, and bioimaging applications.

Project description:Quantum dots (QDs), also known as nanoscale semiconductor crystals, are nanoparticles with unique optical and electronic properties such as bright and intensive fluorescence. Since most conventional organic label dyes do not offer the near-infrared (>650 nm) emission possibility, QDs, with their tunable optical properties, have gained a lot of interest. They possess characteristics such as good chemical and photo-stability, high quantum yield and size-tunable light emission. Different types of QDs can be excited with the same light wavelength, and their narrow emission bands can be detected simultaneously for multiple assays. There is an increasing interest in the development of nano-theranostics platforms for simultaneous sensing, imaging and therapy. QDs have great potential for such applications, with notable results already published in the fields of sensors, drug delivery and biomedical imaging. This review summarizes the latest developments available in literature regarding the use of QDs for medical applications.

Project description: Not available

Project description:To achieve competitive fluorescence carbon dots (CDs), studies on regulating fluorescence of CDs under controlled, comparable conditions are in great demand. Herein, by changing the functional groups and nitrogenous existence forms in the precursors, three efficient yellow-green emissive N-doped CDs which have the same fluorescence peak wavelength but different photoluminescence quantum yields were realized through a facile hydrothermal method. The as-prepared CDs exhibit not only excited-independent emissions but also similar surface states. The best-performing CDs among the three products exhibits photoluminescence quantum yields of up to 24.4% in water and 53.3% in ethanol, abundant surface functional groups and its high N-doping degree would be the reason for its excellent performances. By washing and reduction processes, the emission evolution of the CDs was studied linking the changes of surface states. The fluorescence can certainly be attributed to the surface of the carbon dots, and the surface states control the photoluminescence features. Serving as a yellow-green colour conversion layer, the best CDs in the three products was used to fabricate a white light-emitting diode. The white light-emitting diode shows an excellent colour rendering index up to 93.3, suggesting broad application prospects of the CDs in lighting and display fields.

Project description:BackgroundCarbon-based drug delivery systems have attracted great interest because of their excellent photothermal conversion capability and high specific surface area for drug loading. Herein, we report a multifunctional nanoplatform based on hyaluronic acid (HA)-modified and graphene quantum dot (GQD)-gated hollow mesoporous carbon nanoparticle (HMCN) for anticancer drug encapsulation and targeted chemo-photothermal therapy of CD44 receptor-overexpressed cancer cells.MethodsIn this design, HMCN was not only used as a nanocarrier with high drug loading content to achieve chemotherapy, but also as a near-infrared absorbing agent to realize photothermal therapy. GQDs could not only prevent premature drug release during blood circulation, but also enhance the chemo-photothermal therapeutic efficacy for complete tumor growth suppression. After being modified with HA, the HA-HMCN(DOX)@GQDs could specifically target cancer cells.ResultsAs expected, the as-prepared HMCN exhibited high doxorubicin (DOX)-loading capacity of 410 mg/g and excellent light-to-heat conversion property. The DOX was released from HA-HMCN(DOX)@GQDs in a near-infrared laser and pH stimuli-responsive manner, which could enhance the therapeutic effect. In vitro cell biological experimental results confirmed that the nanoplatform possesses excellent biocompatibility, specifically target CD44 receptor-overexpressing human cervical carcinoma HeLa cells, and has remarkable synergistic chemo-photothermal killing capacity. The in vivo therapeutic studies in HeLa xenografts also showed negligible toxicity of HA-HMCN@GQDs and complete inhibition of tumor growth of HA-HMCN(DOX) @GQDs with near-infrared irradiation.ConclusionThe excellent therapeutic effects demonstrated in vitro and in vivo suggested the HMCN-based nanoplatform holds potential for efficient dual-responsive targeting drug delivery and synergistic chemo-photothermal therapy.

