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D-最优设计作为一种有用的工具,响应面法,用于优化同步荧光信号,以实现阿伐那非和他达拉非的同时测定。

D-optimal design as a useful tool response surface methodology for the optimization of signals from synchronous fluorescence prior to simultaneous determination of avanafil and tadalafil.

机构信息

Pharmaceutical Analytical Chemistry Department, Faculty of Pharmacy, Al-Azhar University, 11751 Nasr City, Cairo, Egypt.

Pharmaceutical Analytical Chemistry Department, Faculty of Pharmacy, Al-Azhar University, 11751 Nasr City, Cairo, Egypt; Pharmaceutical Chemistry Department, Heliopolis University, Cairo-Belbeis Desert Rd El-Nahda, El-Salam, Cairo Governorate 11777, Egypt.

出版信息

Spectrochim Acta A Mol Biomol Spectrosc. 2020 Jul 5;235:118313. doi: 10.1016/j.saa.2020.118313. Epub 2020 Mar 31.

DOI:10.1016/j.saa.2020.118313
PMID:32251891
Abstract

A rapid, smart and sensitive first derivative spectrofluorimetric method has been carried out for the simultaneous estimation of avanafil and tadalafil either in their pure form, tablet dosage form or spiked human plasma. The measurements of normal emission spectra or synchronous fluorescence intensity of both drugs show severe overlap which hindered their determination using normal fluorescence or synchronous intensity. Therefore, a highly sensitive first derivative synchronous fluorescence procedure was used to resolve this overlap. The method is based upon measurement of the amplitude of the first derivative of synchronous fluorescence intensity of both drugs at Δλ = 70 nm and at suitable wavelength of 396 nm and 364 nm for avanafil and tadalafil, respectively. Under the optimum conditions, the linear determination ranges are 50-1800 and 5-400 ng mL with a detection limit of 12.93 and 1.46 ng mL for avanafil and tadalafil, respectively. A response surface methodology was used for optimization using D-optimal design which can be used for determination of the exact optimum parameters specifically designed for this method. In addition; it is a good way to graphically clarify the relationship between various experimental variables and the synchronous fluorescence intensity.

摘要

一种快速、灵敏且敏感的一阶导数分光荧光法已被用于同时测定阿伐那非和他达拉非在纯品、片剂或加标人血浆中的含量。两种药物的正常发射光谱或同步荧光强度的测量存在严重重叠,这阻碍了使用普通荧光或同步强度来测定它们。因此,采用了高灵敏度的一阶导数同步荧光法来解决这种重叠。该方法基于测量两种药物的同步荧光强度一阶导数的振幅,阿伐那非和他达拉非的 Δλ分别为 70nm 和合适的波长 396nm 和 364nm。在最佳条件下,线性测定范围分别为 50-1800ng/mL 和 5-400ng/mL,阿伐那非和他达拉非的检测限分别为 12.93ng/mL 和 1.46ng/mL。响应面法(RSM)采用 D-最优设计进行优化,该设计可用于确定专门为此方法设计的精确最佳参数。此外,它是一种直观地阐明各种实验变量与同步荧光强度之间关系的好方法。

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