Abstract
Simple SummaryThe complement system can be exploited by anticancer antibody-based therapeutics. Activation of the classical complement pathway by the heavy chain of antibodies eventually leads to the lysis of target cells. However, overexpression of complement inhibitors by tumor cells limits the therapeutic efficacy. We designed and produced recombinant gain-of-function variants of complement C2 protein that counteract the activity of complement inhibitors. The dominant character of designed mutations in C2 allows supplementation of human serum with recombinant proteins for enhancing the cytocidal activity of complement-activating antibodies. In vitro functional assays demonstrate that this strategy is compatible with several clinically approved antibodies.The molecular target for the classical complement pathway (CP) is defined by surface-bound immunoglobulins. Therefore, numerous anticancer monoclonal antibodies (mAbs) exploit the CP as their effector mechanism. Conversely, the alternative complement pathway (AP) is spontaneously induced on the host and microbial surfaces, but complement inhibitors on host cells prevent its downstream processing. Gain-of-function (GoF) mutations in the AP components that oppose physiological regulation directly predispose carriers to autoimmune/inflammatory diseases. Based on the homology between AP and CP components, we modified the CP component C2 so that it emulates the known pathogenic mutations in the AP component, factor B. By using tumor cell lines and patient-derived leukemic cells along with a set of clinically approved immunotherapeutics, we showed that the supplementation of serum with recombinant GoF C2 variants not only enhances the cytocidal effect of type I anti-CD20 mAbs rituximab and ofatumumab, but also lowers the threshold of mAbs necessary for the efficient lysis of tumor cells and efficiently exploits the leftovers of the drug accumulated in patients’ sera after the previous infusion. Moreover, we demonstrate that GoF C2 acts in concert with other therapeutic mAbs, such as type II anti-CD20, anti-CD22, and anti-CD38 specimens, for overcoming cancer cells resistance to complement attack.
Highlights
IntroductionThe introduction of complement-activating anticancer monoclonal antibodies (mAbs) as a means of targeted therapy opened a new era in oncology and hematology
This article is an open access articleThe introduction of complement-activating anticancer monoclonal antibodies as a means of targeted therapy opened a new era in oncology and hematology
We verified the effect of single and multiple substitutions in C2 on the activity of complement pathway (CP) convertase formed on the surface of CD20-positive human lymphoma cells sensitized with ofatumumab
Summary
The introduction of complement-activating anticancer monoclonal antibodies (mAbs) as a means of targeted therapy opened a new era in oncology and hematology. Subsequent rounds of therapy, and limited efficacy in other B-cell malignancies imposed studies on new generations of anti-CD20 mAbs [2]. The second-generation anti-CD20 mAb ofatumumab presented superior in vitro complement-dependent cytotoxicity (CDC) [3]. Data from randomized clinical studies demonstrated no superior efficacy versus rituximab [4], suggesting a dispensable role of complement activation in the therapeutic effect of anti-CD20 mAbs. On the other hand, a post-infusion drop in complement activity of patients’ sera together with the observation that rituximab-nonresponsive patients achieved clinical response when the infusion was accompanied with fresh frozen plasma suggest complement exhaustion as an important factor limiting the efficacy of antiCD20 mAbs (reviewed in [5]). Rituximab and ofatumumab are classified as type I anti-CD20 mAbs, i.e., strong activators of CDC and weak direct inducers of cell death. The opposite characteristic is a hallmark of type II specimens represented by glycoengineered, third-generation anti-CD20 mAb obinutuzumab [8]
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