Single-chain vascular endothelial growth factor variant with antagonist activity.

J Biol Chem

Maxygen ApS, Agern Alle 1, DK-2970 Hørsholm, Denmark.

Published: October 2002

AI Article Synopsis

  • Vascular endothelial growth factor (VEGF) is crucial for forming blood vessels and is linked to diseases like cancer in adults.
  • Researchers developed a single-chain version of VEGF that simplifies the creation of two active receptor binding sites, overcoming challenges with the traditional method of making heterodimers.
  • A mutant form of this single-chain VEGF effectively blocks the activity of the wild-type protein on endothelial cells, showcasing a new method to modify proteins for targeted therapeutic purposes.

Article Abstract

Vascular endothelial growth factor is a specific endothelial cell mitogen that is essential for the formation of the vascular system but in the adult individual is involved in several pathological conditions, including cancer. It is a homodimeric protein that activates its receptor by binding two receptor molecules and inducing dimerization. By mixing two vascular endothelial growth factor monomers, each with different substitutions, heterodimers with only one active receptor binding site have previously been prepared. These heterodimers bind the receptor molecule but are unable to induce dimerization and activation. However, preparation of heterodimers is cumbersome, involving separate expression of different monomers, refolding the mixture, and separating heterodimers from homodimers. Here we show that a fully functional ligand can efficiently be expressed as a single protein chain containing two monomers. Single-chain vascular endothelial growth factor is functionally equivalent to the wild-type protein. By monomer-specific mutagenesis, one receptor binding site was altered. This variant competitively and specifically antagonizes the mitogenic effect of the wild-type protein on endothelial cells. The results obtained with the single-chain antagonist show the feasibility of the single-chain approach in directing alterations to single specific regions in natural homodimeric proteins that would be impossible to target in other ways.

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Source
http://dx.doi.org/10.1074/jbc.M204107200DOI Listing

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