Implementation of QbD Approach to the Development of Chromatographic Methods for the Determination of Complete Impurity Profile of Substance on the Preclinical and Clinical Step of Drug Discovery Studies

The purpose of this work was to demonstrate the use of the AQbD with the DOE approach to the methodical step-by-step development of a UHPLC method for the quantitative determination of the impurity profile of new CPL409116 substance (JAK/ROCK inhibitor) on the preclinical and clinical step of drug d...

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Autores principales: Gurba-Bryśkiewicz, Lidia, Dawid, Urszula, Smuga, Damian A., Maruszak, Wioleta, Delis, Monika, Szymczak, Krzysztof, Stypik, Bartosz, Moroz, Aleksandra, Błocka, Aleksandra, Mroczkiewicz, Michał, Dubiel, Krzysztof, Wieczorek, Maciej
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9505031/
https://www.ncbi.nlm.nih.gov/pubmed/36142622
http://dx.doi.org/10.3390/ijms231810720
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author Gurba-Bryśkiewicz, Lidia
Dawid, Urszula
Smuga, Damian A.
Maruszak, Wioleta
Delis, Monika
Szymczak, Krzysztof
Stypik, Bartosz
Moroz, Aleksandra
Błocka, Aleksandra
Mroczkiewicz, Michał
Dubiel, Krzysztof
Wieczorek, Maciej
author_facet Gurba-Bryśkiewicz, Lidia
Dawid, Urszula
Smuga, Damian A.
Maruszak, Wioleta
Delis, Monika
Szymczak, Krzysztof
Stypik, Bartosz
Moroz, Aleksandra
Błocka, Aleksandra
Mroczkiewicz, Michał
Dubiel, Krzysztof
Wieczorek, Maciej
author_sort Gurba-Bryśkiewicz, Lidia
collection PubMed
description The purpose of this work was to demonstrate the use of the AQbD with the DOE approach to the methodical step-by-step development of a UHPLC method for the quantitative determination of the impurity profile of new CPL409116 substance (JAK/ROCK inhibitor) on the preclinical and clinical step of drug discovery studies. The critical method parameters (CMPs) have been tested extensively: the kind of stationary phase (8 different columns), pH of the aqueous mobile phase (2.6, 3.2, 4.0, 6.8), and start (20–25%) and stop (85–90%) percentage of organic mobile phase (ACN). The critical method attributes (CMAs) are the resolution between the peaks (≥2.0) and peak symmetry of analytes (≥0.8 and ≤1.8). In the screening step, the effects of different levels of CMPs on the CMAs were evaluated based on a full fractional design 2(2). The robustness tests were established from the knowledge space of the screening step and performed by application fractional factorial design 2((4−1)). Method operable design region (MODR) was generated. The probability of meeting the specifications for the CMAs was calculated by Monte-Carlo simulations. In relation to literature such a complete AQbD approach including screening, optimization, and validation steps for the development of a new method for the quantitative determination of the full profile of nine impurities of an innovative pharmaceutical substance with the structure-based pre-development pointed out the novelty of our work. The final working conditions were as follows: column Zorbax Eclipse Plus C18, aqueous mobile phase 10 mM ± 1 mM aqueous solution of HCOOH, pH 2.6, 20% ± 1% of ACN at the start and 85% ± 1% of ACN at the end of the gradient, and column temperature 30 °C ± 2 °C. The method was validated in compliance with ICH guideline Q2(R1). The optimized method is specified, linear, precise, and robust. LOQ is on the reporting threshold level of 0.05% and LOD at 0.02% for all impurities.
