Effect of Process Conditions on Particle Size and Shape in Continuous Antisolvent Crystallisation of Lovastatin

John McGinty; Magdalene W. S. Chong; Andrew Manson; Cameron J. Brown; Alison Nordon; Jan Sefcik

doi:10.3390/cryst10100925

Crystals (Oct 2020)

Effect of Process Conditions on Particle Size and Shape in Continuous Antisolvent Crystallisation of Lovastatin

John McGinty,
Magdalene W. S. Chong,
Andrew Manson,
Cameron J. Brown,
Alison Nordon,
Jan Sefcik

Affiliations

John McGinty: Future Manufacturing Research Hub in Continuous Manufacturing and Advanced Crystallisation, Technology and Innovation Centre, University of Strathclyde, 99 George Street, Glasgow G1 1RD, UK
Magdalene W. S. Chong: Future Manufacturing Research Hub in Continuous Manufacturing and Advanced Crystallisation, Technology and Innovation Centre, University of Strathclyde, 99 George Street, Glasgow G1 1RD, UK
Andrew Manson: Department of Chemical and Process Engineering, University of Strathclyde, James Weir Building, 75 Montrose Street, Glasgow G1 1XJ, UK
Cameron J. Brown: Future Manufacturing Research Hub in Continuous Manufacturing and Advanced Crystallisation, Technology and Innovation Centre, University of Strathclyde, 99 George Street, Glasgow G1 1RD, UK
Alison Nordon: Future Manufacturing Research Hub in Continuous Manufacturing and Advanced Crystallisation, Technology and Innovation Centre, University of Strathclyde, 99 George Street, Glasgow G1 1RD, UK
Jan Sefcik: Future Manufacturing Research Hub in Continuous Manufacturing and Advanced Crystallisation, Technology and Innovation Centre, University of Strathclyde, 99 George Street, Glasgow G1 1RD, UK

DOI: https://doi.org/10.3390/cryst10100925
Journal volume & issue: Vol. 10, no. 10
p. 925

Abstract

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Lovastatin crystals often exhibit an undesirable needle-like morphology. Several studies have shown how a needle-like morphology can be modified in antisolvent crystallisation with the use of additives, but there is much less experimental work demonstrating crystal shape modification without the use of additives. In this study, a series of unseeded continuous antisolvent crystallisation experiments were conducted with the process conditions of supersaturation, total flow rate, and ultrasound level being varied to determine their effects on crystal size and shape. This experimental work involved identifying acetone/water as the most suitable solvent/antisolvent system, assessing lovastatin nucleation behaviour by means of induction time measurements, and then designing and implementing the continuous antisolvent crystallisation experiments. It was found that in order to produce the smallest and least needle-like particles, the maximum total flow rate and supersaturation had to be combined with the application of ultrasound. These results should aid development of pharmaceutical manufacturing processes where the ability to control particle size and shape would allow for optimisation of crystal isolation and more efficient downstream processing.

Published in Crystals

ISSN: 2073-4352 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science: Chemistry: Crystallography
Website: http://www.mdpi.com/journal/crystals/

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