NK-cell activation and antibody-dependent cellular cytotoxicity induced by rituximab-coated target cells is inhibited by the C3b component of complement

Wang, Siao-Yi; Racila, Emilian; Taylor, Ronald P.; Weiner, George J.

doi:10.1182/blood-2007-02-074716

Cited by 166 publications

(148 citation statements)

References 43 publications

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“…Moreover, by a strategy of local fH inhibition, putative systemic side effects of an anti-fH strategy may also be reduced. We do not expect that the increased complement activation and thus enhanced C3b deposition will decrease the overall efficacy of ofatumumab by impairing natural killer cell-mediated ADCC 45 as recently published data indicate that monoclonal antibody-dependent amplification of C3 deposition on tumor cells enhanced both macrophagedependent, Fc-mediated ADCC and CDC in vitro and in vivo. 46 Thus, the lack of natural killer cell activation can be compensated for by increased phagocytosis and complement-mediated lysis.…”

Section: Discussionmentioning

confidence: 99%

Complement factor H-derived short consensus repeat 18-20 enhanced complement-dependent cytotoxicity of ofatumumab on chronic lymphocytic leukemia cells

et al. 2013

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The antitumor activity of monoclonal antibodies in the treatment of chronic lymphocytic leukemia is mediated mainly by antibody-dependent cellular cytotoxicity and complement-dependent cytotoxicity. Unfortunately, the efficacy of complement-dependent cytotoxicity is strongly restricted due to the expression and acquisition of regulators of complement activation by lymphocytic leukemia cells. Whereas the role of membrane regulators of complement activation, such as CD55 and CD59, has been investigated in detail in chronic lymphocytic leukemia, the involvement of soluble regulators of complement activation, such as complement factor H, has not yet been reported. Propidium iodide staining was performed to investigate the efficacy of ofatumumab and factor H-derived shortconsensus-repeat 18-20 in the induction of complement-dependent cytotoxicity on primary chronic lymphocytic leukemia cells from 20 patients. Deposition of complement C3 fragments was monitored by western blot analysis. Expression of CD20, CD55 or CD59 was determined by FACS analysis. Replacement of factor H with short consensus repeat 18-20 significantly increased the susceptibility of primary chronic lymphocytic leukemia cells to ofatumumab-induced complement-dependent cytotoxicity. More importantly, addition of short-consensus-repeat 18-20 was able to overcome complement-resistance occurring during treatment with ofatumumab alone. Use of short consensus repeat 18-20 is likely to prolong the turnover time of active C3b fragments generated on the target cells following ofatumumab-induced complement activation, thereby improving specific killing of chronic lymphocytic leukemia cells by complement-dependent cytotoxicity. The relative contribution of factor H to the protection of chronic lymphocytic leukemia cells against complement-dependent cytotoxicity was comparable to that of CD55. Our data suggest that, by abrogating factor H function, short consensus repeat 18-20 may provide a novel approach that improves the complement-dependent efficacy of therapeutic monoclonal antibodies.

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Section: Discussionmentioning

confidence: 99%

Complement factor H-derived short consensus repeat 18-20 enhanced complement-dependent cytotoxicity of ofatumumab on chronic lymphocytic leukemia cells

et al. 2013

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“…This finding is in contrast to human IgG1, the format of Ab used by almost all approved Ab drugs, which at least in vitro mediates target cell killing mainly by recruiting NK cells as effector cells or by complement fixation. For rituximab, first-infusion reactions were correlated with the activation of complement (38), whereas the therapeutic contribution of CDC to the antitumor activity of rituximab in patients remains to be investigated (39,40). Our Ab construct, which does not activate human complement, might be an attractive alternative for clinical applications.…”

Section: Discussionmentioning

confidence: 99%

A Recombinant Bispecific Single-Chain Fragment Variable Specific for HLA Class II and FcαRI (CD89) Recruits Polymorphonuclear Neutrophils for Efficient Lysis of Malignant B Lymphoid Cells

Guettinger

Barbin

Peipp³

et al. 2009

The Journal of Immunology

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Bispecific Abs offer new perspectives for cancer immunotherapy. In this study, we describe a recombinant bispecific single-chain fragment variable (bsscFv) directed against FcαRI (CD89) on polymorphonuclear neutrophils (PMNs) or monocytes/macrophages and HLA class II on lymphoma target cells. FcαRI and HLA class II-directed single-chain fragment variable (scFv) fragments were isolated from phage display libraries, established from the hybridomas A77 and F3.3, respectively. The two scFv molecules were connected with a 20 aa flexible linker sequence. After expression in SF21 insect cells and chromatographic purification, the bispecific molecule showed specific binding to both Ags at KD values of 148 ± 42 nM and 113 ± 25 nM for the anti-FcαRI and anti-HLA class II scFv components in the bsscFv, respectively. In Ab-dependent cytotoxicity assays with PMNs as effectors and a series of lymphoma-derived cell lines (ARH-77, RAJI, REH, NALM-6, RS4;11), the bsscFv was significantly more cytotoxic than the parental murine IgG1 and its chimeric IgG1 derivative. When targeting primary tumor cell isolates from six patients with B cell malignancies, the killing capacity of the (FcαRI × HLA class II) bsscFv compared favorably to conventional HLA class II mAb. Importantly, the cell lines NALM-6 and RS411, as well as two primary tumor cell isolates, were exclusively lysed by the bsscFv. To our knowledge, this is the first report of an FcαRI-directed bsscFv effectively recruiting PMNs for redirected cytotoxicity against human B cell malignancies. Our data show that an (FcαRI × HLA class II) bsscFv is an interesting candidate for further engineering of small, modular immunopharmaceuticals.

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“…Further functional assays confirmed that complement fixation upstream of C5 is responsible for the impaired ADCC activity mediated by NK cells in the presence of serum. 72 In addition, NK-mediated ADCC capacity of the glycoengineered mAb obinutuzumab (GA101), having a decreased ability to fix complement compared with rituximab, was not affected in the presence of complement. 73 To confirm those findings in vivo, a murine anti-idiotype mAb directed against murine 38C13 B cell lymphomas was used to show that serum blocks murine NK cell activation.…”

Section: The Role Of Complement In Ab Immunotherapymentioning

confidence: 99%

Regulation of complement and modulation of its activity in monoclonal antibody therapy of cancer

Meyer

Leusen

Boross

2014

mAbs

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NK-cell activation and antibody-dependent cellular cytotoxicity induced by rituximab-coated target cells is inhibited by the C3b component of complement

Cited by 166 publications

References 43 publications

Complement factor H-derived short consensus repeat 18-20 enhanced complement-dependent cytotoxicity of ofatumumab on chronic lymphocytic leukemia cells

Complement factor H-derived short consensus repeat 18-20 enhanced complement-dependent cytotoxicity of ofatumumab on chronic lymphocytic leukemia cells

A Recombinant Bispecific Single-Chain Fragment Variable Specific for HLA Class II and FcαRI (CD89) Recruits Polymorphonuclear Neutrophils for Efficient Lysis of Malignant B Lymphoid Cells

Regulation of complement and modulation of its activity in monoclonal antibody therapy of cancer

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