Research Update of Emergent Sulfur Quantum Dots in Synthesis and Sensing/Bioimaging Applications
Abstract
:1. Introduction
2. Synthetic Methods of SQDs
2.1. Acid Etching Oxidation Method
2.2. Assembly-Fission Method
2.3. Surface-Etching Method
2.4. Oxygen-Accelerated Method
2.5. Ultrasonication and Microwave Method
2.6. One-Step Hydrothermal Method
2.7. Other Methods
3. Applications
3.1. Sensing
3.1.1. Fluorescence Sensing
3.1.2. Colorimetric and Fluorescence Dual-Channel Sensing
3.1.3. Ratiometric Fluorescent Sensing
3.1.4. Electrochemical Sensing
3.1.5. Electrochemiluminescence Sensing
3.2. Bioimaging
4. Challenges and Prospects
- Currently, as shown in Table 1, for most reported synthetic methods, the synthesis time was shortened but with a relatively low QY, or QY was effectively improved but with a prolonged synthesis process. This suggested that more research efforts should be made to develop faster and simpler synthesis methods with higher QY and well-defined luminescence mechanisms. Meanwhile, the optical characteristics can be affected by side products, so the complex purification process should be simplified to achieve efficient product separation and purification.
- In these reported methods, most of the precursors were bulk sulfur powder, PEG, and NaOH; thus requiring a large amount of bulk sulfur powder. Although Arshad et al. [45] used sodium thiosulfate as precursors to produce elemental sulfur, that is not enough, and it is necessary to find new precursors to design effective reaction systems.
- From the perspective of sensing and bioimaging applications, one limitation for the reported SQDs is that most of their emission colors were focused on blue and green, which could be easily interfered with by the self-fluorescence of biological samples. This problem can be solved by synthesizing SQDs with red or near infrared or even infrared-II fluorescence, and such emission modulation can be achieved by doping heteroatoms, changing passivators and reaction conditions, etc.
- For sensing applications, the target molecules are limited, including metal ions (Fe3+, Ag+, Hg2+, Co2+, Zn2+, Cr6+, Ce4+), Dox, AA, CQ, norfloxacin, BChE, miRNA-21, and GSH. One of the possible reasons for this is the limited functional groups on the surface of SQDs, resulting in their limited ability to recognize the target molecules.
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Conflicts of Interest
References
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Method | Precursor | Solvent | Ligand | Temperature | Reaction Time | QY | Emission Wavelength | Application | Ref. |
---|---|---|---|---|---|---|---|---|---|
Acid etching oxidation | CdS or ZnS QDs, HNO3aqueous solution | n-hexane, H2O | Not mention | RT | 36 h | 0.549% | 428 nm | Quenching by Fe3+ | [19] |
Assembly-fission | Sublimed sulfur, NaOH | H2O | PEG-400 | 70 °C | 125 h | 3.8% | 529−488 nm | ECL inannihilation reaction, CL from oxidation | [30] |
Surface etching | Sulfur powder, NaOH, H2O2 | H2O | PEG | 70 °C | 5 h | 23% | 440–500 nm | LEDs | [27] |
Surface etching | Sulfur powder, NaOH, Cu2+ | H2O | PEG-400 | 70 °C | 72 h | 32.8% | 425–525 nm | No | [31] |
Surface etching | Sulfur powder, NaOH, H2O2 | H2O | PSS | 70 °C | 12 h | 5.13% | 420 nm | Anti-bacteria | [28] |
Oxygen accelerated | Sublimed sulfur, NaOH, pure O2 | H2O | PEG-400 | 90 °C | 10 h | 21.5% | 490 nm | Cellular imaging | [32] |
Oxygen accelerated | Sublimed sulfur, NaOH, N2 or air | H2O | PEG-400 | 70 °C | 72 h | 8% | 425–500 nm | No | [33] |
Oxygen accelerated | Sublimed sulfur, NaOH, pure O2 | H2O | CMC | 90 °C | 24 h | 7.1% | 434 nm | Detection of Cr6+ and AA, cell imaging | [34] |
Oxygen accelerated | Sublimed sulfur, NaOH, pure O2 | H2O | HP-β-CD | 85 °C | 12 h | 4.66% | 443 nm | Detection of TTZ, cell imaging | [35] |
Oxygen accelerated | Sublimed sulfur, NaOH, pure O2 | H2O | PVA | 75 °C | 12 h | 4.62% | 443 nm | Quenching by Fe3+, Nanothermometer to monitor cell temperature | [36] |
Ultrasonication and microwave | Sublimated sulfur, Na2S | H2O | PEG-400 | RT, ultrasonication | 12 h | 2.1% | 515–562 nm | Cellular imaging | [37] |
Ultrasonication and microwave | Sulfur powder, NaOH, H2O2 | H2O | PEG-400 | 70, 80, 90 and 95 °C via microwave, 70 °C | 5 min for microwave, 40 h | 49.25% | 445–506 nm | No | [38] |
Ultrasonication and microwave | Sublimed sulfur, NaOH, H2O2 | H2O | PEG-400 | 70 °C, ultrasound-microwave | 2 h | 58.6% | 440 nm | Ce4+ and AA detection | [39] |
One-step hydrothermal | Sulfur (monoclinic phase), NaOH | H2O | PEG | 170 °C | 4 h | 4.02% | 554 nm | No | [40] |
One-step hydrothermal | Sublimed sulfur, H2O2 | H2O | PEG-400 | 220 °C | 42 h | 10.3% | 365 nm | Fe3+ detection, cellular imaging | [41] |
Situ reaction | Sodium thiosulfate, oxalic acid, NaOH | H2O | PEG-400 | 70 °C | 6 h | 2.5% | 462 nm | Colorimetric discrimination of multiple metal ions | [42] |
Mechanochemical | Sodium thiosulfate, oxalic acid, NaOH | H2O | PEG-400 | RT | 1 h | 4.8% | 461 nm | Cellular imaging | [26] |
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Ning, K.; Sun, Y.; Liu, J.; Fu, Y.; Ye, K.; Liang, J.; Wu, Y. Research Update of Emergent Sulfur Quantum Dots in Synthesis and Sensing/Bioimaging Applications. Molecules 2022, 27, 2822. https://doi.org/10.3390/molecules27092822
Ning K, Sun Y, Liu J, Fu Y, Ye K, Liang J, Wu Y. Research Update of Emergent Sulfur Quantum Dots in Synthesis and Sensing/Bioimaging Applications. Molecules. 2022; 27(9):2822. https://doi.org/10.3390/molecules27092822
Chicago/Turabian StyleNing, Keke, Yujie Sun, Jiaxin Liu, Yao Fu, Kang Ye, Jiangong Liang, and Yuan Wu. 2022. "Research Update of Emergent Sulfur Quantum Dots in Synthesis and Sensing/Bioimaging Applications" Molecules 27, no. 9: 2822. https://doi.org/10.3390/molecules27092822