Development and Validation of Liquid Chromatography-Based Methods to Assess the Lipophilicity of Cytotoxic Platinum(IV) Complexes

Matthias H. M. Klose; Sarah Theiner; Hristo P. Varbanov; Doris Hoefer; Verena Pichler; Mathea Sophia Galanski; Samuel M. Meier-Menches; Bernhard K. Keppler

doi:10.3390/inorganics6040130

Development and Validation of Liquid Chromatography-Based Methods to Assess the Lipophilicity of Cytotoxic Platinum(IV) Complexes

Matthias H. M. Klose, Sarah Theiner, Hristo P. Varbanov, Doris Hoefer, Verena Pichler, Mathea Sophia Galanski, Samuel M. Meier-Menches (Corresponding author), Bernhard K. Keppler (Corresponding author)

Publications: Contribution to book › Chapter › Peer Reviewed

Abstract

Lipophilicity is a crucial parameter for drug discovery, usually determined by the logarithmic partition coefficient (Log P) between octanol and water. However, the available detection methods have restricted the widespread use of the partition coefficient in inorganic medicinal chemistry, and recent investigations have shifted towards chromatographic lipophilicity parameters, frequently without a conversion to derive Log P. As high-performance liquid chromatography (HPLC) instruments are readily available to research groups, a HPLC-based method is presented and validated to derive the partition coefficient of a set of 19 structurally diverse and cytotoxic platinum(IV) complexes exhibiting a dynamic range of at least four orders of magnitude. The chromatographic lipophilicity parameters Φ ₀ and Log k _w were experimentally determined for the same set of compounds, and a correlation was obtained that allows interconversion between the two lipophilicity scales, which was applied to an additional set of 34 platinum(IV) drug candidates. Thereby, a Φ ₀ = 58 corresponds to Log P = 0. The same approacheswere successfully evaluated to determine the distribution coefficient (Log D) of five ionisable platinum(IV) compounds to sample pH-dependent effects on the lipophilicity. This study provides straight-forward HPLC-based methods to determine the lipophilicity of cytotoxic platinum(IV) complexes in the form of Log P and Φ ₀ that can be interconverted and easily expanded to other metal-based compound classes.

Original language	English
Title of host publication	Unconventional Anticancer Metallodrugs and Strategies to Improve their Pharmacological Profile
Editors	Maria Contel
Place of Publication	Basel
Publisher	Multi-disciplinary digital publishing institute (MDPI)
Pages	71-84
Number of pages	14
Volume	6
Edition	4
ISBN (Electronic)	978-3-03921-316-0
ISBN (Print)	978-3-03921-315-3
DOIs	https://doi.org/10.3390/inorganics6040130
Publication status	Published - Dec 2018

Publication series

Series	Inorganics
ISSN	2304-6740

Austrian Fields of Science 2012

104003 Inorganic chemistry
301904 Cancer research

Keywords

phi(0)
anticancer agents
chromatographic lipophilicity parameter
distribution coefficient
HPLC
lipophilicity
Log k(w)
Log P
partition coefficient
platinum(IV)
TETRACARBOXYLATOPLATINUM(IV) COMPLEXES
HYDROPHOBICITY
PT(II)
ACCUMULATION
COEFFICIENT
PREDICTION
PARAMETERS
RETENTION
CHEMISTRY
MOIETY
Partition coefficient
Log k
Platinum(IV)
Distribution coefficient
Φ
Chromatographic lipophilicity parameter
Anticancer agents
Lipophilicity

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.3390/inorganics6040130Licence: CC BY 4.0

Cite this

Klose, M. H. M., Theiner, S., Varbanov, H. P., Hoefer, D., Pichler, V., Galanski, M. S., Meier-Menches, S. M., & Keppler, B. K. (2018). Development and Validation of Liquid Chromatography-Based Methods to Assess the Lipophilicity of Cytotoxic Platinum(IV) Complexes. In M. Contel (Ed.), Unconventional Anticancer Metallodrugs and Strategies to Improve their Pharmacological Profile (4 ed., Vol. 6, pp. 71-84). Article 130 Multi-disciplinary digital publishing institute (MDPI). https://doi.org/10.3390/inorganics6040130

Klose, Matthias H. M. ; Theiner, Sarah ; Varbanov, Hristo P. et al. / Development and Validation of Liquid Chromatography-Based Methods to Assess the Lipophilicity of Cytotoxic Platinum(IV) Complexes. Unconventional Anticancer Metallodrugs and Strategies to Improve their Pharmacological Profile. editor / Maria Contel. Vol. 6 4. ed. Basel : Multi-disciplinary digital publishing institute (MDPI), 2018. pp. 71-84 (Inorganics).

