Your search keyword '"Ronald P. Taylor"' showing total 243 results

1. FcγR-Mediated Trogocytosis 2.0: Revisiting History Gives Rise to a Unifying Hypothesis

Author

Margaret A. Lindorfer and Ronald P. Taylor

Subjects

trogocytosis, Fcγ receptors, liver sinusoidal endothelial cells, immune adherence, Immunologic diseases. Allergy, RC581-607

Abstract

There is increasing interest in the clinical implications and immunology of trogocytosis, a process in which the receptors on acceptor cells remove and internalize cognate ligands from donor cells. We have reported that this phenomenon occurs in cancer immunotherapy, in which cells that express FcγR remove and internalize CD20 and bound mAbs from malignant B cells. This process can be generalized to include other reactions including the immune adherence phenomenon and antibody-induced immunosuppression. We discuss in detail FcγR-mediated trogocytosis and the evidence supporting a proposed predominant role for liver sinusoidal endothelial cells via the action of the inhibitory receptor FcγRIIb2. We describe experiments to test the validity of this hypothesis. The elucidation of the details of FcγR-mediated trogocytosis has the potential to allow for the development of novel therapies that can potentially block or enhance this reaction, depending upon whether the process leads to unfavorable or positive biological effects.

Published

2022

2. Clearance of amyloid‐beta with bispecific antibody constructs bound to erythrocytes

Author

Ronald P. Taylor, Margaret A. Lindorfer, and John P. Atkinson

Subjects

Alzheimer's disease, amyloid beta, bispecific monoclonal antibodies, complement receptor 1, erythrocyte, human, Neurology. Diseases of the nervous system, RC346-429, Geriatrics, RC952-954.6

Abstract

Abstract We propose use of bispecific monoclonal antibody (mAb) complexes bound to erythrocytes to redress the lack of efficacy of anti‐amyloid beta mAbs in Alzheimer's disease treatment. Our paradigm leverages erythrocyte complement receptor 1 to promote rapid and quantitative removal of amyloid beta from the circulation, and its subsequent removal from the brain as well.

Published

2020

3. Special Issue: The Role of Complement in Cancer Immunotherapy

Author

Ronald P. Taylor

Subjects

n/a, Immunologic diseases. Allergy, RC581-607

Abstract

The complement system plays an important role in critical aspects of immune defense and in the maintenance of homeostasis in the bloodstream, as well as in essentially all tissues and organs [...]

Published

2021

4. CD20 and CD37 antibodies synergize to activate complement by Fc-mediated clustering

Author

Simone C. Oostindie, Hilma J. van der Horst, Margaret A. Lindorfer, Erika M. Cook, Jillian C. Tupitza, Clive S. Zent, Richard Burack, Karl R. VanDerMeid, Kristin Strumane, Martine E. D. Chamuleau, Tuna Mutis, Rob N. de Jong, Janine Schuurman, Esther C. W. Breij, Frank J. Beurskens, Paul W. H. I. Parren, and Ronald P. Taylor

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

CD20 monoclonal antibody therapies have significantly improved the outlook for patients with B-cell malignancies. However, many patients acquire resistance, demonstrating the need for new and improved drugs. We previously demonstrated that the natural process of antibody hexamer formation on targeted cells allows for optimal induction of complement-dependent cytotoxicity. Complement-dependent cytotoxicity can be potentiated by introducing a single point mutation such as E430G in the IgG Fc domain that enhances intermolecular Fc-Fc interactions between cell-bound IgG molecules, thereby facilitating IgG hexamer formation. Antibodies specific for CD37, a target that is abundantly expressed on healthy and malignant B cells, are generally poor inducers of complement-dependent cytotoxicity. Here we demonstrate that introduction of the hexamerization-enhancing mutation E430G in CD37-specific antibodies facilitates highly potent complement-dependent cytotoxicity in chronic lymphocytic leukemia cells ex vivo. Strikingly, we observed that combinations of hexamerization-enhanced CD20 and CD37 antibodies cooperated in C1q binding and induced superior and synergistic complement-dependent cytotoxicity in patient-derived cancer cells compared to the single agents. Furthermore, CD20 and CD37 antibodies colocalized on the cell membrane, an effect that was potentiated by the hexamerization-enhancing mutation. Moreover, upon cell surface binding, CD20 and CD37 antibodies were shown to form mixed hexameric antibody complexes consisting of both antibodies each bound to their own cognate target, so-called hetero-hexamers. These findings provide novel insights into the mechanisms of synergy in antibody-mediated complement-dependent cytotoxicity and provide a rationale to explore Fc-engineering and antibody hetero-hexamerization as a tool to enhance the cooperativity and therapeutic efficacy of antibody combinations.

Published

2019

5. The Role of Complement in the Mechanism of Action of Therapeutic Anti-Cancer mAbs

Author

Josée Golay and Ronald P. Taylor

Subjects

therapeutic monoclonal antibodies (mAbs), complement, antibody dependent cellular cytotoxicity, phagocytosis, complement receptors, Immunologic diseases. Allergy, RC581-607

Abstract

Unconjugated anti-cancer IgG1 monoclonal antibodies (mAbs) activate antibody-dependent cellular cytotoxicity (ADCC) by natural killer (NK) cells and antibody-dependent cellular phagocytosis (ADCP) by macrophages, and these activities are thought to be important mechanisms of action for many of these mAbs in vivo. Several mAbs also activate the classical complement pathway and promote complement-dependent cytotoxicity (CDC), although with very different levels of efficacy, depending on the mAb, the target antigen, and the tumor type. Recent studies have unraveled the various structural factors that define why some IgG1 mAbs are strong mediators of CDC, whereas others are not. The role of complement activation and membrane inhibitors expressed by tumor cells, most notably CD55 and CD59, has also been quite extensively studied, but how much these affect the resistance of tumors in vivo to IgG1 therapeutic mAbs still remains incompletely understood. Recent studies have demonstrated that complement activation has multiple effects beyond target cell lysis, affecting both innate and adaptive immunity mediated by soluble complement fragments, such as C3a and C5a, and by stimulating complement receptors expressed by immune cells, including NK cells, neutrophils, macrophages, T cells, and dendritic cells. Complement activation can enhance ADCC and ADCP and may contribute to the vaccine effect of mAbs. These different aspects of complement are also briefly reviewed in the specific context of FDA-approved therapeutic anti-cancer IgG1 mAbs.

Published

2020

6. How Do mAbs Make Use of Complement to Kill Cancer Cells? The Role of Ca2+

Author

Ronald P. Taylor and Margaret A. Lindorfer

Subjects

complement, therapeutic monoclonal antibodies (mAbs), Ca2+, fluorescence microscopy, Immunologic diseases. Allergy, RC581-607

Abstract

We examined the kinetics and mechanisms by which monoclonal antibodies (mAbs) utilize complement to rapidly kill targeted cancer cells. Based on results from flow cytometry, confocal microscopy and high-resolution digital imaging experiments, the general patterns which have emerged reveal cytotoxic activities mediated by substantial and lethal Ca2+ fluxes. The Ca2+ fluxes are common to the reported pathways that have been utilized by other toxins in killing nucleated cells. These reactions terminate in very high levels of cell killing, and based on these considerations, we suggest additional strategies to further enhance mAb-based targeting of cancer with complement.

Published

2020

7. Endothelial Microparticles and Systemic Complement Activation in Patients With Chronic Kidney Disease

Author

Diana Jalal, Brandon Renner, Jennifer Laskowski, Erik Stites, James Cooper, Karissa Valente, Zhiying You, Loni Perrenoud, Moglie Le Quintrec, Ismaeel Muhamed, Uwe Christians, Jelena Klawitter, Margaret A. Lindorfer, Ronald P. Taylor, V. Michael Holers, and Joshua M. Thurman

Subjects

chronic kidney disease, Microparticles complement activation, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Background Endothelial microparticles are associated with chronic kidney disease (CKD) and complement activation. We hypothesized that the complement pathway is activated in patients with CKD via endothelial microparticles and that complement activation correlates with endothelial dysfunction in CKD. Methods and Results We analyzed complement data of 30 healthy subjects, 30 patients with stage III/IV CKD, and 30 renal transplant recipients with stage III/IV CKD, evaluating the potential correlation of complement fragments with brachial artery flow–mediated dilation, Chronic Kidney Disease Epidemiology Collaboration glomerular filtration rate, and urinary albumin/creatinine ratio. Endothelial microparticles were characterized via proteomic analysis and compared between study groups. Complement fragment Ba was significantly increased in CKD and post–kidney transplant CKD. Plasma Ba levels correlated significantly with lower brachial artery flow–mediated dilation, lower Chronic Kidney Disease Epidemiology Collaboration glomerular filtration rate, and higher urinary albumin/creatinine ratio. Factor D levels were significantly higher in the plasma microparticles of patients with CKD versus healthy controls. Plasma microparticles isolated from patients with CKD and containing factor D activated the alternative pathway in vitro. Conclusion The alternative complement pathway is activated in CKD and correlates with endothelial dysfunction and markers of CKD. Future studies are needed to evaluate whether endothelial microparticles with increased factor D play a pathologic role in CKD‐associated vascular disease. Clinical Trial Registration URL: http://www.clinicaltrials.gov. Unique identifier: NCT02230202.

Published

2018

8. CD20 mAb-Mediated Complement Dependent Cytotoxicity of Tumor Cells is Enhanced by Blocking the Action of Factor I

Author

Margaret A. Lindorfer, Paul V. Beum, and Ronald P. Taylor

Subjects

monoclonal antibody, complement, Factor I, rituximab, ofatumumab, Immunologic diseases. Allergy, RC581-607

Abstract

The CD20 mAbs, rituximab (RTX) and ofatumumab (OFA), have been used with success in the clinic in the treatment of B cell malignancies. These mAbs can eliminate B cells only by utilizing the body’s immune effector mechanisms, and there is considerable evidence that OFA is particularly effective at eliminating B cells by mediating complement dependent cytotoxicity (CDC). However, effector mechanisms such as complement can be exhausted or down-regulated. Therefore, several approaches are being investigated with the goal of increasing CDC mediated by these mAbs. We reported that when patients with chronic lymphocytic leukemia (CLL) are treated with RTX or with OFA, complement is rapidly activated on circulating, targeted CLL B cells. However, a substantial fraction of these cells escape CDC and clearance due to degradation of covalently deposited active C3b fragments to inactive fragments iC3b and C3d. This process is mediated by a plasma protease, Factor I. Therefore, a rational approach for increasing CDC would be to block this reaction by inhibiting Factor I with a neutralizing mAb. Indeed, we have demonstrated that use of neutralizing mAb A247, specific for factor I, significantly and substantially increases CD20 mAb-mediated CDC of both cell lines and of primary CLL cells in vitro.

Published

2013

9. Ibrutinib interferes with the cell-mediated anti-tumor activities of therapeutic CD20 antibodies: implications for combination therapy

Author

Fabio Da Roit, Patrick J. Engelberts, Ronald P. Taylor, Esther C.W. Breij, Giuseppe Gritti, Alessandro Rambaldi, Martino Introna, Paul W.H.I. Parren, Frank J. Beurskens, and Josée Golay

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

The novel Bruton tyrosine kinase inhibitor ibrutinib and phosphatidyl-4-5-biphosphate 3-kinase-δ inhibitor idelalisib are promising drugs for the treatment of chronic lymphocytic leukemia and B-cell non-Hodgkin lymphoma, either alone or in combination with anti-CD20 antibodies. We investigated the possible positive or negative impact of these drugs on all known mechanisms of action of both type I and type II anti-CD20 antibodies. Pretreatment with ibrutinib for 1 hour did not increase direct cell death of cell lines or chronic lymphocytic leukemia samples mediated by anti-CD20 antibodies. Pre-treatment with ibrutinib did not inhibit complement activation or complement-mediated lysis. In contrast, ibrutinib strongly inhibited all cell-mediated mechanisms induced by anti-CD20 antibodies rituximab, ofatumumab or obinutuzumab, either in purified systems or whole blood assays. Activation of natural killer cells, and antibody-dependent cellular cytotoxicity by these cells, as well as phagocytosis by macrophages or neutrophils were inhibited by ibrutinib with a half maximal effective concentration of 0.3–3 μM. Analysis of anti-CD20 mediated activation of natural killer cells isolated from patients on continued oral ibrutinib treatment suggested that repeated drug dosing inhibits these cells in vivo. Finally we show that the phosphatidyl-4-5-biphosphate 3-kinase-δ inhibitor idelalisib similarly inhibited the immune cell-mediated mechanisms induced by anti-CD20 antibodies, although the effects of this drug at 10 μM were weaker than those observed with ibrutinib at the same concentration. We conclude that the design of combined treatment schedules of anti-CD20 antibodies with these kinase inhibitors should consider the multiple negative interactions between these two classes of drugs.

Published

2015

10. Rapid clearance of rituximab may contribute to the continued high incidence of autoimmune hematologic complications of chemoimmunotherapy for chronic lymphocytic leukemia

Author

Clifton C. Mo, Ndegwa Njuguna, Paul V. Beum, Margaret A. Lindorfer, Berengere Vire, Elinor Lee, Gerald Marti, Wyndham H Wilson, Ronald P. Taylor, and Adrian Wiestner

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Rituximab is an effective treatment for autoimmune cytopenias associated with chronic lymphocytic leukemia. Despite the incorporation of rituximab into fludarabine-based chemotherapy regimens, the incidence of autoimmune cytopenias has remained high. Inadequate rituximab exposure due to rapid antibody clearance may be a contributing factor. To test this hypothesis, we measured serum rituximab levels in patients treated with fludarabine and rituximab (375 mg/m2). All patients had undetectable rituximab trough levels by the end of cycle 1, and one-third had undetectable levels already on Day 6 of cycle 1. Although rituximab trough levels increased progressively with each cycle, only by cycle 4 did the median trough level exceed 10 ug/mL. The median half-life of rituximab during cycle 1 was 27 hours, compared to 199 hours during cycle 4 (P

Published

2013

11. Fractionated subcutaneous rituximab is well-tolerated and preserves CD20 expression on tumor cells in patients with chronic lymphocytic leukemia

Author

Georg Aue, Margaret A. Lindorfer, Paul V. Beum, Andrew W. Pawluczkowycz, Berengere Vire, Thomas Hughes, Ronald P. Taylor, and Adrian Wiestner

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

A pilot study previously demonstrated that thrice-weekly, fractionated-dose intravenous rituximab (RTX) limits CD20 loss from chronic lymphocytic leukemia (CLL) B cells, thereby enhancing immunotherapeutic targeting. Here, we investigated the feasibility of giving 20 mg rituximab subcutaneously thrice weekly for up to 12 weeks in 4 previously treated CLL patients. Subcutaneous rituximab was well-tolerated with minimal injection site reactions; a variable degree of efficacy was observed, likely influenced by the size of the patients’ B cell/CD20 burden. Subcutaneous RTX largely preserved CD20 expression on leukemic cells but the most effective therapeutic dosing regimen needs to be established (ClinicalTrials.gov Identifier: NCT00366418).

