RAPID: Randomized pharmacophore identification for drug design

P. W. Finn; L. E. Kavraki; J. C. Latombe; R. Motwani; C. Shelton; S. Venkatasubramanian; A. Yao

doi:10.1016/S0925-7721(98)00008-X

RAPID: Randomized pharmacophore identification for drug design

P. W. Finn
, L. E. Kavraki
, J. C. Latombe
, R. Motwani
, C. Shelton
, S. Venkatasubramanian
, A. Yao

电子与信息学部

Pfizer
Stanford University

科研成果: 期刊稿件 › 文章 › 同行评审

16 引用（Scopus）

摘要

This paper describes a randomized approach for finding invariants in a set of flexible and chemically distinct ligands (drug molecules) that underlies an integrated software system called RAPID currently under development. An invariant is a collection of features embedded in ℝ³ which is present in one or more of the possible low-energy conformations of each ligand. Such invariants are called pharmacophores and contain the parts of the ligand that are primarily responsible for its binding with a receptor. The identification of pharmacophores is crucial in drug design since frequently the structure of targeted receptor is unknown but a number of molecules that interact with it have been discovered by experiments. In these cases the pharmacophore is used as a template for building more effective drugs. It is expected that our techniques and results will prove useful in other applications such as molecular database screening and comparative molecular field analysis.

源语言	英语
页（从-至）	263-272
页数	10
期刊	Computational Geometry: Theory and Applications
卷	10
期	4
DOI	https://doi.org/10.1016/S0925-7721(98)00008-X
出版状态	已出版 - 7月 1998

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10.1016/S0925-7721(98)00008-X

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title = "RAPID: Randomized pharmacophore identification for drug design",

abstract = "This paper describes a randomized approach for finding invariants in a set of flexible and chemically distinct ligands (drug molecules) that underlies an integrated software system called RAPID currently under development. An invariant is a collection of features embedded in ℝ3 which is present in one or more of the possible low-energy conformations of each ligand. Such invariants are called pharmacophores and contain the parts of the ligand that are primarily responsible for its binding with a receptor. The identification of pharmacophores is crucial in drug design since frequently the structure of targeted receptor is unknown but a number of molecules that interact with it have been discovered by experiments. In these cases the pharmacophore is used as a template for building more effective drugs. It is expected that our techniques and results will prove useful in other applications such as molecular database screening and comparative molecular field analysis.",

author = "Finn, \{P. W.\} and Kavraki, \{L. E.\} and Latombe, \{J. C.\} and R. Motwani and C. Shelton and S. Venkatasubramanian and A. Yao",

year = "1998",

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doi = "10.1016/S0925-7721(98)00008-X",

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TY - JOUR

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T2 - Randomized pharmacophore identification for drug design

AU - Finn, P. W.

AU - Kavraki, L. E.

AU - Latombe, J. C.

AU - Motwani, R.

AU - Shelton, C.

AU - Venkatasubramanian, S.

AU - Yao, A.

PY - 1998/7

Y1 - 1998/7

N2 - This paper describes a randomized approach for finding invariants in a set of flexible and chemically distinct ligands (drug molecules) that underlies an integrated software system called RAPID currently under development. An invariant is a collection of features embedded in ℝ3 which is present in one or more of the possible low-energy conformations of each ligand. Such invariants are called pharmacophores and contain the parts of the ligand that are primarily responsible for its binding with a receptor. The identification of pharmacophores is crucial in drug design since frequently the structure of targeted receptor is unknown but a number of molecules that interact with it have been discovered by experiments. In these cases the pharmacophore is used as a template for building more effective drugs. It is expected that our techniques and results will prove useful in other applications such as molecular database screening and comparative molecular field analysis.

AB - This paper describes a randomized approach for finding invariants in a set of flexible and chemically distinct ligands (drug molecules) that underlies an integrated software system called RAPID currently under development. An invariant is a collection of features embedded in ℝ3 which is present in one or more of the possible low-energy conformations of each ligand. Such invariants are called pharmacophores and contain the parts of the ligand that are primarily responsible for its binding with a receptor. The identification of pharmacophores is crucial in drug design since frequently the structure of targeted receptor is unknown but a number of molecules that interact with it have been discovered by experiments. In these cases the pharmacophore is used as a template for building more effective drugs. It is expected that our techniques and results will prove useful in other applications such as molecular database screening and comparative molecular field analysis.

UR - https://www.scopus.com/pages/publications/0012418602

U2 - 10.1016/S0925-7721(98)00008-X

DO - 10.1016/S0925-7721(98)00008-X

M3 - 文章

AN - SCOPUS:0012418602

SN - 0925-7721

VL - 10

SP - 263

EP - 272

JO - Computational Geometry: Theory and Applications

JF - Computational Geometry: Theory and Applications

IS - 4

ER -

RAPID: Randomized pharmacophore identification for drug design

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