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spelling pubmed-95050312022-09-24 Implementation of QbD Approach to the Development of Chromatographic Methods for the Determination of Complete Impurity Profile of Substance on the Preclinical and Clinical Step of Drug Discovery Studies Gurba-Bryśkiewicz, Lidia Dawid, Urszula Smuga, Damian A. Maruszak, Wioleta Delis, Monika Szymczak, Krzysztof Stypik, Bartosz Moroz, Aleksandra Błocka, Aleksandra Mroczkiewicz, Michał Dubiel, Krzysztof Wieczorek, Maciej Int J Mol Sci Article The purpose of this work was to demonstrate the use of the AQbD with the DOE approach to the methodical step-by-step development of a UHPLC method for the quantitative determination of the impurity profile of new CPL409116 substance (JAK/ROCK inhibitor) on the preclinical and clinical step of drug discovery studies. The critical method parameters (CMPs) have been tested extensively: the kind of stationary phase (8 different columns), pH of the aqueous mobile phase (2.6, 3.2, 4.0, 6.8), and start (20–25%) and stop (85–90%) percentage of organic mobile phase (ACN). The critical method attributes (CMAs) are the resolution between the peaks (≥2.0) and peak symmetry of analytes (≥0.8 and ≤1.8). In the screening step, the effects of different levels of CMPs on the CMAs were evaluated based on a full fractional design 2(2). The robustness tests were established from the knowledge space of the screening step and performed by application fractional factorial design 2((4−1)). Method operable design region (MODR) was generated. The probability of meeting the specifications for the CMAs was calculated by Monte-Carlo simulations. In relation to literature such a complete AQbD approach including screening, optimization, and validation steps for the development of a new method for the quantitative determination of the full profile of nine impurities of an innovative pharmaceutical substance with the structure-based pre-development pointed out the novelty of our work. The final working conditions were as follows: column Zorbax Eclipse Plus C18, aqueous mobile phase 10 mM ± 1 mM aqueous solution of HCOOH, pH 2.6, 20% ± 1% of ACN at the start and 85% ± 1% of ACN at the end of the gradient, and column temperature 30 °C ± 2 °C. The method was validated in compliance with ICH guideline Q2(R1). The optimized method is specified, linear, precise, and robust. LOQ is on the reporting threshold level of 0.05% and LOD at 0.02% for all impurities. MDPI 2022-09-14 /pmc/articles/PMC9505031/ /pubmed/36142622 http://dx.doi.org/10.3390/ijms231810720 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Gurba-Bryśkiewicz, Lidia
Dawid, Urszula
Smuga, Damian A.
Maruszak, Wioleta
Delis, Monika
Szymczak, Krzysztof
Stypik, Bartosz
Moroz, Aleksandra
Błocka, Aleksandra
Mroczkiewicz, Michał
Dubiel, Krzysztof
Wieczorek, Maciej
Implementation of QbD Approach to the Development of Chromatographic Methods for the Determination of Complete Impurity Profile of Substance on the Preclinical and Clinical Step of Drug Discovery Studies
title Implementation of QbD Approach to the Development of Chromatographic Methods for the Determination of Complete Impurity Profile of Substance on the Preclinical and Clinical Step of Drug Discovery Studies
title_full Implementation of QbD Approach to the Development of Chromatographic Methods for the Determination of Complete Impurity Profile of Substance on the Preclinical and Clinical Step of Drug Discovery Studies
title_fullStr Implementation of QbD Approach to the Development of Chromatographic Methods for the Determination of Complete Impurity Profile of Substance on the Preclinical and Clinical Step of Drug Discovery Studies
title_full_unstemmed Implementation of QbD Approach to the Development of Chromatographic Methods for the Determination of Complete Impurity Profile of Substance on the Preclinical and Clinical Step of Drug Discovery Studies
title_short Implementation of QbD Approach to the Development of Chromatographic Methods for the Determination of Complete Impurity Profile of Substance on the Preclinical and Clinical Step of Drug Discovery Studies
title_sort implementation of qbd approach to the development of chromatographic methods for the determination of complete impurity profile of substance on the preclinical and clinical step of drug discovery studies
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9505031/
https://www.ncbi.nlm.nih.gov/pubmed/36142622
http://dx.doi.org/10.3390/ijms231810720
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