Crystal polymorphism of pharmaceuticals: Probing crystal nucleation at the molecular level

Kevin P. Guiry; Joanne M. Kelleher; Simon E. Lawrence; Marie T. McAuliffe; Humphrey A. Moynihan; Andrea L. Ryan

doi:10.1080/14756360701425147

Crystal polymorphism of pharmaceuticals: Probing crystal nucleation at the molecular level

Kevin P. Guiry
, Joanne M. Kelleher
, Simon E. Lawrence
, Marie T. McAuliffe
, Humphrey A. Moynihan
, Andrea L. Ryan

School of Chemistry

University College Cork

Research output: Contribution to journal › Article › peer-review

Abstract

Paracetamol, sulfathiazole and l-glutamic acid are presented as examples of pharmaceutical crystal polymorphic systems. The effect of N-acylated sulfathiazole derivatives (3-6) on sulfathiazole crystallisation is discussed, and possible modes of action presented. Methods for the control of the crystal polymorphism of l-glutamic acid which utilise the principles of conformation mimicry and co-operative binding are presented. The preparation of a series of bis-amides of EDTA derived from sulfathiazole, 5-aminoisophthalic acid and 4-hydroxyaniline (i.e. compounds 9a-c) is presented, as is data on the effect of these compounds on the crystallisation of, respectively, sulfathiazole, l-glutamic acid and paracetamol.

Original language	English
Pages (from-to)	550-555
Number of pages	6
Journal	Journal of Enzyme Inhibition and Medicinal Chemistry
Volume	22
Issue number	5
DOIs	https://doi.org/10.1080/14756360701425147
Publication status	Published - Oct 2007

Keywords

Crystal polymorphism
EDTA
L-glutamic acid
Paracetamol
Sulfathiazole

Access to Document

10.1080/14756360701425147

Cite this

@article{2c138dccb4b6448381eb0a60e4246e85,

title = "Crystal polymorphism of pharmaceuticals: Probing crystal nucleation at the molecular level",

abstract = "Paracetamol, sulfathiazole and l-glutamic acid are presented as examples of pharmaceutical crystal polymorphic systems. The effect of N-acylated sulfathiazole derivatives (3-6) on sulfathiazole crystallisation is discussed, and possible modes of action presented. Methods for the control of the crystal polymorphism of l-glutamic acid which utilise the principles of conformation mimicry and co-operative binding are presented. The preparation of a series of bis-amides of EDTA derived from sulfathiazole, 5-aminoisophthalic acid and 4-hydroxyaniline (i.e. compounds 9a-c) is presented, as is data on the effect of these compounds on the crystallisation of, respectively, sulfathiazole, l-glutamic acid and paracetamol.",

keywords = "Crystal polymorphism, EDTA, L-glutamic acid, Paracetamol, Sulfathiazole",

author = "Guiry, \{Kevin P.\} and Kelleher, \{Joanne M.\} and Lawrence, \{Simon E.\} and McAuliffe, \{Marie T.\} and Moynihan, \{Humphrey A.\} and Ryan, \{Andrea L.\}",

year = "2007",

month = oct,

doi = "10.1080/14756360701425147",

language = "English",

volume = "22",

pages = "550--555",

journal = "Journal of Enzyme Inhibition and Medicinal Chemistry",

issn = "1475-6366",

publisher = "Taylor and Francis Ltd.",

number = "5",

}

TY - JOUR

T1 - Crystal polymorphism of pharmaceuticals

T2 - Probing crystal nucleation at the molecular level

AU - Guiry, Kevin P.

AU - Kelleher, Joanne M.

AU - Lawrence, Simon E.

AU - McAuliffe, Marie T.

AU - Moynihan, Humphrey A.

AU - Ryan, Andrea L.

PY - 2007/10

Y1 - 2007/10

N2 - Paracetamol, sulfathiazole and l-glutamic acid are presented as examples of pharmaceutical crystal polymorphic systems. The effect of N-acylated sulfathiazole derivatives (3-6) on sulfathiazole crystallisation is discussed, and possible modes of action presented. Methods for the control of the crystal polymorphism of l-glutamic acid which utilise the principles of conformation mimicry and co-operative binding are presented. The preparation of a series of bis-amides of EDTA derived from sulfathiazole, 5-aminoisophthalic acid and 4-hydroxyaniline (i.e. compounds 9a-c) is presented, as is data on the effect of these compounds on the crystallisation of, respectively, sulfathiazole, l-glutamic acid and paracetamol.

AB - Paracetamol, sulfathiazole and l-glutamic acid are presented as examples of pharmaceutical crystal polymorphic systems. The effect of N-acylated sulfathiazole derivatives (3-6) on sulfathiazole crystallisation is discussed, and possible modes of action presented. Methods for the control of the crystal polymorphism of l-glutamic acid which utilise the principles of conformation mimicry and co-operative binding are presented. The preparation of a series of bis-amides of EDTA derived from sulfathiazole, 5-aminoisophthalic acid and 4-hydroxyaniline (i.e. compounds 9a-c) is presented, as is data on the effect of these compounds on the crystallisation of, respectively, sulfathiazole, l-glutamic acid and paracetamol.

KW - Crystal polymorphism

KW - EDTA

KW - L-glutamic acid

KW - Paracetamol

KW - Sulfathiazole

UR - https://www.scopus.com/pages/publications/35348952615

U2 - 10.1080/14756360701425147

DO - 10.1080/14756360701425147

M3 - Article

C2 - 18035822

AN - SCOPUS:35348952615

SN - 1475-6366

VL - 22

SP - 550

EP - 555

JO - Journal of Enzyme Inhibition and Medicinal Chemistry

JF - Journal of Enzyme Inhibition and Medicinal Chemistry

IS - 5

ER -

Crystal polymorphism of pharmaceuticals: Probing crystal nucleation at the molecular level

Abstract

Keywords

Access to Document

Other files and links

Fingerprint

Cite this