Published

2010

12. Phagocytosis via complement receptor 3 enables microbes to evade killing by neutrophils

Author

Asya Smirnov, Kylene P. Daily, Mary C. Gray, Stephanie A. Ragland, Lacie M. Werner, M. Brittany Johnson, Joshua C. Eby, Erik L. Hewlett, Ronald P. Taylor, and Alison K. Criss

Subjects

Immunology, Immunology and Allergy, Cell Biology

Abstract

CR3 (CD11b/CD18; αmβ2 integrin) is a conserved phagocytic receptor. The active conformation of CR3 binds the iC3b fragment of complement C3 as well as many host and microbial ligands, leading to actin-dependent phagocytosis. There are conflicting reports about how CR3 engagement affects the fate of phagocytosed substrates. Using imaging flow cytometry, we confirmed that binding and internalization of iC3b-opsonized polystyrene beads by primary human neutrophils was CR3-dependent. iC3b-opsonized beads did not stimulate neutrophil reactive oxygen species, and most beads were found in primary granule-negative phagosomes. Similarly, Neisseria gonorrhoeae that does not express phase-variable Opa proteins suppresses neutrophil reactive oxygen species and delays phagolysosome formation. Here, binding and internalization of Opa-deleted (Δopa) N. gonorrhoeae by adherent human neutrophils was inhibited using blocking antibodies against CR3 and by adding neutrophil inhibitory factor, which targets the CD11b I-domain. No detectable C3 was deposited on N. gonorrhoeae in the presence of neutrophils alone. Conversely, overexpressing CD11b in HL-60 promyelocytes enhanced Δopa N. gonorrhoeae phagocytosis, which required the CD11b I-domain. Phagocytosis of N. gonorrhoeae was also inhibited in mouse neutrophils that were CD11b-deficient or treated with anti-CD11b. Phorbol ester treatment upregulated surface CR3 on neutrophils in suspension, enabling CR3-dependent phagocytosis of Δopa N. gonorrhoeae. Neutrophils exposed to Δopa N. gonorrhoeae had limited phosphorylation of Erk1/2, p38, and JNK. Neutrophil phagocytosis of unopsonized Mycobacterium smegmatis, which also resides in immature phagosomes, was CR3-dependent and did not elicit reactive oxygen species. We suggest that CR3-mediated phagocytosis is a silent mode of entry into neutrophils, which is appropriated by diverse pathogens to subvert phagocytic killing.

Published

2023

13. Rituximab induced cytokine release with high serum IP-10 (CXCL10) concentrations is associated with infusion reactions

Author

Jeremiah E. Moore, Paige C. Bloom, Charles C. Chu, Jennifer E. Bruno, Christine A. Herne, Andrea M. Baran, Sally A. Quataert, Timothy R. Mosmann, Ronald P. Taylor, Danielle S. Wallace, Michael R. Elliott, Paul M. Barr, and Clive S. Zent

Subjects

Cancer Research, Oncology, Hematology

Published

2023

14. Decision letter: Soluble MAC is primarily released from MAC-resistant bacteria that potently convert complement component C5

Author

Ronald P Taylor

Published

2022

15. Mutation of complement factor B causing massive fluid-phase dysregulation of the alternative complement pathway can result in atypical hemolytic uremic syndrome

Author

Kammi J. Henriksen, Mari Mori, Carla M. Nester, C. John Sperati, Ronald P. Taylor, Gabriella R. Pitcher, Yuzhou Zhang, Cindy Benson, Nicolò Borsa, Robin Kremsdorf, Renee X. Goodfellow, and Richard J.H. Smith

Subjects

Adult, 0301 basic medicine, Complement Pathway, Alternative, 030232 urology & nephrology, Complement factor B, Article, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Atypical hemolytic uremic syndrome, Humans, Medicine, Complement Activation, Atypical Hemolytic Uremic Syndrome, Cesarean Section, business.industry, Microangiopathic hemolytic anemia, Middle Aged, medicine.disease, C3-convertase, Schistocyte, 030104 developmental biology, Nephrology, Child, Preschool, Complement Factor H, Mutation, Immunology, Alternative complement pathway, Properdin, Female, business, Complement Factor B

Abstract

Atypical hemolytic uremic syndrome is an ultra-rare disease characterized by microangiopathic hemolytic anemia, thrombocytopenia and acute kidney injury. Its pathogenesis is driven most frequently by dysregulated cell-surface control of the alternative pathway of complement secondary to inherited and/or acquired factors. Here we evaluated two unrelated patients with atypical hemolytic uremic syndrome. The first, a five-year-old Caucasian female, presented at 10 months with schistocytes, thrombocytopenia and kidney injury. The second, a 55-year-old Caucasian female, presented at age 31 following caesarean section for preeclampsia. Complement biomarker testing was remarkable for undetectable levels of C3 in both. Circulating levels of C5 and properdin were also low consistent with over-activity of the alternative and terminal pathways of complement. Genetic testing identified a heterozygous novel variant in CFB (c.1101 C>A, p.Ser367Arg) in both patients. Functional studies found strong fluid-phase C3 cleavage when normal and proband sera were mixed. Cell-surface C3b deposition was strongly positive when patient serum was supplemented with C3. In vitro control of C3 convertase activity could be restored with increased concentrations of factor H. Thus, CFB p.Ser367Arg is a gain-of-function pathogenic variant that leads to dysregulation of the alternative pathway in the fluid-phase and increased C3b deposition on cell surfaces. Our study highlights the complexities of complement-mediated diseases like atypical hemolytic uremic syndrome and illustrates the importance of functional studies at the variant level to gain insight into the disease phenotype.

Published

2020

16. Risk-adapted, ofatumumab-based chemoimmunotherapy and consolidation in treatment-naïve chronic lymphocytic leukemia: a phase 2 study

Author

Thomas E. Hughes, Gerald E. Marti, Clare Sun, Ronald P. Taylor, Susan Soto, Adrian Wiestner, Inhye E. Ahn, Irina Maric, Jennifer Lotter, Erika M Gaglione, Constance M. Yuan, Clifton C. Mo, Maryalice Stetler-Stevenson, Laura M Wake, Cydney M. Nichols, Janet Valdez, Christopher Pleyer, Xin Tian, Jeanine Superata, Margaret A. Lindorfer, Mohammed Farooqui, Sarah E. M. Herman, Dennis C Drinkwater, Pia Nierman, and Sanjal Desai

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Trogocytosis, Chronic lymphocytic leukemia, Phases of clinical research, Ofatumumab, Antibodies, Monoclonal, Humanized, Article, Therapy naive, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Chemoimmunotherapy, hemic and lymphatic diseases, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, business.industry, Cytogenetics, Hematology, medicine.disease, Minimal residual disease, Leukemia, Lymphocytic, Chronic, B-Cell, Treatment Outcome, chemistry, 030220 oncology & carcinogenesis, Immunotherapy, business, 030215 immunology

Abstract

High-risk cytogenetics and minimal residual disease (MRD) after chemoimmunotherapy (CIT) predict unfavorable outcome in chronic lymphocytic leukemia (CLL). This phase 2 study investigated risk-adapted CIT in treatment-naïve CLL (NCT01145209). Patients with high-risk cytogenetics received induction with fludarabine, cyclophosphamide, and ofatumumab. Those without high-risk cytogenetics received fludarabine and ofatumumab. After induction, MRD positive (MRD+) patients received 4 doses of ofatumumab consolidation. MRD negative (MRD−) patients had no intervention. Of 28 evaluable for response, all responded to induction and 10 (36%) achieved MRD−. Two-year progression-free survival (PFS) was 71.4% (CI(95), 56.5–90.3%). There was no significant difference in median PFS between high-risk and standard-risk group. Ofatumumab consolidation didn’t convert MRD+ to MRD−. In MRD+ group, we saw selective loss of CD20 antigens during therapy. In conclusion, risk-adapted CIT is feasible in treatment-naïve CLL. Ofatumumab consolidation didn’t improve depth of response in MRD+ patients. Loss of targetable CD20 likely reduces efficacy of consolidation therapy.

Published

2021

17. The Role of Complement in the Mechanism of Action of Therapeutic Anti-Cancer mAbs

Author

Ronald P. Taylor and Josée Golay

Subjects

Antibody-dependent cell-mediated cytotoxicity, lcsh:Immunologic diseases. Allergy, Chemistry, therapeutic monoclonal antibodies (mAbs), antibody dependent cellular cytotoxicity, Immunology, phagocytosis, Complement receptor, CD59, Review, Acquired immune system, Cell biology, Complement system, Classical complement pathway, Immune system, complement receptors, Drug Discovery, Immunology and Allergy, complement, Cytotoxicity, lcsh:RC581-607

Abstract

Unconjugated anti-cancer IgG1 monoclonal antibodies (mAbs) activate antibody-dependent cellular cytotoxicity (ADCC) by natural killer (NK) cells and antibody-dependent cellular phagocytosis (ADCP) by macrophages, and these activities are thought to be important mechanisms of action for many of these mAbs in vivo. Several mAbs also activate the classical complement pathway and promote complement-dependent cytotoxicity (CDC), although with very different levels of efficacy, depending on the mAb, the target antigen, and the tumor type. Recent studies have unraveled the various structural factors that define why some IgG1 mAbs are strong mediators of CDC, whereas others are not. The role of complement activation and membrane inhibitors expressed by tumor cells, most notably CD55 and CD59, has also been quite extensively studied, but how much these affect the resistance of tumors in vivo to IgG1 therapeutic mAbs still remains incompletely understood. Recent studies have demonstrated that complement activation has multiple effects beyond target cell lysis, affecting both innate and adaptive immunity mediated by soluble complement fragments, such as C3a and C5a, and by stimulating complement receptors expressed by immune cells, including NK cells, neutrophils, macrophages, T cells, and dendritic cells. Complement activation can enhance ADCC and ADCP and may contribute to the vaccine effect of mAbs. These different aspects of complement are also briefly reviewed in the specific context of FDA-approved therapeutic anti-cancer IgG1 mAbs.

Published

2020

18. DuoHexaBody-CD37(R), a novel biparatopic CD37 antibody with enhanced Fc-mediated hexamerization as a potential therapy for B-cell malignancies

Author

Janine Schuurman, Martine E.D. Chamuleau, Paul W. H. I. Parren, Jeroen van den Brakel, Ronald P. Taylor, Marije B. Overdijk, Hilma J. van der Horst, Simone C. Oostindie, Hendrik J. Rademaker, Frank J. Beurskens, Juliette van den Noort, Berris van Kessel, Esther C.W. Breij, Margaret A. Lindorfer, Kristin Strumane, Laurens P. Kil, Tuna Mutis, Edward Van Den Brink, Hematology, CCA - Cancer biology and immunology, Hematology laboratory, and AII - Cancer immunology

Subjects

biology, Chemistry, Chronic lymphocytic leukemia, Hematology, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, Epitope, medicine.anatomical_structure, Oncology, Antigen, Monoclonal, Cancer cell, medicine, biology.protein, Cancer research, Antibody, Cytotoxicity, B cell

Abstract

Tetraspanin CD37 has recently received renewed interest as a therapeutic target for B-cell malignancies. Although complement-dependent cytotoxicity (CDC) is a powerful Fc-mediated effector function for killing hematological cancer cells, CD37-specific antibodies are generally poor inducers of CDC. To enhance CDC, the E430G mutation was introduced into humanized CD37 monoclonal IgG1 antibodies to drive more efficient IgG hexamer formation through intermolecular Fc-Fc interactions after cell surface antigen binding. DuoHexaBody-CD37, a bispecific CD37 antibody with the E430G hexamerization-enhancing mutation targeting two non-overlapping epitopes on CD37 (biparatopic), demonstrated potent and superior CDC activity compared to other CD37 antibody variants evaluated, in particular ex vivo in patient-derived chronic lymphocytic leukemia cells. The superior CDC potency was attributed to enhanced IgG hexamerization mediated by the E430G mutation in combination with dual epitope targeting. The mechanism of action of DuoHexaBody-CD37 was shown to be multifaceted, as it was additionally capable of inducing efficient antibody-dependent cellular cytotoxicity and antibody-dependent cellular phagocytosis in vitro. Finally, potent anti-tumor activity in vivo was observed in cell line- and patient-derived xenograft models from different B-cell malignancy subtypes. These encouraging preclinical results suggest that DuoHexaBody-CD37 (GEN3009) may serve as a potential therapeutic antibody for the treatment of human B-cell malignancies.

Published

2020

19. Clearance of amyloid‐beta with bispecific antibody constructs bound to erythrocytes

Author

John P. Atkinson, Margaret A. Lindorfer, and Ronald P. Taylor

Subjects

0301 basic medicine, Bispecific antibody, Amyloid beta, medicine.drug_class, Complement receptor 1, Monoclonal antibody, bispecific monoclonal antibodies, 03 medical and health sciences, 0302 clinical medicine, Lack of efficacy, medicine, human, Beta (finance), RC346-429, Disease treatment, biology, Bispecific monoclonal antibody, Chemistry, RC952-954.6, Alzheimer's disease, amyloid beta, Psychiatry and Mental health, complement receptor 1, 030104 developmental biology, Geriatrics, Perspective, biology.protein, Cancer research, Neurology (clinical), erythrocyte, Neurology. Diseases of the nervous system, biology.gene, 030217 neurology & neurosurgery, Perspectives

Abstract

We propose use of bispecific monoclonal antibody (mAb) complexes bound to erythrocytes to redress the lack of efficacy of anti‐amyloid beta mAbs in Alzheimer's disease treatment. Our paradigm leverages erythrocyte complement receptor 1 to promote rapid and quantitative removal of amyloid beta from the circulation, and its subsequent removal from the brain as well.

