AI Article Synopsis
- Obinutuzumab (GA101) is a modified antibody that binds more effectively to CD16B, enhancing the immune response of neutrophils compared to traditional antibodies like rituximab.
- The glycoengineered form of obinutuzumab activates polymorphonuclear neutrophils (PMNs), increasing certain surface markers and promoting the release of inflammatory cytokines without generating harmful reactive oxygen species.
- This study concludes that the heightened phagocytosis of cancer cells by PMNs is a key mechanism by which obinutuzumab exerts its anti-cancer effects, linked to its stronger interaction with CD16B receptors.
Article Abstract
Obinutuzumab (GA101) is a glycoengineered type 2 CD20 antibody with enhanced CD16A-binding and natural killer-mediated cytotoxicity. CD16B is highly homologous to CD16A and a major FcγR on human polymorphonuclear neutrophils (PMNs). We show here that glycoengineered obinutuzumab or rituximab bound CD16B with approximately sevenfold higher affinity, compared with nonglycoengineered wild-type parental antibodies. Furthermore, glycoengineered obinutuzumab activated PMNs, either purified or in chronic lymphoblastic leukemia whole blood, more efficiently than wild-type rituximab. Activation resulted in a 50% increase in CD11b expression and 70% down-modulation of CD62L on neutrophils and in release of tumor necrosis factor alpha, IL-6, and IL-8. Activation was not accompanied by generation of reactive oxygen species or antibody-dependent cellular cytotoxicity activity, but led to up to 47% phagocytosis of glycoengineered anti-CD20 opsonized chronic lymphoblastic leukemia targets by purified PMNs. Significant phagocytosis was observed in whole blood, but only in the presence of glycoengineered antibodies, and was followed by up to 50% PMN death. Finally we show, using anti-CD16B and anti-CD32A Fab and F(ab')2 fragments, that both of these receptors are involved in PMN activation, phagocytosis, and cell death induced by glycoengineered antibodies. We conclude that phagocytosis by PMNs is an additional mechanism of action of obinutuzumab mediated through its higher binding affinity for CD16B.
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| http://dx.doi.org/10.1182/blood-2013-05-504043 | DOI Listing |
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