Evaluation of Differences in Dosage Form Performance of Generics Using BCS-Based Biowaiver Specifications and Biopharmaceutical Modeling–Case Examples Amoxicillin and Doxycycline

Hofsäss, Martin A.; Dressman, Jennifer B.

doi:10.1016/j.xphs.2020.04.011

Cited by 14 publications

(13 citation statements)

References 48 publications

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“…Hofs€ ass and Dressman recently reported building a PBPK absorption model for amoxicillin and doxycycline and conducting virtual BE studies with some modifications to the default model values, i.e., the mean gastric pH was set to 2.7 and varied between 1.2 and 4.5, and the mean gastric transit time of 0.28 h was varied between 0 and 0.8 h. In addition, the percentage of fluid volume in the small and large intestine was set to 7.5% and 2%, respectively. 75 These values are closer to those reported in vivo and the effect of varying these parameters in a population can be assessed better. Depending on the formulation, various GIT parameters may need to be modified accordingly (e.g., gastric transit time may need to be greatly extended for non-disintegrating formulations).…”

Section: Discussionsupporting

confidence: 69%

Evaluating the Impact of Physiological Properties of the Gastrointestinal Tract On Drug In Vivo Performance Using Physiologically Based Biopharmaceutics Modeling and Virtual Clinical Trials

Jereb

Opara²,

Bajc³

et al. 2021

Journal of Pharmaceutical Sciences

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Section: Discussionsupporting

confidence: 69%

Evaluating the Impact of Physiological Properties of the Gastrointestinal Tract On Drug In Vivo Performance Using Physiologically Based Biopharmaceutics Modeling and Virtual Clinical Trials

Jereb

Opara²,

Bajc³

et al. 2021

Journal of Pharmaceutical Sciences

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“…The current BCS-biowaiver approach has been widely criticized for being overdiscriminating and overly strict, excluding opportunities not only for scientifically justified extensions to certain BCS class II compounds but also for drug substances which are in theory eligible for BCS-based biowaivers but failed to comply with criteria in the dissolution performance. − Several publications have implemented PBBM approaches, including VBE, to investigate the variables limiting drug absorption, support possible BCS-based biowaiver extensions, and recommend specifications based on the in vivo performance. ,− On the other hand, it has been suggested that products containing drugs belonging to BCS class I and III might exhibit a high risk of bioequivalence failure due to their intrinsic pharmacokinetic properties (e.g., if they have a high first-pass effect or short half-life) and that the eligibility of their products for biowaiver might need to be revised . Further concerns have been raised, especially for products including BCS class III drugs, on the potential interactions of different excipients with gut transporters, which in turn could lead to increased risk for bioequivalence. − On the whole, it seems that regulatory confidence in the performance of PBPK models for justification of biowaivers is still rather tentative.…”

Section: Current Statusmentioning

confidence: 99%

Physiologically Based Pharmacokinetic/Pharmacodynamic Modeling to Support Waivers of In Vivo Clinical Studies: Current Status, Challenges, and Opportunities

Loisios-Konstantinidis

Dressman

2020

Mol. Pharmaceutics

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Physiologically based pharmacokinetic/pharmacodynamic (PBPK/PD) modeling has been extensively applied to quantitatively translate in vitro data, predict the in vivo performance, and ultimately support waivers of in vivo clinical studies. In the area of biopharmaceutics and within the context of model-informed drug discovery and development (MID3), there is a rapidly growing interest in applying verified and validated mechanistic PBPK models to waive in vivo clinical studies. However, the regulatory acceptance of PBPK analyses for biopharmaceutics and oral drug absorption applications, which is also referred to variously as “PBPK absorption modeling” [CPT: Pharmacometrics Syst. Pharmacol.20176492], “physiologically based absorption modeling”, or “physiologically based biopharmaceutics modeling” (PBBM), remains rather low [J. Pharm. Sci.20161052723] [AAPS J.20192129]. Despite considerable progress in the understanding of gastrointestinal (GI) physiology, in vitro biopharmaceutic and in silico tools, PBPK models for oral absorption often suffer from an incomplete understanding of the physiology, overparameterization, and insufficient model validation and/or platform verification, all of which can represent limitations to their translatability and predictive performance. The complex interactions of drug substances and (bioenabling) formulations with the highly dynamic and heterogeneous environment of the GI tract in different age, ethnic, and genetic groups as well as disease states have not been yet fully elucidated, and they deserve further research. Along with advancements in the understanding of GI physiology and refinement of current or development of fully mechanistic in silico tools, we strongly believe that harmonization, interdisciplinary interaction, and enhancement of the translational link between in vitro, in silico, and in vivo will determine the future of PBBM. This Perspective provides an overview of the current status of PBBM, reflects on challenges and knowledge gaps, and discusses future opportunities around PBPK/PD models for oral absorption of small and large molecules to waive in vivo clinical studies

