Literature DB >> 15643518

Targeting human cancer cells with VEGF receptor-2-directed liposomes.

Alma Rubio Demirovic1, Cornelia Marty, Sandra Console, Steffen M Zeisberger, Claudia Ruch, Rolf Jaussi, Reto A Schwendener, Kurt Ballmer-Hofer.   

Abstract

Antibodies are among the most versatile tools used today to characterize and target molecules in cells and in biological tissues. The development of phage display libraries encoding a large repertoire of single chain antibodies, scFv, allows the rapid and efficient isolation of antibodies specific for almost any type of molecule. A great advantage of such recombinant antibodies is the possibility to functionalize them by introducing new amino acid sequences. This leads to new features that would be difficult to introduce into naturally occurring antibody molecules. This approach has been successfully applied to create molecules with new biological activities, e.g. by generating chimeric scFv antibodies carrying sequences derived from other biomolecules such as blood clotting factors or enzymes. Here, we describe a new antibody isolated from an M13 phage library that recognizes vascular endothelial growth factor receptor 2, VEGFR-2. This antibody, scFvVR-2H9 was coupled to liposomes and used to specifically target VEGFR-2-expressing human cancer cells in culture.

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Year:  2005        PMID: 15643518

Source DB:  PubMed          Journal:  Oncol Rep        ISSN: 1021-335X            Impact factor:   3.906


  1 in total

1.  Highly efficient baculovirus-mediated multigene delivery in primary cells.

Authors:  Maysam Mansouri; Itxaso Bellon-Echeverria; Aurélien Rizk; Zahra Ehsaei; Chiara Cianciolo Cosentino; Catarina S Silva; Ye Xie; Frederick M Boyce; M Wayne Davis; Stephan C F Neuhauss; Verdon Taylor; Kurt Ballmer-Hofer; Imre Berger; Philipp Berger
Journal:  Nat Commun       Date:  2016-05-04       Impact factor: 14.919

  1 in total

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