An Estimation of Baricitinib by AQbD-driven UV SpectrophotometryDevelopment and Validation Process

IF 1.2 4区医学 Q4 CHEMISTRY, MEDICINAL

Letters in Drug Design & Discovery Pub Date : 2023-10-11 DOI:10.2174/0115701808252124231010055104

Laxmi Rani, Ashwini Kumar Mishra, Neha SL, Hitesh Kumar Dewangan, Pravat Kumar Sahoo

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Abstract

Background: Baricitinib (BCTB) is a novel Janus Kinase (JAK) 1 and 2 inhibitor used in the therapy of rheumatoid arthritis, approved by the “Food and Drug Administration” in 2018. It has significant dose-dependent effectiveness and severe side effects. Thus, it is crucial to figure out its concentration in developed dosage forms. The literature search revealed that there has only been one UV spectroscopy technique documented up to this point. Methanol was chosen as the detection medium in this approach, which is not comparable with plasma or serum. As a result, the preliminary research suggested developing a UV spectroscopic approach that can estimate BCTB concentration and compare it to its concentration in the plasma or serum. Thus, in the proposed method, 7.4 pH phosphate buffer was selected as a mobile phase. Aim: Using the Analytical Quality by Design (AQbD) methodology, a simple, robust spectrophotometric method for the detection of BCTB in API form and Niosomes drug delivery system is designed and assessed. Methods: In the AQbD approach, a face-centered CCD design of Design Expert 13 software was used to evaluate two critical method variables: scanning speed and sampling interval. The design space suitability was confirmed by standard error and overlay plots. The 2-D contour and 3-D response surface plots were used to forecast the relationship between the response variable and predictor variables. Results: Baricitinib displays an absorption maximum at 249.40 nm in saline phosphate buffer pH 7.4. The distinguished linearity of the method was obtained over a concentration of 5–30 µg/ml with a correlation coefficient (R2 ) value of 0.998. BCTB % assay was found to be near 99 %. Intraday and Interday precision were found to have % RSDs of 0.067–0.488 and 0.146–0.942, respectively. Conclusion: The established spectrophotometric technique was observed to be precise as per ICH revised guidelines ICH Q2 (R1) and Q14 for analytical method validation. Our findings are instructional for the future design and development of safe and reliable therapeutic dosage forms of BCTB for rheumatoid arthritis.

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aqbd驱动紫外分光光度法测定巴西替尼的研究

背景:Baricitinib (BCTB)是一种用于治疗类风湿性关节炎的新型Janus激酶(JAK) 1和2抑制剂，于2018年获得美国食品药品监督管理局(fda)批准。它具有明显的剂量依赖性和严重的副作用。因此，在已开发的剂型中计算出其浓度是至关重要的。文献检索显示，到目前为止，只有一种紫外光谱技术被记录在案。该方法选择甲醇作为检测介质，与血浆或血清没有可比性。因此，初步研究建议开发一种紫外光谱方法，可以估计BCTB的浓度，并将其与血浆或血清中的浓度进行比较。因此，在所提出的方法中，选择7.4 pH的磷酸盐缓冲液作为流动相。目的:采用设计质量分析(AQbD)方法，设计一种简便、可靠的分光光度法检测原料药剂型和Niosomes给药系统中的BCTB。方法:在AQbD方法中，采用design Expert 13软件的面心CCD设计来评估两个关键的方法变量:扫描速度和采样间隔。通过标准误差和叠加图验证了设计空间的适宜性。利用二维轮廓图和三维响应面图预测响应变量与预测变量之间的关系。结果:Baricitinib在pH 7.4的盐水磷酸盐缓冲液中在249.40 nm处具有最大的吸收。在浓度为5 ~ 30µg/ml范围内，本法的线性关系良好，相关系数(R2)为0.998。bbcb %测定接近99%。日内精密度和日内精密度的% rsd分别为0.067 ~ 0.488和0.146 ~ 0.942。结论:所建立的分光光度法符合ICH修订指南ICH Q2 (R1)和Q14对分析方法验证的要求。我们的研究结果对未来设计和开发安全可靠的类风湿性关节炎bbcb治疗剂型具有指导意义。

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来源期刊

Letters in Drug Design & Discovery 医学-医药化学

CiteScore

1.80

自引率

10.00%

发文量

245

审稿时长

3 months

期刊介绍： Aims & Scope Letters in Drug Design & Discovery publishes letters, mini-reviews, highlights and guest edited thematic issues in all areas of rational drug design and discovery including medicinal chemistry, in-silico drug design, combinatorial chemistry, high-throughput screening, drug targets, and structure-activity relationships. The emphasis is on publishing quality papers very rapidly by taking full advantage of latest Internet technology for both submission and review of manuscripts. The online journal is an essential reading to all pharmaceutical scientists involved in research in drug design and discovery.