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载碳点壳聚糖印迹聚合物作为荧光传感器、分散固相萃取剂和药物载体

Chloramphenicol-imprinted polychitosan bounded with carbon dots as fluorescent sensor, dispersive sorbent, and drug carrier.

机构信息

School of Pharmacy, China Medical University, No. 100, Sec. 1, Jingmao Rd., Beitun Dist, Taichung, 406040, Taiwan.

Department of Beauty and Health Care, Min-Hwei Junior College of Health Care Management, No. 1116, Sec 2, Zhongshan E. Rd, Tainan, 73658, Taiwan.

出版信息

Mikrochim Acta. 2024 Apr 1;191(4):227. doi: 10.1007/s00604-024-06324-1.

Abstract

Chitosan, an abundant natural polysaccharide, was conjugated with carbon dots (CDs) and self-polymerized with chloramphenicol (CAP) templates to synthesize CD-incorporated and molecularly CAP-imprinted polychitosan (CD-MIC). The CD-MIC was used for fluorescent sensing, dispersive sorption, and dosage release of CAP at different pH levels. The sphere of action mechanism, approved by emission and excitation fluorescence, UV-Vis absorption, and fluorescence lifetime measurements, regulated the fluorescence static quenching. By the Perrin model, the quenching extent was linearly correlated to CAP within 0.17 - 33.2 μM (LOD = 37 nM) at pH 7.0. With an imprinting factor of 3.1, the CD-MIC was more selective for CAP than CD, although it was less sensitive to CAP. The recoveries of 5.0 μM CAP from milk matrix were 95% (RSD = 2.3%) for CD-MIC probes and 62% (RSD = 4.5%) for CD. The Langmuir and pseudo-second-order models preferably described the isothermal and kinetic sorptions of CAP into the imprinted cavities in CD-MICs, respectively. The Weber - Morris kinetic model showed three stages involved in intraparticle diffusion, which was pH-dependent and gradually arduous at the later stage, and showed external diffusion partly engaged in the diffusion mechanism. The 20 - 70% of CAP formulated in CAP-embedded CD-MICs were released in 8 - 48 h. The release percentage was lower at pH 7.0 than at pH 5.0 and 9.0, but the equilibrium time was shorter. At pH 7.0, the release percentage reached 45% at 10 min and slowly increased to 51% at 24 h.

摘要

壳聚糖是一种丰富的天然多糖,与碳点(CDs)结合,并与氯霉素(CAP)模板自聚合,合成了包含 CD 的分子印迹聚壳聚糖(CD-MIC)。CD-MIC 用于在不同 pH 值下对 CAP 进行荧光传感、分散吸附和剂量释放。通过发射和激发荧光、紫外-可见吸收和荧光寿命测量证实的作用机制球体调节了荧光静态猝灭。通过 Perrin 模型,在 pH 7.0 时,猝灭程度与 0.17-33.2 μM 范围内的 CAP 呈线性相关(LOD=37 nM)。在具有 3.1 倍印迹因子的情况下,CD-MIC 对 CAP 的选择性高于 CD,尽管对 CAP 的灵敏度较低。从牛奶基质中回收 5.0 μM CAP 的 CD-MIC 探针的回收率为 95%(RSD=2.3%),而 CD 的回收率为 62%(RSD=4.5%)。Langmuir 和拟二级动力学模型分别优选地描述了 CAP 在 CD-MIC 印迹腔中的等温和动力学吸附。Weber-Morris 动力学模型表明,三个阶段涉及颗粒内扩散,这与 pH 有关,在后期阶段逐渐困难,并且显示外部扩散部分参与了扩散机制。在 CAP 嵌入的 CD-MIC 中,20%-70%的 CAP 在 8-48 小时内释放。在 pH 7.0 时的释放百分比低于 pH 5.0 和 9.0,但平衡时间较短。在 pH 7.0 时,在 10 分钟时释放百分比达到 45%,并缓慢增加到 24 小时时的 51%。

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