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dc.contributor.author Shin, Hyun Young -
dc.contributor.author Jang, Seil -
dc.contributor.author Woo, Hyeong Jung -
dc.contributor.author Chung, Jae-Hee -
dc.contributor.author Kim, Woon-Hae -
dc.contributor.author Kim, Dongoh -
dc.contributor.author Kang, Minju -
dc.contributor.author Lim, Yujin -
dc.contributor.author Habib, Omer -
dc.contributor.author Lee, Jungmin -
dc.contributor.author Yang, Sohae -
dc.contributor.author Lee, Dae Hee -
dc.contributor.author Kim, Minseok S. -
dc.date.accessioned 2023-07-23T18:40:18Z -
dc.date.available 2023-07-23T18:40:18Z -
dc.date.created 2023-04-21 -
dc.date.issued 2023-03 -
dc.identifier.issn 1838-7640 -
dc.identifier.uri http://hdl.handle.net/20.500.11750/46225 -
dc.description.abstract Natural killer (NK) cells are an attractive cell source in cancer immunotherapy due to their potent antitumor ability and promising safety for allogenic applications. However, the clinical outcome of NK cell therapy has been limited due to poor persistence and loss of activity in the cytokine-deficient tumor microenvironment. Benefits from exogenous administration of soluble interleukin-2 (IL-2) to stimulate the activity of NK cells have not been significant due to cytokine consumption and activation of other immune cells, compromising both efficacy and safety. Methods: To overcome these drawbacks, we developed a novel membrane-bound protein (MBP) technology to express IL-2 on the surface of NK-92 cells (MBP NK) inducing autocrine signal for proliferation without IL-2 supplementation. Results: The MBP NK cells exhibited not only improved proliferation in IL-2 deficient conditions but also stronger secretion of cytolytic granules leading to enhanced anti-tumor activity both in vitro and in vivo. Furthermore, the experiment with a spheroid solid tumor model exhibited enhanced infiltration by MBP NK cells creating higher local effector-to-target ratio for efficient tumor killing. These results suggest MBP technology can be an effective utility for NK-92 cell engineering to increase anti-tumor activity and reduce potential adverse effects, providing a higher therapeutic index in clinical applications. © 2023 Ivyspring International Publisher. All rights reserved. -
dc.language English -
dc.publisher Ivyspring International Publisher -
dc.title Cytokine engineered NK-92 therapy to improve persistence and anti-tumor activity -
dc.type Article -
dc.identifier.doi 10.7150/thno.79942 -
dc.identifier.wosid 000994913400003 -
dc.identifier.scopusid 2-s2.0-85152210626 -
dc.identifier.bibliographicCitation Theranostics, v.13, no.5, pp.1506 - 1519 -
dc.description.isOpenAccess TRUE -
dc.subject.keywordAuthor membrane-bound protein (MBP) -
dc.subject.keywordAuthor interleukin-2 -
dc.subject.keywordAuthor self-activation -
dc.subject.keywordAuthor tumor-infiltrating lymphocytes -
dc.subject.keywordAuthor microwell array chip -
dc.subject.keywordAuthor natural killer cell -
dc.subject.keywordPlus NK CELLS -
dc.subject.keywordPlus SAFETY -
dc.subject.keywordPlus CANCER -
dc.identifier.url https://www.thno.org/cover/v13i5.jpg -
dc.citation.endPage 1519 -
dc.citation.number 5 -
dc.citation.startPage 1506 -
dc.citation.title Theranostics -
dc.citation.volume 13 -
dc.description.journalRegisteredClass scie -
dc.description.journalRegisteredClass scopus -
dc.relation.journalResearchArea Research & Experimental Medicine -
dc.relation.journalWebOfScienceCategory Medicine, Research & Experimental -
dc.type.docType Article -
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Appears in Collections:
Department of New Biology BioDr. Lab - Nanobiomedicine 1. Journal Articles

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