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Discovery of Highly Potent and Selective IKZF2 Degraders for Cancer Immunotherapy.

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Journal of medicinal chemistry 📖 저널 OA 13.8% 2023: 1/1 OA 2024: 1/8 OA 2025: 14/81 OA 2026: 14/134 OA 2023~2026 2026 Vol.69(8) p. 9615-9634 Protein Degradation and Inhibitors
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PubMed DOI OpenAlex 마지막 보강 2026-04-29
OpenAlex 토픽 · Protein Degradation and Inhibitors interferon and immune responses Nanoplatforms for cancer theranostics

Wang Y, Qi Z, Sun S, Wei T, Wei P, Jia C

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Immunosuppressive Tregs, regulated by IKZF2, facilitate tumor immune evasion and resistance to immune checkpoint therapies.

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APA Yalei Wang, Zhenze Qi, et al. (2026). Discovery of Highly Potent and Selective IKZF2 Degraders for Cancer Immunotherapy.. Journal of medicinal chemistry, 69(8), 9615-9634. https://doi.org/10.1021/acs.jmedchem.6c00500
MLA Yalei Wang, et al.. "Discovery of Highly Potent and Selective IKZF2 Degraders for Cancer Immunotherapy.." Journal of medicinal chemistry, vol. 69, no. 8, 2026, pp. 9615-9634.
PMID 41944524 ↗

Abstract

Immunosuppressive Tregs, regulated by IKZF2, facilitate tumor immune evasion and resistance to immune checkpoint therapies. Targeted IKZF2 degradation represents a promising strategy for the development of innovative cancer immunotherapeutics. Herein, we designed and synthesized a novel series of phthalazinone-based glutarimide derivatives, identifying compound as a potent, highly selective, and rapid-acting IKZF2 molecular glue degrader. Compound induced robust IKZF2 degradation (DC = 1.78 nM and = 93.2%) via a Cullin-CRBN-dependent pathway, while sparing other CRBN neosubstrates and outperforming the benchmark degrader DKY709. Mechanistically, -induced IKZF2 deletion enhanced the proinflammatory IL-2 production and attenuated the immunosuppressive function of Tregs. Oral administration of triggered rapid, profound, and sustained IKZF2 degradation in mice spleen and thymus. As monotherapy, significantly suppressed B16F tumor growth, and combined with anti-PD-1 antibody therapy exhibited marked synergistic effects. Together, our findings demonstrate as a promising IKZF2 degrader for advancing cancer immunotherapy.

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