Published

2020

20. C3(H2O) prevents rescue of complement-mediated C3 glomerulopathy in Cfh-/- Cfd-/- mice

Author

Richard J.H. Smith, Emily E. Anderson, Ronald P. Taylor, John B. Henrich, Kristofer May, Dao-Fu Dai, Yuzhou Zhang, Adam Keenan, Gabriella R. Pitcher, and Margaret A. Lindorfer

Subjects

0301 basic medicine, Nephrology, medicine.medical_specialty, Hereditary Complement Deficiency Diseases, Complement Pathway, Alternative, Kidney, Complement factor B, 03 medical and health sciences, Mice, 0302 clinical medicine, Glomerulopathy, Internal medicine, medicine, Animals, Humans, Mice, Knockout, biology, Chemistry, Complement C5, General Medicine, Chronic renal disease, Complement C3, medicine.disease, Molecular biology, C3-convertase, Complement inhibition, Mice, Inbred C57BL, 030104 developmental biology, 030220 oncology & carcinogenesis, Complement Factor H, Alternative complement pathway, biology.protein, Factor D, Complement Factor D, Kidney Diseases, Research Article

Abstract

Therapeutic complement inhibition is a major focus for novel drug development. Of upstream targets, factor D (FD) is appealing because it circulates in plasma at low concentrations and has a single function: to cleave factor B to generate C3 convertase of the alternative pathway (AP). Mice with a targeted deletion of factor H (FH; Cfh(–/–) mice) develop C3 glomerulopathy (C3G) due to uncontrolled AP activity. To assess the impact of FD inhibition, we studied Cfh(–/–) Cfd(–/–) mice. We show that C3G in Cfh(–/–) mice is not rescued by removing FD. We used serum from Cfh(–/–) Cfd(–/–) mice to demonstrate that residual AP function occurs even when both FD and FH are missing and that hemolytic activity is present due to the action of C3(H(2)O). We propose that uncontrolled tick-over leads to slow activation of the AP in Cfh(–/–) Cfd(–/–) mice and that a minimal threshold of FH is necessary if tissue deposition of C3 is to be prevented. The FD/FH ratio dictates serum C3 level and renal C3b deposition. In C3G patients with chronic renal disease, the FD/FH ratio correlates inversely with C3 and C5 serum levels, suggesting that continuous AP control may be difficult to achieve by targeting FD.

Published

2019

21. Mechanisms of Complement-Mediated Damage in Hematological Disorders

Author

Ronald P. Taylor and Margaret A. Lindorfer

Subjects

0301 basic medicine, biology, business.industry, Autoantibody, Complement System Proteins, Hematology, medicine.disease, Hematologic Diseases, Complement (complexity), Complement system, Pathogenesis, 03 medical and health sciences, 030104 developmental biology, Atypical hemolytic uremic syndrome, Immunology, biology.protein, Paroxysmal nocturnal hemoglobinuria, Humans, Medicine, Antibody, business, Homeostasis

Abstract

The complement cascade is an ancient defense system that destroys and eliminates threats to normal homeostasis in the bloodstream and tissues. Although multiple controls keep complement in check to minimize innocent bystander injury to normal cells and tissues, defects in complement regulation due to mutations in, or autoantibodies to, complement control proteins underlie the pathogenesis of several hemolytic diseases including paroxysmal nocturnal hemoglobinuria, and atypical hemolytic uremic syndrome. In autoimmune hemolytic anemias complement plays an important role in erythrocyte destruction mediated by antierythrocyte antibodies. The pathogenic mechanisms of these hemolytic diseases are discussed, with an emphasis on pivotal steps in complement activation.

Published

2018

22. DuoHexaBody-CD37

Author

Simone C, Oostindie, Hilma J, van der Horst, Laurens P, Kil, Kristin, Strumane, Marije B, Overdijk, Edward N, van den Brink, Jeroen H N, van den Brakel, Hendrik J, Rademaker, Berris, van Kessel, Juliette, van den Noort, Martine E D, Chamuleau, Tuna, Mutis, Margaret A, Lindorfer, Ronald P, Taylor, Janine, Schuurman, Paul W H I, Parren, Frank J, Beurskens, and Esther C W, Breij

Subjects

B-Lymphocytes, Lymphoma, B-Cell, Lymphoma, Tetraspanins, Recombinant Fusion Proteins, Antibody-Dependent Cell Cytotoxicity, Drug development, Mice, SCID, Receptors, Fc, Leukemia, Lymphocytic, Chronic, B-Cell, Article, Mice, HEK293 Cells, Targeted therapies, Drug Development, Antigens, Neoplasm, Cell Line, Tumor, Immunoglobulin G, Antibodies, Bispecific, Animals, Heterografts, Humans, Leukaemia, Molecular Targeted Therapy

Abstract

Tetraspanin CD37 has recently received renewed interest as a therapeutic target for B-cell malignancies. Although complement-dependent cytotoxicity (CDC) is a powerful Fc-mediated effector function for killing hematological cancer cells, CD37-specific antibodies are generally poor inducers of CDC. To enhance CDC, the E430G mutation was introduced into humanized CD37 monoclonal IgG1 antibodies to drive more efficient IgG hexamer formation through intermolecular Fc-Fc interactions after cell surface antigen binding. DuoHexaBody-CD37, a bispecific CD37 antibody with the E430G hexamerization-enhancing mutation targeting two non-overlapping epitopes on CD37 (biparatopic), demonstrated potent and superior CDC activity compared to other CD37 antibody variants evaluated, in particular ex vivo in patient-derived chronic lymphocytic leukemia cells. The superior CDC potency was attributed to enhanced IgG hexamerization mediated by the E430G mutation in combination with dual epitope targeting. The mechanism of action of DuoHexaBody-CD37 was shown to be multifaceted, as it was additionally capable of inducing efficient antibody-dependent cellular cytotoxicity and antibody-dependent cellular phagocytosis in vitro. Finally, potent anti-tumor activity in vivo was observed in cell line- and patient-derived xenograft models from different B-cell malignancy subtypes. These encouraging preclinical results suggest that DuoHexaBody-CD37 (GEN3009) may serve as a potential therapeutic antibody for the treatment of human B-cell malignancies.

Published

2019

23. ‘Stealth’ corporate innovation: an emerging threat for therapeutic drug development

Author

John P. A. Ioannidis, Antonio M. Risitano, Brian V. Geisbrecht, Bo Nilsson, Daniel Ricklin, Alberto Mantovani, B. Paul Morgan, Tom Eirik Mollnes, Ronald P. Taylor, John D. Lambris, Mohamed R. Daha, Taroh Kinoshita, E. Sander Connolly, Dimitrios C. Mastellos, Robert A. Montgomery, Ruben Pio, V. Michael Holers, Piet Gros, Berhane Ghebrehiwet, George Hajishengallis, Anna M. Blom, Markus Huber-Lang, Mastellos, Dimitrios C, Blom, Anna M, Connolly, E Sander, Daha, Mohamed R, Geisbrecht, Brian V, Ghebrehiwet, Berhane, Gros, Piet, Hajishengallis, George, Holers, V Michael, Huber-Lang, Marku, Kinoshita, Taroh, Mollnes, Tom E, Montgomery, Robert A, Morgan, B Paul, Nilsson, Bo, Pio, Ruben, Ricklin, Daniel, Risitano, Antonio M, Taylor, Ronald P, Mantovani, Alberto, Ioannidis, John P A, and Lambris, John D

Subjects

0301 basic medicine, Immunology, Corporate innovation, Article, ComputingMilieux_GENERAL, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Drug development, Data transparency, Accountability, Immunology and Allergy, Engineering ethics, Business, 030215 immunology

Abstract

Therapeutic innovations of potentially great clinical impact should embrace the overarching values of research accountability, data transparency and validation through the scientific peer-review process.

Published

2019

24. CD20 and CD37 antibodies synergize to activate complement by Fc-mediated clustering

Author

Margaret A. Lindorfer, Martine E.D. Chamuleau, Richard Burack, Paul W. H. I. Parren, Clive S. Zent, Ronald P. Taylor, Karl R. VanDerMeid, Tuna Mutis, Rob N. de Jong, Jillian C. Tupitza, Hilma J. van der Horst, Janine Schuurman, Erika M. Cook, Kristin Strumane, Frank J. Beurskens, Esther C.W. Breij, Simone C. Oostindie, Hematology laboratory, CCA - Cancer biology and immunology, Hematology, and Molecular cell biology and Immunology

Subjects

CD20, biology, medicine.drug_class, Chemistry, Hematology, Complement System Proteins, Monoclonal antibody, Antigens, CD20, Article, Antibodies, 03 medical and health sciences, 0302 clinical medicine, Antigen, Cell culture, Cell Therapy & Immunotherapy, Cancer cell, Monoclonal, Cancer research, medicine, biology.protein, Cluster Analysis, Antibody, Cytotoxicity, 030215 immunology

Abstract

CD20 monoclonal antibody therapies have significantly improved the outlook for patients with B-cell malignancies. However, many patients acquire resistance, demonstrating the need for new and improved drugs. We previously demonstrated that the natural process of antibody hexamer formation on targeted cells allows for optimal induction of complement-dependent cytotoxicity. Complement-dependent cytotoxicity can be potentiated by introducing a single point mutation such as E430G in the IgG Fc domain that enhances intermolecular Fc-Fc interactions between cell-bound IgG molecules, thereby facilitating IgG hexamer formation. Antibodies specific for CD37, a target that is abundantly expressed on healthy and malignant B cells, are generally poor inducers of complement-dependent cytotoxicity. Here we demonstrate that introduction of the hexamerization-enhancing mutation E430G in CD37-specific antibodies facilitates highly potent complement-dependent cytotoxicity in chronic lymphocytic leukemia cells ex vivo. Strikingly, we observed that combinations of hexamerization-enhanced CD20 and CD37 antibodies cooperated in C1q binding and induced superior and synergistic complement-dependent cytotoxicity in patient-derived cancer cells compared to the single agents. Furthermore, CD20 and CD37 antibodies colocalized on the cell membrane, an effect that was potentiated by the hexamerization-enhancing mutation. Moreover, upon cell surface binding, CD20 and CD37 antibodies were shown to form mixed hexameric antibody complexes consisting of both antibodies each bound to their own cognate target, so-called hetero-hexamers. These findings provide novel insights into the mechanisms of synergy in antibody-mediated complement-dependent cytotoxicity and provide a rationale to explore Fc-engineering and antibody hetero-hexamerization as a tool to enhance the cooperativity and therapeutic efficacy of antibody combinations.

Published

2019

25. Complement alone drives efficacy of a chimeric antigonococcal monoclonal antibody

Author

Trent M. Woodruff, Xianbao He, Jutamas Shaughnessy, Marcel Roza, Janine Schuurman, Frank J. Beurskens, Bart-Jan de Kreuk, Peter A. Rice, Robin R. Ingalls, Nancy A. Nowak, Wen-Chao Song, Sunita Gulati, Sanjay Ram, Bo Zheng, Ronald P. Taylor, Marina Botto, and Rosane B. DeOliveira

Subjects

0301 basic medicine, Physiology, Complement System, medicine.disease_cause, Pathology and Laboratory Medicine, Biochemistry, Epitope, C5a receptor, Epitopes, Gonorrhea, Mice, 0302 clinical medicine, Mathematical and Statistical Techniques, Immune Physiology, Medicine and Health Sciences, Biology (General), Complement Activation, 11 Medical and Health Sciences, Mice, Inbred BALB C, Immune System Proteins, General Neuroscience, Complement C4b-Binding Protein, Statistics, Antibodies, Monoclonal, Animal Models, Antibodies, Bacterial, Healthy Volunteers, 3. Good health, Bacterial Pathogens, Infectious Diseases, Experimental Organism Systems, Medical Microbiology, Neisseria Gonorrhoeae, Complement Factor H, Physical Sciences, Female, Antibody, Pathogens, General Agricultural and Biological Sciences, Neisseria, Research Article, QH301-705.5, medicine.drug_class, Urology, Immunology, Sexually Transmitted Diseases, Mice, Transgenic, Mouse Models, Biology, Monoclonal antibody, Research and Analysis Methods, Microbiology, General Biochemistry, Genetics and Molecular Biology, Antibodies, 03 medical and health sciences, Model Organisms, Antigen, 07 Agricultural and Veterinary Sciences, medicine, Animals, Humans, Statistical Methods, Microbial Pathogens, Antigens, Bacterial, Analysis of Variance, General Immunology and Microbiology, Bacteria, Genitourinary Infections, Organisms, Biology and Life Sciences, Proteins, Complement System Proteins, 06 Biological Sciences, Virology, Complement system, Monoclonal Antibodies, Mice, Inbred C57BL, 030104 developmental biology, Immunoglobulin G, Immune System, Neisseria gonorrhoeae, biology.protein, Animal Studies, Fc-Gamma Receptor, 030217 neurology & neurosurgery, Mathematics, Developmental Biology

Abstract

Multidrug-resistant Neisseria gonorrhoeae is a global health problem. Monoclonal antibody (mAb) 2C7 recognizes a gonococcal lipooligosaccharide epitope that is expressed by >95% of clinical isolates and hastens gonococcal vaginal clearance in mice. Chimeric mAb 2C7 (human immunoglobulin G1 [IgG1]) with an E430G Fc modification that enhances Fc:Fc interactions and hexamerization following surface-target binding and increases complement activation (HexaBody technology) showed significantly greater C1q engagement and C4 and C3 deposition compared to mAb 2C7 with wild-type Fc. Greater complement activation by 2C7-E430G Fc translated to increased bactericidal activity in vitro and, consequently, enhanced efficacy in mice, compared with “Fc-unmodified” chimeric 2C7. Gonococci bind the complement inhibitors factor H (FH) and C4b-binding protein (C4BP) in a human-specific manner, which dampens antibody (Ab)-mediated complement-dependent killing. The variant 2C7-E430G Fc overcame the barrier posed by these inhibitors in human FH/C4BP transgenic mice, for which a single 1 μg intravenous dose cleared established infection. Chlamydia frequently coexists with and exacerbates gonorrhea; 2C7-E430G Fc also proved effective against gonorrhea in gonorrhea/chlamydia-coinfected mice. Complement activation alone was necessary and sufficient for 2C7 function, evidenced by the fact that (1) “complement-inactive” Fc modifications that engaged Fc gamma receptor (FcγR) rendered 2C7 ineffective, nonetheless; (2) 2C7 was nonfunctional in C1q−/− mice, when C5 function was blocked, or in C9−/− mice; and (3) 2C7 remained effective in neutrophil-depleted mice and in mice treated with PMX205, a C5a receptor (C5aR1) inhibitor. We highlight the importance of complement activation for antigonococcal Ab function in the genital tract. Elucidating the correlates of protection against gonorrhea will inform the development of Ab-based gonococcal vaccines and immunotherapeutics., A chimeric antibody that contains a "complement-enhancing" mutation in Fc (so-called HexaBody technology) shows increased bactericidal activity compared to antibody bearing wild-type Fc and may represent a promising immunotherapeutic approach against multidrug-resistant gonorrhea.

