Epitope and Fc-Mediated Cross-linking, but Not High Affinity, Are Critical for Antitumor Activity of CD137 Agonist Antibody with Reduced Liver Toxicity

Ho, Sun K.; Xu, Zhenghai; Thakur, Archana; Fox, Melvin; Tan, Siu Sze; DiGiammarino, Enrico L.; Zhou, Li; Sho, Mien; Cairns, Belinda; Zhao, Vivian; Xiong, Mengli; Samayoa, Josue; Forsyth, Charles M.; Powers, David B.; Chao, Debra T.; Hollenbaugh, Diane; Alvarez, Hamsell M.; Akamatsu, Yoshiko

doi:10.1158/1535-7163.mct-19-0608

Cited by 31 publications

(39 citation statements)

References 48 publications

(51 reference statements)

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“…Accumulated clinical data was not promising for either antibody [53]. Efforts have been made to mitigate the liver toxicity and improve the efficacy of 4-1BB antibodies [52,54] by engineering the Fc portion of the antibody to eliminate binding to the activating FcγRs, including FcγRI, FcγRIIA, and FcγRIIIA, while retaining binding to the inhibitory Fc receptor FcγRIIB [52]. Alternatively, antibodies targeting different epitopes away from the ligand-binding sites may have better efficacy as well as safety profiles if they are IgG4, which have better binding affinity to FcγRIIB than IgG2, which only binds to FcγRIIA [54].…”

Section: Selection Of Igg Subclasses For Targets Expressed In Immune mentioning

confidence: 99%

How to select IgG subclasses in developing anti-tumor therapeutic antibodies

2020

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The intact antibody of human immunoglobulin (IgG) is composed of the fragment for antigen binding (Fab) and the crystallizable fragment (Fc) for binding of Fcγ receptors. Among the four subclasses of human IgG (IgG1, IgG2, IgG3, IgG4), which differ in their constant regions, particularly in their hinges and CH2 domains, IgG1 has the highest FcγRbinding affinity, followed by IgG3, IgG2, and IgG4. As a result, different subclasses have different effector functions such as antibody-dependent cell-mediated cytotoxicity (ADCC) and antibody-dependent cellular phagocytosis (ADCP). Fcγ receptors include six subtypes (FcγRI, FcγRIIA, FcγRIIB, FcγRIIC, FcγRIIIA, FcγRIIIB) which differ in cellular distribution, binding affinity to Fc, and the resulting biological activity. Therefore, when developing anti-tumor therapeutic antibodies, including single-targeted antibodies, bi-specific antibodies (BsAbs), and antibody-drug conjugates (ADCs), many factors, such as target biology, cellular distribution of the targets, the environments of particular tumor types, as well as the proposed mechanism of action (MOA), must be taken into consideration. This review outlines fundamental strategies that are required to select IgG subclasses in developing anti-tumor therapeutic antibodies.

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Section: Selection Of Igg Subclasses For Targets Expressed In Immune mentioning

confidence: 99%

How to select IgG subclasses in developing anti-tumor therapeutic antibodies

2020

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“…Efforts are underway to develop 4-1BB agonists with more favorable toxicity profiles that retain potent costimulatory capacities (80)(81)(82). In addition to the optimization of anti-4-1BB immunoglobulins (80,81), various formats of targeted 4-1BB agonists are being investigated.…”

Section: Discussionmentioning

confidence: 99%

An engineered 4-1BBL fusion protein with “activity on demand”

Mock

Stringhini

Villa

et al. 2020

Proc. Natl. Acad. Sci. U.S.A.

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Engineered cytokines are gaining importance in cancer therapy, but these products are often limited by toxicity, especially at early time points after intravenous administration. 4-1BB is a member of the tumor necrosis factor receptor superfamily, which has been considered as a target for therapeutic strategies with agonistic antibodies or using its cognate cytokine ligand, 4-1BBL. Here we describe the engineering of an antibody fusion protein, termed F8-4-1BBL, that does not exhibit cytokine activity in solution but regains biological activity on antigen binding. F8-4-1BBL bound specifically to its cognate antigen, the alternatively spliced EDA domain of fibronectin, and selectively localized to tumors in vivo, as evidenced by quantitative biodistribution experiments. The product promoted a potent antitumor activity in various mouse models of cancer without apparent toxicity at the doses used. F8-4-1BBL represents a prototype for antibody-cytokine fusion proteins, which conditionally display “activity on demand” properties at the site of disease on antigen binding and reduce toxicity to normal tissues.

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“…Studies have focused on the development of bispecific agonists promoting agonist localisation to the tumour microenvironment 56,58 , or have sought to understand the relative roles of Fab region binding versus FcR clustering. New preclinical studies of 4-1BB agonists have shown that strong anti-tumor efficacy can be generated whilst avoiding both 4-1BBL ligand-blocking and liver toxicity due to crosslinking 57,59 . One study has indicted that 4-1BB antibodies that are weak agonists from Fab binding alone, but require inhibitory Fcreceptor FcgRIIB-mediated crosslinking, retain anti-tumour activity in the absence of liver toxicity 57 .…”

Section: Discussionmentioning

confidence: 99%

4-1BB is a target for immunotherapy in patients with undifferentiated pleomorphic sarcoma

Melake

Smith

Mansfield

et al. 2020

Preprint

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Systemic relapse, after treatment of a localised primary tumour with neo-adjuvant radiotherapy and surgery, is the major cause of disease related mortality in patients with sarcoma. As with other cancers, many sarcoma patients derive no benefit from anti-PD-1 treatment. Combining radiotherapy and immunotherapy is under investigation as a means to improve response rates and control metastatic disease. Here, we use a retrospective cohort of sarcoma patients, treated with neoadjuvant radiotherapy, and TCGA data to explore patient stratification for immunotherapy and therapeutic targets of relevance to sarcoma. We show a group of patients with immune-hot undifferentiated pleomorphic sarcoma as one of the highest-ranking candidates for emerging 4-1BB targeting agents. A binary hot/cold classification method indicates 4-1BB-high hot sarcomas share many characteristics with immunotherapy responsive cancers of other pathologies. Hot tumours in sarcoma are however substantially less prevalent. Patient stratification, of intense interest for immunotherapies, is therefore even more important in sarcoma.

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Epitope and Fc-Mediated Cross-linking, but Not High Affinity, Are Critical for Antitumor Activity of CD137 Agonist Antibody with Reduced Liver Toxicity

Cited by 31 publications

References 48 publications

How to select IgG subclasses in developing anti-tumor therapeutic antibodies

How to select IgG subclasses in developing anti-tumor therapeutic antibodies

An engineered 4-1BBL fusion protein with “activity on demand”

4-1BB is a target for immunotherapy in patients with undifferentiated pleomorphic sarcoma

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