Literature DB >> 15204035

G-protein coupled receptors as allosteric machines.

Terry Kenakin1.   

Abstract

Allosterism, whereby small molecule ligands produce global changes in the conformations of receptors, is a powerful mechanism for drug effect. This is illustrated by the recent data describing CCR5 antagonists as blockers of HIV infection. Allosteric effects are described in terms of a change in the tertiary conformation of the receptor. This paper outlines some unique features of allosteric antagonists as new drug entities. These include the fact that allosteric ligands have texture in antagonism (not all allosterically blocked receptors are alike), allosteric blockade is probe dependent (not all agonists and radioligands are blocked equally), and the fact that allosteric binding involves a separate site on the receptor may have relevance to duration of effect and selectivity. Dissociation between receptor function and binding also can be encountered with allosteric ligands.

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Year:  2004        PMID: 15204035     DOI: 10.1080/10606820490464316

Source DB:  PubMed          Journal:  Receptors Channels        ISSN: 1060-6823


  14 in total

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Authors:  Catherine J Hutchings; Gabriella Cseke; Greg Osborne; Jeanette Woolard; Andrei Zhukov; Markus Koglin; Ali Jazayeri; Jahnavi Pandya-Pathak; Christopher J Langmead; Stephen J Hill; Malcolm Weir; Fiona H Marshall
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7.  Bitopic ligands: all-in-one orthosteric and allosteric.

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9.  Cell surface expression of CCR5 and other host factors influence the inhibition of HIV-1 infection of human lymphocytes by CCR5 ligands.

Authors:  Thomas J Ketas; Shawn E Kuhmann; Ashley Palmer; Juan Zurita; Weijing He; Sunil K Ahuja; Per Johan Klasse; John P Moore
Journal:  Virology       Date:  2007-04-10       Impact factor: 3.616

Review 10.  A pièce de resistance: how HIV-1 escapes small molecule CCR5 inhibitors.

Authors:  John P Moore; Daniel R Kuritzkes
Journal:  Curr Opin HIV AIDS       Date:  2009-03       Impact factor: 4.283

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