Published

2019

26. Critical role of C5a in sickle cell disease

Author

Margaret A. Lindorfer, Marna E. Ericson, Julia Nguyen, Trevor Killeen, Gregory M. Vercellotti, Terry Robert Schaid, Fuad Abdulla, Chunsheng Chen, John D. Belcher, Ronald P. Taylor, and Agustin P. Dalmasso

Subjects

Male, Vascular Cell Adhesion Molecule-1, Inflammation, Complement C5a, Mice, Transgenic, Anemia, Sickle Cell, Complement Membrane Attack Complex, Pharmacology, Kidney, Article, Recombinant C5a, 03 medical and health sciences, Mice, 0302 clinical medicine, hemic and lymphatic diseases, Blocking antibody, medicine, Animals, Humans, Anaphylatoxin, Lung, Receptor, Anaphylatoxin C5a, Innate immune system, biology, Chemistry, NF-kappa B, Hematology, Complement C3, Intercellular Adhesion Molecule-1, Antibodies, Neutralizing, Immunity, Innate, Complement system, Toll-Like Receptor 4, Cerebrovascular Disorders, Disease Models, Animal, P-Selectin, Gene Expression Regulation, Liver, 030220 oncology & carcinogenesis, Alternative complement pathway, biology.protein, medicine.symptom, Antibody, E-Selectin, 030215 immunology, Signal Transduction

Abstract

Innate immune complement activation may contribute to sickle cell disease (SCD) pathogenesis. Ischemia-reperfusion physiology is a key component of the inflammatory and vaso-occlusive milieu in SCD and is associated with complement activation. C5a is an anaphylatoxin, a potent pro-inflammatory mediator that can activate leukocytes, platelets, and endothelial cells, all of which play a role in vaso-occlusion. We hypothesize that hypoxia-reoxygenation (H/R) in SCD mice activates complement, promoting inflammation and vaso-occlusion. At baseline and after H/R, sickle Townes-SS mice had increased C3 activation fragments and C5b-9 deposition in kidneys, livers and lungs and alternative pathway Bb fragments in plasma compared to control AA-mice. Activated complement promoted vaso-occlusion (microvascular stasis) in SS-mice; infusion of zymosan-activated, but not heat-inactivated serum, induced substantial vaso-occlusion in the skin venules of SS-mice. Infusion of recombinant C5a induced stasis in SS, but not AA-mice that was blocked by anti-C5a receptor (C5aR) IgG. C5a-mediated stasis was accompanied by inflammatory responses in SS-mice including NF-κB activation and increased expression of TLR4 and adhesion molecules VCAM-1, ICAM-1, and E-selectin in the liver. Anti-C5aR IgG blocked these inflammatory responses. Also, C5a rapidly up-regulated Weibel-Palade body P-selectin and von Willebrand factor on the surface of human umbilical vein endothelial cells in vitro and on vascular endothelium in vivo. In SS-mice, a blocking antibody to P-selectin inhibited C5a-induced stasis. Similarly, an antibody to C5 that blocks murine C5 cleavage or an antibody that blocks C5aR inhibited H/R-induced stasis in SS-mice. These results suggest that inhibition of C5a may be beneficial in SCD.

Published

2019

27. Antibodies That Efficiently Form Hexamers upon Antigen Binding Can Induce Complement-Dependent Cytotoxicity under Complement-Limiting Conditions

Author

Paul W. H. I. Parren, Ronald P. Taylor, Janine Schuurman, Erika M. Cook, Margaret A. Lindorfer, Clive S. Zent, Richard Burack, Hilma J. van der Horst, Frank J. Beurskens, and Simone C. Oostindie

Subjects

0301 basic medicine, medicine.drug_class, Immunology, Antibodies, Monoclonal, Humanized, Monoclonal antibody, 03 medical and health sciences, Classical complement pathway, Antigen, Cell Line, Tumor, medicine, Humans, Immunology and Allergy, Antigens, Cytotoxicity, Alemtuzumab, Complement Activation, B cell, Immunotherapy and Vaccines, B-Lymphocytes, Membrane Glycoproteins, biology, Chemistry, Antibody-Dependent Cell Cytotoxicity, Antibodies, Monoclonal, Complement System Proteins, Hematology, Limiting, Antigens, CD20, Complement C9, Antigen binding, ADP-ribosyl Cyclase 1, Molecular biology, Complement-dependent cytotoxicity, Complement (complexity), Cell biology, Complement system, 030104 developmental biology, medicine.anatomical_structure, Complement C3b, biology.protein, Binding Sites, Antibody, Antibody

Abstract

Recently, we demonstrated that IgG Abs can organize into ordered hexamers after binding their cognate Ags expressed on cell surfaces. This process is dependent on Fc:Fc interactions, which promote C1q binding, the first step in classical pathway complement activation. We went on to engineer point mutations that stimulated IgG hexamer formation and complement-dependent cytotoxicity (CDC). The hexamer formation–enhanced (HexaBody) CD20 and CD38 mAbs support faster, more robust CDC than their wild-type counterparts. To further investigate the CDC potential of these mAbs, we used flow cytometry, high-resolution digital imaging, and four-color confocal microscopy to examine their activity against B cell lines and primary chronic lymphocytic leukemia cells in sera depleted of single complement components. We also examined the CDC activity of alemtuzumab (anti-CD52) and mAb W6/32 (anti-HLA), which bind at high density to cells and promote substantial complement activation. Although we observed little CDC for mAb-opsonized cells reacted with sera depleted of early complement components, we were surprised to discover that the Hexabody mAbs, as well as ALM and W6/32, were all quite effective at promoting CDC in sera depleted of individual complement components C6 to C9. However, neutralization studies conducted with an anti-C9 mAb verified that C9 is required for CDC activity against cell lines. These highly effective complement-activating mAbs efficiently focus activated complement components on the cell, including C3b and C9, and promote CDC with a very low threshold of MAC binding, thus providing additional insight into their enhanced efficacy in promoting CDC.

Published

2016

28. Echocardiographic Ischemic Memory Imaging Through Complement-Mediated Vascular Adhesion of Phosphatidylserine-Containing Microbubbles

Author

Brian P. Davidson, Ronald P. Taylor, Yan Zhao, William Packwood, Aris Xie, Brian Mott, Jonathan R. Lindner, and J. Todd Belcik

Subjects

Male, Pathology, Time Factors, Intravital Microscopy, Myocardial Infarction, Contrast Media, Infarction, 030204 cardiovascular system & hematology, Chest pain, Ferric Compounds, chemistry.chemical_compound, 0302 clinical medicine, 030212 general & internal medicine, Membrane Glycoproteins, Microbubbles, medicine.diagnostic_test, Oxides, Complement C3, Phosphatidylserine, Flow Cytometry, Coronary Vessels, Molecular Imaging, Echocardiography, Cardiology, medicine.symptom, Cardiology and Cardiovascular Medicine, Intravital microscopy, medicine.medical_specialty, Iron, Ischemia, Myocardial Reperfusion Injury, Phosphatidylserines, Flow cytometry, 03 medical and health sciences, Dogs, Predictive Value of Tests, Internal medicine, medicine, Animals, Radiology, Nuclear Medicine and imaging, business.industry, Complement C1q, Complement System Proteins, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, chemistry, Molecular imaging, business

Abstract

This study hypothesized that microvascular retention of phosphatidylserine-containing microbubbles (MB-PS) would allow detection of recent but resolved myocardial ischemia with myocardial contrast echocardiographic (MCE) molecular imaging.Techniques for ischemic memory imaging which can detect and spatially assess resolved myocardial ischemia are being developed for rapid evaluation of patients with chest pain.MCE molecular imaging with MB-PS was performed 1.5 h, 3.0 h, and 6.0 h after brief (10 min) myocardial ischemia in mice; data were compared to selectin-targeted microbubbles. MCE molecular imaging with Sonazoid (GE Healthcare, Amersham, United Kingdom), a commercially produced phosphatidylserine (PS) - containing agent, was performed in separate mice at 1.5 h and 3.0 h after ischemia-reperfusion; and in dogs undergoing 135 min of ischemia and 60 min of reflow as well as in closed-chest nonischemic control dogs. The mechanism for MB-PS attachment was assessed by intravital microscopy of post-ischemic muscle and by flow cytometry analysis of cell-MB interactions.In mice undergoing ischemia-reperfusion without infarction, signal enhancement in the risk area for MB-PS and p-selectin glycoprotein ligand-1-targeted microbubbles was similar at reflow times of 1.5 h (23.3 ± 7.3 IU vs. 30.7 ± 4.1 IU), 3.0 h (42.2 ± 6.2 IU vs. 33.9 ± 7.4 IU), and 6.0 h (24.1 ± 4.3 IU vs. 25.5 ± 4.7 IU). For both agents, signal in the risk area was significantly (p 0.05) higher than remote region at all reflow times. Sonazoid also produced strong risk area enhancement at 1.5 h (34.7 ± 5.0 IU) and 3.0 h (52.5 ± 4.5 IU) which was approximately 3-fold greater than in the control region, and which correlated spatially with the microsphere-derived risk area. In dogs, Sonazoid signal in the risk area was5-fold higher than in closed-chest control myocardium (42.2 ± 8.1 IU vs. 7.9 ± 3.3 IU; p 0.001). Mechanistic studies indicated that MB-PS attached directly to venular endothelium and adherent leukocytes which was dependent on serum complement components C1q and C3.Ischemic memory imaging with MCE is possible using MB-PS which may obviate the need for ligand-directed targeting.

Published

2016

29. Abstract 4544: Multifaceted mechanism of action of DuoHexaBody-CD37 involves both complement- and Fc gamma receptor-mediated cytotoxicity in pre-clinical B-cell lymphoma models

Author

Tuna Mutis, Paul W. H. I. Parren, Andreas Lingnau, Marije B. Overdijk, Ronald P. Taylor, Martine E.D. Chamuleau, Frank J. Beurskens, Marcel Brandhorst, A. Kate Sasser, Janine Schuurman, Margaret A. Lindorfer, Kristin Strumane, Simone C. Oostindie, Jeroen van den Brakel, Berris van Kessel, Esther C.W. Breij, Hilma J. van der Horst, and Laurens P. Kil

Subjects

Antibody-dependent cell-mediated cytotoxicity, Cancer Research, Plasma membrane organization, biology, Chemistry, medicine.disease, Peripheral blood mononuclear cell, Raji cell, Antibody opsonization, Oncology, Cancer research, biology.protein, medicine, Antibody, Cytotoxicity, B-cell lymphoma

Abstract

CD37 is a tetraspanin expressed on mature B cells where it orchestrates plasma membrane organization, receptor signaling, cell migration and adhesion. As CD37 is abundantly expressed on many mature B cell-derived malignancies, it represents an attractive target for new antibody therapies. DuoHexaBody®-CD37 is a novel biparatopic bispecific CD37 antibody with an Fc domain engineered to enhance antibody hexamerization upon binding to CD37 on the plasma membrane. DuoHexaBody-CD37 was shown to induce potent complement-dependent cytotoxicity (CDC) of malignant B-cell lines and primary chronic lymphocytic leukemia and non-Hodgkin lymphoma patient samples (Oostindie et al., Blood 2018 132:4170; van der Horst et al., Blood 2018 132:4179). Here, we demonstrate that the DuoHexaBody-CD37 mechanism of action also encompasses FcγR-mediated effector functions, including antibody-dependent cellular cytotoxicity (ADCC) and antibody-dependent cellular phagocytosis (ADCP). Daudi and Raji cells opsonized with DuoHexaBody-CD37 induced FcγRIIa and FcγRIIIa signaling in luciferase reporter assays. In agreement with efficient FcγR engagement, opsonization with DuoHexaBody-CD37 resulted in dose-dependent ADCC and ADCP by human healthy donor peripheral blood mononuclear cells (PBMCs) and monocyte-derived macrophages (MDMs), respectively. In a 4-hour Chromium-51 release assay, DuoHexaBody-CD37 induced ADCC in Daudi cells with PMBCs from 11 out of 12 tested donors (average EC50 of 9.87 [±9.98] ng/mL; maximum kill 20.4 [±9.2]%), and in Raji cells with 1 out of 3 donors. Image- and flow cytometry-based assays with MDMs illustrated that in presence of DuoHexaBody-CD37, Daudi cells were efficiently engulfed by effector cells from 3 different donors (average percentage phagocytic macrophages 29.7 ± 7.6%) resulting in target cell depletion (maximum depletion 75.9 [±18.0]%). Potent anti-tumor activity of DuoHexaBody-CD37 in vivo was reported in a screening approach using B-cell lymphoma patient-derived xenograft (PDX) models with single-mouse treatment groups. Two weekly doses of 5 mg/kg DuoHexaBody-CD37 resulted in strong tumor growth inhibition (tumor stasis or tumor regression) in 3/9 models compared to untreated tumors. Follow-up cohort PDX studies with eight mice per group confirmed potent, dose-dependent anti-tumor activity of DuoHexaBody-CD37 at doses as low as 1 mg/kg. In summary, DuoHexaBody-CD37 induces efficient tumor cell kill through CDC, ADCC and ADCP in vitro and shows potent anti-tumor activity in B-cell lymphoma PDX models in vivo. These data further strengthen the rationale for exploring the safety and efficacy of DuoHexaBody-CD37 in B-cell malignancy patients. Citation Format: Laurens P. Kil, Simone C. Oostindie, Kristin Strumane, Hilma J. van der Horst, Berris van Kessel, Marije B. Overdijk, Andreas Lingnau, Marcel Brandhorst, Jeroen van den Brakel, Margaret A. Lindorfer, Ronald P. Taylor, Martine E. Chamuleau, Tuna Mutis, A. Kate Sasser, Janine Schuurman, Paul W. Parren, Frank J. Beurskens, Esther C. Breij. Multifaceted mechanism of action of DuoHexaBody-CD37 involves both complement- and Fc gamma receptor-mediated cytotoxicity in pre-clinical B-cell lymphoma models [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 4544.