Project description:This work assessed the fabrication of nitrogen-doped CQDs (NCQDs) from alkali lignin (AL) obtained from spruce, representing a green, low-cost biomass generated by the pulp and biorefinery industries. The AL was found to retain its original lignin skeleton and could be used to produce NCQDs with excellent photoluminescence properties by one-pot hydrothermal treatment of AL and m-phenylenediamine. These NCQDs exhibited blue-green fluorescence (FL) with excitation/emission of 390/490 nm under optimal conditions. The NCQDs showed pH and excitation wavelength-dependent FL emission behaviors. On the basis of the exceptional selective response of these NCQDs to specific solvents, we developed a FL probe for the detection of formaldehyde (FA). The FL intensity of NCQDs was found to be directly proportional to the concentration of FA in the range of 0.05 to 2 mM (R 2 = 0.993), with a detection limit of 4.64 µM (based on 3σ/K). A composite film comprising NCQDs with poly(vinyl alcohol) was found to act as a sensor with a good FL response to FA gas. When exposed to gaseous FA, this film exhibited increased FL intensity and transitioned from blue-green to blue. A mechanism is proposed in which the NCQDs react rapidly with FA to generate Schiff bases that result in enhanced FL emission and the observed blue shift in color.

Project description:IntroductionThe anti-cancer potency of copper-doped carbon quantum dots (Cu-CDs) against breast cancer progression needs more detailed investigations.MethodsWith urea and ethylene glycol applied as carbon sources and copper sulfate used as a reactive dopant, Cu-CDs were synthesized in the current study by a one-step hydrothermal synthesis method, followed by the characterization and biocompatibility evaluations of Cu-CDs. Subsequently, the anti-cancer potency of Cu-CDs against breast cancer progression was confirmed by these biochemical, molecular, and transcriptomic assessments, including viability, proliferation, migration, invasion, adhesion, clonogenicity, cell cycle distribution, apoptosis, redox homeostasis, and transcriptomic assays of MDA-MB-231 cells.ResultsThe biocompatibility of Cu-CDs was confirmed based on the non-significant changes in the pathological and physiological parameters in the Cu-CDs treated mice, as well as the noncytotoxic effect of Cu-CDs on normal cells. Moreover, the Cu-CDs treatments not only decreased the viability, proliferation, migration, invasion, adhesion, and clonogenicity of MDA-MB-231 cells but also induced the redox imbalance, cell cycle arrest, and apoptosis of MDA-MB-231 cells via ameliorating the mitochondrial dysfunctions and regulating the MAPK signaling pathway.ConclusionOur findings confirmed the biosafety and excellent anti-cancer potency of Cu-CDs against breast cancer progression by tapping into mechanisms that disrupt malignant behaviors and oxidative homeostasis of breast cancer cells.

Project description:Effective antitumor nanomedicines maximize therapeutic efficacy by prolonging drug circulation time and transporting drugs to target sites. Although numerous nanocarriers have been developed for accurate tumor targeting, their limited water solubility makes their stable storage challenging, and poses biosafety risks in clinical translation. Herein, we choose reduced glutathione (GSH) to quick synthesize gram-scale water-soluble large amino acids mimicking carbon quantum dots (LAAM GSH-CQDs) enriched in steric chain amino acid groups with solubility of up to 2.0 g mL-1. The water-solubility arises from a hexagonal arrangement formed between amino acid groups and water molecules through hydrogen bonding, producing chair-form hexamer hydration layers covering LAAM GSH-CQDs. This endows a noticeable stability against long-term storage and adding electrolytes. Specifically, they exhibit negligible protein absorption, immunogenicity, and hemolysis, with stealth effect, showing an extraordinarily tolerated dose (5000 mg kg-1) in female mice. The rich amino acid groups simultaneously endow them considerable tumor-specific targeting. The loading of first-line chemotherapeutic drug doxorubicin onto LAAM GSH-CQDs through π-π stacking without sacrificing their merits achieves superior tumor inhibition and minimal side effects compared to commercial doxorubicin liposomal. The tumor-targeted drug delivery platform offered by LAAM GSH-CQDs holds significant promise for advancing clinical applications in cancer treatment.