PO.IM01.13 · 免疫学

A first-in-class PD-L1/B7-H3/VEGF tri-specific ADC achieves enhanced preclinical antitumor efficacy through direct cytotoxicity, immune checkpoint blockade and VEGF inhibition

海报缩略图:A first-in-class PD-L1/B7-H3/VEGF tri-specific ADC achieves enhanced preclinical antitumor efficacy through direct cytotoxicity, immune checkpoint blockade and VEGF inhibition
编号 6940 展板 21 时间 4/22 09:00–12:00 区域 Section 6 主讲 Jiajia Pan, PhD
分会场 Antibody-Drug Conjugates 2
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作者与单位

Jiajia Pan, Pengfei Wang, Hongwang He, Mengfan Peng, Meng Cheng, Jie Zhang, Chengyi Ju, Jun Wang, Li Li, Hui Feng

Allink Biotherapeutics, Shanghai, China

摘要 Abstract

PD-L1 is an established immunotherapy target highly expressed in various solid tumors, while B7-H3 is another extensively investigated target overexpressed on a wide range of tumor cells. ADCs targeting PD-L1 or B7-H3 have entered clinical development and shown promising efficacy. PD-L1-directed ADCs may combine direct cytotoxicity and immunotherapy, demonstrating antitumor activity even in PD-L1-negative patients. However, ADC-related toxicity may limit their clinical dosing and thus restrict the full immune-mediated effects. Meanwhile, VEGF/PD-(L)1 bispecific antibodies are emerging as next-generation immunotherapies, with multiple trials exploring their combination with ADCs. Here, we developed ALK208, a trispecific ADC targeting PD-L1, B7-H3, and VEGF, conjugated to a topoisomerase I inhibitor payload. It is designed to integrate direct tumor cell killing, immune checkpoint blockade, and anti-angiogenic activity for maximal antitumor efficacy. Through optimized linker-payload design and DAR, ALK208 exhibited an improved safety profile, enabling higher dose levels to support robust PD-L1 blockade and VEGF neutralization. In preclinical studies, ALK208 simultaneously bound B7-H3, PD-L1, and VEGF with affinity comparable to monospecific antibodies. It effectively blocked VEGF/VEGFR and PD-1/PD-L1 interactions in reporter assays. Concurrent binding of B7-H3 and PD-L1 enhanced cellular binding and internalization in B7-H3/PD-L1 double-positive tumor cells, leading to more potent cytotoxicity than monospecific ADCs. VEGF-mediated crosslinking further strengthened binding, internalization, and cell-killing activity compared to a PD-L1/B7-H3 bispecific ADC. In the presence of VEGF homodimer, ALK208 also showed enhanced PD-L1 blockade in functional assays. Importantly, it did not kill activated T cells or APCs in vitro, suggesting a favorable immune safety profile. In xenograft models, ALK208 outperformed clinical-stage PD-L1 and PD-L1/B7-H3 ADCs. In summary, ALK208 is a first-in-class PD-L1/B7-H3/VEGF trispecific ADC that integrates multiple complementary mechanisms to maximize antitumor efficacy while maintaining a promising safety profile.
利益披露 Disclosure
J. Pan, Shanghai Allink Biotherapeutics Co., Ltd Employment. P. Wang, Shanghai Allink Biotherapeutics Co., Ltd Employment. H. He, Shanghai Allink Biotherapeutics Co., Ltd Employment. M. Peng, Shanghai Allink Biotherapeutics Co., Ltd Employment. M. Cheng, Shanghai Allink Biotherapeutics Co., Ltd Employment. J. Zhang, Shanghai Allink Biotherapeutics Co., Ltd Employment. C. Ju, Shanghai Allink Biotherapeutics Co., Ltd Employment. J. Wang, Shanghai Allink Biotherapeutics Co., Ltd Employment. L. Li, Shanghai Allink Biotherapeutics Co., Ltd Employment. H. Feng, Shanghai Allink Biotherapeutics Co., Ltd Employment, Stock. Shanghai Junshi Biosciences Co., Ltd. Stock.

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