PO.ET02.09 · 实验与分子治疗

SONNET 5010, a novel proprietary peptide drug conjugate lock and load platform

编号 479 展板 22 时间 4/19 02:00–05:00 区域 Section 19 主讲 John Cini, PhD
分会场 RNA, Gene and Cell Therapies, and Enabling Assay Technologies
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作者与单位

John K. Cini1, Susan Dexter1, Stephen McAndrew1, Arron Hearn2, Evert Bokma2, Gavin Birch2, Grant Harradence2, Christopher Sayer2, Rosa Gonzalez-Serrano2, Joao Nunes2

1Sonnet Biotherapeutics, Inc., Princeton, NJ,2Abzena, Cambridge, United Kingdom

摘要 Abstract

Background: Conventional IgG-based antibody-drug conjugates (ADCs) face major limitations, including heterogeneous drug-to-antibody ratios (DAR), variable pharmacokinetics, limited tumor penetration, and linker instability that can lead to off-target toxicity. To overcome these challenges, Sonnet has developed a non-IgG peptide drug conjugate (PDC) platform that enables precise drug loading and improved distribution. SON-5010 is the first proof-of-concept PDC generated using this approach and incorporates Sonnet's F H AB® (Fully Human Albumin Binding) domain to enhance half-life, tumor accumulation, and overall pharmacokinetics. Methods: SON-5010 consists of a dual anti-HER2 single-chain variable fragment (scFv) targeting domain flanking the F H AB motif, combined with an 18-amino-acid Docking Peptide-Payload Domain (DPPD). The DPPD contains three lysine residues that enable deterministic DAR3 conjugation with MMAE. The scFv-F H AB-scFv targeting domain was expressed in CHO cells, while the MMAE-loaded DPPD was chemically synthesized. The components were linked through standard conjugation chemistry to generate an ~88 kDa PDC. In vitro assessments included serum stability at 37°C and cytotoxicity testing in HER2-high (SKBR3) and HER2-negative (A549) cells. In vivo antitumor activity was evaluated in the HER2-positive BT-474 breast carcinoma xenograft model. SON-5010 was designed for direct comparison with trastuzumab, which contains the same anti-HER2 domain and Lys linker chemistry as MMAE (DAR3), except that it is attached to the DPPD rather than an IgG. Results: SON-5010 demonstrated strong serum stability and potent cytotoxicity in HER2-expressing SKBR3 cells, with no activity in HER2-negative A549 cells. In vivo, SON-5010 produced tumor growth inhibition comparable to HER2-directed MMAE ADC control of trastuzumab. At 10 mg/kg, SON-5010 showed no detectable toxicity, with stable body weight and no adverse clinical signs. The smaller size of the PDC and the F H AB-mediated albumin binding likely contributed to improved tumor penetration and favorable tolerability. Conclusions: SON-5010 demonstrates the potential of Sonnet's modular PDC platform to address key limitations of IgG-based ADCs. The architecture enables full DAR control, enhanced penetration, and flexible engineering of targeting domains and payload chemistries. The platform also supports dual-payload and multispecific designs, offering opportunities to overcome resistance and improve therapeutic index. Early results indicate that SON-5010 is a promising next-generation targeted therapeutic candidate.
利益披露 Disclosure
J. K. Cini, None.. S. Dexter, None.. S. McAndrew, None.. A. Hearn, None.. E. Bokma, None.. G. Birch, None.. G. Harradence, None.. C. Sayer, None.. R. Gonzalez-Serrano, None.. J. Nunes, None.

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