In this work, highly luminescent carbon dots (CDs) were synthesized by the hydrothermal method at 170 °C for 12 h using pasteurized milk as a carbon source. The prepared CDs exhibited bright blue fluorescence under UV light illumination at 365 nm. The CDs show fluorescence life time of ~4.89 ns at excitation wavelength of 370 nm. The effect of different solvents on the fluorescence property of CDs was also investigated. The lisinopril (Lis)-loaded CDs were fabricated by self-assembly of lisinopril on the surfaces of CDs, which were characterized by UV-visible and FT-IR spectroscopic techniques. The controlled release of lisinopril from the Lis-CDs was realized at pH values of 5.2, 6.2 and 7.4, respectively. The results of the cytotoxicity and confocal laser scanning microscopic images indicate that the Lis-CDs were successfully uptaken by HeLa cells without apparent cytotoxicity. The synthesized CDs show great potential as drug vehicles with good biocompatibility, sustained release of lisinopril from CDs, indicating that the CDs can act as a promising drug delivery system for therapeutic delivery and/or bioimaging applications. 相似文献
Fluorescent carbon dots (CDs) have acquired growing interest from different areas over decades. Their fascinating property of tunable fluorescence by changing the excitation wavelength has attracted researchers worldwide. Understanding the mechanisms behind fluorescence is of great importance, as they help with the synthesis and applications, significantly when narrowed down to applications with color-tunable mechanisms. But, due to a lack of practical and theoretical information, the fluorescence mechanisms of CDs remain unknown, preventing the production of CDs with desired optical qualities. This review focuses on the PL mechanisms of carbon dots. The quantum confinement effect determined the carbon core, the surface and edge states determined by various surface defects and the connected functional/chemical groups on the surface/edges, the molecular state solely determined the fluorophores in the interior or surface of the CDs, and the Crosslink Enhanced Emission Effect are the currently confirmed PL mechanisms.
The ability to precisely sense physiological pH changes in the cellular environment is exceedingly difficult. Novel technologies are thus required to address this challenge. Fluorescent nanomaterials can be exploited to this effect because their optical properties can exhibit strong pH dependence. Herein, an intracellular pH-sensing probe is developed via a facile microwave-reaction synthesis method for the preparation of carbon dots (CDs) using glutathione and formamide. The CDs possess unique optical properties allowing for concomitant fluorescence in the blue and red regions of the spectrum. These dots are investigated as pH-sensors using the red fluorescence signatures at 650 and 680 nm. The two fluorescence bands respond differently following pH changes in their environment and could thus be used for ratiometric measurements. Cytotoxicity studies of the CDs in glioblastoma cells show no decrease in cell viability up to 100 μg mL−1 (24 h). Fluorescence imaging reveals that the dots localize in lysosomal compartments. Moreover, they can sense changes in lysosomal pH in response to serum and amino acid starvation, as well as administration of diclofenac and metformin, drugs currently in clinical trials for combination treatments of cancer. These CDs offer a new self-referencing approach for live intracellular pH sensing in 2D- and 3D-cell models. 相似文献