Discovery of leukotriene A4 hydrolase inhibitors using metabolomics biased fragment crystallography

Douglas R. Davies; Bjorn Mamat; Olafur T. Magnusson; Jeff Christensen; Magnus H. Haraldsson; Rama Mishra; Brian Pease; Erik Hansen; Jasbir Singh; David Zembower; Hidong Kim; Alex S. Kiselyov; Alex B. Burgin; Mark E. Gurney; Lance J. Stewart

doi:10.1021/jm900259h

Discovery of leukotriene A4 hydrolase inhibitors using metabolomics biased fragment crystallography

Douglas R. Davies
, Bjorn Mamat
, Olafur T. Magnusson
, Jeff Christensen
, Magnus H. Haraldsson
, Rama Mishra
, Brian Pease
, Erik Hansen
, Jasbir Singh
, David Zembower
, Hidong Kim
, Alex S. Kiselyov
, Alex B. Burgin
, Mark E. Gurney
, Lance J. Stewart

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Rannsóknarafurð: Framlag til fræðitímarits › Grein › ritrýni

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We describe a novel fragment library termed fragments of life (FOL) for structure-based drug discovery. The FOL library includes natural small molecules of life, derivatives thereof, and biaryl protein architecture mimetics. The choice of fragments facilitates the interrogation of protein active sites, allosteric binding sites, and protein-protein interaction surfaces for fragment binding. We screened the FOL library against leukotriene A4 hydrolase (LTA4H) by X-ray crystallography. A diverse set of fragments including derivatives of resveratrol, nicotinamide, and indole were identified as efficient ligands for LTA4H. These fragments were elaborated in a small number of synthetic cycles into potent inhibitors of LTA4H representing multiple novel chemotypes for modulating leukotriene biosynthesis. Analysis of the fragment-bound structures also showed that the fragments comprehensively recapitulated key chemical features and binding modes of several reported LTA4H inhibitors.

Upprunalegt tungumál	Enska
Síður (frá-til)	4694-4715
Síðufjöldi	22
Fræðitímarit	Journal of Medicinal Chemistry
Bindi	52
Númer tölublaðs	15
DOI	https://doi.org/10.1021/jm900259h
Útgáfustaða	Útgefið - 13 ágú. 2009

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10.1021/jm900259h

Vitna í þetta

Davies, D. R., Mamat, B., Magnusson, O. T., Christensen, J., Haraldsson, M. H., Mishra, R., Pease, B., Hansen, E., Singh, J., Zembower, D., Kim, H., Kiselyov, A. S., Burgin, A. B., Gurney, M. E., & Stewart, L. J. (2009). Discovery of leukotriene A4 hydrolase inhibitors using metabolomics biased fragment crystallography. Journal of Medicinal Chemistry, 52(15), 4694-4715. https://doi.org/10.1021/jm900259h

@article{a2f680545940450cafb87096f64a2548,

title = "Discovery of leukotriene A4 hydrolase inhibitors using metabolomics biased fragment crystallography",

abstract = "We describe a novel fragment library termed fragments of life (FOL) for structure-based drug discovery. The FOL library includes natural small molecules of life, derivatives thereof, and biaryl protein architecture mimetics. The choice of fragments facilitates the interrogation of protein active sites, allosteric binding sites, and protein-protein interaction surfaces for fragment binding. We screened the FOL library against leukotriene A4 hydrolase (LTA4H) by X-ray crystallography. A diverse set of fragments including derivatives of resveratrol, nicotinamide, and indole were identified as efficient ligands for LTA4H. These fragments were elaborated in a small number of synthetic cycles into potent inhibitors of LTA4H representing multiple novel chemotypes for modulating leukotriene biosynthesis. Analysis of the fragment-bound structures also showed that the fragments comprehensively recapitulated key chemical features and binding modes of several reported LTA4H inhibitors.",

