A nanoadjuvant that dynamically coordinates innate immune stimuli activation enhances cancer immunotherapy and reduces immune cell exhaustion

Seung Mo Jin; Yeon Jeong Yoo; Hong Sik Shin; Sohyun Kim; Sang Nam Lee; Chang Hoon Lee; Hyunji Kim; Jung Eun Kim; Yong Soo Bae; Jung Hyub Hong; Young Woock Noh; Yong Taik Lim

doi:10.1038/s41565-022-01296-w

A nanoadjuvant that dynamically coordinates innate immune stimuli activation enhances cancer immunotherapy and reduces immune cell exhaustion

Seung Mo Jin
, Yeon Jeong Yoo
, Hong Sik Shin
, Sohyun Kim
, Sang Nam Lee
, Chang Hoon Lee
, Hyunji Kim
, Jung Eun Kim
, Yong Soo Bae
, Jung Hyub Hong
, Young Woock Noh
, Yong Taik Lim

Research output: Contribution to journal › Article › peer-review

97 Scopus citations

Abstract

Although conventional innate immune stimuli contribute to immune activation, they induce exhausted immune cells, resulting in suboptimal cancer immunotherapy. Here we suggest a kinetically activating nanoadjuvant (K-nanoadjuvant) that can dynamically integrate two waves of innate immune stimuli, resulting in effective antitumour immunity without immune cell exhaustion. The combinatorial code of K-nanoadjuvant is optimized in terms of the order, duration and time window between spatiotemporally activating Toll-like receptor 7/8 agonist and other Toll-like receptor agonists. K-nanoadjuvant induces effector/non-exhausted dendritic cells that programme the magnitude and persistence of interleukin-12 secretion, generate effector/non-exhausted CD8⁺ T cells, and activate natural killer cells. Treatment with K-nanoadjuvant as a monotherapy or in combination therapy with anti-PD-L1 or liposomes (doxorubicin) results in strong antitumour immunity in murine models, with minimal systemic toxicity, providing a strategy for synchronous and dynamic tailoring of innate immunity for enhanced cancer immunotherapy.

Original language	English
Pages (from-to)	390-402
Number of pages	13
Journal	Nature Nanotechnology
Volume	18
Issue number	4
DOIs	https://doi.org/10.1038/s41565-022-01296-w
State	Published - Apr 2023
Externally published	Yes

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Jin, S. M., Yoo, Y. J., Shin, H. S., Kim, S., Lee, S. N., Lee, C. H., Kim, H., Kim, J. E., Bae, Y. S., Hong, J. H., Noh, Y. W., & Lim, Y. T. (2023). A nanoadjuvant that dynamically coordinates innate immune stimuli activation enhances cancer immunotherapy and reduces immune cell exhaustion. Nature Nanotechnology, 18(4), 390-402. https://doi.org/10.1038/s41565-022-01296-w

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title = "A nanoadjuvant that dynamically coordinates innate immune stimuli activation enhances cancer immunotherapy and reduces immune cell exhaustion",

abstract = "Although conventional innate immune stimuli contribute to immune activation, they induce exhausted immune cells, resulting in suboptimal cancer immunotherapy. Here we suggest a kinetically activating nanoadjuvant (K-nanoadjuvant) that can dynamically integrate two waves of innate immune stimuli, resulting in effective antitumour immunity without immune cell exhaustion. The combinatorial code of K-nanoadjuvant is optimized in terms of the order, duration and time window between spatiotemporally activating Toll-like receptor 7/8 agonist and other Toll-like receptor agonists. K-nanoadjuvant induces effector/non-exhausted dendritic cells that programme the magnitude and persistence of interleukin-12 secretion, generate effector/non-exhausted CD8+ T cells, and activate natural killer cells. Treatment with K-nanoadjuvant as a monotherapy or in combination therapy with anti-PD-L1 or liposomes (doxorubicin) results in strong antitumour immunity in murine models, with minimal systemic toxicity, providing a strategy for synchronous and dynamic tailoring of innate immunity for enhanced cancer immunotherapy.",

author = "Jin, \{Seung Mo\} and Yoo, \{Yeon Jeong\} and Shin, \{Hong Sik\} and Sohyun Kim and Lee, \{Sang Nam\} and Lee, \{Chang Hoon\} and Hyunji Kim and Kim, \{Jung Eun\} and Bae, \{Yong Soo\} and Hong, \{Jung Hyub\} and Noh, \{Young Woock\} and Lim, \{Yong Taik\}",

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year = "2023",

month = apr,

doi = "10.1038/s41565-022-01296-w",

language = "English",

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AU - Jin, Seung Mo

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AU - Kim, Sohyun

AU - Lee, Sang Nam

AU - Lee, Chang Hoon

AU - Kim, Hyunji

AU - Kim, Jung Eun

AU - Bae, Yong Soo

AU - Hong, Jung Hyub

AU - Noh, Young Woock

AU - Lim, Yong Taik

PY - 2023/4

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AB - Although conventional innate immune stimuli contribute to immune activation, they induce exhausted immune cells, resulting in suboptimal cancer immunotherapy. Here we suggest a kinetically activating nanoadjuvant (K-nanoadjuvant) that can dynamically integrate two waves of innate immune stimuli, resulting in effective antitumour immunity without immune cell exhaustion. The combinatorial code of K-nanoadjuvant is optimized in terms of the order, duration and time window between spatiotemporally activating Toll-like receptor 7/8 agonist and other Toll-like receptor agonists. K-nanoadjuvant induces effector/non-exhausted dendritic cells that programme the magnitude and persistence of interleukin-12 secretion, generate effector/non-exhausted CD8+ T cells, and activate natural killer cells. Treatment with K-nanoadjuvant as a monotherapy or in combination therapy with anti-PD-L1 or liposomes (doxorubicin) results in strong antitumour immunity in murine models, with minimal systemic toxicity, providing a strategy for synchronous and dynamic tailoring of innate immunity for enhanced cancer immunotherapy.

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JO - Nature Nanotechnology

JF - Nature Nanotechnology

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ER -

A nanoadjuvant that dynamically coordinates innate immune stimuli activation enhances cancer immunotherapy and reduces immune cell exhaustion

Abstract

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