4.8 Article Retracted Publication

被撤回的出版物: Synthesis of Multivalent Glycoconjugates Containing the Immunoactive LELTE Peptide: Effect of Glycosylation on Cellular Activation and Natural Killing by Human Peripheral Blood Mononuclear Cells (Retracted article. See vol. 136, pg. 1156, 2014)

Journal

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY
Volume 132, Issue 19, Pages 6800-6808

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/ja101296t

Keywords

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Funding

  1. Universite Joseph Fourier
  2. Centre National de la Recherche Scientifique (CNRS)
  3. EU ESF [D-34]
  4. Ministry of Education of the Czech Republic [LC06010, MSM21620808, 1M0505]
  5. Agency of the Academy of Sciences of the Czech Republic [IAA400200503]
  6. Czech Science Foundation [303/09/0477, 305/09/H008]
  7. Institutional Research Concept for the Institute of Microbiology [AVOZ50200510]

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Pentapeptide diacidic sequence LELTE, derived from the mycobacterial heat shock protein hsp65, has been recently identified as a danger signal of the immune system effective via specific binding to the universal leukocyte triggering receptor CD69. This sequence is not active per se, only after its presentation within the multivalent environment of its parent protein, or after artificial dimerization using a standard bifunctional reagents. Here we describe an entirely new way of presenting of this peptide based on its attachment to a cyclopeptide RAFT scaffold (K-K-K-P-G)2 through the c-amino group of lysine residues, alone or in combination with the carbohydrate epitope alpha GaINAc. The ability of such RAFT scaffolds to precipitate the target CD69 receptor or to activate CD69-positive cells is enhanced in compounds 2 and 4 possessing combined peptide/carbohydrate expression. Compounds 2 and 4 are highly efficient activators of natural killer lymphocytes, but they are completely inactive from the point of view of activation-induced apoptosis of lymphocytes by the target cells. These unique properties make the combined peptide/carbohydrate RAFTs highly suitable for future evaluation in animal tumor therapies in vivo and predict them to be readily available and efficient immunoactivators.

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