“Pharmacophore”的意思、由来-开放百科全书

A pharmacophore is an abstract description of molecular features that are necessary for molecular recognition of a ligand by a biological macromolecule. IUPAC defines a pharmacophore to be "an ensemble of steric and electronic features that is necessary to ensure the optimal supramolecular interactions with a specific biological target and to trigger (or block) its biological response".^[1] A pharmacophore model explains how structurally diverse ligands can bind to a common receptor site. Furthermore, pharmacophore models can be used to identify through de novo design or virtual screening novel ligands that will bind to the same receptor.

Features

Typical pharmacophore features include hydrophobic centroids, aromatic rings, hydrogen bond acceptors or donors, cations, and anions. These pharmacophoric points may be located on the ligand itself or may be projected points presumed to be located in the receptor.

The features need to match different chemical groups with similar properties, in order to identify novel ligands. Ligand-receptor interactions are typically “polar positive”, “polar negative” or “hydrophobic”. A well-defined pharmacophore model includes both hydrophobic volumes and hydrogen bond vectors.

Model development

The process for developing a pharmacophore model generally involves the following steps:

As the biological activities of new molecules become available, the pharmacophore model can be updated to further refine it.

Applications

In modern computational chemistry, pharmacophores are used to define the essential features of one or more molecules with the same biological activity. A database of diverse chemical compounds can then be searched for more molecules which share the same features arranged in the same relative orientation. Pharmacophores are also used as the starting point for developing 3D-QSAR models. Such tools and a related concept of "privileged structures", which are "defined as molecular frameworks which are able of providing useful ligands for more than one type of receptor or enzyme target by judicious structural modifications",^[3] aid in drug discovery.

History

Historically, pharmacophores were established by Lemont Kier, who first mentions the concept in 1967^[4]

The development of the concept is often erroneously accredited to Paul Ehrlich. However neither the alleged source^[6] nor any of his other works mention the term "pharmacophore" or make use of the concept.^[7]

See also

References

1. ^{{cite journal |vauthors=Wermuth CG, Ganellin CR, Lindberg P, Mitscher LA | title = Glossary of terms used in medicinal chemistry (IUPAC Recommendations 1998) | journal=Pure and Applied Chemistry |year = 1998 | volume=70 | issue = 5 | pages = 1129–1143 | doi = 10.1351/pac199870051129 }}
2. ^{{cite book |vauthors=Madsen U, Bräuner-Osborne H, Greenwood JR, Johansen TN, Krogsgaard-Larsen P, Liljefors T, Nielsen M, Frølund B |editor=Gad SC |title=Drug Discovery Handbook |publisher=Wiley-Interscience/J. Wiley |location=Hoboken, N.J |year=2005 |pages=797–907 |chapter=GABA and Glutamate receptor ligands and their therapeutic potential in CNS disorders |isbn=0-471-21384-5 }}
3. ^{{Citation |last=Duarte |first=CD |display-authors=etal |year=2007 |title=Privileged structures: a useful concept for the rational design of new lead drug candidates |journal=Mini Rev Med Chem |volume=7 |issue=11 |pages=1108-1119 |pmid=18045214 |pmc= |doi=10.2174/138955707782331722 |postscript=.}}
4. ^{{cite journal | author = Kier LB | title = Molecular orbital calculation of preferred conformations of acetylcholine, muscarine, and muscarone | journal = Mol. Pharmacol. | volume = 3 | issue = 5 | pages = 487–94 |date=September 1967 | pmid = 6052710 | doi = }}
5. ^{{cite book | author = Kier LB | title = Molecular orbital theory in drug research | publisher = Academic Press | location = Boston | year = 1971 | pages = 164–169 | isbn = 0-12-406550-3 }}
6. ^{{cite journal | author = Ehrlich P | title=Über den jetzigen Stand der Chemotherapie | journal = Ber. Dtsch. Chem. Ges. | year = 1909 | volume = 42 | pages = 17–47 | doi=10.1002/cber.19090420105}}
7. ^{{cite journal|authors=J.H. van Drie | title = Monty Kier and the Origin of the Pharmacophore Concept | journal = Internet Electronic Journal of Molecular Design | volume = 6 | year = 2007 | pages = 271–279 | url = http://biochempress.com/Files/iejmd_2007_6_0271.pdf }}