BAR-Bodies: B-Cell Receptor Antigens As the Targeting Moiety of Antibodies in Substitution for the Variable Region of Heavy and Light Chains

Abstract: Background Chronic antigenic stimulation of the B-cell receptor (BCR) seems to play a critical role in the pathogenesis of B-cell lymphomas. We recently identified ARS2 and LRPAP1 as the autoantigenic targets of the B-cell receptors of approximately 25% of diffuse large B cell lymphomas (DLBCLs) of the ABC type and 45% of mantle cell lymphomas (MCLs), respectively. These BCR antigens can be used to target lymphoma cells in an approach we designated as BAR (B-cell receptor antigens for reverse ta… Show more

“…Although this review focuses mainly on what the literature refers to as ligand-based CAR-T cells, it is necessary to mention other approaches in which ligands are incorporated as the binding moiety of the CAR structure. In this regard, we found the so-called chimeric autoantibody receptor (CAAR) ( 103 ), B-cell receptor antigen for reverse targeting (BAR) ( 104 ), and chimeric HLA antibody receptor (CHAR) ( Figure 3 ) .…”

“…BCR signaling has been identified as an important pathway in B-cell lymphomagenesis, and there is increasing evidence that antigenic stimulation of the BCR is a trigger for proliferation. Several autoantigens, such as ARS2 and LRPAP1, have been proposed as stimulatory ligands of the BCR and its pathway in one quarter of diffuse large B-cell lymphomas (DLBCLs) and almost half of the mantle cell lymphomas (MCLs), respectively ( 104 – 106 ).…”

“…Further research has led to the construction of an antibody-like structure that incorporates the sequence of these identified BCR antigens, or at least their BCR-binding epitope, replacing the variable fragments of the scFv heavy and light chains, with the aim of transducing T cells and targeting malignant B-clones with unique specificity for these BCRs responsible for tumor expansion ( 104 , 106 ). Since approaches such as that of Bewarder et al.…”

Ligand-based CAR-T cell: Different strategies to drive T cells in future new treatments

“…Although this review focuses mainly on what the literature refers to as ligand-based CAR-T cells, it is necessary to mention other approaches in which ligands are incorporated as the binding moiety of the CAR structure. In this regard, we found the so-called chimeric autoantibody receptor (CAAR) ( 103 ), B-cell receptor antigen for reverse targeting (BAR) ( 104 ), and chimeric HLA antibody receptor (CHAR) ( Figure 3 ) .…”

“…BCR signaling has been identified as an important pathway in B-cell lymphomagenesis, and there is increasing evidence that antigenic stimulation of the BCR is a trigger for proliferation. Several autoantigens, such as ARS2 and LRPAP1, have been proposed as stimulatory ligands of the BCR and its pathway in one quarter of diffuse large B-cell lymphomas (DLBCLs) and almost half of the mantle cell lymphomas (MCLs), respectively ( 104 – 106 ).…”

“…Further research has led to the construction of an antibody-like structure that incorporates the sequence of these identified BCR antigens, or at least their BCR-binding epitope, replacing the variable fragments of the scFv heavy and light chains, with the aim of transducing T cells and targeting malignant B-clones with unique specificity for these BCRs responsible for tumor expansion ( 104 , 106 ). Since approaches such as that of Bewarder et al.…”

Ligand-based CAR-T cell: Different strategies to drive T cells in future new treatments