FILLING THE GAPS IN ANTAGONIST CCR5 BINDING, A RETROSPECTIVE AND PERSPECTIVE ANALYSIS
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Amerzhanova, Yerkezhan
Vangelista, Luca
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Frontiers in Immunology
Abstract
The large number of pathologies that position CCR5 as a central molecular determinant
substantiates the studies aimed at understanding receptor-ligand interactions, as well as
the development of compounds that efficiently block this receptor. This perspective
focuses on CCR5 antagonism as the preferred landscape for therapeutic intervention,
thus the receptor active site occupancy by known antagonists of different origins is
overviewed. CCL5 is a natural agonist ligand for CCR5 and an extensively studied scaffold
for CCR5 antagonists production through chemokine N-terminus modification. A
retrospective 3D modeling analysis on recently developed CCL5 mutants and their
contribution to enhanced anti-HIV-1 activity is reported here. These results allow us to
prospect the development of conceptually novel amino acid substitutions outside the
CCL5 N-terminus hotspot. CCR5 interaction improvement in regions distal to the
chemokine N-terminus, as well as the stabilization of the chemokine hydrophobic core
are strategies that influence binding affinity and stability beyond the agonist/antagonist
dualism. Furthermore, the development of allosteric antagonists topologically remote from
the orthosteric site (e.g., intracellular or membrane-embedded) is an intriguing new
avenue in GPCR druggability and thus a conceivable novel direction for CCR5
blockade. Ultimately, the three-dimensional structure elucidation of the interaction
between various ligands and CCR5 helps illuminate the active site occupancy and
mechanism of action.
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Amerzhanova, Y., & Vangelista, L. (2022). Filling the Gaps in Antagonist CCR5 Binding, a Retrospective and Perspective Analysis. Frontiers in Immunology, 13. https://doi.org/10.3389/fimmu.2022.826418
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