Antibodies specifically targeting a locally misfolded region of tumor associated EGFR

Garrett, T.P.J.; Burgess, Anthony W; Gan, Hui; Luwor, Rodney B; Cartwright, Glenn A.; Walker, Francesca; Orchard, Suzanne G; Clayton, Andrew H. A.; Nice, Edouard C.; Rothacker, Julie; Catimel, Bruno; Cavenee, Webster K.; Old, Lloyd J.; Stockert, Elisabeth; Ritter, Gerd; Adams, Timothy E.; Hoyne, Peter A.; Wittrup, Dane; Chao, Ginger; Cochran, Jennifer R.; Luo, Chu; Lou, Mezhen; Huyton, Trevor; Xu, Yibin; Fairlie, W. Douglas; Yao, Shenggen; Scott, Andrew M.; Johns, Terrance G.

doi:10.1073/pnas.0811559106

Cited by 73 publications

(86 citation statements)

References 36 publications

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“…The different epitopes that these antibodies recognize underlie their distinct mechanisms of action and consequent efficacies against human xenograft tumors overexpressing EGFRvIII. Previous studies suggest that binding to the ABT-806 epitope blocks receptor dimerization and subsequent activation (8). In contrast, cetuximab exerts its antitumor activity, at least in part, by binding to its epitope on domain III of the EGFR preventing ligand binding (27).…”

Section: Discussionmentioning

confidence: 99%

“…Details of EGFR protein forms (based on numbering from accession# NP_005219.2) are as follows: wild-type EGFR comprised the entire extracellular binding domain (amino acids 1-645); EGFRvIII contained an in-frame deletion generating a truncated protein with a novel glycine (residues 1-29 and G-298-645); EGFR 1-501 (the first 1-525 amino acids inclusive 24 amino acid leader); and a double mutant EGFR C271A,C283A (containing EGFR 1-645, C295A, C307A) replacing cysteine at 271 and 283 in the processed protein with alanine (8) …”

Section: Antibodies and Reagentsmentioning

confidence: 99%

“…The targeted epitope is accessible in tumors with wild-type EGFR amplification or in tumors that express EGFRvIII, the most common deletion mutant of EGFR that lacks the ligand-binding domain of exons 2-7 and retains constitutive kinase activity (8)(9)(10). Thus mAb806 has tumor-specific binding properties and would not be expected to elicit the side effects, including skin rash, observed with other cetuximab-like EGFR targeting (mAbs) associated with targeting of normal tissues.…”

Section: Introductionmentioning

confidence: 99%

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Characterization of ABT-806, a Humanized Tumor-Specific Anti-EGFR Monoclonal Antibody

Reilly

Phillips

Buchanan

et al. 2015

Molecular Cancer Therapeutics

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Despite clinical efficacy, current approved agents targeting EGFR are associated with on-target toxicities as a consequence of disrupting normal EGFR function. MAb 806 is a novel EGFR antibody that selectively targets a tumor-selective epitope suggesting that a mAb 806-based therapeutic would retain antitumor activity without the on-target toxicities associated with EGFR inhibition. To enable clinical development, a humanized variant of mAb 806 designated ABT-806 was generated and is currently in phase 1 trials. We describe the characterization of binding and functional properties of ABT-806 compared with the clinically validated anti-EGFR antibody cetuximab. ABT-806 binds the mutant EGFRvIII with high affinity and, relative to cetuximab, exhibits increased potency against glioblastoma multiforme cell line and patient-derived xenografts expressing this form of the receptor. ABT-806 also inhibits the growth of squamous cell carcinoma xenograft models expressing high levels of wild-type EGFR, associated with inhibition of EGFR signaling, although higher doses of ABT-806 than cetuximab are required for similar activity. ABT-806 enhances in vivo potency of standard-of-care therapies used to treat glioblastoma multiforme and head and neck squamous cell carcinoma. An indiumlabeled version of ABT-806, [ 111 In]-ABT-806, used to investigate the relationship between dose and receptor occupancy, revealed greater receptor occupancy at lowers doses in an EGFRvIII-expressing model and significant uptake in an orthotopic model. Collectively, these results suggest that ABT-806 may have antitumor activity superior to cetuximab in EGFRvIIIexpressing tumors, and similar activity to cetuximab in tumors highly overexpressing wild-type EGFR with reduced toxicity.

