4.6 Article

Rational Design and Synthesis of Optimized Glycoclusters for Multivalent Lectin-Carbohydrate Interactions: Influence of the Linker Arm

Journal

CHEMISTRY-A EUROPEAN JOURNAL
Volume 18, Issue 20, Pages 6250-6263

Publisher

WILEY-V C H VERLAG GMBH
DOI: 10.1002/chem.201200010

Keywords

carbohydrates; click chemistry; glycoclusters; lectin; multivalency

Funding

  1. Universite Claude Bernard Lyon
  2. CNRS
  3. Region Rhone-Alpes (Cluster de Recherche Chimie)
  4. Vaincre la Mucoviscidose
  5. GDR Pseudomonas
  6. COST Action [CM-1102 MultiGlycoNano]
  7. ANR Glycoasterix
  8. Czech Ministry of Education [MSM0021622413, ME08008]
  9. European Community [205872]

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The design of multivalent glycoclusters requires the conjugation of biologically relevant carbohydrate epitopes functionalized with linker arms to multivalent core scaffolds. The multigram-scale syntheses of three structurally modified triethyleneglycol analogues that incorporate amide moiety(ies) and/or a phenyl ring offer convenient access to a series of carbohydrate probes with different water solubilities and rigidities. Evaluation of flexibility and determination of preferred conformations were performed by conformational analysis. Conjugation of the azido-functionalized carbohydrates with tetra-propargylated core scaffolds afforded a library of 18 tetravalent glycoclusters, in high yields, by CuI-catalyzed azidealkyne cycloaddition (CuAAC). The compounds were evaluated for their ability to bind to PA-IL (the LecA lectin from the opportunistic pathogen Pseudomonas aeruginosa). Biochemical evaluation through inhibition of hemagglutination assays (HIA), enzyme-linked lectin assays (ELLA), surface plasmon resonance (SPR), and isothermal titration microcalorimetry (ITC) revealed improved and unprecedented affinities for one of the monovalent probes (K-d=5.8 mu M) and also for a number of the tetravalent compounds that provide several new nanomolar ligands for this tetrameric lectin.

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