Published

2020

30. Duohexabody-CD37, a Novel Bispecific Antibody with a Hexamerization-Enhancing Mutation Targeting CD37, Demonstrates Superior Complement-Dependent Cytotoxicity in Preclinical B-Cell Malignancy Models

Author

Frank J. Beurskens, Simone C. Oostindie, Margaret A. Lindorfer, Janine Schuurman, Martine E.D. Chamuleau, Hilma J. van der Horst, Kristin Strumane, Paul W. H. I. Parren, Ronald P. Taylor, A. Kate Sasser, Esther C.W. Breij, Marije B. Overdijk, Erica M. Cook, Sandra Verploegen, and Tuna Mutis

Subjects

Mutation, biology, Chemistry, medicine.drug_class, Chronic lymphocytic leukemia, Immunology, Cell Biology, Hematology, CD37, medicine.disease, medicine.disease_cause, Monoclonal antibody, Biochemistry, Epitope, Complement-dependent cytotoxicity, Immunoglobulin G, biology.protein, medicine, Cancer research, Antibody

Abstract

CD37 is a tetraspanin plasma membrane protein abundantly expressed on B-cells and represents a promising therapeutic target for the treatment of B-cell malignancies. Although complement-dependent cytotoxicity (CDC) has proven to be a powerful Fc-mediated effector function for killing hematological cancer cells, CD37 antibody-based therapeutics currently in clinical development are poor inducers of CDC. Here we present DuoHexaBody-CD37, a novel humanized IgG1 bispecific antibody targeting two different CD37 epitopes, with an E430G hexamerization-enhancing mutation, for the potential treatment of B-cell malignancies. The natural process of antibody hexamer formation through intermolecular Fc-Fc interactions between IgG molecules after cell surface antigen binding can be improved by introducing a single point mutation such as E430G in the IgG Fc domain, thereby facilitating more efficient C1q binding and complement activation (Diebolder et al., Science 2014; de Jong et al., PLoS Biol 2016). The hexamerization-enhancing mutation E430G was introduced into two humanized CD37 monoclonal antibodies (mAbs) that bind non-overlapping CD37 epitopes. Different antibody formats and combinations, including the single antibodies, combinations of the mAbs and bispecific mAbs were tested for their capacity to induce CDC and antibody-dependent cellular cytotoxicity (ADCC). The bispecific hexamerization-enhanced antibody variant DuoHexaBody-CD37, showed superior CDC activity compared to the single hexamerization-enhanced mAbs and the combination thereof, both in vitro over a range of different B-cell lines, and ex vivo in tumor cell samples obtained from patients with chronic lymphocytic leukemia (CLL). In a CDC assay using tumor cells obtained from a relapsed/refractory CLL patient who received prior treatment with rituximab, ibrutinib and idelalisib, DuoHexaBody-CD37 induced almost complete lysis (84% lysis at a concentration 100 µg/mL), thereby outperforming the single HexaBody molecules (15% and 23% lysis) and the combination (57%) (Figure 1). In addition to its potent CDC activity, DuoHexaBody-CD37 was also capable of inducing potent ADCC of Daudi cells (EC50 = 12.3 ± 9.5 ng/mL), as assessed using peripheral blood mononuclear cells from 8 healthy human donors in a standard chromium release assay. In assays using whole blood from 6 healthy human donors, DuoHexaBody-CD37 showed efficient B-cell binding and potent and specific depletion of the B-cell population (98% ± 1.3% depletion at 10 µg/mL, EC50 = 0.85 ± 0.284 µg/mL). Furthermore, DuoHexaBody-CD37 induced significant inhibition of tumor growth in vivo in Daudi-luc Burkitt's lymphoma and JVM-3 CLL mouse xenograft models, at doses as low as 0.1 and 1 mg/kg (p In summary, we present a novel therapeutic antibody that, for the first time, combines proprietary DuoBody® and HexaBody® platforms. DuoHexaBody-CD37 induced highly potent CDC and efficient ADCC in preclinical models, suggesting that DuoHexaBody-CD37 may serve as a potential therapeutic mAb for the treatment of human B-cell malignancies. Disclosures Oostindie: Genmab: Employment, Equity Ownership. Van Der Horst:Genmab: Research Funding. Overdijk:Genmab: Employment, Equity Ownership. Strumane:Genmab: Employment, Equity Ownership. Verploegen:Genmab: Employment, Equity Ownership. Lindorfer:Genmab: Research Funding. Cook:Genmab: Research Funding. Chamuleau:Gilead: Research Funding; BMS: Research Funding; celgene: Research Funding; Genmab: Research Funding. Mutis:Gilead: Research Funding; Celgene: Research Funding; Janssen: Membership on an entity's Board of Directors or advisory committees, Research Funding; Genmab: Research Funding; Novartis: Research Funding; OnkImmune: Research Funding. Schuurman:Genmab: Employment, Other: Warrants. Sasser:Genmab: Employment, Equity Ownership. Taylor:Genmab: Research Funding. Parren:Genmab: Equity Ownership; Lava Therapeutics: Employment. Beurskens:Genmab: Employment, Equity Ownership. Breij:Genmab: Employment, Equity Ownership.

Published

2018

31. Endothelial Microparticles and Systemic Complement Activation in Patients With Chronic Kidney Disease

Author

Ismaeel Muhamed, V. Michael Holers, Jennifer Laskowski, Jelena Klawitter, James E. Cooper, Ronald P. Taylor, Karissa Valente, Joshua M. Thurman, Zhiying You, Moglie Le Quintrec, Margaret A. Lindorfer, Brandon Renner, Uwe Christians, Diana Jalal, Loni Perrenoud, Erik Stites, Carver College of Medicine, University of Iowa, University of Colorado Anschutz [Aurora], Centre Hospitalier Régional Universitaire [Montpellier] (CHRU Montpellier), Cellules Souches, Plasticité Cellulaire, Médecine Régénératrice et Immunothérapies (IRMB), Université de Montpellier (UM)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre Hospitalier Régional Universitaire [Montpellier] (CHRU Montpellier), North Carolina State University [Raleigh] (NC State), University of North Carolina System (UNC), University of North Carolina [Chapel Hill] (UNC), University of Virginia [Charlottesville], This work was supported by a grant from the American HeartAssociation (14GRNT20120018) and National Institutes ofHealth Grant R01 DK076690 (Thurman). It was also supportedby NIH T32 DK007135, Philips, Alexandre, Centre Hospitalier Régional Universitaire [Montpellier] (CHRU Montpellier)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Montpellier (UM), and University of Virginia

Subjects

Male, Proteomics, 0301 basic medicine, Brachial Artery, Complement Pathway, Alternative, Pilot Projects, Complement Membrane Attack Complex, 030204 cardiovascular system & hematology, urologic and male genital diseases, Severity of Illness Index, [SDV.MHEP.UN]Life Sciences [q-bio]/Human health and pathology/Urology and Nephrology, [SDV.IMM.II]Life Sciences [q-bio]/Immunology/Innate immunity, 0302 clinical medicine, Cell-Derived Microparticles, Medicine, Complement Activation, Original Research, Complement C4a, Middle Aged, female genital diseases and pregnancy complications, Vasodilation, Endothelium/Vascular Type/Nitric Oxide, Complement Factor D, Female, Cardiology and Cardiovascular Medicine, Complement Factor B, Glomerular Filtration Rate, Adult, Complement C5a, 03 medical and health sciences, Humans, In patient, Renal Insufficiency, Chronic, [SDV.IMM.II] Life Sciences [q-bio]/Immunology/Innate immunity, Aged, Inflammation, Kidney in Cardiovascular Disease, business.industry, Endothelial Cells, Complement System Proteins, medicine.disease, Kidney Transplantation, [SDV.MHEP.UN] Life Sciences [q-bio]/Human health and pathology/Urology and Nephrology, Complement system, Microparticles complement activation, 030104 developmental biology, Case-Control Studies, Immunology, Endothelium, Vascular, business, chronic kidney disease, Kidney disease

Abstract

Background Endothelial microparticles are associated with chronic kidney disease ( CKD ) and complement activation. We hypothesized that the complement pathway is activated in patients with CKD via endothelial microparticles and that complement activation correlates with endothelial dysfunction in CKD . Methods and Results We analyzed complement data of 30 healthy subjects, 30 patients with stage III / IV CKD , and 30 renal transplant recipients with stage III / IV CKD , evaluating the potential correlation of complement fragments with brachial artery flow–mediated dilation, Chronic Kidney Disease Epidemiology Collaboration glomerular filtration rate, and urinary albumin/creatinine ratio. Endothelial microparticles were characterized via proteomic analysis and compared between study groups. Complement fragment Ba was significantly increased in CKD and post–kidney transplant CKD . Plasma Ba levels correlated significantly with lower brachial artery flow–mediated dilation, lower Chronic Kidney Disease Epidemiology Collaboration glomerular filtration rate, and higher urinary albumin/creatinine ratio. Factor D levels were significantly higher in the plasma microparticles of patients with CKD versus healthy controls. Plasma microparticles isolated from patients with CKD and containing factor D activated the alternative pathway in vitro. Conclusion The alternative complement pathway is activated in CKD and correlates with endothelial dysfunction and markers of CKD . Future studies are needed to evaluate whether endothelial microparticles with increased factor D play a pathologic role in CKD ‐associated vascular disease. Clinical Trial Registration URL : http://www.clinicaltrials.gov . Unique identifier: NCT 02230202.

Published

2018

32. Mechanisms of Complement Activation in Malaria

Author

Ronald P. Taylor, José A. Stoute, and Margaret A. Lindorfer

Subjects

Antibody opsonization, Classical complement pathway, Immune system, biology, Chemistry, Complement receptor 1, parasitic diseases, Alternative complement pathway, biology.gene, Decay-accelerating factor, Complement (complexity), Complement system, Microbiology

Abstract

Activation of the classical pathway of complement, mediated by immune complexes, is very well-documented in malaria. In addition, several of the breakdown products that are produced upon rupture of malaria-infected erythrocytes, including hemin and the digestive vacuole, activate the alternative pathway of complement. Evidence for complement activation in malaria includes reduction in serum titers of total complement hemolytic activity and of individual complement components as well as increases in soluble complement activation products in the serum. In addition, C3 activation fragments have been demonstrated to be covalently bound to both infected and uninfected erythrocytes under a variety of conditions in malaria, thus leading to the extravascular clearance of erythrocytes to the spleen. This erythrocyte opsonization reaction, mediated by both the classical and alternative pathways of complement, may be additionally amplified in severe cases of malaria complicated by acidosis due to increased activation of the alternative pathway of complement.

Published

2018

33. Null donors favor prepared immunologists

Author

Ronald P. Taylor

Subjects

0301 basic medicine, Immunology, Null (mathematics), Cell Biology, Hematology, Biology, Biochemistry, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Binary Golay code, Effector functions, Receptor, 030215 immunology

Abstract

In this issue of Blood, Golay et al carefully examine activation and effector functions of normal neutrophils and of FcγRIIIB (CD16B)–negative neutrophils isolated from the blood of a rare null donor.1 Their work reveals, for the first time, that normal neutrophils also express FcγRIIIA (CD16A) and that the 2 receptors on neutrophils mediate distinctly different effector functions for processing antibody-opsonized substrates.

