Rituximab Infusion Promotes Rapid Complement Depletion and Acute CD20 Loss in Chronic Lymphocytic Leukemia

Kennedy, Adam D.; Beum, Paul V.; Solga, Michael D.; DiLillo, David J.; Lindorfer, Margaret A.; Hess, Charles E.; Densmore, John; Williams, Michael E.; Taylor, Ronald P.

doi:10.4049/jimmunol.172.5.3280

Cited by 317 publications

(361 citation statements)

References 48 publications

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“…The role of complement-dependent cytotoxicity (CDC) is suggested by the consumption of complement observed after rituximab administration but in vitro CDC does not correlate with clinical response in lymphomas (Winkler et al, 1999;Weng and Levy, 2001). However, CDC seems to be the most important mechanism of cell lysis in chronic lymphocytic leukemia (CLL) patients (Kennedy et al, 2004). CDC is probably involved in the cytokine-release syndrome and its toxicity (Bienvenu et al, 2001).…”

Section: Mechanisms Of Action Of Rituximabmentioning

confidence: 99%

Rituximab therapy in malignant lymphoma

2007

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Section: Mechanisms Of Action Of Rituximabmentioning

confidence: 99%

Rituximab therapy in malignant lymphoma

2007

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“…This poor efficacy has been explained by low CD20 expression levels of CLL cells, 9,10 the presence of complement inactivating molecules (CD55, CD59) on CLL cells, 11 the presence of soluble CD20 (ref. 12), shaving and downmodulation of CD20 after rituximab treatment, 13,14 resistance to antibody dependent cellular cytotoxicity by natural killer cells in vitro 15 andFlast but not leastF the intrinsic anti-apoptotic profile of CLL cells. 16 In this study, we show that, in sharp contrast to the induction of resistance to cytotoxic drugs, CD40 stimulation of CLL cells considerably increases sensitivity to anti-CD20-mediated cell death.…”

Section: Introductionmentioning

confidence: 99%

CD40 stimulation sensitizes CLL cells to rituximab-induced cell death

et al. 2011

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In vitro CD40-stimulated chronic lymphocytic leukemia (CLL) cells are resistant to cytotoxic drugs. In sharp contrast, we here show that CD40 stimulation sensitizes CLL cells to rituximabmediated cell death. This increased sensitivity is specific for anti-CD20 treatment. Rituximab-mediated death in CD40-stimulated CLL cells shows rapid kinetics (within hours), and is caspase and p53 independent, but depends on extracellular Ca 2 þ and reactive oxygen species (ROS) production. By increasing basal ROS production, CD40 stimulation sensitizes CLL cells to rituximab-mediated death. Our findings provide a rationale for combination treatment of CLL with cytotoxic drugs and anti-CD20 monoclonal antibodies.

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“…Extensive preclinical evidence showed that it is neither internalized nor shed when bound to B cells (9,27,33). We recently reported that during the standard infusion of RTX in patients with chronic lymphocytic leukemia (CLL), a large fraction of B cells was rapidly cleared from the circulation after only 30 mg of RTX was infused (34). However, immediately after the total dose of ϳ700 mg of RTX had been infused, when the concentration of RTX in the bloodstream was quite high (Ͼ100 g/ml), substantial B cell recrudescence was evident.…”

Section: T Argeting Of Ags On Cancer Cells By Mabs Has Been a Key Strmentioning

confidence: 99%

The Shaving Reaction: Rituximab/CD20 Complexes Are Removed from Mantle Cell Lymphoma and Chronic Lymphocytic Leukemia Cells by THP-1 Monocytes

Beum

Kennedy

Williams

et al. 2006

The Journal of Immunology

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Clinical investigations have revealed that infusion of immunotherapeutic mAbs directed to normal or tumor cells can lead to loss of targeted epitopes, a phenomenon called antigenic modulation. Recently, we reported that rituximab treatment of chronic lymphocytic leukemia patients induced substantial loss of CD20 on B cells found in the circulation after rituximab infusion, when rituximab plasma concentrations were high. Such antigenic modulation can severely compromise therapeutic efficacy, and we postulated that B cells had been stripped (shaved) of the rituximab/CD20 complex by monocytes or macrophages in a reaction mediated by FcγR. We developed an in vitro model to replicate this in vivo shaving process, based on reacting rituximab-opsonized CD20+ cells with acceptor THP-1 monocytes. After 45 min at 37°C, rituximab and CD20 are removed from opsonized cells, and both are demonstrable on acceptor THP-1 cells. The reaction occurs equally well in the presence and absence of normal human serum, and monocytes isolated from peripheral blood also promote shaving of CD20 from rituximab-opsonized cells. Tests with inhibitors and use of F(ab′)2 of rituximab indicate transfer of rituximab/CD20 complexes to THP-1 cells is mediated by FcγR. Antigenic modulation described in previous reports may have been mediated by such shaving, and our findings may have profound implications for the use of mAbs in the immunotherapy of cancer.

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Rituximab Infusion Promotes Rapid Complement Depletion and Acute CD20 Loss in Chronic Lymphocytic Leukemia

Cited by 317 publications

References 48 publications

Rituximab therapy in malignant lymphoma

Rituximab therapy in malignant lymphoma

CD40 stimulation sensitizes CLL cells to rituximab-induced cell death

The Shaving Reaction: Rituximab/CD20 Complexes Are Removed from Mantle Cell Lymphoma and Chronic Lymphocytic Leukemia Cells by THP-1 Monocytes

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