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. 2022 Dec 23;61(52):e202214992.
doi: 10.1002/anie.202214992. Epub 2022 Nov 24.

Tumor-Selective Activation of Toll-Like Receptor 7/8 Agonist Nano-Immunomodulator Generates Safe Anti-Tumor Immune Responses upon Systemic Administration

Yanyun Hao  1 Hui Li  1 Xiaoyan Ge  1 Yang Liu  1 Xia Li  1 Yutong Liu  1 Hongfei Chen  1 Shiying Zhang  1 Jing Zou  1 Lingling Huang  1 Fabao Zhao  2 Dongwei Kang  2 Bruno G De Geest  3 Zhiyue Zhang  1
Affiliations

Tumor-Selective Activation of Toll-Like Receptor 7/8 Agonist Nano-Immunomodulator Generates Safe Anti-Tumor Immune Responses upon Systemic Administration

Yanyun Hao et al. Angew Chem Int Ed Engl. .

Abstract

Agonists of innate pattern recognition receptors such as toll-like receptors (TLRs) prime adaptive anti-tumor immunity and hold promise for cancer immunotherapy. However, small-molecule TLR agonists cause immune-related adverse effects (irAEs) after systemic administration. Herein, we report a polymeric nano-immunomodulator (cN@SS-IMQ) that is inactive until it is selectively metabolized to an active immunostimulant within the tumor. cN@SS-IMQ was obtained via self-assembly of a cyclo(Arg-Gly-Asp-D-Phe-Lys)-modified amphiphilic copolymeric prodrug. Upon systemic administration, cN@SS-IMQ preferentially accumulated at tumor sites and responded to high intracellular glutathione levels to release native imidazoquinolines for dendritic cell maturation, thereby enhancing the infiltration of T lymphocytes. Collectively, cN@SS-IMQ tends to activate the immune system without irAEs, thus suggesting its promising potential for safe systemic targeting delivery.

Keywords: Glutathione-Responsiveness; Imidazoquinolines; Immunotherapy; Systemic Administration; Toll-Like Receptors.

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References

    1. F. Baharom, R. A. Ramirez-Valdez, K. K. S. Tobin, H. Yamane, C. A. Dutertre, A. Khalilnezhad, G. V. Reynoso, V. L. Coble, G. M. Lynn, M. P. Mule, A. J. Martins, J. P. Finnigan, X. M. Zhang, J. A. Hamerman, N. Bhardwaj, J. S. Tsang, H. D. Hickman, F. Ginhoux, A. S. Ishizuka, R. A. Seder, Nat. Immunol. 2021, 22, 41-52.
    1. L. A. O′Neill, D. Golenbock, A. G. Bowie, Nat. Rev. Immunol. 2013, 13, 453-460.
    1. None
    1. W. G. Kerr, J. D. Chisholm, J. Immunol. 2019, 202, 11-19;
    1. B. Singh, S. Maharjan, D. C. Pan, Z. Zhao, Y. Gao, Y. S. Zhang, S. Mitragotri, Biomaterials 2022, 280, 121302.

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