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Open Access

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Year : July 18, 2024 at 12:50 pm | [if 1553 equals=””] Volume :14 [else] Volume :14[/if 1553] | [if 424 equals=”Regular Issue”]Issue[/if 424][if 424 equals=”Special Issue”]Special Issue[/if 424] [if 424 equals=”Conference”][/if 424] : 02 | Page : 1-9

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H. Padma Latha, S. Deepa, CH. Sri Divya, S. Raja Sree, G. Aruna

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Professor, Associate Professor, Associate Professor, Associate Professor, Associate Professor Department of pharmaceutics, Gyana Jyothi College of Pharmacy, Hyderabad, Department of pharmaceutics, Gyana Jyothi College of Pharmacy, Hyderabad, Department of pharmaceutics, Gyana Jyothi College of Pharmacy, Hyderabad, Department of pharmaceutics, Gyana Jyothi College of Pharmacy, Hyderabad, Department of pharmaceutics, Gyana Jyothi College of Pharmacy, Hyderabad Telangana, Telangana, Telangana, Telangana, Telangana India, India, India, India, India

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Abstract

nA straightforward, precise method was developed to simultaneously assess Bempedoic acid and Rosuvastatin in both bulk and tablet forms. Utilizing a DIKMA Spursil C18 column (4.6 mm x 250 mm, 3.0 μm), chromatography was conducted with a mobile phase comprising 30% phosphate buffer and 70% acetonitrile, flowing at 1 ml/min. Operating at ambient temperature, the optimized wavelength for detection was set at 240 nm, revealing retention times of 4.418 min for Bempedoic acid and 3.524 min for Rosuvastatin. Both compounds exhibited high purity levels, with Bempedoic acid at 100.57% and Rosuvastatin at 100.15%. The system’s suitability parameters, such as theoretical plates and tailing factor, fell within acceptable thresholds at 4402.39 and 6959.54, respectively, with values of 1.12 and 3.60.Linearity studies demonstrated strong correlation coefficients (r2) of 0.999 for both Bempedoic acid and Rosuvastatin, with mean recovery percentages of 100.33% and 100.74%, respectively. Repeatability showed low % RSD values of 1.0 and 0.3, while intermediate precision displayed % RSD values of 0.7 and 1.2, respectively. Overall, the precision study affirmed the method’s reliability, robustness, and repeatability. These findings validate the proposed RP‐HPLC method as a dependable, rapid, and reproducible technique suitable for routine estimation of Bempedoic acid and Rosuvastatin in both bulk and tablet forms.

Keywords: Bempedoic acid, Rosuvastatin, RP‐HPLC, Simultaneous estimation.

n[if 424 equals=”Regular Issue”][This article belongs to Research & Reviews: A Journal of Toxicology(rrjot)]

[/if 424][if 424 equals=”Special Issue”][This article belongs to Special Issue under section in Research & Reviews: A Journal of Toxicology(rrjot)][/if 424][if 424 equals=”Conference”]This article belongs to Conference [/if 424]

How to cite this article: H. Padma Latha, S. Deepa, CH. Sri Divya, S. Raja Sree, G. Aruna. Toxicology-Focused Development and Validation of an RP-HPLC Technique for Quantifying Bempefoic Acid and Rosuvastatin in a Fixed-Dose Combination. Research & Reviews: A Journal of Toxicology. July 18, 2024; 14(02):1-9.

How to cite this URL: H. Padma Latha, S. Deepa, CH. Sri Divya, S. Raja Sree, G. Aruna. Toxicology-Focused Development and Validation of an RP-HPLC Technique for Quantifying Bempefoic Acid and Rosuvastatin in a Fixed-Dose Combination. Research & Reviews: A Journal of Toxicology. July 18, 2024; 14(02):1-9. Available from: https://journals.stmjournals.com/rrjot/article=July 18, 2024/view=0

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References

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Citrate Lyase. Curr Atheroscler Rep. 2016 Oct;18(10):61. doi: 10.1007/s11883-016-0611-4.
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7. Uma Sai Teja Yarra and Sowjanya Gummadi: Stability indicating RP-HPLC method for
simultaneous quantification of bempedoic acid and ezetimibe in bulk and pharmaceutical
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DOI: https://doi.org/10.37591/RRJoT.v14i02.0

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[if 424 not_equal=””]Regular Issue[else]Published[/if 424] Subscription Original Research

Research & Reviews: A Journal of Toxicology

[if 344 not_equal=””]ISSN: 2231-3834[/if 344]

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Volume	14
[if 424 equals=”Regular Issue”]Issue[/if 424][if 424 equals=”Special Issue”]Special Issue[/if 424] [if 424 equals=”Conference”][/if 424]	02
Received	March 26, 2024
Accepted	April 2, 2024
Published		July 18, 2024

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