Bevacizumab

Immunoglobulin G (IgG) Fc receptors play a critical role in linking IgG antibody-mediated immune responses with cellular effector functions. A high resolution map of the binding site on human IgG1 for human Fc␥RI, Fc␥RIIA, Fc␥RIIB, Fc␥RIIIA, and FcRn receptors has been determined. A common set of IgG1 residues is involved in binding to all Fc␥R; Fc␥RII and Fc␥RIII also utilize residues outside this common set. In addition to residues which, when altered, abrogated binding to one or more of the receptors, several residues were found that improved binding only to specific receptors or simultaneously improved binding to one type of receptor and reduced binding to another type. Select IgG1 variants with improved binding to Fc␥RIIIA exhibited up to 100% enhancement in antibody-dependent cell cytotoxicity using human effector cells; these variants included changes at residues not found at the binding interface in the IgG/Fc␥RIIIA co-crystal structure (Sondermann, P., Huber, R., Oosthuizen, V., and Jacob, U. (2000) Nature 406, 267-273). These engineered antibodies may have important implications for improving antibody therapeutic efficacy.

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Engineering therapeutic antibodies for improved function

Presta¹,

Shields²,

Namenuk³

et al. 2002

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The binding sites on human IgG1 for human Fc gamma receptor (Fc gamma R) I, Fc gamma RIIa, Fc gamma RIIb, Fc gamma RIIIa and neonatal FcR have been mapped. A common set of IgG1 residues is involved in binding to all Fc gamma Rs, while Fc gamma RII and Fc gamma RIII utilize distinct sites outside this common set. In addition to residues which abrogated binding to the Fc gamma R, several positions were found which improved binding only to specific Fc gamma Rs or simultaneously improved binding to one type of Fc gamma R and reduced binding to another type. Selected IgG1 variants with improved binding to Fc gamma RIIIa were then tested in an in vitro antibody-dependent cellular cytotoxicity (ADCC) assay and showed an enhancement in ADCC when either peripheral blood mononuclear cells or natural killer cells were used.

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Analysis of mixture sequences derived from edman degradation data

Henzel¹,

Stults²,

Wong³

et al. 1996

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Rapid assembly of “subtiligase” substrates to elucidate optimal ligation junctures

Judice¹,

Namenuk²,

Burnier³

1996

Bioorganic & Medicinal Chemistry Letters

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Angela K. Namenuk

High Resolution Mapping of the Binding Site on Human IgG1 for FcγRI, FcγRII, FcγRIII, and FcRn and Design of IgG1 Variants with Improved Binding to the FcγR

Engineering therapeutic antibodies for improved function

Analysis of mixture sequences derived from edman degradation data

Rapid assembly of “subtiligase” substrates to elucidate optimal ligation junctures

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