Candidate Selection and Preclinical Evaluation of N-tert-Butyl Isoquine (GSK369796), An Affordable and Effective 4-Aminoquinoline Antimalarial for the 21st Century

Paul M. O'Neill; B. Kevin Park; Alison E. Shone; James L. Maggs; Phillip Roberts; Paul A. Stocks; Giancarlo Biagini; Patrick G. Bray; Peter Gibbons; Neil Berry; Peter A. Winstanley; Amira Mukhtar; Richard Bonar-Law; Stephen Hindley; Ramesh B. Bambal; Charles B. Davis; Martin Bates; Timothy K. Hart; Stephanie L. Gresham; Ron M. Lawrence; Richard A. Brigandi; Federico M. Gomez-delas-Heras; Domingo V. Gargallo; Steve Ward

doi:10.1021/jm8012618

Candidate Selection and Preclinical Evaluation of N-tert-Butyl Isoquine (GSK369796), An Affordable and Effective 4-Aminoquinoline Antimalarial for the 21st Century

Paul M. O'Neill
, B. Kevin Park
, Alison E. Shone
, James L. Maggs
, Phillip Roberts
, Paul A. Stocks
, Giancarlo Biagini
, Patrick G. Bray
, Peter Gibbons
, Neil Berry
, Peter A. Winstanley
, Amira Mukhtar
, Richard Bonar-Law
, Stephen Hindley
, Ramesh B. Bambal
, Charles B. Davis
, Martin Bates
, Timothy K. Hart
, Stephanie L. Gresham
, Ron M. Lawrence

Richard A. Brigandi, Federico M. Gomez-delas-Heras, Domingo V. Gargallo, Steve Ward

Tropical Disease Biology

University of Liverpool
Liverpool School of Tropical Medicine
GlaxoSmithKline

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

86 Citations (Scopus)

Abstract

N-tert-Butyl isoquine (4) (GSK369796) is a 4-aminoquinoline drug candidate selected and developed as part of a public−private partnership between academics at Liverpool, MMV, and GSK pharmaceuticals. This molecule was rationally designed based on chemical, toxicological, pharmacokinetic, and pharmacodynamic considerations and was selected based on excellent activity against Plasmodium falciparum in vitro and rodent malaria parasites in vivo. The optimized chemistry delivered this novel synthetic quinoline in a two-step procedure from cheap and readily available starting materials. The molecule has a full industry standard preclinical development program allowing first into humans to proceed. Employing chloroquine (1) and amodiaquine (2) as comparator molecules in the preclinical plan, the first preclinical dossier of pharmacokinetic, toxicity, and safety pharmacology has also been established for the 4-aminoquinoline antimalarial class. These studies have revealed preclinical liabilities that have never translated into the human experience. This has resulted in the availability of critical information to other drug development teams interested in developing antimalarials within this class.

Original language	English
Pages (from-to)	1408-1415
Number of pages	8
Journal	Journal of Medicinal Chemistry
Volume	52
Issue number	5
DOIs	https://doi.org/10.1021/jm8012618
Publication status	Published - 17 Feb 2009

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SDG 3 Good Health and Well-being

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10.1021/jm8012618

Cite this

O'Neill, P. M., Park, B. K., Shone, A. E., Maggs, J. L., Roberts, P., Stocks, P. A., Biagini, G., Bray, P. G., Gibbons, P., Berry, N., Winstanley, P. A., Mukhtar, A., Bonar-Law, R., Hindley, S., Bambal, R. B., Davis, C. B., Bates, M., Hart, T. K., Gresham, S. L., ... Ward, S. (2009). Candidate Selection and Preclinical Evaluation of N-tert-Butyl Isoquine (GSK369796), An Affordable and Effective 4-Aminoquinoline Antimalarial for the 21st Century. Journal of Medicinal Chemistry, 52(5), 1408-1415. https://doi.org/10.1021/jm8012618

@article{4ff9a46dee4047eabecf70776104f80c,

title = "Candidate Selection and Preclinical Evaluation of N-tert-Butyl Isoquine (GSK369796), An Affordable and Effective 4-Aminoquinoline Antimalarial for the 21st Century",

abstract = "N-tert-Butyl isoquine (4) (GSK369796) is a 4-aminoquinoline drug candidate selected and developed as part of a public−private partnership between academics at Liverpool, MMV, and GSK pharmaceuticals. This molecule was rationally designed based on chemical, toxicological, pharmacokinetic, and pharmacodynamic considerations and was selected based on excellent activity against Plasmodium falciparum in vitro and rodent malaria parasites in vivo. The optimized chemistry delivered this novel synthetic quinoline in a two-step procedure from cheap and readily available starting materials. The molecule has a full industry standard preclinical development program allowing first into humans to proceed. Employing chloroquine (1) and amodiaquine (2) as comparator molecules in the preclinical plan, the first preclinical dossier of pharmacokinetic, toxicity, and safety pharmacology has also been established for the 4-aminoquinoline antimalarial class. These studies have revealed preclinical liabilities that have never translated into the human experience. This has resulted in the availability of critical information to other drug development teams interested in developing antimalarials within this class.",

