基于设计的反相高效液相色谱法测定大鼠血浆和粪便微生物群提取物为基础的固体自纳米乳化给药体系中姜黄素的质量。

Q3 Medicine

Current Drug Research Reviews Pub Date : 2023-01-01 DOI:10.2174/2589977515666230120140543

Leander Corrie, Monica Gulati, Jaskiran Kaur, Ankit Awasthi, Sukriti Vishwas, Arya Kadukkattil Ramanunny, Rubiya Khursheed, Kamal Dua, Dinesh Kumar Chellappan, Sachin Kumar Singh

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引用次数: 3

摘要

背景:姜黄素(Curcumin, CRM)被认为具有多种治疗特性，如抗炎和抗糖尿病特性，因此被认为是一种有效的治疗药物。目的:首次报道了一种灵敏的血浆及粪便基固体自纳米乳化给药系统(S-SNEDDS)中CRM的测定方法。方法:采用Box-Behnken设计优化生物分析方法，共13次运行，3次响应。以甲醇和水(70:30 v/v)为溶剂，流速为1 mL/min。槲皮素作为内标。并对所研制的CRM固体自纳米乳化给药系统进行了特异性试验。结果:中药留置时间为14.18 min。结果表明，该方法在50 ~ 250 ng/mL范围内呈线性关系，R2为0.999。准确性研究表明，CRM的回收率分别小于105%和大于95%。精密度研究进行了间，日内和分析师间的精密度，并发现%RSD小于2%。检测限和定量限分别为3.37 ng/mL和10.23 ng/mL。短期、长期和冻融循环的稳定性研究显示，RSD小于2%，表明CRM在血浆基质中的稳定性。此外，在含有粪便微生物群提取物的固体纳米乳化给药系统中，空白粪便微生物群提取物浆液在CRM的保留时间内没有出现任何峰值，表明其特异性。结论:该方法可用于血液样品中黄酮含量的估算，同时也为植物类黄酮及粪便微生物群提取物的估算提供了一种简便、灵敏的方法，具有一定的临床应用价值。

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Quality by Design-based RP-HPLC Method for Estimation of Curcumin in Rat Plasma and Fecal Microbiota Extract-based Solid Self-nano Emulsifying Drug Delivery System.

Background: Curcumin (CRM) is known to possess various therapeutic properties, such as anti-inflammatory and antidiabetic properties, and is, therefore, considered to be an effective therapeutic.

Objective: A sensitive method for the estimation of CRM in plasma, as well as fecal matter-based solid self-nano emulsifying drug delivery system (S-SNEDDS), has been reported for the first time.

Methods: A bioanalytical method was optimized using Box-Behnken Design having 13 runs and 3 responses. The optimized method was developed using methanol and water (70:30 v/v) with a flow rate of 1 mL/min. Quercetin was used as an internal standard. A specificity test was also performed for the developed CRM solid self-nano emulsifying drug delivery system.

Results: The retention time of CRM was found to be 14.18 minutes. The developed method was validated and found to be linear in the range of 50-250 ng/mL with an R² of 0.999. Accuracy studies indicated that CRM had a percentage recovery of less than 105% and more than 95%, respectively. Precision studies were carried out for inter, intraday, and inter-analyst precision, and the %RSD was found to be less than 2%. The limit of detection (LOD) and limit of quantification (LOQ) were found to be 3.37 ng/mL and 10.23 ng/mL, respectively. Stability studies for shortterm, long term and freeze-thaw cycles showed a %RSD of less than 2%, indicating the stability of CRM in the plasma matrix. Moreover, the blank fecal microbiota extract slurry did not show any peak at the retention time of CRM in a CRM-loaded solid nanoemulsifying drug delivery system containing fecal microbiota extract indicating its specificity.

Conclusion: Hence, the developed method can have clinical implications as it helps estimate CRM in blood samples and also provides a simple and sensitive method for the estimation of plant-based flavonoids along with fecal microbiota extract formulations.

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来源期刊

Current Drug Research Reviews Medicine-Psychiatry and Mental Health

CiteScore

3.70

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0.00%

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