Rational CCL5 mutagenesis integration in a lactobacilli platform generates extremely potent HIV-1 blockers

Secchi, Massimiliano; Grampa, Valentina; Vangelista, Luca

doi:10.1038/s41598-018-20300-9

Cited by 13 publications

(21 citation statements)

References 52 publications

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“…LukED mechanism of action satisfies previously proposed models where the S subunit initiates the binding and recruits the F subunit to proceed with pore formation [53,55]. In addition, it was shown that the FDA-approved CCR5 antagonist maraviroc can block the interaction between LukE and CCR5 [53], and recently developed potent CCL5 derivatives are presently being investigated in this context [56,57]. These data confirm the specificity of this interaction and proves that a drug currently used as HIV-1 inhibitor has repositioning potentials as a treatment option for S. aureus infections [53].…”

Section: Genetic Organizationsupporting

confidence: 65%

Genetic organization and cellular specificity of S. aureus leukocidins

Bulanin¹,

Marchenko²,

Abitayeva³

et al. 2020

Bul. Kar.Univ. “BioMedGeo” Ser

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Currently, infections produced by the gram-positive bacteria S. aureus represent a significant healthcare burden throughout the world. This is attributed to the ability of this bacterium to develop antibiotic resistance and efficiently evade human immune response. Therefore, research effort of many scientific laboratories worldwide is directed toward characterization of the genetic organization and molecular mechanisms responsible for S. aureus pathogenesis. This report is aimed to describe the growing body of evidence related to our understanding of the genetic organization and molecular interactions of the S. aureus leukocidins with the human cells that play an important role in bacterial pathogenesis, and represent a significant healthcare burden. Understanding of the genetic organization linked with additional mechanisms responsible for the realization of toxic potential, can help us to develop a better personalized approach for therapy against S. aureus infections. Thus, improved understanding of the molecular interactions between S. aureus leucocidins, and cell surface receptors may lead to the development of the alternative anti-microbial agents, that either independently or in combination with the current antibiotic treatment regimens will be used as an effective treatment strategy in clinic.

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Section: Genetic Organizationsupporting

confidence: 65%

Genetic organization and cellular specificity of S. aureus leukocidins

Bulanin¹,

Marchenko²,

Abitayeva³

et al. 2020

Bul. Kar.Univ. “BioMedGeo” Ser

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“…Among the CCL5 derivatives efficiently blocking CCR5, the most potent HIV-1 entry inhibitors reported to date are CCL5 5P12 5M and CCL5 6P4 5M, a CCR5 antagonist and a superagonist, respectively ( 11 ). Five mutated hotspots (5M) were selected to enhance different features related to the CCL5:CCR5 interaction.…”

Section: Resultsmentioning

confidence: 99%

“…The high-resolution structure of CCR5 in complex with 5P7 CCL5 (a CCR5 antagonist) (PDB ID: 5UIW) ( 16 ) was used as template for the modeling of CCL5 5P12 5M, the most potent CCR5 antagonist reported to date ( 11 ). Six separate 3D models (T7L, F12Y, A13V, Y27W, F28W and E66S), accounting for the differences between 5P7 CCL5 and CCL5 5P12 5M were built using SWISS-MODEL.…”

Section: Methodsmentioning

confidence: 99%

“…Initially, CCL5 variants retained CCR5 agonist activity, later followed by efforts to attain a switch to antagonism ( 9 ). Last generation CCL5 derivatives acting as CCR5 antagonists could be a valid alternative to MVC, as they present in vitro anti-HIV-1 activity largely superior to MVC ( 10 , 11 ). Monoclonal antibodies (mAbs) acting as CCR5 antagonists have been the subject of intense investigation ( 12 ) leading to promising therapeutic perspectives ( 13 , 14 ).…”

Section: Introductionmentioning

confidence: 99%

“…In this study, we investigated both retroactively and in perspective the innovative role of selected point mutations inserted in CCL5 regions distal to the classically targeted N-terminus ( 11 ). We also briefly discuss emerging allosteric strategies to block GPCRs alternative to the active site occupancy and that could be of interest to tackle CCR5 in pathology.…”

Section: Introductionmentioning

confidence: 99%

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Filling the Gaps in Antagonist CCR5 Binding, a Retrospective and Perspective Analysis

Amerzhanova

Vangelista

2022

Front. Immunol.

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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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