2009
DOI: 10.1007/s00216-009-2634-y
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Analytical tools for the physicochemical profiling of drug candidates to predict absorption/distribution

Abstract: The measurement of physicochemical properties at an early phase of drug discovery and development is crucial to reduce attrition rates due to poor biopharmaceutical properties. Among these properties, ionization, lipophilicity, solubility and permeability are mandatory to predict the pharmacokinetic behavior of NCEs (new chemical entities). Due to the high number of NCEs, the analytical tools used to measure these properties are automated and progressively adapted to high-throughput technologies. The present r… Show more

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Cited by 72 publications
(47 citation statements)
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References 293 publications
(372 reference statements)
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“…The experimental conditions effect the pK a determination such as buffer type and ionic strength, applied voltage, detection method, etc. are discussed as detailed by Henchoz et al [16].…”
Section: Capillary Electrophoresis (Ce)mentioning
confidence: 99%
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“…The experimental conditions effect the pK a determination such as buffer type and ionic strength, applied voltage, detection method, etc. are discussed as detailed by Henchoz et al [16].…”
Section: Capillary Electrophoresis (Ce)mentioning
confidence: 99%
“…This book can be considered as the most competent and detailed compilation of advanced knowledge required by physical chemists involved in drug development. Numerous reviews summarized the state-of-the-art of new HT experimental techniques [12][13][14][15], the most recent was published by Y. Henchoz et al [16]. So, various literature sources are available for all who would expand their understanding of physicochemical profiling according to their need.…”
Section: Figure 12 Drug Research Processmentioning
confidence: 99%
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“…Diese Messungen sind essenziell, um die derzeitigen hohen Ausfallraten von neuen Arzneimittelkandidaten zu verringern. [30] Die Anwendung von Imaging-Methoden bei der Arzneimittelentdeckung hat eine Perspektive, um präklinische medizinische Chemieoptimierungszyklen zu beschleunigen und eine in vitro zu in vivo Tr anslation von Arzneimittelkandidaten zu verbessern. [31,32] Darüber hinaus erfolgte in den durch LC-MS identifizierten Neratinib-Metaboliten Hydroxylierung,N -Oxidation und Dealkylierung des Chinolinrings (Tabelle S1 und Abbildungen S32-S35).…”
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