Published

2019

34. Human IgG is produced in a pro-form that requires clipping of C-terminal lysines for maximal complement activation

Author

Burt G van der Boom, Patrick Van Berkel, Patrick J. Engelberts, Paul W. H. I. Parren, Ronald P. Taylor, Marleen Voorhorst, Margaret A. Lindorfer, Rob N. de Jong, Frank J. Beurskens, Ewald T. J. van den Bremer, and Erika M. Cook

Subjects

capillary isoelectric focusing, Cytotoxicity, Immunologic, Immunology, Mutant, Mutation, Missense, electrospray ionization mass spectrometry, antibody-dependent cell-mediated cytotoxicity, Random hexamer, Report, Humans, Immunology and Allergy, Cytotoxic T cell, isoelectric focusing, Cytotoxicity, complement activation herapeutic antibody post-translational control ADCC antibody-dependent cell-mediated cytotoxicity CDC complement-dependent cytotoxicity CEX cation-exchange cIEF capillary isoelectric focusing CPB carboxy peptidase B ESI-MS electrospray ionization mass spectrometry IEF isoelectric focusing SDS-PAGE sodium dodecyl sulfate polyacrylamide gel electrophoresis HUMAN MONOCLONAL-ANTIBODY MAMMALIAN-CELL CULTURE MASS-SPECTROMETRY IN-VIVO THERAPEUTIC ANTIBODIES CHARGE VARIANTS BINDING-SITE RECOMBINANT PROTEINS MOLECULE, complement-dependent cytotoxicity, cation-exchange, Opsonin, post-translational control, sodium dodecyl sulfate polyacrylamide gel electrophoresis, complement activation, biology, Chemistry, IEF, Complement C1q, Lysine, CPB, ESI-MS, Antibodies, Monoclonal, CEX, Carboxypeptidase, Molecular biology, Complement system, cIEF, HEK293 Cells, Amino Acid Substitution, Immunoglobulin G, biology.protein, carboxy peptidase B, herapeutic antibody, bacteria, Antibody, ADCC, CDC, SDS-PAGE

Abstract

Human IgG is produced with C-terminal lysines that are cleaved off in circulation. The function of this modification was unknown and generally thought not to affect antibody function. We recently reported that efficient C1q binding and complement-dependent cytotoxicity (CDC) requires IgG hexamerization at the cell surface. Here we demonstrate that C-terminal lysines may interfere with this process, leading to suboptimal C1q binding and CDC of cells opsonized with C-terminal lysine-containing IgG. After we removed these lysines with a carboxypeptidase, maximal complement activation was observed. Interestingly, IgG1 mutants containing either a negative C-terminal charge or multiple positive charges lost CDC almost completely; however, CDC was fully restored by mixing C-terminal mutants of opposite charge. Our data indicate a novel post-translational control mechanism of human IgG: human IgG molecules are produced in a pro-form in which charged C-termini interfere with IgG hexamer formation, C1q binding and CDC. To allow maximal complement activation, C-terminal lysine processing is required to release the antibody's full cytotoxic potential.

Published

2015

35. Fcγ-receptor–mediated trogocytosis impacts mAb-based therapies: historical precedence and recent developments

Author

Ronald P. Taylor and Margaret A. Lindorfer

Subjects

Immunological Synapses, Trogocytosis, Neutrophils, medicine.drug_class, medicine.medical_treatment, Immunology, Antigen presentation, Gene Expression, Antineoplastic Agents, Antigen-Antibody Complex, Biology, Antibodies, Monoclonal, Humanized, Ofatumumab, Monoclonal antibody, History, 21st Century, Biochemistry, Monocytes, Antibodies, Monoclonal, Murine-Derived, chemistry.chemical_compound, Cancer immunotherapy, Antigen, medicine, Humans, Antigen Presentation, Receptors, IgG, Antibodies, Monoclonal, Dendritic Cells, Cell Biology, Hematology, Antigens, CD20, Lymphocyte Subsets, Killer Cells, Natural, Protein Transport, chemistry, Monoclonal, Antigenic Modulation, Immunotherapy, Rituximab

Abstract

A specialized form of trogocytosis occurs when Fcγ receptors on acceptor cells take up and internalize donor cell-associated immune complexes composed of specific monoclonal antibodies (mAbs) bound to target antigens on donor cells. This trogocytosis reaction, an example of antigenic modulation, has been described in recent clinical correlative studies and in vitro investigations for several mAbs used in cancer immunotherapy, including rituximab and ofatumumab. We discuss the impact of Fcγ-receptor–mediated trogocytosis on the efficacy of cancer immunotherapy and other mAb-based therapies.

Published

2015

36. Complement C5a-induced changes in neutrophil morphology during inflammation

Author

Miriam Kalbitz, Tim Eiseler, Florian Gebhard, David A. C. Messerer, Holger Barth, Rebecca Wiegner, Stephanie Denk, Manfred Weiss, John D. Lambris, Stephan Paschke, Ronald P. Taylor, Eberhard Barth, Markus Huber-Lang, Tobias Martin, Katharina Pfeiffer, Erika M. Cook, and Margaret A. Lindorfer

Subjects

0301 basic medicine, Neutrophils, Immunology, Inflammation, Complement C5a, chemical and pharmacologic phenomena, Biology, C5a receptor, Article, Neutrophil Activation, 03 medical and health sciences, Adenosine Triphosphate, medicine, Humans, Chloride-Bicarbonate Antiporters, Cell Shape, Receptor, Anaphylatoxin C5a, Cells, Cultured, Innate immune system, Chemotaxis, hemic and immune systems, General Medicine, Neutrophil extracellular traps, Actin cytoskeleton, Actins, Complement system, Cell biology, Actin Cytoskeleton, 030104 developmental biology, Receptors, Purinergic P2X, sense organs, medicine.symptom, Signal Transduction

Abstract

The complement and neutrophil defence systems, as major components of innate immunity, are activated during inflammation and infection. For neutrophil migration to the inflamed region, we hypothesized that the complement activation product C5a induces significant changes in cellular morphology before chemotaxis. Exposure of human neutrophils to C5a dose- and time-dependently resulted in a rapid C5a receptor-1 (C5aR1)-dependent shape change, indicated by enhanced flow cytometric forward-scatter area values. Similar changes were observed after incubation with zymosan-activated serum and in blood neutrophils during murine sepsis, but not in mice lacking the C5aR1. In human neutrophils, Amnis high-resolution digital imaging revealed a C5a-induced decrease in circularity and increase in the cellular length/width ratio. Biomechanically, microfluidic optical stretching experiments indicated significantly increased neutrophil deformability early after C5a stimulation. The C5a-induced shape changes were inhibited by pharmacological blockade of either the Cl-/HCO3--exchanger or the Cl- -channel. Furthermore, actin polymerization assays revealed that C5a exposure resulted in a significant polarization of the neutrophils. The functional polarization process triggered by ATP-P2X/Y-purinoceptor interaction was also involved in the C5a-induced shape changes, because pretreatment with suramin blocked not only the shape changes but also the subsequent C5a-dependent chemotactic activity. In conclusion, the data suggest that the anaphylatoxin C5a regulates basic neutrophil cell processes by increasing the membrane elasticity and cell size as a consequence of actin-cytoskeleton polymerization and reorganization, transforming the neutrophil into a migratory cell able to invade the inflammatory site and subsequently clear pathogens and molecular debris.

Published

2017

37. IgG Fc domains that bind C1q but not effector Fcγ receptors delineate the importance of complement-mediated effector functions

Author

Bianca Balbino, George Delidakis, Tae Hyun Kang, Makiko Watanabe, Kendra Triplett, Anja Lux, Navin Varadarajan, Odile Richard-Le Goff, Oana I. Lungu, Pierre Bruhns, George Georgiou, Corrine Alford, Gabrielle Romain, Margaret A. Lindorfer, Wissam Charab, Falk Nimmerjahn, Yan Jessie Zhang, Hidetaka Tanno, Wupeng Yan, Nicholas M. Marshall, Moses Donkor, Chang-Han Lee, Jiwon Lee, Ronald P. Taylor, Biliana Todorova, University of Texas at Austin [Austin], University of Houston, Anticorps en Thérapie et Pathologie, Institut Pasteur [Paris]-Institut National de la Santé et de la Recherche Médicale (INSERM), University of Erlangen-Nürnberg [Germany], University of Virginia School of Medicine [US], Université Pierre et Marie Curie - Paris 6 - UFR de Médecine Pierre et Marie Curie (UPMC), Université Pierre et Marie Curie - Paris 6 (UPMC), University of Virginia, Department of Biochemistry and Molecular Genetics (xxx), University of Virginia [Charlottesville], We thank Y. Tanno for assistance with protein expression, A. Bui for assistance with liquid chromatography–tandem mass spectrometry, P. Tucker (University of Texas at Austin) for cancer cell lines, D. Lee (MD Anderson Cancer Center) for patient-derived primary acute lymphocytic leukemia cells, the Macromolecular Crystallography Facility of the University of Texas at Austin, the Berkeley Center for Structural Biology, the Advanced Light Source (supported by the Director, Office of Science, Office of Basic Energy Sciences, of the US Department of Energy under contract DE-AC02-05CH11231), the Proteomics Facility at the University of Texas at Austin (supported by grant RP110782 from the Cancer Prevention Research Training Program), and A. Nicola and the Plate-Forme d'Imagerie Dynamique (Institut Pasteur, Paris) for help with the bioluminescence experiments. Supported by the Clayton Foundation, the Institut Pasteur (P.B. laboratory), the Institut National de la Santé et de la Recherche Médicale (P.B. laboratory), the European Research Council Seventh Frame-work Program (ERC-2013-CoG 616050 for the P.B. laboratory), the Pasteur–Paris University International PhD program (B.B.), the Cancer Prevention Research Training Program (RP140108 to M.D., RP160015 to H.T., and RP130570 to N.V.), the American Cancer Society (123506-PF-13-354-01-CDD to N.M.), Uehara Memorial Foundation (H.T.), Japan Society for the Promotion of Science (H.T.), Deutsche Forschungsgemeinschaft (CRC1181-A07 to F.N.), the US National Institutes of Health (R01CA174385 to N.V., and R01 GM104896 to Y.J.Z.) and the Welch Foundation (F-1778 to Y.J.Z.). The content is solely the responsibility of the authors and does not necessarily represent the official views of the Cancer Prevention and Research Institute of Texas., European Project: 616050,EC:FP7:ERC,ERC-2013-CoG,MYELOSHOCK(2014), Friedrich-Alexander Universität Erlangen-Nürnberg (FAU), Institut Pasteur [Paris] (IP)-Institut National de la Santé et de la Recherche Médicale (INSERM), University of Virginia, Martin, Marie, and Role of myeloid cells, their mediators and their antibody receptors in allergic shock (anaphylaxis) using humanized mouse models and clinical samples - MYELOSHOCK - - EC:FP7:ERC2014-09-01 - 2019-08-31 - 616050 - VALID

Subjects

Cytotoxicity, Immunologic, 0301 basic medicine, Cellular immunity, MESH: Complement C1q, MESH: Immunotherapy, Crystallography, X-Ray, Mass Spectrometry, MESH: Antibodies, Monoclonal, Mice, Tandem Mass Spectrometry, Neoplasms, Immunology and Allergy, MESH: Animals, MESH: Neoplasms, Cytotoxicity, Receptor, MESH: Phagocytosis, MESH: Crystallization, MESH: Immunoglobulin G, biology, Effector, Antibodies, Monoclonal, MESH: Enzyme-Linked Immunosorbent Assay, MESH: Chromatography, Gel, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Burkitt Lymphoma, 3. Good health, Cell biology, MESH: Surface Plasmon Resonance, Chromatography, Gel, [SDV.IMM]Life Sciences [q-bio]/Immunology, Immunotherapy, Lymphoma, Large B-Cell, Diffuse, Antibody, Crystallization, Lymphoma, B-Cell, MESH: Cell Line, Tumor, [SDV.IMM] Life Sciences [q-bio]/Immunology, Immunology, Enzyme-Linked Immunosorbent Assay, In Vitro Techniques, MESH: Receptors, IgG, MESH: Immunoglobulin Fc Fragments, 03 medical and health sciences, Classical complement pathway, Immune system, Phagocytosis, Cell Line, Tumor, Animals, Humans, MESH: Cytotoxicity, Immunologic, MESH: Mice, MESH: Lymphoma, B-Cell, MESH: In Vitro Techniques, MESH: Mass Spectrometry, MESH: Precursor Cell Lymphoblastic Leukemia-Lymphoma, MESH: Humans, Complement C1q, Receptors, IgG, MESH: Tandem Mass Spectrometry, Surface Plasmon Resonance, MESH: Crystallography, X-Ray, Immunoglobulin Fc Fragments, Complement system, MESH: Burkitt Lymphoma, 030104 developmental biology, Immunoglobulin G, biology.protein, MESH: Lymphoma, Large B-Cell, Diffuse, MESH: Chromatography, Liquid, Chromatography, Liquid

Abstract

International audience; Engineered crystallizable fragment (Fc) regions of antibody domains, which assume a unique and unprecedented asymmetric structure within the homodimeric Fc polypeptide, enable completely selective binding to the complement component C1q and activation of complement via the classical pathway without any concomitant engagement of the Fcγ receptor (FcγR). We used the engineered Fc domains to demonstrate in vitro and in mouse models that for therapeutic antibodies, complement-dependent cell-mediated cytotoxicity (CDCC) and complement-dependent cell-mediated phagocytosis (CDCP) by immunological effector molecules mediated the clearance of target cells with kinetics and efficacy comparable to those of the FcγR-dependent effector functions that are much better studied, while they circumvented certain adverse reactions associated with FcγR engagement. Collectively, our data highlight the importance of CDCC and CDCP in monoclonal-antibody function and provide an experimental approach for delineating the effect of complement-dependent effector-cell engagement in various therapeutic settings.

