Publication | Closed Access
Generation of human high‐affinity antibodies specific for the fibroblast activation protein by guided selection
39
Citations
37
References
2001
Year
Immunocytochemical TechniqueImmunologyImmunotherapyHuman High‐affinity AntibodiesSynthetic ImmunologyProtein ExpressionImmunochemistryAntibody EngineeringHuman Antibody DerivativesMolecular DiagnosticsRadiation OncologyGuided SelectionCancer ResearchHuman ScfvsTumor TargetingAntibody DerivativesAntibody ScreeningCell BiologyTumor MicroenvironmentFibroblast Activation ProteinAntibody BiologyProtein EngineeringMedicine
Four completely human antibody derivatives [single-chain-antibody fragments (scFvs)] with specificity for the general tumor stroma marker fibroblast activation protein (FAP) were isolated by guided selection. Highly diverse IgG, IgM and IgD isotypes comprising heavy-chain variable domain libraries were generated using cDNAs derived from diverse lymphoid organs of a multitude of donors. Three of the human scFvs were converted into bivalent minibodies and expressed in eukaryotic cells for further functional characterization. Binding-competition studies and analysis by fluorescence-activated cell sorting showed high-affinity binding (10--20 nM) for two clones and recognition of the same epitope as the murine guiding antibody. The minibodies were successfully used for immunohistology of a variety of human carcinoma biopsies, revealing specific staining of stromal fibroblasts. Therefore, they should be suitable for in vivo diagnostic and tumor-targeting studies and, because of their completely human origin, be superior to murine or humanized antibody derivatives.
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