Novel type II anti-CD20 monoclonal antibody (GA101) evokes homotypic adhesion and actin-dependent, lysosome-mediated cell death in B-cell malignancies

Alduaij, Waleed; Иванов, А. В.; Honeychurch, Jamie; Cheadle, Eleanor J.; Potluri, Sandeep; Lim, Sean H.; Shimada, Kazuyuki; Chan, H T Claude; Tutt, Alison L.; Beers, Stephen A.; Glennie, Martin J.; Cragg, Mark S.; Illidge, Tim

doi:10.1182/blood-2010-07-296913

Cited by 259 publications

(259 citation statements)

References 45 publications

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“…26 Obinutuzumab not only possesses ADCC activity, but also exhibits multiple MOAs in vitro, including enhanced noncaspase-dependent induction of direct cell death. 25 Similarly, IGN523 possesses multiple mechanisms of action, as shown here in several cell lines in vitro (Fig. 6).…”

Section: Discussionmentioning

confidence: 56%

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Antitumor activity of an anti‐CD98 antibody

et al. 2015

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CD98 is expressed on several tissue types and specifically upregulated on fast-cycling cells undergoing clonal expansion. Various solid (e.g., nonsmall cell lung carcinoma) as well as hematological malignancies (e.g., acute myeloid leukemia) overexpress CD98. We have identified a CD98-specific mouse monoclonal antibody that exhibits potent preclinical antitumor activity against established lymphoma tumor xenografts. Additionally, the humanized antibody designated IGN523 demonstrated robust tumor growth inhibition in leukemic cell-line derived xenograft models and was as efficacious as standard of care carboplatin in patient-derived nonsmall lung cancer xenografts. In vitro studies revealed that IGN523 elicited strong ADCC activity, induced lysosomal membrane permeabilization and inhibited essential amino acid transport function, ultimately resulting in caspase-3 and -7-mediated apoptosis of tumor cells. IGN523 is currently being evaluated in a Phase I clinical trial for acute myeloid leukemia (NCT02040506). Furthermore, preclinical data support the therapeutic potential of IGN523 in solid tumors.CD98 is a heterodimeric protein that comprises a heavy and light chain. The CD98 heavy chain is a type II transmembrane glycoprotein that forms a heterodimer via covalent linkage to one of 6 amino acid transporters. 1,2 CD98 is overexpressed on the cell surface of almost all tumor cells, regardless of tissue origin and increased expression of a CD98-light chain, L-type amino acid transporter 1 (LAT-1) occurs in many types of human cancers, including breast, colon, oral, ovarian, esophageal, glioma and leukemia. 3,4 Increased uptake of amino acids supports the high growth rate of cancer cells by providing the building blocks for protein synthesis. [4][5][6] Moreover, the higher expression of CD98 heavy chain and LAT-1 in metastatic vs. primary tumors suggests that over-expression of CD98/LAT-1 may facilitate progression and metastasis of human cancers.CD98 also regulates integrin signaling by association with integrin b-subunits, thereby controlling cell proliferation, survival, migration, epithelial adhesion and polarity. 3,7 The function of CD98 in regulating both amino acid transport and integrin signaling can contribute to the rapid proliferation and clonal expansion of lymphocytes and tumor cells. 3 The expression pattern and pleiotropic function of CD98 heavy and light chains suggest these proteins are promising targets for treatment of a variety of human cancers. Although small molecule inhibitors of LAT-1 activity have demonstrated preclinical antitumor activity in a number of cancer cell types, including NSCLC, colon cancer, oral cancer and breast cancer, development of antibodies against CD98 heavy chain has received less focus. 5,[8][9][10] Murine monoclonal antibodies to CD98 inhibit lymphocyte proliferation and the growth of bladder cancer, lymphoma, glioma, prostate and colon cancer cells in preclinical models. [11][12][13] To identify therapeutic anti-CD98 antibodies with significant antitumor activity, we ...