Published

2017

38. Neutrophils: positive or negative?

Author

Ronald P. Taylor

Subjects

0301 basic medicine, medicine.drug_class, Neutrophils, Chronic lymphocytic leukemia, Immunology, Monoclonal antibody, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, immune system diseases, Obinutuzumab, hemic and lymphatic diseases, Medicine, Humans, Opsonin, CD20, biology, business.industry, Cell Biology, Hematology, medicine.disease, Virology, 030104 developmental biology, chemistry, biology.protein, Rituximab, business, 030215 immunology, medicine.drug

Abstract

In this issue of Blood, Valgardsdottir et al demonstrate that human neutrophils do not kill chronic lymphocytic leukemia (CLL) B cells opsonized with the CD20 monoclonal antibody (mAb) rituximab (RTX) or obinutuzumab (OBZ); instead, the neutrophils remove both CD20 and bound mAbs from B cells by trogocytosis.1

Published

2017

39. Ibrutinib interferes with the cell-mediated anti-tumor activities of therapeutic CD20 antibodies: implications for combination therapy

Author

Martino Introna, Paul W. H. I. Parren, Fabio Da Roit, Alessandro Rambaldi, Ronald P. Taylor, Giuseppe Gritti, Josée Golay, Frank J. Beurskens, Esther C.W. Breij, and Patrick J. Engelberts

Subjects

Pyrazoles/pharmacology, Neutrophils, Chronic lymphocytic leukemia, Fluorescent Antibody Technique, Lymphoma, B-Cell/drug therapy, Apoptosis, Pharmacology, Complement Activation/drug effects, Cell Proliferation/drug effects, chemistry.chemical_compound, Piperidines, Obinutuzumab, hemic and lymphatic diseases, Antineoplastic Combined Chemotherapy Protocols, Pyrimidines/pharmacology, Complement Activation, Cells, Cultured, Killer Cells, Natural/drug effects, CD20, biology, Neutrophils/cytology, Antibodies, Monoclonal, Articles, Hematology, Flow Cytometry, Quinazolinones/pharmacology, Killer Cells, Natural, Leukemia, Ibrutinib, Idelalisib, Purines/pharmacology, Lymphoma, B-Cell, Phagocytosis/drug effects, Blotting, Western, Ofatumumab, Phagocytosis, medicine, Humans, Bruton's tyrosine kinase, Cell Proliferation, Quinazolinones, Adenine, Macrophages, Apoptosis/drug effects, Antibody-Dependent Cell Cytotoxicity, Macrophages/cytology, Leukemia, Lymphocytic, Chronic, B-Cell/drug therapy, Antigens, CD20, medicine.disease, Leukemia, Lymphocytic, Chronic, B-Cell, Antibodies, Monoclonal/pharmacology, Pyrimidines, chemistry, Purines, Case-Control Studies, biology.protein, Pyrazoles, Antigens, CD20/immunology

Abstract

The novel Bruton tyrosine kinase inhibitor ibrutinib and phosphatidyl-4-5-biphosphate 3-kinase-δ inhibitor idelalisib are promising drugs for the treatment of chronic lymphocytic leukemia and B-cell non-Hodgkin lymphoma, either alone or in combination with anti-CD20 antibodies. We investigated the possible positive or negative impact of these drugs on all known mechanisms of action of both type I and type II anti-CD20 antibodies. Pretreatment with ibrutinib for 1 hour did not increase direct cell death of cell lines or chronic lymphocytic leukemia samples mediated by anti-CD20 antibodies. Pre-treatment with ibrutinib did not inhibit complement activation or complement-mediated lysis. In contrast, ibrutinib strongly inhibited all cell-mediated mechanisms induced by anti- CD20 antibodies rituximab, ofatumumab or obinutuzumab, either in purified systems or whole blood assays. Activation of natural killer cells, and antibody-dependent cellular cytotoxicity by these cells, as well as phagocytosis by macrophages or neutrophils were inhibited by ibrutinib with a half maximal effective concentration of 0.3-3 μM. Analysis of anti-CD20 mediated activation of natural killer cells isolated from patients on continued oral ibrutinib treatment suggested that repeated drug dosing inhibits these cells in vivo. Finally we show that the phosphatidyl- 4-5-biphosphate 3-kinase-δ inhibitor idelalisib similarly inhibited the immune cell-mediated mechanisms induced by anti-CD20 antibodies, although the effects of this drug at 10 μM were weaker than those observed with ibrutinib at the same concentration. We conclude that the design of combined treatment schedules of anti- CD20 antibodies with these kinase inhibitors should consider the multiple negative interactions between these two classes of drugs.

Published

2014

40. A Humanized Antibody That Regulates the Alternative Pathway Convertase: Potential for Therapy of Renal Disease Associated with Nephritic Factors

Author

Claire L. Harris, Santiago Rodríguez de Córdoba, B. Paul Morgan, Eva Torreira, Oscar Llorca, Danielle Paixão-Cavalcante, Margaret A. Lindorfer, and Ronald P. Taylor

Subjects

Complement C3 Convertase, Alternative Pathway, Complement Pathway, Alternative, Immunology, Complement C3-C5 Convertases, Biology, Antibodies, Monoclonal, Humanized, Complement factor B, Article, C3-convertase, Complement system, Cell biology, Biochemistry, Factor H, Alternative complement pathway, Humans, Immunology and Allergy, Kidney Diseases, Complement membrane attack complex, CFHR5, Complement Factor B

Abstract

Dysregulation of the complement alternative pathway can cause disease in various organs that may be life-threatening. Severe alternative pathway dysregulation can be triggered by autoantibodies to the C3 convertase, termed nephritic factors, which cause pathological stabilization of the convertase enzyme and confer resistance to innate control mechanisms; unregulated complement consumption followed by deposition of C3 fragments in tissues ensues. The mAb, 3E7, and its humanized derivative, H17, have been shown previously to specifically bind activated C3 and prevent binding of both the activating protein, factor B, and the inhibitor, factor H, which are opposite effects that complicate its potential for therapy. Using ligand binding assays, functional assays, and electron microscopy, we show that these Abs bind C3b via a site that overlaps the binding site on C3 for the Ba domain within factor B, thereby blocking an interaction essential for convertase formation. Both Abs also bind the preformed convertase, C3bBb, and provide powerful inhibition of complement activation by preventing cleavage of C3. Critically, the Abs also bound and inhibited C3 cleavage by the nephritic factor–stabilized convertase. We suggest that by preventing enzyme formation and/or cleavage of C3 to its active downstream fragments, H17 may be an effective therapy for conditions caused by severe dysregulation of the C3 convertase and, in particular, those that involve nephritic factors, such as dense deposit disease.

Published

2014

41. Induced Resistance to Ofatumumab-Mediated Cell Clearance Mechanisms, Including Complement-Dependent Cytotoxicity, in Chronic Lymphocytic Leukemia

Author

Ronald P. Taylor, Clive S. Zent, Margaret A. Lindorfer, Adam Pettinger, Nisar A. Baig, Tait D. Shanafelt, Grzegorz S. Nowakowski, Betsy LaPlant, and Amy K. Church

Subjects

Adult, Cytotoxicity, Immunologic, Male, Chronic lymphocytic leukemia, Immunology, Antineoplastic Agents, Antibodies, Monoclonal, Humanized, Ofatumumab, Article, chemistry.chemical_compound, Antigens, CD, Antigens, Neoplasm, immune system diseases, hemic and lymphatic diseases, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Immunology and Allergy, Cytotoxic T cell, Lymphocyte Count, Alemtuzumab, Cyclophosphamide, Aged, Glycoproteins, Aged, 80 and over, CD20, B-Lymphocytes, biology, business.industry, Antibodies, Monoclonal, Complement System Proteins, Middle Aged, Antigens, CD20, medicine.disease, Leukemia, Lymphocytic, Chronic, B-Cell, Complement-dependent cytotoxicity, Complement system, Leukemia, Treatment Outcome, CD52 Antigen, chemistry, Drug Resistance, Neoplasm, Monoclonal, biology.protein, Female, business, Pentostatin

Abstract

Ofatumumab (OFA), a human CD20-targeting mAb, kills B lymphocytes using the innate immune system including complement-dependent cytotoxicity (CDC). The efficacy of OFA in patients with chronic lymphocytic leukemia (CLL) is limited by drug resistance, which is not well characterized. To better understand mechanisms of resistance, we prospectively studied CLL cells isolated from blood samples collected before and after in vivo exposure to the initial dose of OFA therapy in 25 patients undergoing their first treatment for progressive CLL. As previously reported, OFA therapy rapidly decreased the absolute lymphocyte count, CD20 expression by CLL cells, and serum complement levels. We now show that after administration of the first dose of OFA, there was a modest rebound in the absolute lymphocyte count and serum complement levels, but substantial ongoing loss of CD20 expression by CLL cells. These post-OFA treatment CLL cells were highly resistant to OFA-mediated CDC but retained sensitivity to alemtuzumab-mediated CDC in vitro. Posttherapy serum OFA levels correlated inversely with both the amount of pretreatment circulating cell-bound CD20 and with the decrease in this value following treatment. In vitro OFA-mediated CDC did not predict clinical responses, and the patients with first-dose reactions to OFA did not have markers of increased complement activation in vivo. We propose that optimal efficacy of CD20- targeted therapy for CLL requires determining an mAb dose size and frequency that optimizes CLL killing without exceeding the capacity of the cytotoxic mechanisms and thus minimizes loss of CD20 expression in the surviving CLL cells.

Published

2014

42. Mechanisms of enhanced neutralization of botulinum neurotoxin by monoclonal antibodies conjugated to antibodies specific for the erythrocyte complement receptor

Author

Scott K. Dessain, Sharad P. Adekar, Margaret A. Lindorfer, Andrew T. Segan, Rama Devudu Puligedda, Ronald P. Taylor, Ahmed Syed Ubaid, Rodney Bermudez, Huiwu Zhao, Fetweh H. Al-Saleem, Rashmi Sharma, Md. Elias, and Lance L. Simpson

Subjects

Botulinum Toxins, Erythrocytes, medicine.drug_class, Immunology, Mice, Transgenic, Antigen-Antibody Complex, Complement receptor, Monoclonal antibody, Article, Neutralization, Mice, Immune system, Antigen, In vivo, medicine, Animals, Humans, Molecular Biology, biology, Chemistry, Macrophages, Immune adherence, Antibodies, Monoclonal, Botulism, Antibodies, Neutralizing, Molecular biology, Receptors, Complement, Receptors, Complement 3b, biology.protein, Antibody

Abstract

Immune complexes formed between monoclonal antibodies (mAbs) and toxins can neutralize toxicity in vivo by multiple mechanisms. Toxin sequestration and clearance by mAbs may be improved by enhancing their ability to bind to red blood cells (RBCs) through immune adherence. This can be achieved by converting the mAbs to heteropolymers (HPs), which are antigen-specific mAbs cross-linked to mAbs targeting the complement receptor (CR1), a protein that is expressed on the surface of RBCs in primates and mediates delivery of complement C3b-containing immune complexes to tissue macrophages. Conversion of mAbs to HPs has been shown to enhance clearance of multivalent antigens from the blood circulation, but the interaction of HPs with monovalent toxins has not been examined. Using botulinum neurotoxin (BoNT) as a model system, we studied the effect of conversion of a pair of BoNT-specific mAbs into HPs on toxin neutralization and handling in vivo. Two HPs given in combination had 166-fold greater potency than un-modified mAbs, neutralizing 5,000 LD50 BoNT, when tested in transgenic mice expressing human CR1 on RBC membranes. Improvement required adherence of BoNT to the RBC in vivo and 2 HPs, rather than an HP + mAb pair. The HP pair bound BoNT to RBCs in the circulation for 2 hours, in comparison to BoNT-neutralizing anti-serum, which induced no detectable RBC binding. HP pairs exhibited enhanced uptake by peritoneal macrophages in vitro, compared to pairs of mAbs or mAb + HP pairs. In a post-exposure therapeutic model, HPs gave complete protection from a lethal BoNT dose up to 3 hours after toxin exposure. In a pre-exposure prophylaxis model, mice given HP up to 5 days prior to BoNT administration were fully protected from a lethal BoNT dose. These studies elucidate general mechanisms for the neutralization of toxins by HP pairs and demonstrate the potential utility of HPs as BoNT therapeutics.

Published

2014

43. Hexamerization-enhanced CD20 antibody mediates complement-dependent cytotoxicity in serum genetically deficient in C9

Author

Masashi Mizuno, B. Paul Morgan, Frank J. Beurskens, Richard Burack, Paul W. H. I. Parren, Ronald P. Taylor, Erika M. Cook, Margaret A. Lindorfer, Karl R. VanDerMeid, Clive S. Zent, and Janine Schuurman

Subjects

0301 basic medicine, Programmed cell death, Hereditary Complement Deficiency Diseases, Cell Survival, Immunology, Cell, Complement Membrane Attack Complex, Random hexamer, Biology, Polymerization, 03 medical and health sciences, 0302 clinical medicine, medicine, Immunology and Allergy, Humans, Cytotoxicity, CD20, Immunologic Deficiency Syndromes, Complement System Proteins, Complement C9, Molecular biology, Leukemia, Lymphocytic, Chronic, B-Cell, Complement-dependent cytotoxicity, 030104 developmental biology, medicine.anatomical_structure, biology.protein, Calcium, Immunotherapy, Antibody, Rituximab, Intracellular, 030215 immunology

Abstract

We examined complement-dependent cytotoxicity (CDC) by hexamer formation-enhanced CD20 mAb Hx-7D8 of patient-derived chronic lymphocytic leukemia (CLL) cells that are relatively resistant to CDC. CDC was analyzed in normal human serum (NHS) and serum from an individual genetically deficient for C9. Hx-7D8 was able to kill up to 80% of CLL cells in complete absence of C9. We conclude that the narrow C5b-8 pores formed without C9 are sufficient for CDC due to efficient antibody-mediated hexamer formation. In the absence of C9, we observed transient intracellular increases of Ca2 + during CDC (as assessed with FLUO-4) that were extended in time. This suggests that small C5b-8 pores allow Ca2 + to enter the cell, while dissipation of the fluorescent signal accompanying cell disintegration is delayed. The Ca2 + signal is retained concomitantly with TOPRO-3 (viability dye) staining, thereby confirming that Ca2 + influx represents the most proximate mediator of cell death by CDC.