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Section: Discussionmentioning

confidence: 99%

Section: Antibodies and Reagentsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Characterization of ABT-806, a Humanized Tumor-Specific Anti-EGFR Monoclonal Antibody

Reilly

Phillips

Buchanan

et al. 2015

Molecular Cancer Therapeutics

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“…Additionally, this epitope is not known to be targeted by current anti-EGFR therapeutics such as cetuximab (21,22). The m806 antibody displayed no targeting of normal tissues and produced minimal toxicities in a phase I clinical trial (23), while demonstrating activity against cancers exhibiting resistance to cetuximab or with EGFR kinase domain mutations (19,24). These properties suggest that m806 might be uniquely suited for delivery of cytotoxins to cancers that overexpress EGFR while sparing healthy cells.…”

mentioning

confidence: 96%

“…The m806 epitope is not accessible when the receptor is in an inactive monomer or activated dimer but is exposed in the locally misfolded (transitional), or "untethered," conformation, which preferentially occurs under oncogenic conditions (19,20). Additionally, this epitope is not known to be targeted by current anti-EGFR therapeutics such as cetuximab (21,22).…”

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confidence: 99%

Targeting a Cancer-Specific Epitope of the Epidermal Growth Factor Receptor in Triple-Negative Breast Cancer

Simon

Antignani

Sarnovsky

et al. 2016

JNCI J Natl Cancer Inst

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Background: Triple-negative breast cancers (TNBCs) are typically more aggressive and result in poorer outcomes than other breast cancers because treatment options are limited due to lack of hormone receptors or amplified human epidermal growth factor receptor 2 (HER2). Many TNBCs overexpress the epidermal growth factor receptor (EGFR) or manifest amplification of the EGFR gene, supporting EGFR as a therapeutic target. While EGFR-directed small molecule inhibitors have shown limited effectiveness in clinical settings, use of EGFR as a mechanism of delivering enzymatic cytotoxins to TNBC has not been demonstrated. Methods: Using the single-chain variable fragment (scFv) of the 806 antibody that binds only cells with overexpressed, misfolded, or mutant variants of the EGFR, a recombinant immunotoxin was engineered through gene fusion with Pseudomonas aeruginosa Exotoxin A (806-PE38). The potency of 806-PE38 on reducing TNBC cell growth in vitro and in xenograft models (n 6) was examined for six TNBC cell lines. All statistical tests were two-sided. Results: 806-PE38 statistically significantly reduced the viability of all tested TNBC lines, with IC 50 values below 10 ng/mL for three of six cell lines, while not affecting cells with wild-type EGFR (IC 50 >300 ng/mL). Systemic treatments with 806-PE38 vs vehicle resulted in statistically significantly reduced tumor burdens (806-PE38 mean ¼ 128 mm 3 [SD ¼ 46 mm 3 ] vs vehicle mean ¼ 749 mm 3 [SD ¼ 395 mm 3 ], P ¼ .001) and increased median survival (806-PE38 median ¼ 82 days vs vehicle median ¼ 50 days, P ¼ .01) in a MDA-MB-468 TNBC mouse xenograft. Deletion of the catalytic residue eliminated both cytotoxic activity in vitro and the reduction in tumor burden and survival (P ¼ .52). Conclusions: These data support the further development of the 806-PE38 immunotoxin as a therapeutic agent for the treatment of patients with EGFR-positive TNBC. Follow-up experiments with combination therapies will be attempted to achieve full remissions.

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A biparatopic anti‐EGFR nanobody efficiently inhibits solid tumour growth

Roovers

Vosjan

Laeremans

et al. 2011

Intl Journal of Cancer

224

182

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The epidermal growth factor receptor (EGFR) has been shown to be a valid cancer target for antibody-based therapy. At present, several anti-EGFR monoclonal antibodies (mAbs) have been successfully used, among which cetuximab and matuzumab. X-ray crystallography data show that these antibodies bind to different epitopes on the ecto-domain of EGFR, providing a rationale for the combined use of these two antibody specificities. We have previously reported on the successful isolation of antagonistic anti-EGFR nanobodies. In the present study, we aimed to improve on these molecules by combining nanobodies with specificities similar to both cetuximab and matuzumab into a single bi-paratopic molecule. Carefully designed phage nanobody selections resulted in two sets of nanobodies that specifically blocked the binding of either matuzumab or of cetuximab to EGFR and that did not compete for each others binding. A combination of nanobodies from both epitope groups into the bi-paratopic nanobody CONAN-1 was shown to block EGFR activation more efficiently than monovalent or bivalent (monospecific) nanobodies. In addition, this bi-paratopic nanobody potently inhibited EGF-dependent cell proliferation. Importantly, in an in vivo model of athymic mice bearing A431 xenografts, CONAN-1 inhibited tumour outgrowth with an almost similar potency as the whole mAb cetuximab, despite the fact that CONAN-1 is devoid of an Fc portion that could mediate immune effector functions. Compared to therapy using bivalent, mono-specific nanobodies, CONAN-1 was clearly more potent in tumour growth inhibition. These results show that the rational design of bi-paratopic nanobody-based anti-cancer therapeutics may yield potent lead molecules for further development.

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Antibodies specifically targeting a locally misfolded region of tumor associated EGFR

Cited by 73 publications

References 36 publications

Characterization of ABT-806, a Humanized Tumor-Specific Anti-EGFR Monoclonal Antibody

Characterization of ABT-806, a Humanized Tumor-Specific Anti-EGFR Monoclonal Antibody

Targeting a Cancer-Specific Epitope of the Epidermal Growth Factor Receptor in Triple-Negative Breast Cancer

A biparatopic anti‐EGFR nanobody efficiently inhibits solid tumour growth

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