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Section: Discussionmentioning

confidence: 56%

“…25 To assess whether similar effects are seen with IGN523 plus crosslinker, we investigated if the CD98-IGN523 complex was internalized to lysosomes and whether this led to increased lysosomal permeability (Fig. 5).…”

Section: Ign523 Elicits Caspase-dependent Apoptosis Increases Lysosomentioning

confidence: 99%

Antitumor activity of an anti‐CD98 antibody

et al. 2015

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“…Also direct cytotoxicity is enhanced. CD20 binding leads to homotypic adhesion and following cell death induction is non-apoptotic, actin-dependent and lysosome mediated [23]. Further in vitro studies showed depletion of CLL cells in whole blood assays and the superior efficacy of GA-101 compared to rituximab [24].…”

Section: Ga-101mentioning

confidence: 99%

Refractory chronic lymphocytic leukemia - new therapeutic strategies

Schnaiter

Stilgenbauer

2010

Oncotarget

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AbstrAct:Treatment outcome of chronic lymphocytic leukemia (CLL) has considerably improved since the introduction of fludarabine (F) as part of the standard therapy. Nevertheless, refractoriness to fludarabine occurs in a significant number of patients and is associated with an unfavorable prognosis. Important risk factors are 17p deletion and/or mutation of TP53. For this subgroup the CD52 antibody alemtuzumab (A) presents a new treatment approach and has already been approved. Meanwhile we have to face also refractoriness to alemtuzumab. Importantly, the monoclonal CD20 antibody ofatumumab has now shown efficacy in F and A double-refractory CLL. The next generation CD20 antibody GA-101 is currently compared to rituximab (R) and will possibly be its more potent successor. Further B-cell antigens are targeted by lumiliximab (CD23), TRU-016 (CD37) and blinatumomab (CD19). Apart from monoclonal antibody therapies, a great number of small molecules are examined for the treatment of refractory and relapsed CLL. Most of these agents aim to overcome apoptosis resistance in CLL cells or influence the microenvironment. Typical targets are regulators of the cell cycle and antiapoptotic molecules like the members of the Bcl-2 family. Up to now the most promising agents appear to be flavopiridol and lenalidomide among others.

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“…Type I display a potent ability to activate complement through enhanced recruitment of C1q [12] due to the efficient clustering of antibody Fc regions [13]; an activity directly linked to their ability to redistribute CD20 to lipid raft microdomains of the plasma membrane. In contrast, type II anti-CD20 mAb do not display either of these properties but instead evoke strong homotypic adhesion [14] and a non-apoptotic form of lysosomal cell death [14][15][16][17]. In addition, we observed that type I anti-CD20 mAb undergo more rapid internalization from the cell surface, in contrast to type II mAb [18][19][20].…”

Section: Introductionmentioning

confidence: 98%

Antibody modulation: Limiting the efficacy of therapeutic antibodies

Vaughan

Cragg

Beers

2015

Pharmacological Research

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Monoclonal antibodies (mAb) have revolutionised the way in which we treat disease.From cancer to autoimmunity, antibody therapy has been responsible for some of the most impressive clinical responses observed in the last 2 decades. A key component of this success has been their generally low levels of toxicity, and unique mechanisms of action. These two facets have allowed them to a) be integrated rapidly into clinical practice in combination with conventional radio-and chemotherapies and b) to avoid the resistance mechanisms typically observed with classical small molecule drugs, such as upregulation of drug efflux transporters, dysregulation of apoptosis and mutations in key target enzymes/pathways.Although success with mAb therapies has been impressive, they are also subject to their own resistance mechanisms. In this perspective we discuss the various ways in which mAb therapeutics can be inhibited, concentrating mainly on the ways in which they can be removed from the target cell surface -a process called modulation. This can be achieved either in a cis-fashion on a single cell or in trans, precipitated by engagement with a second phagocytic cell. The evidence for each of these processes will be discussed, in addition to possible therapeutic strategies that might be employed to inhibit or reverse them.Abbreviations: Fc gamma receptor, FcR; monoclonal antibody, mAb

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Novel type II anti-CD20 monoclonal antibody (GA101) evokes homotypic adhesion and actin-dependent, lysosome-mediated cell death in B-cell malignancies

Cited by 259 publications

References 45 publications

Antitumor activity of an anti‐CD98 antibody

Antitumor activity of an anti‐CD98 antibody

Refractory chronic lymphocytic leukemia - new therapeutic strategies

Antibody modulation: Limiting the efficacy of therapeutic antibodies

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