4.5 Article

A convenient route towards deoxygalactosyl-functionalised ortho-carbaborane: Synthesis of a building block for peptide conjugation

Journal

JOURNAL OF ORGANOMETALLIC CHEMISTRY
Volume 798, Issue -, Pages 46-50

Publisher

ELSEVIER SCIENCE SA
DOI: 10.1016/j.jorganchem.2015.08.011

Keywords

Carbaboranes; Carboranes; Monosubstitution; Galactose; Water solubility; Peptide; Bioconjugation

Funding

  1. Fonds der Chemischen Industrie (FCI)
  2. Europaischer Fonds fur regionale Entwicklung (EFRE)
  3. Graduate School Leipzig, School of Natural Sciences - Building with Molecules and Nano-objects (BuildMoNa)

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In the treatment of cancer, boron neutron capture therapy (BNCT) is a mild and promising alternative to established harsh therapeutic methods such as chemo- and radiation therapy. However, successful BNCT procedures strongly depend on efficient, tumour-selective boron-delivery systems, and recently we have demonstrated that the breast tumour-selective peptide [F-7,P-34]-NPY is a promising boron-shuttle system after conjugation with three ortho-carbaborane clusters (1,2-closo-C2B10H10). The extreme hydrophobicity of the latter, however, causes problems in medicinal applications in vivo. Therefore, we have elaborated a synthetic protocol towards a deoxygalactosyl-modified (and thus more hydrophilic) building block that can readily be conjugated with the shuttle peptide. A key intermediate, i.e., ortho-carbaborane functionalised with a bis-isopropylidene-protected deoxygalactosyl moiety, was synthesised by both a silyl protection strategy (which is generally recommended for monosubstitution) and direct reaction of metallated ortho-carbaborane in acceptable yield. (C) 2015 Elsevier B.V. All rights reserved.

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