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| Author | : Eiman Atiek |
| Publisher | : |
| Total Pages | : |
| Release | : 2021 |
| Genre | : Amino acids |
| ISBN | : |
| Author | : Robert O. Williams III |
| Publisher | : Springer Science & Business Media |
| Total Pages | : 656 |
| Release | : 2011-12-04 |
| Genre | : Medical |
| ISBN | : 1461411440 |
This volume is intended to provide the reader with a breadth of understanding regarding the many challenges faced with the formulation of poorly water-soluble drugs as well as in-depth knowledge in the critical areas of development with these compounds. Further, this book is designed to provide practical guidance for overcoming formulation challenges toward the end goal of improving drug therapies with poorly water-soluble drugs. Enhancing solubility via formulation intervention is a unique opportunity in which formulation scientists can enable drug therapies by creating viable medicines from seemingly undeliverable molecules. With the ever increasing number of poorly water-soluble compounds entering development, the role of the formulation scientist is growing in importance. Also, knowledge of the advanced analytical, formulation, and process technologies as well as specific regulatory considerations related to the formulation of these compounds is increasing in value. Ideally, this book will serve as a useful tool in the education of current and future generations of scientists, and in this context contribute toward providing patients with new and better medicines.
| Author | : Robert O. Williams III |
| Publisher | : Springer |
| Total Pages | : 648 |
| Release | : 2011-12-03 |
| Genre | : Medical |
| ISBN | : 9781461411451 |
This volume is intended to provide the reader with a breadth of understanding regarding the many challenges faced with the formulation of poorly water-soluble drugs as well as in-depth knowledge in the critical areas of development with these compounds. Further, this book is designed to provide practical guidance for overcoming formulation challenges toward the end goal of improving drug therapies with poorly water-soluble drugs. Enhancing solubility via formulation intervention is a unique opportunity in which formulation scientists can enable drug therapies by creating viable medicines from seemingly undeliverable molecules. With the ever increasing number of poorly water-soluble compounds entering development, the role of the formulation scientist is growing in importance. Also, knowledge of the advanced analytical, formulation, and process technologies as well as specific regulatory considerations related to the formulation of these compounds is increasing in value. Ideally, this book will serve as a useful tool in the education of current and future generations of scientists, and in this context contribute toward providing patients with new and better medicines.
| Author | : Navnit Shah |
| Publisher | : Springer |
| Total Pages | : 702 |
| Release | : 2014-11-21 |
| Genre | : Medical |
| ISBN | : 1493915983 |
This volume offers a comprehensive guide on the theory and practice of amorphous solid dispersions (ASD) for handling challenges associated with poorly soluble drugs. In twenty-three inclusive chapters, the book examines thermodynamics and kinetics of the amorphous state and amorphous solid dispersions, ASD technologies, excipients for stabilizing amorphous solid dispersions such as polymers, and ASD manufacturing technologies, including spray drying, hot melt extrusion, fluid bed layering and solvent-controlled micro-precipitation technology (MBP). Each technology is illustrated by specific case studies. In addition, dedicated sections cover analytical tools and technologies for characterization of amorphous solid dispersions, the prediction of long-term stability, and the development of suitable dissolution methods and regulatory aspects. The book also highlights future technologies on the horizon, such as supercritical fluid processing, mesoporous silica, KinetiSol®, and the use of non-salt-forming organic acids and amino acids for the stabilization of amorphous systems. Amorphous Solid Dispersions: Theory and Practice is a valuable reference to pharmaceutical scientists interested in developing bioavailable and therapeutically effective formulations of poorly soluble molecules in order to advance these technologies and develop better medicines for the future.
