Targeting and Suppression of Survivin in Cancer Cells Based on the Interaction of Cell Surface Vimentin with N-Acetylglucosamine-Bearing Polymers - 九大コレクション | 九州大学附属図書館

＜学術雑誌論文＞
Targeting and Suppression of Survivin in Cancer Cells Based on the Interaction of Cell Surface Vimentin with N-Acetylglucosamine-Bearing Polymers

作成者	作成者名 Kitagawa, Karera 北川, 佳玲良キタガワ, カレラ所属機関所属機関名 Applied Chemistry, Graduate School of Engineering, Kyushu University 九州大学大学院工学府応用化学専攻
	著者識別子 0000-0002-8357-8654 作成者名 Kobayashi, Shingo 小林, 慎吾コバヤシ, シンゴ所属機関所属機関名 Institute for Materials Chemistry and Engineering, Kyushu University 九州大学先導物質化学研究所
	著者識別子 100020077 0000-0001-8590-6079 作成者名 Miura, Yoshiko 三浦, 佳子ミウラ, ヨシコ所属機関所属機関名 Chemical Engineering, Graduate School of Engineering, Kyushu University 九州大学大学院工学研究院化学工学部門
	著者識別子 100022941 0000-0002-1115-2080 作成者名 Tanaka, Masaru 田中, 賢タナカ, マサル所属機関所属機関名 Institute for Materials Chemistry and Engineering, Kyushu University 九州大学先導物質化学研究所
	著者識別子 100022773 0000-0002-4948-9375 作成者名 Ise, Hirohiko 伊勢, 裕彦イセ, ヒロヒコ所属機関所属機関名 Institute for Materials Chemistry and Engineering, Kyushu University 九州大学先導物質化学研究所
本文言語	英語
出版者	American Chemical Society (ACS)
発行日	2025-08-13
収録物名	ACS Omega
出版タイプ	Version of Record
アクセス権	open access
権利関係	© 2025 The Authors.
権利関係	Creative Commons Attribution-NonCommercial-NoDerivs 4.0 International
関連DOI	以下と同一 https://doi.org/10.1021/acsomega.5c02098
関連URI
関連HDL
概要	Survivin, a protein overexpressed in various fetal and malignant tumor tissues, induces tumor progression and resistance to cancer therapy. Cell surface vimentin has N-acetylglucosamine (GlcNAc)-bindi...ng activities in several cell types including tumor cells. Furthermore, GlcNAc-bearing polymers downregulate the expression of the survivin-encoding baculoviral inhibitor of apoptosis protein repeat-containing protein 5 (BIRC5). Thus, cell surface vimentin is a target for cancer therapy. The downregulation of survivin expression in cancer cells by selectively targeting cell surface vimentin with GlcNAc-bearing polymers may mitigate drug resistance. However, the ability of GlcNAc to bind to cell surface vimentin depends on its valency in GlcNAc-bearing polymers. The optimal GlcNAc valency for the interaction remains unknown. Therefore, we aimed to develop optimal GlcNAc-bearing polymers for effective cancer therapy. In this study, GlcNAc polymers of various lengths were synthesized through reversible addition/fragmentation chain-transfer polymerization. We found that a low-molecular-weight GlcNAc polymer (5 GlcNAc-mer) interacted with cell surface vimentin-expressing cells to a greater extent than high-molecular-weight GlcNAc polymers (10 and 20 GlcNAc-mer). These interactions upregulated the expression of p53, an upstream signal transducer. Moreover, they inhibited the phosphorylation of signal transducers and activators of transcription 3 and downregulated survivin expression. In addition, low-molecular-weight GlcNAc polymers decreased the viability of 3LL cells, mouse lung carcinoma cell lines, and MCF-7 cells, human breast cancer lines, but not that of MCF10A, nontumorigenic breast cells. These findings suggest that low-molecular-weight GlcNAc polymers, which selectively target cancer cells and downregulate survivin expression, are promising tools for cancer therapy.続きを見る

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詳細

PISSN	2470-1343
EISSN	2470-1343
レコードID	7378069
主題	Cancer
	Cells
	Genetics
	Peptides and proteins
	Polymers
タイプ	Article
助成情報	助成機関名 Japan Society for the Promotion of Science (JSPS) 日本学術振興会研究課題番号 JP22K12818 研究課題名 O-GlcNAc化タンパク質の生体修復機構解明とそれに基づいた線維症治療戦略創成
助成情報	助成機関名 Japan Society for the Promotion of Science (JSPS) 日本学術振興会研究課題名 Cooperative Research Program of the Network Joint Research Center for Materials and Devices 物質・デバイス領域共同研究拠点
登録日	2025.08.22
更新日	2025.08.22