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Dual membrane receptor degradation via folate receptor targeting chimera

Zhen Wang, Zhixin Li, Jenny Högström, Hiroyuki Inuzuka, Rui Jing, Peiqiang Yan, Tao Hou, Yihang Qi, Daoyuan Huang, Jingchao Wang, Ting Wu, Xiaoying Shi, Bolin Liu, Taru Muranen, Dingpeng Zhang, Wenyi Wei

2025Nature Communications9 citationsDOIOpen Access PDF

Abstract

Cancer drug resistance poses a significant challenge in oncology, often driven by intricate cross-talk among membrane-bound receptors that compromise mono-targeted therapies. We develop a dual membrane receptor degradation strategy leveraging Folate Receptor α (FRα) to address this issue. Folate Receptor α Targeting Chimeras-dual (FolTAC-dual) are engineered degraders designed to selectively and simultaneously degrade distinct receptor pairs: (1) EGFR/HER2 and (2) PD-L1/VISTA. Through modular optimization of modality configurations and geometries, we identify the "string" format as the most effective construct. Mechanistic studies demonstrate an ~85% increase in EGFR-binding affinity compared to the conventional knob-into-hole design, likely contributing to the improved efficiency of dual-target degradation. Proof-of-concept studies reveal that EGFR and HER2 FolTAC-dual effectively counteracts resistance in Trastuzumab/Lapatinib-resistant HER2-positive breast cancer models, while PD-L1 and VISTA FolTAC-dual rejuvenates immune responses in PD-L1 antibody-resistant syngeneic mouse models. These findings establish FolTAC-dual as a promising dual-degradation platform for clinical translation.

Topics & Concepts

Folate receptorReceptorChimera (genetics)Cell biologyChemistryCancer researchHEK 293 cellsChimeric antigen receptorImmune systemCell surface receptorDegradation (telecommunications)Computational biologyDual roleCancer cellBiologyCell membraneDrug resistanceCancerImmune receptorDual (grammatical number)Synthetic biologyCancer therapyFolic acidModular designBiochemistryCancer treatmentMembraneProtein Degradation and InhibitorsMonoclonal and Polyclonal Antibodies ResearchHER2/EGFR in Cancer Research
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