Exosome-mediated delivery of inflammation-responsive Il-10 mRNA for controlled atherosclerosis treatment

Rationale: Tailored inflammation control is badly needed for the treatment of kinds of inflammatory diseases, such as atherosclerosis. IL-10 is a potent anti-inflammatory cytokine, while systemic and repeated delivery could cause detrimental side-effects due to immune repression. In this study, we h...

Descripción completa

Detalles Bibliográficos
Autores principales: Bu, Te, Li, Zhelong, Hou, Ying, Sun, Wenqi, Zhang, Rongxin, Zhao, Lianbi, Wei, Mengying, Yang, Guodong, Yuan, Lijun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2021
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8581418/
https://www.ncbi.nlm.nih.gov/pubmed/34815799
http://dx.doi.org/10.7150/thno.64229
_version_ 1784596803940777984
author Bu, Te
Li, Zhelong
Hou, Ying
Sun, Wenqi
Zhang, Rongxin
Zhao, Lianbi
Wei, Mengying
Yang, Guodong
Yuan, Lijun
author_facet Bu, Te
Li, Zhelong
Hou, Ying
Sun, Wenqi
Zhang, Rongxin
Zhao, Lianbi
Wei, Mengying
Yang, Guodong
Yuan, Lijun
author_sort Bu, Te
collection PubMed
description Rationale: Tailored inflammation control is badly needed for the treatment of kinds of inflammatory diseases, such as atherosclerosis. IL-10 is a potent anti-inflammatory cytokine, while systemic and repeated delivery could cause detrimental side-effects due to immune repression. In this study, we have developed a nano-system to deliver inflammation-responsive Il-10 mRNA preferentially into macrophages for tailored inflammation control. Methods: Il-10 was engineered to harbor a modified HCV-IRES (hepatitis C virus internal ribosome entry site), in which the two miR-122 recognition sites were replaced by two miR-155 recognition sites. The translational responsiveness of the engineered mRNA to miR-155 was tested by Western blot or ELISA. Moreover, the engineered Il-10 mRNA was passively encapsulated into exosomes by forced expression in donor cells. Therapeutic effects on atherosclerosis and the systemic leaky expression effects in vivo of the functionalized exosomes were analyzed in ApoE(-/-) (Apolipoprotein E-deficient) mice. Results: The engineered IRES-Il-10 mRNA could be translationally activated in cells when miR-155 was forced expressed or in M1 polarized macrophages with endogenous miR-155 induced. In addition, the engineered IRES-Il-10 mRNA, when encapsulated into the exosomes, could be efficiently delivered into macrophages and some other cell types in the plaque in ApoE(-/-) mice. In the recipient cells of the plaque, the encapsulated Il-10 mRNA was functionally translated into protein, with relatively low leaky in other tissues/organs without obvious inflammation. Consistent with the robust Il-10 induction in the plaque, exosome-based delivery of the engineered Il-10 could alleviate the atherosclerosis in ApoE(-/-) mice. Conclusion: Our study established a potent platform for controlled inflammation control via exosome-based systemic and repeated delivery of engineered Il-10 mRNA, which could be a promising strategy for atherosclerosis treatment.
format Online
Article
Text
id pubmed-8581418
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Ivyspring International Publisher
record_format MEDLINE/PubMed
spelling pubmed-85814182021-11-22 Exosome-mediated delivery of inflammation-responsive Il-10 mRNA for controlled atherosclerosis treatment Bu, Te Li, Zhelong Hou, Ying Sun, Wenqi Zhang, Rongxin Zhao, Lianbi Wei, Mengying Yang, Guodong Yuan, Lijun Theranostics Research Paper Rationale: Tailored inflammation control is badly needed for the treatment of kinds of inflammatory diseases, such as atherosclerosis. IL-10 is a potent anti-inflammatory cytokine, while systemic and repeated delivery could cause detrimental side-effects due to immune repression. In this study, we have developed a nano-system to deliver inflammation-responsive