| Author | : Gregory K. Webster |
| Publisher | : CRC Press |
| Total Pages | : 728 |
| Release | : 2017-01-06 |
| Genre | : Medical |
| ISBN | : 9814745464 |
This book is the first text to provide a comprehensive assessment of the application of fundamental principles of dissolution and drug release testing to poorly soluble compounds and formulations. Such drug products are, vis-à-vis their physical and chemical properties, inherently incompatible with aqueous dissolution. However, dissolution methods are required for product development and selection, as well as for the fulfillment of regulatory obligations with respect to biopharmaceutical assessment and product quality understanding. The percentage of poorly soluble drugs, defined in classes 2 and 4 of the Biopharmaceutics Classification System (BCS), has significantly increased in the modern pharmaceutical development pipeline. This book provides a thorough exposition of general method development strategies for such drugs, including instrumentation and media selection, the use of compendial and non-compendial techniques in product development, and phase-appropriate approaches to dissolution development. Emerging topics in the field of dissolution are also discussed, including biorelevant and biphasic dissolution, the use on enzymes in dissolution testing, dissolution of suspensions, and drug release of non-oral products. Of particular interest to the industrial pharmaceutical professional, a brief overview of the formulation and solubilization techniques employed in the development of BCS class 2 and 4 drugs to overcome solubility challenges is provided and is complemented by a collection of chapters that survey the approaches and considerations in developing dissolution methodologies for enabling drug delivery technologies, including nanosuspensions, lipid-based formulations, and stabilized amorphous drug formulations.
| Author | : Scott Victor Jermain |
| Publisher | : |
| Total Pages | : 0 |
| Release | : 2019 |
| Genre | : |
| ISBN | : |
Poorly water-soluble drugs continue to dominate today’s drug development pipelines, and thus a multitude of technologies and solubility-enhancing methodologies have been commercialized to address this issue. One-such methodology to enhance the solubility of poorly water-soluble drugs is the development of amorphous solid dispersions. What was once considered a risky method of drug delivery (due to lack of drug kinetic stability in its amorphous state), formulating drugs as amorphous solid dispersions has grown significantly over the past two decades. Two amorphous solid dispersion-producing technologies have become well-understood for the development and successful delivery of poorly water-soluble drugs, and thus an overwhelming majority of commercialized amorphous solid dispersion products are processed by these two technologies; hot melt extrusion and spray drying. Each technology has distinct advantages and disadvantages, and thus many poorly water-soluble drugs are unable to process by either technology using conventional techniques. Thus, novel utilization of excipients and processing methods is necessary to continually expand the formulation design space. Furthermore, the development and commercialization of novel amorphous solid dispersion-producing technologies is necessary to further-expand the formulation design space. Therefore, the following research is an effort to expand the formulation design space of poorly water-soluble drugs while forming amorphous solid dispersions. The following research focuses on continued innovation in the field of amorphous solid dispersions to enhance the bioavailability of poorly water-soluble drugs. These research directions demonstrate innovative use of an ordinary excipient to enhance delivery of amorphous solid dispersions processed by hot melt extrusion. Additionally, these studies demonstrate the use (and further understanding) of a novel technology, KinetiSol, that allows for processing amorphous solid dispersions without the necessity of external thermal input or solvent(s). KinetiSol-processed materials are compared with spray dried materials to evaluate the kinetics behind drug release of a weakly basic drug processed with an ionic polymer, and findings from this study will be essential for future delivery of amorphous solid dispersions of weakly basic drugs in ionic polymers
| Author | : Gregory K. Webster |
| Publisher | : Jenny Stanford Publishing |
| Total Pages | : 0 |
| Release | : 2016-12-16 |
| Genre | : Bioavailability |
| ISBN | : 9789814745451 |
This book is the first text to provide a comprehensive assessment of the application of fundamental principles of dissolution and drug release testing to poorly soluble compounds and formulations. Such drug products are, vis-à-vis their physical and chemical properties, inherently incompatible with aqueous dissolution. However, dissolution methods are required for product development and selection, as well as for the fulfillment of regulatory obligations with respect to biopharmaceutical assessment and product quality understanding. The percentage of poorly soluble drugs, defined in classes 2 and 4 of the Biopharmaceutics Classification System (BCS), has significantly increased in the modern pharmaceutical development pipeline. This book provides a thorough exposition of general method development strategies for such drugs, including instrumentation and media selection, the use of compendial and non-compendial techniques in product development, and phase-appropriate approaches to dissolution development. Emerging topics in the field of dissolution are also discussed, including biorelevant and biphasic dissolution, the use on enzymes in dissolution testing, dissolution of suspensions, and drug release of non-oral products. Of particular interest to the industrial pharmaceutical professional, a brief overview of the formulation and solubilization techniques employed in the development of BCS class 2 and 4 drugs to overcome solubility challenges is provided and is complemented by a collection of chapters that survey the approaches and considerations in developing dissolution methodologies for enabling drug delivery technologies, including nanosuspensions, lipid-based formulations, and stabilized amorphous drug formulations.