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title = "Development and Validation of Liquid Chromatography-Based Methods to Assess the Lipophilicity of Cytotoxic Platinum(IV) Complexes",

abstract = "Lipophilicity is a crucial parameter for drug discovery, usually determined by the logarithmic partition coefficient (Log P) between octanol and water. However, the available detection methods have restricted the widespread use of the partition coefficient in inorganic medicinal chemistry, and recent investigations have shifted towards chromatographic lipophilicity parameters, frequently without a conversion to derive Log P. As high-performance liquid chromatography (HPLC) instruments are readily available to research groups, a HPLC-based method is presented and validated to derive the partition coefficient of a set of 19 structurally diverse and cytotoxic platinum(IV) complexes exhibiting a dynamic range of at least four orders of magnitude. The chromatographic lipophilicity parameters Φ 0 and Log k w were experimentally determined for the same set of compounds, and a correlation was obtained that allows interconversion between the two lipophilicity scales, which was applied to an additional set of 34 platinum(IV) drug candidates. Thereby, a Φ 0 = 58 corresponds to Log P = 0. The same approacheswere successfully evaluated to determine the distribution coefficient (Log D) of five ionisable platinum(IV) compounds to sample pH-dependent effects on the lipophilicity. This study provides straight-forward HPLC-based methods to determine the lipophilicity of cytotoxic platinum(IV) complexes in the form of Log P and Φ 0 that can be interconverted and easily expanded to other metal-based compound classes. ",

keywords = "phi(0), anticancer agents, chromatographic lipophilicity parameter, distribution coefficient, HPLC, lipophilicity, Log k(w), Log P, partition coefficient, platinum(IV), TETRACARBOXYLATOPLATINUM(IV) COMPLEXES, HYDROPHOBICITY, PT(II), ACCUMULATION, COEFFICIENT, PREDICTION, PARAMETERS, RETENTION, CHEMISTRY, MOIETY, Partition coefficient, Log k, Platinum(IV), Distribution coefficient, Φ, Chromatographic lipophilicity parameter, Anticancer agents, Lipophilicity",

author = "Klose, \{Matthias H. M.\} and Sarah Theiner and Varbanov, \{Hristo P.\} and Doris Hoefer and Verena Pichler and Galanski, \{Mathea Sophia\} and Meier-Menches, \{Samuel M.\} and Keppler, \{Bernhard K.\}",

note = "Publisher Copyright: {\textcopyright} 2018 by the authors.",

year = "2018",

month = dec,

doi = "10.3390/inorganics6040130",

language = "English",

isbn = "978-3-03921-315-3",

volume = "6",

series = "Inorganics",

publisher = "Multi-disciplinary digital publishing institute (MDPI)",

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editor = "Maria Contel",

booktitle = "Unconventional Anticancer Metallodrugs and Strategies to Improve their Pharmacological Profile",

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}

Klose, MHM, Theiner, S, Varbanov, HP, Hoefer, D, Pichler, V , Galanski, MS , Meier-Menches, SM & Keppler, BK 2018, Development and Validation of Liquid Chromatography-Based Methods to Assess the Lipophilicity of Cytotoxic Platinum(IV) Complexes. in M Contel (ed.), Unconventional Anticancer Metallodrugs and Strategies to Improve their Pharmacological Profile. 4 edn, vol. 6, 130, Multi-disciplinary digital publishing institute (MDPI), Basel, Inorganics, pp. 71-84. https://doi.org/10.3390/inorganics6040130

Development and Validation of Liquid Chromatography-Based Methods to Assess the Lipophilicity of Cytotoxic Platinum(IV) Complexes. / Klose, Matthias H. M.; Theiner, Sarah; Varbanov, Hristo P. et al.
Unconventional Anticancer Metallodrugs and Strategies to Improve their Pharmacological Profile. ed. / Maria Contel. Vol. 6 4. ed. Basel: Multi-disciplinary digital publishing institute (MDPI), 2018. p. 71-84 130 (Inorganics).

Publications: Contribution to book › Chapter › Peer Reviewed

TY - CHAP

T1 - Development and Validation of Liquid Chromatography-Based Methods to Assess the Lipophilicity of Cytotoxic Platinum(IV) Complexes

AU - Klose, Matthias H. M.

AU - Theiner, Sarah

AU - Varbanov, Hristo P.

AU - Hoefer, Doris

AU - Pichler, Verena

AU - Galanski, Mathea Sophia

AU - Meier-Menches, Samuel M.

AU - Keppler, Bernhard K.

