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Experimental Hematology & Oncology

Experimental Hematology & Oncology

IF: 13.5
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TLR7/8 signaling activation enhances the potency of human pluripotent stem cell-derived eosinophils in cancer immunotherapy for solid tumors

Published:1 March 2025 DOI: 10.1186/s40164-025-00613-y PMID: 40025520
Sheng Zhu,?Zhengyang Zhou,?Ruixin Gu,?Zixin Zhao,?Yingfeng Zhang,?Yudi Miao,?Qi Lei,?Tianxing Liu,?Guokai Wang,?Chenyi Dai,?Yi Huo,?Jinghao You,?Lejun Lv,?Cheng Li,?Ming Yin,?Chengyan Wang,?Hongkui Deng

Abstract

Background: Efficient tumor T-cell infiltration is crucial for the effectiveness of T-cell-based therapies against solid tumors. Eosinophils play crucial roles in recruiting T cells in solid tumors. Our group has previously generated induced eosinophils (iEOs) from human pluripotent stem cells and exhibited synergistic efficacy with CAR-T cells in solid tumor inhibition. However, administrated eosinophils might influx into inflammatory lungs, posing a potential safety risk. Mitigating the safety concern and enhancing efficacy is a promising development direction for further application of eosinophils.

Methods: We developed a new approach to generate eosinophils with enhanced potency from human chemically reprogrammed induced pluripotent stem cells (hCiPSCs) with the Toll-like receptor (TLR) 7/8 signaling agonist R848.

Results: R848-activated iEOs (R-iEOs) showed significantly decreased influx to the inflamed lungs, indicating a lower risk of causing airway disorders. Furthermore, these R-iEOs had enhanced anti-tumor functions, preferably accumulated at tumor sites, and further increased T-cell infiltration. The combination of R-iEOs and CAR-T cells suppressed tumor growth in mice. Moreover, the chemo-trafficking signaling increased in R-iEOs, which may contribute to the decreased lung influx of R-iEOs and the increased tumor recruitment of T cells.

Conclusion: Our study provides a novel approach to alleviate the potential safety concerns associated with eosinophils while increasing T-cell infiltration in solid tumors. This finding offers a prospective strategy for incorporating eosinophils to improve CAR-T-cell immunotherapy for solid tumors in the future.

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Materials
Procduct Name CAS Molecular Formula Supplier Price
AMG 487 473719-41-4 C32H28F3N5O4 93 suppliers $43.00-$2500.00
AMG 487 473719-41-4 C32H28F3N5O4 93 suppliers $43.00-$2500.00
AMG 487 473719-41-4 C32H28F3N5O4 93 suppliers $43.00-$2500.00
AMG 487 473719-41-4 C32H28F3N5O4 93 suppliers $43.00-$2500.00
(±)-NBI 74330 473722-68-8 C32H27F4N5O3 22 suppliers $91.00-$1622.50
(±)-NBI 74330 473722-68-8 C32H27F4N5O3 22 suppliers $91.00-$1622.50
(±)-NBI 74330 473722-68-8 C32H27F4N5O3 22 suppliers $91.00-$1622.50
(±)-NBI 74330 473722-68-8 C32H27F4N5O3 22 suppliers $91.00-$1622.50

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