Il-10 mRNA preferentially into macrophages for tailored inflammation control. Methods: Il-10 was engineered to harbor a modified HCV-IRES (hepatitis C virus internal ribosome entry site), in which the two miR-122 recognition sites were replaced by two miR-155 recognition sites. The translational responsiveness of the engineered mRNA to miR-155 was tested by Western blot or ELISA. Moreover, the engineered Il-10 mRNA was passively encapsulated into exosomes by forced expression in donor cells. Therapeutic effects on atherosclerosis and the systemic leaky expression effects in vivo of the functionalized exosomes were analyzed in ApoE(-/-) (Apolipoprotein E-deficient) mice. Results: The engineered IRES-Il-10 mRNA could be translationally activated in cells when miR-155 was forced expressed or in M1 polarized macrophages with endogenous miR-155 induced. In addition, the engineered IRES-Il-10 mRNA, when encapsulated into the exosomes, could be efficiently delivered into macrophages and some other cell types in the plaque in ApoE(-/-) mice. In the recipient cells of the plaque, the encapsulated Il-10 mRNA was functionally translated into protein, with relatively low leaky in other tissues/organs without obvious inflammation. Consistent with the robust Il-10 induction in the plaque, exosome-based delivery of the engineered Il-10 could alleviate the atherosclerosis in ApoE(-/-) mice. Conclusion: Our study established a potent platform for controlled inflammation control via exosome-based systemic and repeated delivery of engineered Il-10 mRNA, which could be a promising strategy for atherosclerosis treatment. Ivyspring International Publisher 2021-10-25 /pmc/articles/PMC8581418/ /pubmed/34815799 http://dx.doi.org/10.7150/thno.64229 Text en © The author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Bu, Te
Li, Zhelong
Hou, Ying
Sun, Wenqi
Zhang, Rongxin
Zhao, Lianbi
Wei, Mengying
Yang, Guodong
Yuan, Lijun
Exosome-mediated delivery of inflammation-responsive Il-10 mRNA for controlled atherosclerosis treatment
title Exosome-mediated delivery of inflammation-responsive Il-10 mRNA for controlled atherosclerosis treatment
title_full Exosome-mediated delivery of inflammation-responsive Il-10 mRNA for controlled atherosclerosis treatment
title_fullStr Exosome-mediated delivery of inflammation-responsive Il-10 mRNA for controlled atherosclerosis treatment
title_full_unstemmed Exosome-mediated delivery of inflammation-responsive Il-10 mRNA for controlled atherosclerosis treatment
title_short Exosome-mediated delivery of inflammation-responsive Il-10 mRNA for controlled atherosclerosis treatment
title_sort exosome-mediated delivery of inflammation-responsive il-10 mrna for controlled atherosclerosis treatment
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8581418/
https://www.ncbi.nlm.nih.gov/pubmed/34815799
http://dx.doi.org/10.7150/thno.64229
work_keys_str_mv AT bute exosomemediateddeliveryofinflammationresponsiveil10mrnaforcontrolledatherosclerosistreatment
AT lizhelong exosomemediateddeliveryofinflammationresponsiveil10mrnaforcontrolledatherosclerosistreatment
AT houying exosomemediateddeliveryofinflammationresponsiveil10mrnaforcontrolledatherosclerosistreatment
AT sunwenqi exosomemediateddeliveryofinflammationresponsiveil10mrnaforcontrolledatherosclerosistreatment
AT zhangrongxin exosomemediateddeliveryofinflammationresponsiveil10mrnaforcontrolledatherosclerosistreatment
AT zhaolianbi exosomemediateddeliveryofinflammationresponsiveil10mrnaforcontrolledatherosclerosistreatment
AT weimengying exosomemediateddeliveryofinflammationresponsiveil10mrnaforcontrolledatherosclerosistreatment
AT yangguodong exosomemediateddeliveryofinflammationresponsiveil10mrnaforcontrolledatherosclerosistreatment
AT yuanlijun exosomemediateddeliveryofinflammationresponsiveil10mrnaforcontrolledatherosclerosistreatment

Ejemplares similares