Eco-friendly-assessed micellar-fluorimetric platform for concurrent analysis of empagliflozin and prucalopride succinate in biological fluids: Docking simulation

[Display omitted] •Ultrasensitive and eco-friendly spectrofluorimetric platform.•Simultaneous analysis of empagliflozin and prucalopride succinate at nanogram scale.•The proposed platform was assessed for its greenness using the eco-scale tool.•The proposed platform was validated as per ICH guidelin...

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Veröffentlicht in:Spectrochimica acta. Part A, Molecular and biomolecular spectroscopy Molecular and biomolecular spectroscopy, 2023-08, Vol.296, p.122715, Article 122715
Hauptverfasser: Nour, Israa M., Mohamed, Ahmed R., Hasan, Mohamed A., Badrawy, Mohamed
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Sprache:eng
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Zusammenfassung:[Display omitted] •Ultrasensitive and eco-friendly spectrofluorimetric platform.•Simultaneous analysis of empagliflozin and prucalopride succinate at nanogram scale.•The proposed platform was assessed for its greenness using the eco-scale tool.•The proposed platform was validated as per ICH guidelines. Fluorescence spectroscopy has an important role in the determination of very small quantities of substances, especially in biological fluids. For this reason, most analysts have adopted the use of this technique in their biological studies and research, which helps them in the determination of any substance found in trace amounts. In addition to the high sensitivity of the fluorimetric technique, it has the advantages of simplicity and being green for the environment. All these reasons encourage the use of fluorimetric spectroscopy for quantifying co-administered therapy in biological fluids, which is considered a crucial step for patients, particularly in emergent cases requiring monitoring of administered therapeutic drugs. In this work, a sensitive, simple, economic, and environmentally friendly fluorimetric analytical technique was developed for the simultaneous determination of prucalopride succinate (a novel anti-constipation agent) and empagliflozin (an anti-diabetic agent) in pharmaceutical forms and spiked plasma depending on third-derivative signal processing at 333 and 314 nm, respectively. Conventional fluorescence spectra of both drugs showed a large overlap that hindered their simultaneous determination. So, third-order derivative fluorescence was adopted to overcome this overlap. The third-derivative corresponding to each spectrum was recorded using data points = 17 and a scaling factor of 10. The greenness of the proposed method was evaluated using an eco-scale scoring system, revealing excellent greenness. Analytical method parameters were validated following ICH guidelines. The method showed high sensitivity, covering a concentration range of 50–1100 ng/mL and 4–500 ng/mL for empagliflozin and prucalopride, respectively, allowing the pharmacokinetic study of both drugs in biological fluids. The LOD values were 14.09 and 0.91 ng/mL, while the LOQ values were 42.72 and 2.77 ng/mL for empagliflozin and prucalopride, respectively.
ISSN:1386-1425
1873-3557
DOI:10.1016/j.saa.2023.122715