PY - 2018/12

Y1 - 2018/12

N2 - Lipophilicity is a crucial parameter for drug discovery, usually determined by the logarithmic partition coefficient (Log P) between octanol and water. However, the available detection methods have restricted the widespread use of the partition coefficient in inorganic medicinal chemistry, and recent investigations have shifted towards chromatographic lipophilicity parameters, frequently without a conversion to derive Log P. As high-performance liquid chromatography (HPLC) instruments are readily available to research groups, a HPLC-based method is presented and validated to derive the partition coefficient of a set of 19 structurally diverse and cytotoxic platinum(IV) complexes exhibiting a dynamic range of at least four orders of magnitude. The chromatographic lipophilicity parameters Φ 0 and Log k w were experimentally determined for the same set of compounds, and a correlation was obtained that allows interconversion between the two lipophilicity scales, which was applied to an additional set of 34 platinum(IV) drug candidates. Thereby, a Φ 0 = 58 corresponds to Log P = 0. The same approacheswere successfully evaluated to determine the distribution coefficient (Log D) of five ionisable platinum(IV) compounds to sample pH-dependent effects on the lipophilicity. This study provides straight-forward HPLC-based methods to determine the lipophilicity of cytotoxic platinum(IV) complexes in the form of Log P and Φ 0 that can be interconverted and easily expanded to other metal-based compound classes.

AB - Lipophilicity is a crucial parameter for drug discovery, usually determined by the logarithmic partition coefficient (Log P) between octanol and water. However, the available detection methods have restricted the widespread use of the partition coefficient in inorganic medicinal chemistry, and recent investigations have shifted towards chromatographic lipophilicity parameters, frequently without a conversion to derive Log P. As high-performance liquid chromatography (HPLC) instruments are readily available to research groups, a HPLC-based method is presented and validated to derive the partition coefficient of a set of 19 structurally diverse and cytotoxic platinum(IV) complexes exhibiting a dynamic range of at least four orders of magnitude. The chromatographic lipophilicity parameters Φ 0 and Log k w were experimentally determined for the same set of compounds, and a correlation was obtained that allows interconversion between the two lipophilicity scales, which was applied to an additional set of 34 platinum(IV) drug candidates. Thereby, a Φ 0 = 58 corresponds to Log P = 0. The same approacheswere successfully evaluated to determine the distribution coefficient (Log D) of five ionisable platinum(IV) compounds to sample pH-dependent effects on the lipophilicity. This study provides straight-forward HPLC-based methods to determine the lipophilicity of cytotoxic platinum(IV) complexes in the form of Log P and Φ 0 that can be interconverted and easily expanded to other metal-based compound classes.

KW - phi(0)

KW - anticancer agents

KW - chromatographic lipophilicity parameter

KW - distribution coefficient

KW - HPLC

KW - lipophilicity

KW - Log k(w)

KW - Log P

KW - partition coefficient

KW - platinum(IV)

KW - TETRACARBOXYLATOPLATINUM(IV) COMPLEXES

KW - HYDROPHOBICITY

KW - PT(II)

KW - ACCUMULATION

KW - COEFFICIENT

KW - PREDICTION

KW - PARAMETERS

KW - RETENTION

KW - CHEMISTRY

KW - MOIETY

KW - Partition coefficient

KW - Log k

KW - Platinum(IV)

KW - Distribution coefficient

KW - Φ

KW - Chromatographic lipophilicity parameter

KW - Anticancer agents

KW - Lipophilicity

UR - https://www.scopus.com/pages/publications/85058791775

U2 - 10.3390/inorganics6040130

DO - 10.3390/inorganics6040130

M3 - Chapter

SN - 978-3-03921-315-3

VL - 6

T3 - Inorganics

SP - 71

EP - 84

BT - Unconventional Anticancer Metallodrugs and Strategies to Improve their Pharmacological Profile

A2 - Contel, Maria

PB - Multi-disciplinary digital publishing institute (MDPI)

CY - Basel

ER -

Klose MHM, Theiner S, Varbanov HP, Hoefer D, Pichler V , Galanski MS et al. Development and Validation of Liquid Chromatography-Based Methods to Assess the Lipophilicity of Cytotoxic Platinum(IV) Complexes. In Contel M, editor, Unconventional Anticancer Metallodrugs and Strategies to Improve their Pharmacological Profile. 4 ed. Vol. 6. Basel: Multi-disciplinary digital publishing institute (MDPI). 2018. p. 71-84. 130. (Inorganics). doi: 10.3390/inorganics6040130

Development and Validation of Liquid Chromatography-Based Methods to Assess the Lipophilicity of Cytotoxic Platinum(IV) Complexes

Abstract

Publication series

Austrian Fields of Science 2012

Keywords

UN SDGs

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