Davies, Matthew N. ; Bayry, Jagadeesh ; Tchilian, Elma Z. ; Vani, Janakiraman ; Shaila, Melkote S. ; Forbes, Emily K. ; Draper, Simon J. ; Beverley, Peter C. L. ; Tough, David F. ; Flower, Darren R. (2009) Toward the discovery of vaccine adjuvants: coupling In Silico screening and In Vitro analysis of antagonist binding to human and mouse CCR4 receptors PLos One, 4 (11). e8084_1-e8084_12. ISSN 1932-6203
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Official URL: http://www.plosone.org/article/info%3Adoi%2F10.137...
Related URL: http://dx.doi.org/10.1371/journal.pone.0008084
Abstract
Background: Adjuvants enhance or modify an immune response that is made to an antigen. An antagonist of the chemokine CCR4 receptor can display adjuvant-like properties by diminishing the ability of CD4+CD25+ regulatory T cells (Tregs) to down-regulate immune responses. Methodology: Here, we have used protein modelling to create a plausible chemokine receptor model with the aim of using virtual screening to identify potential small molecule chemokine antagonists. A combination of homology modelling and molecular docking was used to create a model of the CCR4 receptor in order to investigate potential lead compounds that display antagonistic properties. Three-dimensional structure-based virtual screening of the CCR4 receptor identified 116 small molecules that were calculated to have a high affinity for the receptor; these were tested experimentally for CCR4 antagonism. Fifteen of these small molecules were shown to inhibit specifically CCR4-mediated cell migration, including that of CCR4+ Tregs. Significance: Our CCR4 antagonists act as adjuvants augmenting human T cell proliferation in an in vitro immune response model and compound SP50 increases T cell and antibody responses in vivo when combined with vaccine antigens of Mycobacterium tuberculosis and Plasmodium yoelii in mice.
Item Type: | Article |
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Source: | Copyright of this article belongs to Public Library of Science. |
ID Code: | 49354 |
Deposited On: | 20 Jul 2011 06:20 |
Last Modified: | 18 May 2016 04:06 |
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