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. 1999 Jun 18;453(1-2):164-8.
doi: 10.1016/s0014-5793(99)00713-9.

Di-, tri- and tetrameric single chain Fv antibody fragments against human CD19: effect of valency on cell binding

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Di-, tri- and tetrameric single chain Fv antibody fragments against human CD19: effect of valency on cell binding

F Le Gall et al. FEBS Lett. .
Free article

Abstract

Single chain variable fragments (scFv) of the murine monoclonal antibody HD37 specific to human B-cell antigen CD19 were constructed by joining the VH and VL domains with linkers of 18, 10, 1 and 0 residues. ScFv-18 formed monomers, dimers and small amounts of tetramers; scFv-10 formed dimers and small amounts of tetramers; scFv-1 formed exclusively tetramers; scFv-0 formed exclusively trimers. The affinities of the scFv-10 (diabody) and scFv-1 (tetrabody) were approximately 1.5- and 2.5-fold higher, respectively, than that of the scFv-0 (triabody). The tetrabody displayed a significantly prolonged association with cell-bound antigen (t1/2 cell surface retention at 37 degrees C of 26.6 min) compared to both the diabody (13.3 min) and triabody (6.7 min). This increase in avidity of the tetrabody combined with its larger size could prove to be particularly advantageous for imaging and the immunotherapy of B-cell malignancies.

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