author = "Davies, \{Douglas R.\} and Bjorn Mamat and Magnusson, \{Olafur T.\} and Jeff Christensen and Haraldsson, \{Magnus H.\} and Rama Mishra and Brian Pease and Erik Hansen and Jasbir Singh and David Zembower and Hidong Kim and Kiselyov, \{Alex S.\} and Burgin, \{Alex B.\} and Gurney, \{Mark E.\} and Stewart, \{Lance J.\}",

year = "2009",

month = aug,

day = "13",

doi = "10.1021/jm900259h",

language = "English",

volume = "52",

pages = "4694--4715",

journal = "Journal of Medicinal Chemistry",

issn = "0022-2623",

publisher = "American Chemical Society",

number = "15",

}

Davies, DR, Mamat, B, Magnusson, OT, Christensen, J, Haraldsson, MH, Mishra, R, Pease, B, Hansen, E, Singh, J, Zembower, D, Kim, H, Kiselyov, AS, Burgin, AB, Gurney, ME & Stewart, LJ 2009, 'Discovery of leukotriene A4 hydrolase inhibitors using metabolomics biased fragment crystallography', Journal of Medicinal Chemistry, bind. 52, nr. 15, bls. 4694-4715. https://doi.org/10.1021/jm900259h

TY - JOUR

T1 - Discovery of leukotriene A4 hydrolase inhibitors using metabolomics biased fragment crystallography

AU - Davies, Douglas R.

AU - Mamat, Bjorn

AU - Magnusson, Olafur T.

AU - Christensen, Jeff

AU - Haraldsson, Magnus H.

AU - Mishra, Rama

AU - Pease, Brian

AU - Hansen, Erik

AU - Singh, Jasbir

AU - Zembower, David

AU - Kim, Hidong

AU - Kiselyov, Alex S.

AU - Burgin, Alex B.

AU - Gurney, Mark E.

AU - Stewart, Lance J.

PY - 2009/8/13

Y1 - 2009/8/13

N2 - We describe a novel fragment library termed fragments of life (FOL) for structure-based drug discovery. The FOL library includes natural small molecules of life, derivatives thereof, and biaryl protein architecture mimetics. The choice of fragments facilitates the interrogation of protein active sites, allosteric binding sites, and protein-protein interaction surfaces for fragment binding. We screened the FOL library against leukotriene A4 hydrolase (LTA4H) by X-ray crystallography. A diverse set of fragments including derivatives of resveratrol, nicotinamide, and indole were identified as efficient ligands for LTA4H. These fragments were elaborated in a small number of synthetic cycles into potent inhibitors of LTA4H representing multiple novel chemotypes for modulating leukotriene biosynthesis. Analysis of the fragment-bound structures also showed that the fragments comprehensively recapitulated key chemical features and binding modes of several reported LTA4H inhibitors.

AB - We describe a novel fragment library termed fragments of life (FOL) for structure-based drug discovery. The FOL library includes natural small molecules of life, derivatives thereof, and biaryl protein architecture mimetics. The choice of fragments facilitates the interrogation of protein active sites, allosteric binding sites, and protein-protein interaction surfaces for fragment binding. We screened the FOL library against leukotriene A4 hydrolase (LTA4H) by X-ray crystallography. A diverse set of fragments including derivatives of resveratrol, nicotinamide, and indole were identified as efficient ligands for LTA4H. These fragments were elaborated in a small number of synthetic cycles into potent inhibitors of LTA4H representing multiple novel chemotypes for modulating leukotriene biosynthesis. Analysis of the fragment-bound structures also showed that the fragments comprehensively recapitulated key chemical features and binding modes of several reported LTA4H inhibitors.

UR - https://www.scopus.com/pages/publications/68549132502

U2 - 10.1021/jm900259h

DO - 10.1021/jm900259h

M3 - Article

C2 - 19618939

SN - 0022-2623

VL - 52

SP - 4694

EP - 4715

JO - Journal of Medicinal Chemistry

JF - Journal of Medicinal Chemistry

IS - 15

ER -

Discovery of leukotriene A4 hydrolase inhibitors using metabolomics biased fragment crystallography

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