2013
DOI: 10.1016/j.ctrv.2012.10.008
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Effector mechanisms of anti-CD20 monoclonal antibodies in B cell malignancies

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Cited by 66 publications
(46 citation statements)
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“…Using sandwich ELISAs, we analysed plasma collected from 31 patients with various B cell malignancies treated with the CD20 mAbs rituximab or ofatumumab. Upon binding to target cell, anti-CD20 mAbs are expected to activate the classical complement pathway but it is not clear, which effector arm of the complement system contribute to the therapeutic effect (Okroj et al, 2013b). Also, it is not always the case that complement attack on tumor cells will proceed to the lytic stage, as malignant B cells may shed CD20-mAb complexes (Taylor and Lindorfer, 2014) and widely express the complement inhibitors CD46 and CD55 preventing C5 cleavage (Okroj et al, 2013a).…”
Section: Measurement Of Soluble Markers Of Complement Activation In Pmentioning
confidence: 99%
“…Using sandwich ELISAs, we analysed plasma collected from 31 patients with various B cell malignancies treated with the CD20 mAbs rituximab or ofatumumab. Upon binding to target cell, anti-CD20 mAbs are expected to activate the classical complement pathway but it is not clear, which effector arm of the complement system contribute to the therapeutic effect (Okroj et al, 2013b). Also, it is not always the case that complement attack on tumor cells will proceed to the lytic stage, as malignant B cells may shed CD20-mAb complexes (Taylor and Lindorfer, 2014) and widely express the complement inhibitors CD46 and CD55 preventing C5 cleavage (Okroj et al, 2013a).…”
Section: Measurement Of Soluble Markers Of Complement Activation In Pmentioning
confidence: 99%
“…Such protection may be overrun by tumor-targeted monoclonal antibodies (mAbs), which enhance the efficacy of complement-dependent cytotoxicity (CDC, attributable to lysis of target cells due to membrane attack complex formation) and lead to establishment of successful therapies. Therapeutic mAbs may exert at least two more modes of target cell killing: antibody-dependent cellular cytotoxicity (ADCC) or direct effects such as apoptotic cell death upon antibody binding [5]. Moreover, phagocytes engulf cells opsonized by antibodies and/or complement more readily.…”
Section: Introductionmentioning
confidence: 99%
“…IPH4102 was effective in autologous killing assays in which it induces NK cell-based lysis of autologous S ezary cells, demonstrating both the functional integrity of patients' NK cells, and the sensitivity of primary tumors to ADCC through KIR3DL2 targeting. ADCC is known to contribute to the clinical efficacy of many approved therapeutic mAbs, including anti-HER2 trastuzumab (46), anti-CD20 rituximab and obinutuzumab (44,(47)(48)(49)(50), anti-CCR4 mogamulizumab (45), or anti-EGFR cetuximab (51). Moreover, IPH4102 was found to reproducibly promote S ezary tumor cells lysis when directly incubated with patients' unsorted PBMC, hence at much less favorable effector to target ratios, unequivocally confirming the potency of this therapeutic candidate.…”
Section: Discussionmentioning
confidence: 99%