Molecular construction of HIV-gp120 discontinuous epitope mimics by assembly of cyclic peptides on an orthogonal alkyne functionalized TAC-scaffold

Publication date

2016

Authors

Werkhoven, P. R.ISNI 0000000493229006
Elwakiel, M.
Meuleman, T. J.
Quarles Van Ufford, H. C.ISNI 0000000389772666
Kruijtzer, JohnISNI 0000000387953981
Liskamp, RobISNI 0000000393845493

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Document Type

Article
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Abstract

Mimics of discontinuous epitopes of for example bacterial or viral proteins may have considerable potential for the development of synthetic vaccines, especially if conserved epitopes can be mimicked. However, due to the structural complexity and size of discontinuous epitopes molecular construction of these mimics remains challeging. We present here a convergent route for the assembly of discontinuous epitope mimics by successive azide alkyne cycloaddition on an orthogonal alkyne functionalized scaffold. Here the synthesis of mimics of the HIV gp120 discontinuous epitope that interacts with the CD4 receptor is described. The resulting protein mimics are capable of inhibition of the gp120-CD4 interaction. The route is convergent, robust and should be applicable to other discontinuous epitopes.

Keywords

Physical and Theoretical Chemistry, Organic Chemistry, Biochemistry, SDG 3 - Good Health and Well-being

Citation

Werkhoven, P R, Elwakiel, M, Meuleman, T J, Quarles Van Ufford, H C, Kruijtzer, J A W & Liskamp, R M J 2016, 'Molecular construction of HIV-gp120 discontinuous epitope mimics by assembly of cyclic peptides on an orthogonal alkyne functionalized TAC-scaffold', Organic & Biomolecular Chemistry, vol. 14, no. 2, pp. 701-710. https://doi.org/10.1039/c5ob02014j