What question did this study set out to answer?

To develop and evaluate NL019, a novel dual-target ADC utilizing the NanoOne™ platform for improved efficacy in cancer treatment.

April 5, 2026

Abstract 1677: NL019: A next-generation TROP2/NECTIN4 dual-target nanobody-based ADC developed from the NanoOne™ Platform

Key Points

To develop and evaluate NL019, a novel dual-target ADC utilizing the NanoOne™ platform for improved efficacy in cancer treatment.
Utilized NanoOne™ platform to create dual-target nanobody-based ADC.
Employed VHH nanobody modules for enhanced tumor penetration and antigen recognition.
Conducted in vitro tests for dual-target binding and cytotoxicity.
Tested NL019 efficacy in xenograft and CDX models against benchmark ADCs.
NL019 showed potent synergistic activity in vitro with reduced on-target toxicities.
Achieved superior antitumor efficacy in preclinical models compared to benchmark ADCs targeting TROP2 or NECTIN4.
Demonstrated dose-dependent effects in tumor models, supporting its potential as a broad-spectrum therapeutic.

Abstract

Abstract Background: While antibody-drug conjugates (ADCs) have transformed oncology treatment, conventional IgG-based ADCs are constrained by suboptimal tumor penetration, heterogeneous antigen expression, and Fc receptor-mediated immune toxicity. NanoOne™, developed by Naliean Therapeutics, is an innovative nanobody-based modular ADC platform that redefines ADC engineering through molecular miniaturization, structural precision, and payload flexibility. Methods: NanoOne™ integrates multiple VHH nanobody modules (54 kDa) to achieve deep tumor penetration and broad recognition of tumors with diverse tumor-associated antigen (TAA) profiles. Its proprietary Site-Specific Dual-Payload Conjugation enables precise stoichiometric control (1:2, 2:1, 2:2, etc.) for single or dual payloads with outstanding homogeneity. The design incorporates a highly hydrophilic and stable linker that confers excellent developability. Fc domains are removed to avoid Fc receptor-mediated toxicity to immune cells while maintaining optimal half-life and enhancing tumor microenvironment accumulation. Results: NL019, a TROP2/NECTIN4 dual-target ADC armed with a microtubule inhibitor, demonstrated potent and synergistic activity in vitro—including dual-target binding, internalization, and cytotoxicity—while minimizing on-target toxicities seen in single-target ADCs. In multiple xenograft and CDX models, NL019 achieved superior, dose-dependent antitumor efficacy versus benchmark ADCs targeting TROP2 or NECTIN4. Conclusions: NL019 exemplifies the disruptive potential of NanoOne™, combining advanced molecular architecture, precision one/dual-payload conjugation, and superior tumor selectivity. Supported by strong preclinical efficacy and developability, NL019 is advancing toward first-in-human trials. Given the broad expression of TROP2 and NECTIN4 across epithelial malignancies, NL019 has the potential to establish a new generation of broad-spectrum ADC therapeutics. Citation Format: Meiguang Xiong, Binbin Wang, Jie Ni, Chenchen Lu, Fang Yu, Yu Zhang, . NL019: A next-generation TROP2/NECTIN4 dual-target nanobody-based ADC developed from the NanoOne™ Platform abstract. In: Proceedings of the American Association for Cancer Research Annual Meeting 2026; Part 1 (Regular Abstracts); 2026 Apr 17-22; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2026;86(7 Suppl):Abstract nr 1677.

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Abstract 1677: NL019: A next-generation TROP2/NECTIN4 dual-target nanobody-based ADC developed from the NanoOne™ Platform

Key Points

Abstract

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