Preclinical studies of BB-1701, a HER2-targeting eribulin-containing ADC with potent bystander effect and ICD activity

Author:

Wang Yang1ORCID,Xia Bing1,Cao Lixia1,Yang Jianfeng1,Feng Cui1,Jiang Fangdun1,Li Chen1,Gu Lixia1,Yang Yifan1,Tian Jing1,Cheng Xin23,Furuuchi Keiji23,Fulmer James23,Verdi Arielle23,Rybinski Katherine23,Soto Allis23,Albone Earl23,Uenaka Toshimitsu23,Gong Likun4,Liu Tingting4,Qin Qiuping4,Wei Ziping1,Zhou Yuhong1

Affiliation:

1. Bliss Biopharmaceutical (Hangzhou) Co., Ltd, Hexiang Technology Center , Hangzhou 310018 , China

2. Epochal Precision Anti-Cancer Therapeutics (EPAT) , Cell Lineage and Differentiation (CLD) Domain, , Exton, PA 19341 , United States

3. Eisai Inc. , Cell Lineage and Differentiation (CLD) Domain, , Exton, PA 19341 , United States

4. Shanghai Institute of Materia Medica, Chinese Academy of Sciences , Shanghai 201203 , China

Abstract

Abstract Background: Several HER2-targeting antibody–drug conjugates (ADC) have gained market approval for the treatment of HER2-expressing metastasis. Promising responses have been reported with the new generation of ADCs in patients who do not respond well to other HER2-targeting therapeutics. However, these ADCs still face challenges of resistance and/or severe adverse effects associated with their particular payload toxins. Eribulin, a therapeutic agent for the treatment of metastatic breast cancer and liposarcoma, is a new choice of ADC payload with a distinct mechanism of action and safety profile. Methods: We’ve generated a novel HER2-tageting eribulin-containing ADC, BB-1701. The potency of BB-1701 was tested in vitro and in vivo against cancer cells where HER2-expressing levels vary in a large range. Bystander killing effect and toxin-induced immunogenic cell death (ICD) of BB-1701 were also tested. Results: In comparison with HER2-targeting ADCs with DM1 and Dxd payload, eribulin-containing ADC demonstrated higher in vitro cytotoxicity in HER2-low cancer cell lines. BB-1701 also effectively suppressed tumors in models resistant to DM1 or Dxd containing ADCs. Mode of action studies showed that BB-1701 had a significant bystander effect on HER2-null cells adjacent to HER2-high cells. In addition, BB-1701 treatment induced ICD. Repeated doses of BB-1701 in nonhuman primates showed favorable pharmacokinetics and safety profiles at the intended clinical dosage, route of administration, and schedule. Conclusions: The preclinical data support the test of BB-1701 in patients with various HER2-expressing cancers, including those resistant to other HER2-targeting ADCs. A phase I clinical trial of BB-1701 (NCT04257110) in patients is currently underway.

Funder

Bliss Biopharmaceutical (Hangzhou) Co., Ltd

Publisher

Oxford University Press (OUP)

Reference39 articles.

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