A Novel HER3-Targeting Antibody–Drug Conjugate, U3-1402, Exhibits Potent Therapeutic Efficacy through the Delivery of Cytotoxic Payload by Efficient Internalization

Hashimoto, Yuichi; Koyama, Kumiko; Kamai, Yasuki; Hirotani, Kenji; Ogitani, Yusuke; Zembutsu, Akiko; Abe, Manabu; Kaneda, Yoshihisa; Maeda, Naoyuki; Shiose, Yoshinobu; Iguchi, Takuma; Ishizaka, Tomomichi; Karibe, Tsuyoshi; Hayakawa, Ichiro; Morita, Koji; Nakada, Takashi; Nomura, Taisei; Wakita, Kenichi; Kagari, Takashi; Abe, Yuki; Murakami, Masato; Ueno, Suguru; Agatsuma, Toshinori

doi:10.1158/1078-0432.ccr-19-1745

Cited by 94 publications

(51 citation statements)

References 41 publications

(56 reference statements)

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“…Proof of clinical concept has already been achieved with approvals of anti-HER2 ADCs, such as trastuzumab–emtansine (T-DM1) and trastuzumab–deruxtecan (T-DXd) for breast cancer 217 , 218 , in which the anti-HER2 is linked to a cytotoxic microtubule inhibitor and a topoisomerase 1 inhibitor, respectively. Similarly, patritumab, a HER3 antibody linked to DXd (HER3–DXd) is in early clinical development for the treatment of solid tumours such as colorectal cancer 219 .…”

Section: The Next 20 Years Of Kinase Drug Discoverymentioning

confidence: 99%

Kinase drug discovery 20 years after imatinib: progress and future directions

Cohen

Cross

Jänne

2021

Nat Rev Drug Discov

543

399

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Section: The Next 20 Years Of Kinase Drug Discoverymentioning

confidence: 99%

Kinase drug discovery 20 years after imatinib: progress and future directions

Cohen

Cross

Jänne

2021

Nat Rev Drug Discov

543

399

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show abstract

“…In NSCLC, HER3-overexpression has been reported in 80% of EGFR-mutated adenocarcinomas [78]. HER3-DXd demonstrated to inhibit tumor growth in HER3+, EGFRmutated, EGFR-TKI resistant patient-derived xenograft (PDX) models, while it was ineffective in HER3-negative models [79]. A phase I trial then investigated this ADC in EGFR-mutated NSCLC progressing to first generation EGFR-TKIs and negative for T790M mutation, or after osimertinib failure [80].…”

Section: Patritumab Deruxtecan (U3-1402)mentioning

confidence: 99%

Antibody–drug conjugates in solid tumors: a look into novel targets

2021

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Antibody–drug conjugates (ADCs) are a relatively new class of anticancer agents designed to merge the selectivity of monoclonal antibodies with cell killing properties of chemotherapy. They are commonly described as the “Trojan Horses” of therapeutic armamentarium, because of their capability of directly conveying cytotoxic drug (payloads) into the tumor space, thus transforming chemotherapy into a targeted agent. Three novel ADCs have been recently approved, i.e., trastuzumab deruxtecan, sacituzumab govitecan and enfortumab vedotin, respectively, targeting HER2, Trop2 and Nectin4. Thanks to progressive advances in engineering technologies these drugs rely on, the spectrum of diseases sensitive to these drugs as well as their indications are in continuous expansion. Several novel ADCs are under evaluation, exploring new potential targets along with innovative payloads. This review aims at providing a summary of the technology behind these compounds and at presenting the latest ADCs approved in solid tumors, as well as at describing novel targets for ADCs under investigation and new strategies to optimize their efficacy in solid tumors.

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“…Additionally, differences in the internalization rate were observed for the studied variants in a panel of cell lines with varying levels of HER3 expression. The ability to induce rapid internalization is of relevance when designing payload delivery, which could be a viable strategy for HER3-targeted therapy [25]. Based on our results, we hypothesized that the molecular design of affibody-based therapeutics targeting HER3 in terms of the relative position of functional domains and valency has an impact on tumor targeting, biodistribution properties, and internalization rates.…”

Section: Introductionmentioning

confidence: 86%

Evaluating the Therapeutic Efficacy of Mono- and Bivalent Affibody-Based Fusion Proteins Targeting HER3 in a Pancreatic Cancer Xenograft Model

et al. 2020

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Human epidermal growth factor receptor 3 (HER3) has been increasingly scrutinized as a potential drug target since the elucidation of its role in mediating tumor growth and acquired therapy resistance. Affibody molecules are so-called scaffold proteins with favorable biophysical properties, such as a small size for improved tissue penetration and extravasation, thermal and chemical stability, and a high tolerance to modifications. Additionally, affibody molecules are efficiently produced in prokaryotic hosts or by chemical peptide synthesis. We have previously evaluated the biodistribution profiles of five mono- and bivalent anti-HER3 affibody molecules (designated as 3) fused to an albumin-binding domain (designated as A), 3A, 33A, 3A3, A33, and A3, that inhibit ligand-dependent phosphorylation. In the present study, we examined the therapeutic efficacy of the three most promising variants, 3A, 33A, and 3A3, in a direct comparison with the HER3-targeting monoclonal antibody seribantumab (MM-121) in a preclinical BxPC-3 pancreatic cancer model. Xenografted mice were treated with either an affibody construct or MM-121 and the tumor growth was compared to a vehicle group. Receptor occupancy was estimated by positron emission tomography/computed tomography (PET/CT) imaging using a HER3-targeting affibody imaging agent [68Ga]Ga-(HE)3-Z08698-NODAGA. The affibody molecules could inhibit ligand-dependent phosphorylation and cell proliferation in vitro and demonstrated tumor growth inhibition in vivo comparable to that of MM-121. PET/CT imaging showed full receptor occupancy for all tested drug candidates. Treatment with 3A and 3A3 affibody constructs was more efficient than with 33A and similar to the anti-HER3 antibody seribantumab, showing that the molecular design of affibody-based therapeutics targeting HER3 in terms of the relative position of functional domains and valency has an impact on therapeutic effect.

show abstract

A Novel HER3-Targeting Antibody–Drug Conjugate, U3-1402, Exhibits Potent Therapeutic Efficacy through the Delivery of Cytotoxic Payload by Efficient Internalization

Cited by 94 publications

References 41 publications

Kinase drug discovery 20 years after imatinib: progress and future directions

Kinase drug discovery 20 years after imatinib: progress and future directions

Antibody–drug conjugates in solid tumors: a look into novel targets

Evaluating the Therapeutic Efficacy of Mono- and Bivalent Affibody-Based Fusion Proteins Targeting HER3 in a Pancreatic Cancer Xenograft Model

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