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Dive into the research topics where Hans-Juergen Mair is active.

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Featured researches published by Hans-Juergen Mair.


Journal of Pharmaceutical Sciences | 2013

Improved Human Bioavailability of Vemurafenib, a Practically Insoluble Drug, Using an Amorphous Polymer-Stabilized Solid Dispersion Prepared by a Solvent-Controlled Coprecipitation Process

Navnit Shah; Raman Mahadevan Iyer; Hans-Juergen Mair; Duk Soon Choi; Hung Tian; Ralph Diodone; Karsten Fähnrich; Anni Pabst-Ravot; Kin Tang; Emmanuel Scheubel; Joseph F. Grippo; Sebastian A. Moreira; Zenaida Go; James Mouskountakis; Theresa Louie; Prabha N. Ibrahim; Harpreet K. Sandhu; Linda Rubia; Hitesh Chokshi; Dharmendra Singhal; Waseem Malick

The present work deals with improving the solubility of vemurafenib, a practically insoluble drug, by converting it into an amorphous-solid dispersion using a solvent-controlled precipitation process. The dispersion containing vemurafenib and hypromellose acetate succinate (HPMCAS), an enteric polymer, is termed microprecipitated bulk powder (MBP), in which the drug is uniformly dispersed within the polymeric substrate. HPMCAS was found to be the most suitable polymer for vemurafenib MBP, among a series of enteric polymers based on superior physical stability and drug-release characteristics of the MBP. The MBP provided a greater rate and extent of dissolution than crystalline drug, reaching an apparent drug concentration of 28-35 µg/mL, almost 30-fold higher than solubility of crystalline drug at 1 µg/mL. The supersaturation was also maintained for more than 4 h. Upon exposure to high temperature and humidity, the MBP was destabilized, resulting in crystallization and lower dissolution rate. The control of moisture and temperature is essential to maintain the stability of the MBP. In a relative human bioavailability study, vemurafenib MBP provided a four- to fivefold increase in exposure compared with crystalline drug. Improving solubility with an amorphous-solid dispersion is a viable strategy for the development of practically insoluble compounds.


Archive | 2010

Compositions and uses thereof

Dipen Desai; Ralph Diodone; Zenaida Go; Prabha N. Ibrahim; Raman Mahadevan Iyer; Hans-Juergen Mair; Harpreet K. Sandhu; Navnit Shah; Gary Conard Visor; Nicole Wyttenbach; Stephan Lauper; Johannes Pudewell; Frank Wierschem


Archive | 1978

NOVEL PROCESS FOR THE MANUFACTURE OF PHARMACEUTICAL PREPARATIONS

Ralph Diodone; Stephan Lauper; Hans-Juergen Mair; Johannes Pudewell; Frank Wierschem


Archive | 2012

Process for the manufacture of pharmaceutically active compounds

Stefan Hildbrand; Hans-Juergen Mair; Roumen Nikolaev Radinov; Yi Ren; James Anderson Wright


Archive | 2010

Propane-i-sulfonic acid {3-[5-(4-chloro-phenyl)-1h-pyrrolo[2,3-b]pyridine-3-carbonyl]-2,4-difluoro-phenyl}-amide compositions and uses thereof

Ralph Diodone; Stephan Lauper; Hans-Juergen Mair; Johannes Pudewell; Frank Wierschem


Archive | 2000

Process for the preparation of 4,5-diamino shikimic acid derivatives

Hans-Juergen Mair


Archive | 2007

Processes for the manufacture of a pyrrolidine-3,4-dicarboxamide derivative

Jean-Michel Adam; Pascal Dott; Hans Iding; Hans-Juergen Mair; Reinhard Reents; Beat Wirz


Archive | 2007

Processes for the preparation of (3r, 4r) -n- (4-chlorophenyl) -1- (2, 2-difluoroethyl) -n'- [2-fluoro-4- (2-oxo-1 (2h) -pyridinyl) phenyl] -3 , 4-pyrrolidinedicarboxamide

Jean-Michel Adam; Pascal Dott; Hans Iding; Hans-Juergen Mair; Reinhard Reents; Beat Wirz


Archive | 2000

Phosphine reduction of azides to amines

Hans-Juergen Mair


Archive | 2013

PROCESS FOR THE PREPARATION OF AROMATIC THIOL DERIVATIVES BY HYDROGENATION OF DISULFIDES

Hans-Juergen Mair; Reinhard Reents; Michelangelo Scalone; Shaoning Wang; Andreas Zogg

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Dipen Desai

University of Rhode Island

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