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“…Additionally, the influence of external factors (for example vibration) and internal factors (for example air bubbles in the dissolution medium, vibration, stirring speed) is lower compared to conventional round-bottom vessels (7). Therefore, not only is the dissolution rate increased when peak vessels are used, it will also be more complete (6,7,20). As this simple modification reduces several artifactual effects commonly encountered in dissolution, peak vessels have often been recommended as a good alternative to increasing the rotation speed.…”

Section: Does Increasing the Rotation Speed Consistently Increase Thementioning

confidence: 99%

“…However, the disadvantages of using a sinker for the dissolution test (as discussed in sections 2 and 3 above) should be considered, and a sinker should be identified that does not artifactually change the dissolution in other ways. With respect to coning, the use of a sinker should be discouraged because there are more efficient ways to counteract this problem such as increasing the rotation speed or using peak vessels (6,7,20).…”

Section: Some Tips For the Use Of Sinkersmentioning

confidence: 99%

“…But, as this beneficial effect on the coning was only observed for one sinker type (CLIPS sinker, acetaminophen capsules, 75 and 100 rpm), the negative effects appear to outweigh any positive effect for most of the sinker types. Thus, we cannot recommend using a sinker to overcome coning; increasing the rotation speed or peak vessels should be considered instead (6,7,20).…”

Section: Which Sinker?mentioning

confidence: 99%

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Investigation of Dissolution Performance of Hard Gelatin Capsule Products Using Various Sinkers

Mansuroglu¹,

Dressman²

2020

Dissolution Technol.

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Dissolution testing is a commonly used tool for the quality control of various dosage forms. For this purpose, consistent test conditions are necessary to obtain reproducible test results. Typical issues that can affect the dissolution performance of tested capsule formulations are floating and coning. Recently, the International Conference on Harmonisation (ICH) guideline recommended the use of sinkers to prevent coning, although no accompanying data to support the recommendation has been published in the open literature to date. Therefore, we initiated studies designed to address the following key questions. A) Do all sinkers prevent flotation of the dosage form? B) Does using sinkers consistently increase the dissolution rate? C) Do sinkers consistently decrease coning? Three commercially available hard capsule drug products were studied: acetaminophen, fluconazole, and ketoprofen. Dissolution was performed without a sinker and with four commercially available sinkers (CLIPS, CAPLOTH, CAPWAST, and JP). Analysis of the results revealed that, although three of the four sinkers were able to adequately address flotation problems, in many cases their use led to artifactual increases or decreases in the dissolution of the capsules. Further, sinkers do not seem to be generally useful for addressing coning issues. Instead, an increase in the stirring speed or use of peak vessels should be considered.

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Evaluation of Differences in Dosage Form Performance of Generics Using BCS-Based Biowaiver Specifications and Biopharmaceutical Modeling–Case Examples Amoxicillin and Doxycycline

Cited by 14 publications

References 48 publications

Evaluating the Impact of Physiological Properties of the Gastrointestinal Tract On Drug In Vivo Performance Using Physiologically Based Biopharmaceutics Modeling and Virtual Clinical Trials

Evaluating the Impact of Physiological Properties of the Gastrointestinal Tract On Drug In Vivo Performance Using Physiologically Based Biopharmaceutics Modeling and Virtual Clinical Trials

Physiologically Based Pharmacokinetic/Pharmacodynamic Modeling to Support Waivers of In Vivo Clinical Studies: Current Status, Challenges, and Opportunities

Investigation of Dissolution Performance of Hard Gelatin Capsule Products Using Various Sinkers

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