Authors:
R. Hilfiker Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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J. Berghausen Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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F. Blatter Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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A. Burkhard Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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S. De Paul Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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B. Freiermuth Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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A. Geoffroy Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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U. Hofmeier Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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C. Marcolli Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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B. Siebenhaar Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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M. Szelagiewicz Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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A. Vit Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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M. von Raumer Solvias AG Klybeckstrasse 191 4002 Basel Switzerland Klybeckstrasse 191 4002 Basel Switzerland

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Abstract  

Crystal structure (polymorphism) as well as crystal shape (morphology) and size have a huge practical and commercial impact on active substances all the way from research to manufacture of the final product. For an optimal development process, it is important to have an integrated approach to these issues ranging from a systematic polymorphism screening to a controlled scale-up of the crystallization process. The polymorphism program has to be tailored according to the development stage. Particularly suitable for an early development stage is a high-throughput polymorphism screening, which is the basis for a more thorough investigation if the product proceeds further in development. Such a comprehensive polymorphism investigation involves further crystallization experiments and extensive physicochemical characterization of the various forms. In this article the high-throughput polymorphism screening method that we have developed is described. Using carbamazepine as an example, the power of this high-throughput polymorphism screening system is demonstrated. Not only were all published forms found, but also new forms were identified. In the second part of the article, important considerations for crystallization optimization are discussed, again using the example of carbamazepine.

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Journal of Thermal Analysis and Calorimetry
Language English
Size A4
Year of
Foundation
1969
Volumes
per Year
1
Issues
per Year
24
Founder Akadémiai Kiadó
Founder's
Address
H-1117 Budapest, Hungary 1516 Budapest, PO Box 245.
Publisher Akadémiai Kiadó
Springer Nature Switzerland AG
Publisher's
Address
H-1117 Budapest, Hungary 1516 Budapest, PO Box 245.
CH-6330 Cham, Switzerland Gewerbestrasse 11.
Responsible
Publisher
Chief Executive Officer, Akadémiai Kiadó
ISSN 1388-6150 (Print)
ISSN 1588-2926 (Online)

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