IL-2K35C-moFA, a Long-Acting Engineered Cytokine with Decreased Interleukin 2 Receptor α Binding, Improved the Cellular Selectivity Profile and Antitumor Efficacy in a Mouse Tumor Model

SIMPLE SUMMARY: The application of IL-2 for treating cancer is limited owing to its toxicity and short half-life. Its high binding ability to IL-2 receptor α expands immunosuppressive Treg cells, which represents an undesirable toxicity in cancer immunotherapy. Moreover, its small molecular size is...

Descripción completa

Detalles Bibliográficos
Autores principales: Wang, Xiaoze, Chen, Gang, Nie, Lei, Wu, Zhenhua, Wang, Xinzeng, Pan, Chenxiao, Chen, Xuchen, Zhao, Xiaobei, Zhu, Jie, He, Qiaojun, Wang, Haibin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9563011/
https://www.ncbi.nlm.nih.gov/pubmed/36230665
http://dx.doi.org/10.3390/cancers14194742
_version_ 1784808305171890176
author Wang, Xiaoze
Chen, Gang
Nie, Lei
Wu, Zhenhua
Wang, Xinzeng
Pan, Chenxiao
Chen, Xuchen
Zhao, Xiaobei
Zhu, Jie
He, Qiaojun
Wang, Haibin
author_facet Wang, Xiaoze
Chen, Gang
Nie, Lei
Wu, Zhenhua
Wang, Xinzeng
Pan, Chenxiao
Chen, Xuchen
Zhao, Xiaobei
Zhu, Jie
He, Qiaojun
Wang, Haibin
author_sort Wang, Xiaoze
collection PubMed
description SIMPLE SUMMARY: The application of IL-2 for treating cancer is limited owing to its toxicity and short half-life. Its high binding ability to IL-2 receptor α expands immunosuppressive Treg cells, which represents an undesirable toxicity in cancer immunotherapy. Moreover, its small molecular size is the reason for its short half-life. We solved these problems by using a covalent modification strategy of IL-2 variant IL-2K35C with fatty acid by maleimide chemistry, namely, IL-2K35C-moFA. The experiments performed in vitro and in vivo proved that IL-2K35C-moFA is a novel immunotherapeutic agent with the potential to selectively stimulate CD8(+) T cells and NK cells. Compared to IL-2WT, IL-2K35C-moFA showed a specifically reduced potency for the stimulation of Treg cells. Our results also showed that fatty acid conjugation appears to be effective in half-life extension. The combination of selective lymphocyte expansion and its long half-life means IL-2K35C-moFA should be evaluated as a potential human immunotherapeutic in the future. ABSTRACT: Human interleukin 2 (IL-2) has shown impressive results as a therapeutic agent for cancer. However, IL-2-based cancer therapy is limited by strong Treg amplification owing to its high binding affinity to IL-2 receptor α (IL-2Rα) and its short half-life owing to its small molecular size. In this study, we solved these problems using a covalent modification strategy of the IL-2 variant, i.e., substituting cysteine (C) for lysine (K) at position 35, using octadecanedicarboxylic acid through maleimide chemistry, creating IL-2K35C-moFA. IL-2K35C-moFA was equipotent to human IL-2 wild type (IL-2WT) in activating tumor-killing CD8(+) memory effector T cells (CD8(+) T) and NK cells bearing the intermediate affinity IL-2 receptors, and less potent than IL-2WT on CTLL-2 cells bearing the high-affinity IL-2 receptors. Moreover, it was shown to support the preferential activation of IL-2 receptor β (IL-2Rβ) over IL-2Rα because of the mutation and fatty acid conjugation. In a B16F10 murine tumor model, IL-2K35C-moFA showed efficacy as a single dose and provided durable immunity for 1 week. Our results support the further evaluation of IL-2K35C-moFA as a novel cancer immunotherapy.
format Online
Article
Text
id pubmed-9563011
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-95630112022-10-15 IL-2K35C-moFA, a Long-Acting Engineered Cytokine with Decreased Interleukin 2 Receptor α Binding, Improved the Cellular Selectivity Profile and Antitumor Efficacy in a Mouse Tumor Model Wang, Xiaoze Chen, Gang Nie, Lei Wu, Zhenhua Wang, Xinzeng Pan, Chenxiao Chen, Xuchen Zhao, Xiaobei Zhu, Jie He, Qiaojun Wang, Haibin Cancers (Basel) Article SIMPLE SUMMARY: The application of IL-2 for treating cancer is limited owing to its toxicity and short half-life. Its high binding ability to IL-2 receptor α expands immunosuppressive Treg cells, which represents an undesirable toxicity in cancer immunotherapy. Moreover, its small molecular size is the reason for its short half-life. We solved these problems by using a covalent modification strategy of IL-2 variant IL-2K35C with fatty acid by maleimide chemistry, namely, IL-2K35C-moFA. The experiments performed in vitro and in vivo proved that IL-2K35C-moFA is a novel immunotherapeutic agent with the potential to selectively stimulate CD8(+) T cells and NK cells. Compared to IL-2WT, IL-2K35C-moFA showed a specifically reduced potency for the stimulation of Treg cells. Our results also showed that fatty acid conjugation appears to be effective in half-life extension. The combination of selective lymphocyte expansion and its long half-life means IL-2K35C-moFA should be evaluated as a potential human