Published

2016

44. Risk-Adapted, Ofatumumab-Based Chemoimmunotherapy and Maintenance in Treatment-Naïve CLL: A Phase II Study

Author

Erika M Gaglione, Inhye E. Ahn, Adrian Wiestner, Dennis C Drinkwater, Constance M. Yuan, Cydney M. Nichols, Pia Nierman, Margaret A. Lindorfer, Mohammed Farooqui, Irina Maric, Ronald P. Taylor, Susan Soto, Sarah E. M. Herman, Gerald E. Marti, Maryalice Stetler-Stevenson, Thomas E. Hughes, Laura M Wake, Xin Tian, Sanjal Desai, Janet Valdez, Alankrita Taneja, Jennifer Lotter, and Clifton C. Mo

Subjects

Oncology, medicine.medical_specialty, business.industry, Immunology, Complete remission, Phases of clinical research, Cell Biology, Hematology, Ofatumumab, Biochemistry, Fludarabine, Therapy naive, chemistry.chemical_compound, chemistry, Chemoimmunotherapy, hemic and lymphatic diseases, Internal medicine, Disease remission, medicine, Genetic risk, business, medicine.drug

Abstract

Introduction: Anti-CD20 monoclonal antibodies (mAb) are an essential component of CLL therapy. Addition of anti-CD20 mAb to induction chemotherapy improves progression-free survival (PFS) and overall survival (OS) in treatment-naïve CLL. Patients who achieve minimal residual disease negativity (MRD-) after induction chemoimmunotherapy (CIT) have prolonged PFS and OS. It is unclear, whether an extended therapy with an anti-CD20 mAb after induction CIT can improve the depth of response and long-term outcomes in patients with detectable residual disease (MRD+). Here we report results from a phase II study using risk-adapted, ofatumumab-based CIT induction followed by ofatumumab maintenance in treatment-naïve CLL patients. (NCT01145209) Methods: Treatment-naïve CLL patients were stratified twice: first, based on pre-treatment FISH, and second, based on post-induction peripheral blood (PB) MRD status. Patients with high-risk FISH (17p or 11q deletion) received up to 6 cycles of fludarabine, cyclophosphamide and ofatumumab (FCO). Patients without high-risk FISH received fludarabine, and ofatumumab (FO). Ofatumumab was dosed at 300mg for the first cycle, and 1000mg for subsequent cycles. After induction, patients were re-stratified based on PB MRD status using flow cytometry. MRD- was defined Results: We enrolled 32 patients. Twenty-eight patients received 3 or more cycles of induction CIT and were evaluable for outcomes. The overall response rate was 100%, including 8 (28.6%) patients achieving a complete response. The median PFS was 42.8 months and was significantly longer for patients who achieved MRD- after induction CIT compared to those with MRD+ (Not reached vs 36.2 months, p Antigen loss through Fc-gamma receptor-mediated uptake of antibody-antigen complexes into effector cells, referred to as trogocytosis, allows tumor cells to escape antibody-dependent cytotoxicity. At the same time, trogocytosis contributes to rapid clearance of circulating mAb. Investigating whether residual cells still expressed CD20, we measured expression of CD20 on CLL cells at the end of CIT. Most residual CLL in PB showed virtually complete loss of CD20 expression. We also stained BM biopsies obtained after 3 and 6 cycles of CIT for CD20 confirming absent or markedly reduced CD20 expressions on residual CD79+ CLL cells. In addition, the median trough level of ofatumumab on day 28 of each cycle increased with each advancing cycle (0, 13, and 51 mcg/mL after cycle 1, 2, and 3, respectively). Similarly, clearance of ofatumumab below the limit of detection (< 0.5mcg/mL) was observed in 60% of patients after the initial dose, and only 20% after cycle 3. Conclusions: Scaling intensity of CIT to genetic risk profiles achieved comparable outcomes for high-risk and standard-risk patients. MRD- remissions were associated with superior PFS, irrespective of the induction CIT regimen used. Maintenance therapy with ofatumumab did not improve the depth of response in MRD+ patients. Antibody induced antigen loss on tumor cells limits the efficacy of anti-CD20 mAbs even in settings with low tumor burden. Disclosures Farooqui: Merck: Employment. Lindorfer:Genmab: Research Funding. Wiestner:Pharmayclics: Research Funding; Acerta: Research Funding; Merck: Research Funding; Nurix: Research Funding.

Published

2019

45. Author Correction: ‘Stealth’ corporate innovation: an emerging threat for therapeutic drug development

Author

Dimitrios C. Mastellos, Anna M. Blom, Mohamed R. Daha, John D. Lambris, Antonio M. Risitano, Brian V. Geisbrecht, Daniel Ricklin, Berhane Ghebrehiwet, John P. A. Ioannidis, Ronald P. Taylor, Alberto Mantovani, Tom Eirik Mollnes, George Hajishengallis, B. Paul Morgan, Taroh Kinoshita, E. Sander Connolly, Piet Gros, Robert A. Montgomery, Bo Nilsson, Ruben Pio, V. Michael Holers, and Markus Huber-Lang

Subjects

Drug development, business.industry, Immunology, Immunology and Allergy, Business, Public relations, Corporate innovation

Published

2019

46. Activation of complement by monoclonal antibodies that target cell-associated β2-microglobulin: Implications for cancer immunotherapy

Author

Ronald P. Taylor, Monica F. Liu, Margaret A. Lindorfer, and Michael J. Pokrass

Subjects

biology, Chemistry, medicine.drug_class, medicine.medical_treatment, Immunology, Cell, Human leukocyte antigen, Monoclonal antibody, Major histocompatibility complex, Molecular biology, Complement-dependent cytotoxicity, medicine.anatomical_structure, Cancer immunotherapy, medicine, biology.protein, Cytotoxic T cell, Antibody, Molecular Biology

Abstract

β2-Microglobulin (β2M), the light chain of the class I major histocompatibilty complex (MHC-I), is a promising tumor target for monoclonal antibodies (mAbs) in cancer immunotherapy. Several reports indicate that chelation of cell-associated β2M by specific mouse mAbs promotes tumor cell destruction by inducing apoptosis or other cytotoxic signaling pathways. Human mAbs employed in cancer therapy are usually IgG1, which mediates cell-killing by effector mechanisms including complement dependent cytotoxicity (CDC). The analogous mouse IgG2a and IgG2b isotypes are similarly effective in activating complement. Therefore, we examined the complement-activating properties of anti-β2M mouse mAbs 1B749 (IgG2a) and HB28 (IgG2b) when either mAb was bound to tumor cell lines or normal cells; we compared these β2M-specific mAbs with mouse mAb W6/32 (IgG2a), specific for human leukocyte antigens in the MHC-I heavy chain. All three mAbs bind to most human cell lines and normal cells in approximately equal amounts, consistent with a 1:1 stoichiometry for the HLA heavy chain in association with β2M. The three mAbs promote rapid C3b deposition and substantial CDC of human cell lines, and mAbs 1B749 and W6/32 have robust cytotoxic activity on reaction with normal mononuclear cells and platelets. Curiously, mAb HB28 induces modest C3b deposition and little CDC of normal cells, and its weaker complement-fixing activity was confirmed by ELISA. Based on these findings, we suggest that human IgG mAbs that target β2M for cancer immunotherapy be selected or engineered so as not to activate complement, thus eliminating the potential adverse effects of complement-mediated lysis of normal cells.

Published

2013

47. CD20 mAb-Mediated Complement Dependent Cytotoxicity of Tumor Cells is Enhanced by Blocking the Action of Factor I

Author

Paul V. Beum, Ronald P. Taylor, and Margaret A. Lindorfer

Subjects

lcsh:Immunologic diseases. Allergy, Chronic lymphocytic leukemia, Immunology, Complement factor I, Ofatumumab, chemistry.chemical_compound, rituximab, hemic and lymphatic diseases, Drug Discovery, medicine, Immunology and Allergy, complement, B cell, CD20, biology, Chemistry, Factor I, medicine.disease, Complement-dependent cytotoxicity, medicine.anatomical_structure, monoclonal antibody, Cell culture, ofatumumab, biology.protein, Cancer research, iC3b, lcsh:RC581-607

Abstract

The CD20 mAbs, rituximab (RTX) and ofatumumab (OFA), have been used with success in the clinic in the treatment of B cell malignancies. These mAbs can eliminate B cells only by utilizing the body’s immune effector mechanisms, and there is considerable evidence that OFA is particularly effective at eliminating B cells by mediating complement dependent cytotoxicity (CDC). However, effector mechanisms such as complement can be exhausted or down-regulated. Therefore, several approaches are being investigated with the goal of increasing CDC mediated by these mAbs. We reported that when patients with chronic lymphocytic leukemia (CLL) are treated with RTX or with OFA, complement is rapidly activated on circulating, targeted CLL B cells. However, a substantial fraction of these cells escape CDC and clearance due to degradation of covalently deposited active C3b fragments to inactive fragments iC3b and C3d. This process is mediated by a plasma protease, Factor I. Therefore, a rational approach for increasing CDC would be to block this reaction by inhibiting Factor I with a neutralizing mAb. Indeed, we have demonstrated that use of neutralizing mAb A247, specific for factor I, significantly and substantially increases CD20 mAb-mediated CDC of both cell lines and of primary CLL cells in vitro.

Published

2013

48. Rapid clearance of rituximab may contribute to the continued high incidence of autoimmune hematologic complications of chemoimmunotherapy for chronic lymphocytic leukemia

Author

Wyndham H. Wilson, Adrian Wiestner, Clifton C. Mo, Gerald E. Marti, Margaret A. Lindorfer, Berengere Vire, Elinor Lee, Ronald P. Taylor, Paul V. Beum, and Ndegwa Njuguna

Subjects

Adult, Male, medicine.medical_specialty, Time Factors, Metabolic Clearance Rate, medicine.medical_treatment, Chronic lymphocytic leukemia, Antineoplastic Agents, Gastroenterology, Cohort Studies, Antibodies, Monoclonal, Murine-Derived, immune system diseases, Chemoimmunotherapy, hemic and lymphatic diseases, Internal medicine, medicine, Humans, Aged, Chemotherapy, business.industry, Incidence, Hematology, Immunotherapy, Middle Aged, medicine.disease, Leukemia, Lymphocytic, Chronic, B-Cell, Fludarabine, Leukemia, Treatment Outcome, Immunology, Trough level, Female, Rituximab, Anemia, Hemolytic, Autoimmune, Original Articles and Brief Reports, business, Vidarabine, medicine.drug

Abstract

Rituximab is an effective treatment for autoimmune cytopenias associated with chronic lymphocytic leukemia. Despite the incorporation of rituximab into fludarabine-based chemotherapy regimens, the incidence of autoimmune cytopenias has remained high. Inadequate rituximab exposure due to rapid antibody clearance may be a contributing factor. To test this hypothesis, we measured serum rituximab levels in patients treated with fludarabine and rituximab (375 mg/m(2)). All patients had undetectable rituximab trough levels by the end of cycle 1, and one-third had undetectable levels already on Day 6 of cycle 1. Although rituximab trough levels increased progressively with each cycle, only by cycle 4 did the median trough level exceed 10 ug/mL. The median half-life of rituximab during cycle 1 was 27 hours, compared to 199 hours during cycle 4 (P

Published

2013

49. Pericytes and immune cells contribute to complement activation in tubulointerstitial fibrosis

Author

Jing Yu, Didier Portilla, Ranjit K Sahu, Edimara S. Reis, Srinivas Ayyadevara, Judit Megyesi, Jeremy S. Duffield, John D. Lambris, Ronald P. Taylor, William B. Stallcup, Sandhya Xavier, and Susan G. Landes

Subjects

0301 basic medicine, Male, Pathology, medicine.medical_specialty, Time Factors, Genotype, Physiology, 030232 urology & nephrology, Cell Communication, Biology, Proinflammatory cytokine, Extracellular matrix, Receptor, Platelet-Derived Growth Factor beta, 03 medical and health sciences, 0302 clinical medicine, Immune system, Folic Acid, Fibrosis, Wnt3A Protein, medicine, Animals, Renal Insufficiency, Chronic, Complement Activation, Wnt Signaling Pathway, Mice, Knockout, Kidney, Extracellular Matrix Proteins, Complement C1q, Macrophages, Complement C3, medicine.disease, Complement system, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Kidney Tubules, Phenotype, Tubulointerstitial fibrosis, Cancer research, Disease Progression, Cytokines, Leukocyte Common Antigens, Inflammation Mediators, Pericytes, Myofibroblast, Ureteral Obstruction, Research Article

Abstract

We have examined the pathogenic role of increased complement expression and activation during kidney fibrosis. Here, we show that PDGFRβ-positive pericytes isolated from mice subjected to obstructive or folic acid injury secrete C1q. This was associated with increased production of proinflammatory cytokines, extracellular matrix components, collagens, and increased Wnt3a-mediated activation of Wnt/β-catenin signaling, which are hallmarks of myofibroblast activation. Real-time PCR, immunoblots, immunohistochemistry, and flow cytometry analysis performed in whole kidney tissue confirmed increased expression of C1q, C1r, and C1s as well as complement activation, which is measured as increased synthesis of C3 fragments predominantly in the interstitial compartment. Flow studies localized increased C1q expression to PDGFRβ-positive pericytes as well as to CD45-positive cells. Although deletion of C1qA did not prevent kidney fibrosis, global deletion of C3 reduced macrophage infiltration, reduced synthesis of C3 fragments, and reduced fibrosis. Clodronate mediated depletion of CD11bF4/80 high macrophages in UUO mice also reduced complement gene expression and reduced fibrosis. Our studies demonstrate local synthesis of complement by both PDGFRβ-positive pericytes and CD45-positive cells in kidney fibrosis. Inhibition of complement activation represents a novel therapeutic target to ameliorate fibrosis and progression of chronic kidney disease.

Published

2016

50. Cytotoxic mechanisms of immunotherapy: Harnessing complement in the action of anti-tumor monoclonal antibodies

Author

Ronald P. Taylor and Margaret A. Lindorfer

Subjects

0301 basic medicine, Cytotoxicity, Immunologic, medicine.drug_class, medicine.medical_treatment, Immunology, Monoclonal antibody, 03 medical and health sciences, 0302 clinical medicine, Antigens, Neoplasm, Neoplasms, medicine, Immunology and Allergy, Cytotoxic T cell, Animals, Humans, Cytotoxicity, Complement Activation, Antibody-dependent cell-mediated cytotoxicity, business.industry, Antibody-Dependent Cell Cytotoxicity, Cancer, Antibodies, Monoclonal, Immunotherapy, Complement System Proteins, medicine.disease, In vitro, Complement system, 030104 developmental biology, business, Genetic Engineering, 030215 immunology

Abstract

Several mAbs that have been approved for the treatment of cancer make use of complement-dependent cytotoxicity (CDC) to eliminate tumor cells. Comprehensive investigations, based on in vitro studies, mouse models and analyses of patient blood samples after mAb treatment have provided key insights into the details of individual steps in the CDC reaction. Based on the lessons learned from these studies, new and innovative approaches are now being developed to increase the clinical efficacy of next generation mAbs with respect to CDC. These improvements include engineering changes in the mAbs to enhance their ability to activate complement. In addition, mAb dosing paradigms are being developed that take into account the capacity as well as the limitations of the complement system to eliminate a substantial burden of mAb-opsonized cells. Over the next few years it is likely these approaches will lead to mAbs that are far more effective in the treatment of cancer.

Published

2016