Abstract
More than 20 years ago clinical investigations in the immunotherapy of cancer revealed that infusion of certain immunotherapeutic mAbs directed to tumor cells induced loss of targeted epitopes. This phenomenon, called antigenic modulation, can compromise mAb-based therapies. Recently we reported that rituximab (RTX) treatment of chronic lymphocytic leukemia patients induced substantial loss of targeted CD20 on B cells found in the circulation after RTX infusion; this "shaving" of RTX-CD20 complexes from B cells is also promoted in vitro by THP-1 monocytes and by PBMC in a reaction mediated by Fcgamma receptors. The mechanism responsible for shaving appears to be trogocytosis, a process in which receptors on effector cells remove and internalize cognate ligands and cell membrane fragments from target cells. We now report that three therapeutic mAbs approved by the U.S. Food and Drug Administration for the treatment of cancer, RTX, cetuximab, and trastuzumab, as well as mAb T101, which has been shown to induce antigenic modulation in the clinic, promote trogocytosis in vitro upon binding to their respective target cells. Trogocytosis of the mAb-opsonized cells is mediated by THP-1 monocytes and by primary monocytes isolated from PBMC. In view of these results, it is likely that these mAbs and possibly other anticancer mAbs now used in the clinic may promote trogocytic removal of the therapeutic mAbs and their cognate Ags from tumor cells in vivo. Our findings may have important implications with respect to the use of mAbs in cancer immunotherapy.
Highlights
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We have recently demonstrated that a similar transfer occurs in vitro when B cells opsonized with anti-CD20 mAb rituximab (RTX)3 are reacted with either PBMC or monocytic THP-1 cells [5]
Since CD20 is an integral membrane protein, we investigated whether donor B cell membrane lipids are transferred
Summary
RTX, rituximab; Al, Alexa; bt, biotinylated; CET, cetuximab; CLL, chronic lymphocytic leukemia; Gt, goat; IC, immune complex(es); MESF, molecules of equivalent soluble fluorochome; Ms, mouse; RA, retinoic acid; SA, streptavidin; TRA, trastuzumab. To further characterize shaving of RTX-CD20 complexes and the relationship of this reaction to trogocytosis, we used the membrane dye PKH26 to test for the transfer of membrane fragments from RTX-opsonized donor cells to acceptor THP-1 cells. Flow cytometry and fluorescence microscopy were employed to examine three different mAb-opsonized/donor cell pairs: mAb T-101/MOLT-4 cells; trastuzumab (TRA, used in the treatment of breast cancer [15, 16])/BT-474 cells; and cetuximab (CET, used in the treatment of colorectal and other cancers [17, 18])/. In all three cases we observe similar reactions that closely follow the tenets defined for trogocytosis: transfer of donor cell-bound mAb/target Ag IC and membrane fragments to the acceptor cells, as well as internalization of acceptor cell Fc␥RI
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