| Form of presentation | Articles in international journals and collections |
| Year of publication | 2021 |
| Язык | английский |
|
Kurbangalieva Almira Rafaelovna, author
Nasibullin Igor Olegovich, author
Tanaka Kacunori , author
|
|
Nakao Yoichi , author
Onoe Hirotaka , author
Tahara Tsuyoshi , author
Tsubokura Kazuki , author
Urano Sayaka , author
Vong Kenward , author
Watanabe Yasuyoshi , author
|
| Bibliographic description in the original language |
Vong, K. Disrupting tumor onset and growth via selective cell tagging (SeCT) therapy / K. Vong, T. Tahara, S. Urano, I. Nasibullin, K. Tsubokura, Y. Nakao, A. Kurbangalieva, H. Onoe, Y. Watanabe, K. Tanaka // Sci. Adv. – 2021. – V. 7, № 17. – Art. № eabg4038. |
| Annotation |
This study presents the early framework of selective cell tagging (SeCT) therapy, which is the concept of preferentially labeling specific cells in vivo with chemical moieties that can elicit a therapeutic response. Using glycosylated artificial metalloenzyme (GArM)–based protein labeling, this study reports two separate functional strategies. In one approach, early tumor onset can be suppressed by tagging cancer cells in living mice with an integrin-blocking cyclic–Arg-Gly-Asp (cRGD) moiety, thereby disrupting cell adhesion onto the extracellular matrix. In another approach, tumor growth in mice can be reduced by tagging with a cytotoxic doxorubicin moiety. Subsequent cell death occurs following internalization and drug release. Overall, experiments have shown that mouse populations receiving the mixture of SeCT labeling reagents exhibited a significant delay/reduction in tumor onset and growth compared with controls. Highlighting its adaptability, this work represents a foundational step for further development of SeCT therapy and its potential therapeutic applications. |
| Keywords |
cell tagging (SeCT) therapy, glycosylated artificial metalloenzyme, protein labeling, |
| The name of the journal |
Science advances
|
| URL |
https://www.science.org/doi/10.1126/sciadv.abg4038 |
| Please use this ID to quote from or refer to the card |
https://repository.kpfu.ru/eng/?p_id=253584&p_lang=2 |
Full metadata record  |
| Field DC |
Value |
Language |
| dc.contributor.author |
Kurbangalieva Almira Rafaelovna |
ru_RU |
| dc.contributor.author |
Nasibullin Igor Olegovich |
ru_RU |
| dc.contributor.author |
Tanaka Kacunori |
ru_RU |
| dc.contributor.author |
Nakao Yoichi |
ru_RU |
| dc.contributor.author |
Onoe Hirotaka |
ru_RU |
| dc.contributor.author |
Tahara Tsuyoshi |
ru_RU |
| dc.contributor.author |
Tsubokura Kazuki |
ru_RU |
| dc.contributor.author |
Urano Sayaka |
ru_RU |
| dc.contributor.author |
Vong Kenward |
ru_RU |
| dc.contributor.author |
Watanabe Yasuyoshi |
ru_RU |
| dc.date.accessioned |
2021-01-01T00:00:00Z |
ru_RU |
| dc.date.available |
2021-01-01T00:00:00Z |
ru_RU |
| dc.date.issued |
2021 |
ru_RU |
| dc.identifier.citation |
Vong, K. Disrupting tumor onset and growth via selective cell tagging (SeCT) therapy / K. Vong, T. Tahara, S. Urano, I. Nasibullin, K. Tsubokura, Y. Nakao, A. Kurbangalieva, H. Onoe, Y. Watanabe, K. Tanaka // Sci. Adv. – 2021. – V. 7, № 17. – Art. № eabg4038. |
ru_RU |
| dc.identifier.uri |
https://repository.kpfu.ru/eng/?p_id=253584&p_lang=2 |
ru_RU |
| dc.description.abstract |
Science advances |
ru_RU |
| dc.description.abstract |
This study presents the early framework of selective cell tagging (SeCT) therapy, which is the concept of preferentially labeling specific cells in vivo with chemical moieties that can elicit a therapeutic response. Using glycosylated artificial metalloenzyme (GArM)–based protein labeling, this study reports two separate functional strategies. In one approach, early tumor onset can be suppressed by tagging cancer cells in living mice with an integrin-blocking cyclic–Arg-Gly-Asp (cRGD) moiety, thereby disrupting cell adhesion onto the extracellular matrix. In another approach, tumor growth in mice can be reduced by tagging with a cytotoxic doxorubicin moiety. Subsequent cell death occurs following internalization and drug release. Overall, experiments have shown that mouse populations receiving the mixture of SeCT labeling reagents exhibited a significant delay/reduction in tumor onset and growth compared with controls. Highlighting its adaptability, this work represents a foundational step for further development of SeCT therapy and its potential therapeutic applications. |
ru_RU |
| dc.language.iso |
ru |
ru_RU |
| dc.subject |
cell tagging (SeCT) therapy |
ru_RU |
| dc.subject |
glycosylated artificial metalloenzyme |
ru_RU |
| dc.subject |
protein labeling |
ru_RU |
| dc.subject |
|
ru_RU |
| dc.title |
Disrupting tumor onset and growth via selective cell tagging (SeCT) therapy |
ru_RU |
| dc.type |
Articles in international journals and collections |
ru_RU |
|
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