author = "O'Neill, \{Paul M.\} and Park, \{B. Kevin\} and Shone, \{Alison E.\} and Maggs, \{James L.\} and Phillip Roberts and Stocks, \{Paul A.\} and Giancarlo Biagini and Bray, \{Patrick G.\} and Peter Gibbons and Neil Berry and Winstanley, \{Peter A.\} and Amira Mukhtar and Richard Bonar-Law and Stephen Hindley and Bambal, \{Ramesh B.\} and Davis, \{Charles B.\} and Martin Bates and Hart, \{Timothy K.\} and Gresham, \{Stephanie L.\} and Lawrence, \{Ron M.\} and Brigandi, \{Richard A.\} and Gomez-delas-Heras, \{Federico M.\} and Gargallo, \{Domingo V.\} and Steve Ward",

year = "2009",

month = feb,

day = "17",

doi = "10.1021/jm8012618",

language = "English",

volume = "52",

pages = "1408--1415",

journal = "Journal of Medicinal Chemistry",

issn = "0022-2623",

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O'Neill, PM, Park, BK, Shone, AE, Maggs, JL, Roberts, P, Stocks, PA, Biagini, G, Bray, PG, Gibbons, P, Berry, N, Winstanley, PA, Mukhtar, A, Bonar-Law, R, Hindley, S, Bambal, RB, Davis, CB, Bates, M, Hart, TK, Gresham, SL, Lawrence, RM, Brigandi, RA, Gomez-delas-Heras, FM, Gargallo, DV & Ward, S 2009, 'Candidate Selection and Preclinical Evaluation of N-tert-Butyl Isoquine (GSK369796), An Affordable and Effective 4-Aminoquinoline Antimalarial for the 21st Century', Journal of Medicinal Chemistry, vol. 52, no. 5, pp. 1408-1415. https://doi.org/10.1021/jm8012618

Candidate Selection and Preclinical Evaluation of N-tert-Butyl Isoquine (GSK369796), An Affordable and Effective 4-Aminoquinoline Antimalarial for the 21st Century. / O'Neill, Paul M.; Park, B. Kevin; Shone, Alison E. et al.
In: Journal of Medicinal Chemistry, Vol. 52, No. 5, 17.02.2009, p. 1408-1415.

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

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AU - O'Neill, Paul M.

AU - Park, B. Kevin

AU - Shone, Alison E.

AU - Maggs, James L.

AU - Roberts, Phillip

AU - Stocks, Paul A.

AU - Biagini, Giancarlo

AU - Bray, Patrick G.

AU - Gibbons, Peter

AU - Berry, Neil

AU - Winstanley, Peter A.

AU - Mukhtar, Amira

AU - Bonar-Law, Richard

AU - Hindley, Stephen

AU - Bambal, Ramesh B.

AU - Davis, Charles B.

AU - Bates, Martin

AU - Hart, Timothy K.

AU - Gresham, Stephanie L.

AU - Lawrence, Ron M.

AU - Brigandi, Richard A.

AU - Gomez-delas-Heras, Federico M.

AU - Gargallo, Domingo V.

AU - Ward, Steve

PY - 2009/2/17

Y1 - 2009/2/17

N2 - N-tert-Butyl isoquine (4) (GSK369796) is a 4-aminoquinoline drug candidate selected and developed as part of a public−private partnership between academics at Liverpool, MMV, and GSK pharmaceuticals. This molecule was rationally designed based on chemical, toxicological, pharmacokinetic, and pharmacodynamic considerations and was selected based on excellent activity against Plasmodium falciparum in vitro and rodent malaria parasites in vivo. The optimized chemistry delivered this novel synthetic quinoline in a two-step procedure from cheap and readily available starting materials. The molecule has a full industry standard preclinical development program allowing first into humans to proceed. Employing chloroquine (1) and amodiaquine (2) as comparator molecules in the preclinical plan, the first preclinical dossier of pharmacokinetic, toxicity, and safety pharmacology has also been established for the 4-aminoquinoline antimalarial class. These studies have revealed preclinical liabilities that have never translated into the human experience. This has resulted in the availability of critical information to other drug development teams interested in developing antimalarials within this class.

AB - N-tert-Butyl isoquine (4) (GSK369796) is a 4-aminoquinoline drug candidate selected and developed as part of a public−private partnership between academics at Liverpool, MMV, and GSK pharmaceuticals. This molecule was rationally designed based on chemical, toxicological, pharmacokinetic, and pharmacodynamic considerations and was selected based on excellent activity against Plasmodium falciparum in vitro and rodent malaria parasites in vivo. The optimized chemistry delivered this novel synthetic quinoline in a two-step procedure from cheap and readily available starting materials. The molecule has a full industry standard preclinical development program allowing first into humans to proceed. Employing chloroquine (1) and amodiaquine (2) as comparator molecules in the preclinical plan, the first preclinical dossier of pharmacokinetic, toxicity, and safety pharmacology has also been established for the 4-aminoquinoline antimalarial class. These studies have revealed preclinical liabilities that have never translated into the human experience. This has resulted in the availability of critical information to other drug development teams interested in developing antimalarials within this class.

U2 - 10.1021/jm8012618

DO - 10.1021/jm8012618

M3 - Article

SN - 0022-2623

VL - 52

SP - 1408

EP - 1415

JO - Journal of Medicinal Chemistry

JF - Journal of Medicinal Chemistry

IS - 5

ER -

Candidate Selection and Preclinical Evaluation of N-tert-Butyl Isoquine (GSK369796), An Affordable and Effective 4-Aminoquinoline Antimalarial for the 21st Century

Abstract

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