Salt Solubility Products of Diprenorphine Hydrochloride, Codeine and Lidocaine Hydrochlorides and Phosphates – Novel Method of Data Analysis Not Dependent on Explicit Solubility Equations

A novel general approach was described to address many of the challenges of salt solubility determination of drug substances, with data processing and refinement of equilibrium constants encoded in the computer program pDISOL-XTM. The new approach was illustrated by the determinations of the solubil...

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Main Authors: Gergely Völgyi, Attila Marosi, Krisztina Takács-Novák, Alex Avdeef
Format: Article
Language:English
Published: International Association of Physical Chemists (IAPC) 2013-12-01
Series:ADMET and DMPK
Online Access:http://pub.iapchem.org/ojs/index.php/admet/article/view/24
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spelling doaj-d9643a5cfe2f4ba78d5ed3234236aa0d2020-11-24T21:25:05ZengInternational Association of Physical Chemists (IAPC)ADMET and DMPK1848-77182013-12-0114486210.5599/admet.1.4.2410Salt Solubility Products of Diprenorphine Hydrochloride, Codeine and Lidocaine Hydrochlorides and Phosphates – Novel Method of Data Analysis Not Dependent on Explicit Solubility EquationsGergely Völgyi0Attila Marosi1Krisztina Takács-Novák2Alex Avdeef3Semmelweis University, Dept. of Pharmaceutical Chemistry, H-1092 Budapest, Högyes E. u.9, HungarySemmelweis University, Dept. of Pharmaceutical Chemistry, H-1092 Budapest, Högyes E. u.9, HungarySemmelweis University, Dept. of Pharmaceutical Chemistry, H-1092 Budapest, Högyes E. u.9, Hungaryin-ADME ResearchA novel general approach was described to address many of the challenges of salt solubility determination of drug substances, with data processing and refinement of equilibrium constants encoded in the computer program pDISOL-XTM. The new approach was illustrated by the determinations of the solubility products of diprenorphine hydrochloride, codeine hydrochloride and phosphate, lidocaine hydrochloride and phosphate at 25 oC, using a recently-optimized saturation shake-flask protocol.  The effects of different buffers (Britton-Robinson universal and Sörensen phosphate) were compared. Lidocaine precipitates were characterized by X-ray powder diffraction (XRPD) and polarization light microscopy. The ionic strength in the studied systems ranged from 0.25 to 4.3 M. Codeine (and possibly diprenorphine) chloride were less soluble than the phosphates for pH > 2. The reverse trend was evident with lidocaine.  Diprenorphine saturated solutions showed departure from the predictions of the Henderson-Hasselbalch equation in alkaline (pH > 9) solutions, consistent with the formation of a mixed-charge anionic dimer.http://pub.iapchem.org/ojs/index.php/admet/article/view/24
collection DOAJ
language English
format Article
sources DOAJ
author Gergely Völgyi
Attila Marosi
Krisztina Takács-Novák
Alex Avdeef
spellingShingle Gergely Völgyi
Attila Marosi
Krisztina Takács-Novák
Alex Avdeef
Salt Solubility Products of Diprenorphine Hydrochloride, Codeine and Lidocaine Hydrochlorides and Phosphates – Novel Method of Data Analysis Not Dependent on Explicit Solubility Equations
ADMET and DMPK
author_facet Gergely Völgyi
Attila Marosi
Krisztina Takács-Novák
Alex Avdeef
author_sort Gergely Völgyi
title Salt Solubility Products of Diprenorphine Hydrochloride, Codeine and Lidocaine Hydrochlorides and Phosphates – Novel Method of Data Analysis Not Dependent on Explicit Solubility Equations
title_short Salt Solubility Products of Diprenorphine Hydrochloride, Codeine and Lidocaine Hydrochlorides and Phosphates – Novel Method of Data Analysis Not Dependent on Explicit Solubility Equations
title_full Salt Solubility Products of Diprenorphine Hydrochloride, Codeine and Lidocaine Hydrochlorides and Phosphates – Novel Method of Data Analysis Not Dependent on Explicit Solubility Equations
title_fullStr Salt Solubility Products of Diprenorphine Hydrochloride, Codeine and Lidocaine Hydrochlorides and Phosphates – Novel Method of Data Analysis Not Dependent on Explicit Solubility Equations
title_full_unstemmed Salt Solubility Products of Diprenorphine Hydrochloride, Codeine and Lidocaine Hydrochlorides and Phosphates – Novel Method of Data Analysis Not Dependent on Explicit Solubility Equations
title_sort salt solubility products of diprenorphine hydrochloride, codeine and lidocaine hydrochlorides and phosphates – novel method of data analysis not dependent on explicit solubility equations
publisher International Association of Physical Chemists (IAPC)
series ADMET and DMPK
issn 1848-7718
publishDate 2013-12-01
description A novel general approach was described to address many of the challenges of salt solubility determination of drug substances, with data processing and refinement of equilibrium constants encoded in the computer program pDISOL-XTM. The new approach was illustrated by the determinations of the solubility products of diprenorphine hydrochloride, codeine hydrochloride and phosphate, lidocaine hydrochloride and phosphate at 25 oC, using a recently-optimized saturation shake-flask protocol.  The effects of different buffers (Britton-Robinson universal and Sörensen phosphate) were compared. Lidocaine precipitates were characterized by X-ray powder diffraction (XRPD) and polarization light microscopy. The ionic strength in the studied systems ranged from 0.25 to 4.3 M. Codeine (and possibly diprenorphine) chloride were less soluble than the phosphates for pH > 2. The reverse trend was evident with lidocaine.  Diprenorphine saturated solutions showed departure from the predictions of the Henderson-Hasselbalch equation in alkaline (pH > 9) solutions, consistent with the formation of a mixed-charge anionic dimer.
url http://pub.iapchem.org/ojs/index.php/admet/article/view/24
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