Engineered immunomodulatory extracellular vesicles derived from epithelial cells acquire capacity for positive and negative T cell co-stimulation in cancer and autoimmunity

Extracellular vesicles (EVs) are generated by all cells and systemic administration of allogenic EVs derived from epithelial and mesenchymal cells have been shown to be safe, despite carrying an array of functional molecules, including thousands of proteins. To address whether epithelial cells deriv...

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Autores principales: Kugeratski, Fernanda G., LeBleu, Valerie S., Dowlatshahi, Dara P., Sugimoto, Hikaru, Arian, Kent A., Fan, Yibo, Huang, Li, Wells, Danielle, Lilla, Sergio, Hodge, Kelly, Zanivan, Sara, McAndrews, Kathleen M., Kalluri, Raghu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory 2023
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10635085/
https://www.ncbi.nlm.nih.gov/pubmed/37961535
http://dx.doi.org/10.1101/2023.11.02.565371
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author Kugeratski, Fernanda G.
LeBleu, Valerie S.
Dowlatshahi, Dara P.
Sugimoto, Hikaru
Arian, Kent A.
Fan, Yibo
Huang, Li
Wells, Danielle
Lilla, Sergio
Hodge, Kelly
Zanivan, Sara
McAndrews, Kathleen M.
Kalluri, Raghu
author_facet Kugeratski, Fernanda G.
LeBleu, Valerie S.
Dowlatshahi, Dara P.
Sugimoto, Hikaru
Arian, Kent A.
Fan, Yibo
Huang, Li
Wells, Danielle
Lilla, Sergio
Hodge, Kelly
Zanivan, Sara
McAndrews, Kathleen M.
Kalluri, Raghu
author_sort Kugeratski, Fernanda G.
collection PubMed
description Extracellular vesicles (EVs) are generated by all cells and systemic administration of allogenic EVs derived from epithelial and mesenchymal cells have been shown to be safe, despite carrying an array of functional molecules, including thousands of proteins. To address whether epithelial cells derived EVs can be modified to acquire the capacity to induce immune response, we engineered 293T EVs to harbor the immunomodulatory CD80, OX40L and PD-L1 molecules. We demonstrated abundant levels of these proteins on the engineered cells and EVs. Functionally, the engineered EVs efficiently elicit positive and negative co-stimulation in human and murine T cells. In the setting of cancer and auto-immune hepatitis, the engineered EVs modulate T cell functions and alter disease progression. Moreover, OX40L EVs provide additional benefit to anti-CTLA-4 treatment in melanoma-bearing mice. Our work provides evidence that epithelial cell derived EVs can be engineered to induce immune responses with translational potential to modulate T cell functions in distinct pathological settings.
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spelling pubmed-106350852023-11-13 Engineered immunomodulatory extracellular vesicles derived from epithelial cells acquire capacity for positive and negative T cell co-stimulation in cancer and autoimmunity Kugeratski, Fernanda G. LeBleu, Valerie S. Dowlatshahi, Dara P. Sugimoto, Hikaru Arian, Kent A. Fan, Yibo Huang, Li Wells, Danielle Lilla, Sergio Hodge, Kelly Zanivan, Sara McAndrews, Kathleen M. Kalluri, Raghu bioRxiv Article Extracellular vesicles (EVs) are generated by all cells and systemic administration of allogenic EVs derived from epithelial and mesenchymal cells have been shown to be safe, despite carrying an array of functional molecules, including thousands of proteins. To address whether epithelial cells derived EVs can be modified to acquire the capacity to induce immune response, we engineered 293T EVs to harbor the immunomodulatory CD80, OX40L and PD-L1 molecules. We demonstrated abundant levels of these proteins on the engineered cells and EVs. Functionally, the engineered EVs efficiently elicit positive and negative co-stimulation in human and murine T cells. In the setting of cancer and auto-immune hepatitis, the engineered EVs modulate T cell functions and alter disease progression. Moreover, OX40L EVs provide additional benefit to anti-CTLA-4 treatment in melanoma-bearing mice. Our work provides evidence that epithelial cell derived EVs can be engineered to induce immune responses with translational potential to modulate T cell functions in distinct pathological settings. Cold Spring Harbor Laboratory 2023-11-04 /pmc/articles/PMC10635085/ /pubmed/37961535 http://dx.doi.org/10.1101/2023.11.02.565371 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (https://creativecommons.org/licenses/by-nc-nd/4.0/) , which allows reusers to copy and distribute the material in any medium or format in unadapted form only, for noncommercial purposes only, and only so long as attribution is given to the creator.
spellingShingle Article
Kugeratski, Fernanda G.
LeBleu, Valerie S.
Dowlatshahi, Dara P.
Sugimoto, Hikaru
Arian, Kent A.
Fan, Yibo
Huang, Li
Wells, Danielle
Lilla, Sergio
Hodge, Kelly
Zanivan, Sara
McAndrews, Kathleen M.
Kalluri, Raghu
Engineered immunomodulatory extracellular vesicles derived from epithelial cells acquire capacity for positive and negative T cell co-stimulation in cancer and autoimmunity
title Engineered immunomodulatory extracellular vesicles derived from epithelial cells acquire capacity for positive and negative T cell co-stimulation in cancer and autoimmunity
title_full Engineered immunomodulatory extracellular vesicles derived from epithelial cells acquire capacity for positive and negative T cell co-stimulation in cancer and autoimmunity
title_fullStr Engineered immunomodulatory extracellular vesicles derived from epithelial cells acquire capacity for positive and negative T cell co-stimulation in cancer and autoimmunity
title_full_unstemmed Engineered immunomodulatory extracellular vesicles derived from epithelial cells acquire capacity for positive and negative T cell co-stimulation in cancer and autoimmunity
title_short Engineered immunomodulatory extracellular vesicles derived from epithelial cells acquire capacity for positive and negative T cell co-stimulation in cancer and autoimmunity
title_sort engineered immunomodulatory extracellular vesicles derived from epithelial cells acquire capacity for positive and negative t cell co-stimulation in cancer and autoimmunity
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10635085/
https://www.ncbi.nlm.nih.gov/pubmed/37961535
http://dx.doi.org/10.1101/2023.11.02.565371
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