| Author | : David J. Hauss |
| Publisher | : CRC Press |
| Total Pages | : 370 |
| Release | : 2007-06-08 |
| Genre | : Medical |
| ISBN | : 1420017268 |
Oral lipid-based formulations are attracting considerable attention due to their capacity to facilitate gastrointestinal absorption and reduce or eliminate the effect of food on the absorption of poorly water-soluble, lipophilic drugs. Despite the obvious and demonstrated utility of these formulations for addressing a persistent and growing problem
| Author | : Andrew Olutoye Ojo |
| Publisher | : |
| Total Pages | : 0 |
| Release | : 2021 |
| Genre | : |
| ISBN | : |
The preparation of amorphous solid dispersions (ASDs) has enabled the development of oral dosage forms for many poorly water-soluble compounds. The aim of the work presented in this dissertation is to advance our understanding of ASDs, specifically their long-term stability with respect to crystallization and the implications of instability on product performance. Advancing knowledge in these areas is pivotal for the pharmaceutical industry and its efforts in drug discovery. Much of our understanding of ASD stability results from empirical or extrapolative models that have been applied to describe stability. Their application has been limited and they do not provide fundamental insights into the recrystallization process to aid in the rationale development in ASDs. Notably, they fail to consider supersaturation as the driving force for crystallization, diffusivity in viscous systems, and interfacial effects. The works presented in this dissertation model the mechanisms of crystal nucleation and growth in ASDs by incorporating these concepts, develop and apply characterization tools to determine critical model parameters, and study the effects of crystallization on product performance.
| Author | : Justin Roy Hughey |
| Publisher | : |
| Total Pages | : 458 |
| Release | : 2012 |
| Genre | : |
| ISBN | : |
The number of newly developed chemical entities exhibiting poor water solubility has increased dramatically in recent years. In many cases this intrinsic property results in poor or erratic dissolution in biological fluids. Improving aqueous solubility of these compounds, even temporarily, can have a significant impact on in vivo performance. Single phase amorphous solid dispersions of a drug and polymer have emerged as a technique to not only increase the level of drug supersaturation but also maintain these levels for extended periods of time. Hot-melt extrusion (HME) has become the preferred processing technique to prepare systems such as these but has a number of limitations that prevent the successful formulation of many drug substances. Within this dissertation, the use of concentration enhancing polymers was investigated in parallel with a thorough evaluation of a novel fusion-based processing technique, KinetiSol® Dispersing (KSD), to prepare single phase amorphous solid dispersions that could not be successfully prepared by HME. Studies showed that the KSD technique is suitable for rendering thermally labile and high melting point drug substances amorphous through a combination of frictional and shearing energy. Compounds such as these were shown to degrade during HME processing due to relatively long residence times and low shear forces. Similarly, the KSD process was shown to successfully process solid dispersion compositions containing a high viscosity polymer with significantly lower levels of polymer degradation than obtained by HME processing. In the final study, KSD processing was used to prepare solid dispersions containing the hydrophilic polymer Soluplus[superscript TM] and methods were evaluated to formulate a tablet with rapid tablet disintegration characteristics, a requirement for sufficient dissolution enhancement. Combined, the studies demonstrated the effectiveness of combining proper polymer selection and formulation approaches with a suitable processing technique to form solid dispersion systems that provide rapid and extended durations of supersaturation.