immunotherapeutic in the future. ABSTRACT: Human interleukin 2 (IL-2) has shown impressive results as a therapeutic agent for cancer. However, IL-2-based cancer therapy is limited by strong Treg amplification owing to its high binding affinity to IL-2 receptor α (IL-2Rα) and its short half-life owing to its small molecular size. In this study, we solved these problems using a covalent modification strategy of the IL-2 variant, i.e., substituting cysteine (C) for lysine (K) at position 35, using octadecanedicarboxylic acid through maleimide chemistry, creating IL-2K35C-moFA. IL-2K35C-moFA was equipotent to human IL-2 wild type (IL-2WT) in activating tumor-killing CD8(+) memory effector T cells (CD8(+) T) and NK cells bearing the intermediate affinity IL-2 receptors, and less potent than IL-2WT on CTLL-2 cells bearing the high-affinity IL-2 receptors. Moreover, it was shown to support the preferential activation of IL-2 receptor β (IL-2Rβ) over IL-2Rα because of the mutation and fatty acid conjugation. In a B16F10 murine tumor model, IL-2K35C-moFA showed efficacy as a single dose and provided durable immunity for 1 week. Our results support the further evaluation of IL-2K35C-moFA as a novel cancer immunotherapy. MDPI 2022-09-28 /pmc/articles/PMC9563011/ /pubmed/36230665 http://dx.doi.org/10.3390/cancers14194742 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Wang, Xiaoze
Chen, Gang
Nie, Lei
Wu, Zhenhua
Wang, Xinzeng
Pan, Chenxiao
Chen, Xuchen
Zhao, Xiaobei
Zhu, Jie
He, Qiaojun
Wang, Haibin
IL-2K35C-moFA, a Long-Acting Engineered Cytokine with Decreased Interleukin 2 Receptor α Binding, Improved the Cellular Selectivity Profile and Antitumor Efficacy in a Mouse Tumor Model
title IL-2K35C-moFA, a Long-Acting Engineered Cytokine with Decreased Interleukin 2 Receptor α Binding, Improved the Cellular Selectivity Profile and Antitumor Efficacy in a Mouse Tumor Model
title_full IL-2K35C-moFA, a Long-Acting Engineered Cytokine with Decreased Interleukin 2 Receptor α Binding, Improved the Cellular Selectivity Profile and Antitumor Efficacy in a Mouse Tumor Model
title_fullStr IL-2K35C-moFA, a Long-Acting Engineered Cytokine with Decreased Interleukin 2 Receptor α Binding, Improved the Cellular Selectivity Profile and Antitumor Efficacy in a Mouse Tumor Model
title_full_unstemmed IL-2K35C-moFA, a Long-Acting Engineered Cytokine with Decreased Interleukin 2 Receptor α Binding, Improved the Cellular Selectivity Profile and Antitumor Efficacy in a Mouse Tumor Model
title_short IL-2K35C-moFA, a Long-Acting Engineered Cytokine with Decreased Interleukin 2 Receptor α Binding, Improved the Cellular Selectivity Profile and Antitumor Efficacy in a Mouse Tumor Model
title_sort il-2k35c-mofa, a long-acting engineered cytokine with decreased interleukin 2 receptor α binding, improved the cellular selectivity profile and antitumor efficacy in a mouse tumor model
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9563011/
https://www.ncbi.nlm.nih.gov/pubmed/36230665
http://dx.doi.org/10.3390/cancers14194742
work_keys_str_mv AT wangxiaoze il2k35cmofaalongactingengineeredcytokinewithdecreasedinterleukin2receptorabindingimprovedthecellularselectivityprofileandantitumorefficacyinamousetumormodel
AT chengang il2k35cmofaalongactingengineeredcytokinewithdecreasedinterleukin2receptorabindingimprovedthecellularselectivityprofileandantitumorefficacyinamousetumormodel
AT nielei il2k35cmofaalongactingengineeredcytokinewithdecreasedinterleukin2receptorabindingimprovedthecellularselectivityprofileandantitumorefficacyinamousetumormodel
AT wuzhenhua il2k35cmofaalongactingengineeredcytokinewithdecreasedinterleukin2receptorabindingimprovedthecellularselectivityprofileandantitumorefficacyinamousetumormodel
AT wangxinzeng il2k35cmofaalongactingengineeredcytokinewithdecreasedinterleukin2receptorabindingimprovedthecellularselectivityprofileandantitumorefficacyinamousetumormodel
AT panchenxiao il2k35cmofaalongactingengineeredcytokinewithdecreasedinterleukin2receptorabindingimprovedthecellularselectivityprofileandantitumorefficacyinamousetumormodel
AT chenxuchen il2k35cmofaalongactingengineeredcytokinewithdecreasedinterleukin2receptorabindingimprovedthecellularselectivityprofileandantitumorefficacyinamousetumormodel
AT zhaoxiaobei il2k35cmofaalongactingengineeredcytokinewithdecreasedinterleukin2receptorabindingimprovedthecellularselectivityprofileandantitumorefficacyinamousetumormodel
AT zhujie il2k35cmofaalongactingengineeredcytokinewithdecreasedinterleukin2receptorabindingimprovedthecellularselectivityprofileandantitumorefficacyinamousetumormodel
AT heqiaojun il2k35cmofaalongactingengineeredcytokinewithdecreasedinterleukin2receptorabindingimprovedthecellularselectivityprofileandantitumorefficacyinamousetumormodel
AT wanghaibin il2k35cmofaalongactingengineeredcytokinewithdecreasedinterleukin2receptorabindingimprovedthecellularselectivityprofileandantitumorefficacyinamousetumormodel

Ejemplares similares