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2022 年度 実施状況報告書

Application of gold-catalyzed hydroamination in sialic acids for the cancer-localized in vivo release of an immunotherapy drug

研究課題

研究課題/領域番号 21K05302
研究機関国立研究開発法人理化学研究所

研究代表者

張 宗哲  国立研究開発法人理化学研究所, 開拓研究本部, 特別研究員 (00774853)

研究期間 (年度) 2021-04-01 – 2024-03-31
キーワードSialyltransferase / Prodrug / Acrolein / In vivo synthesis
研究実績の概要

One of the glycan moieties generally overexpressed in cancer are sialic acids, which can induce immunomodulatory properties via binding to Siglec receptors. Therapies are being proposed and tested in animal models that aim to decrease sialic acid on cancer cells that are crucial for maintaining the inflammatory environment in tumors. However, sialyltransferase inhibitors that have been reported to reduce the amount of sialic acid are not selective for cancer cells and could cause side effects such as kidney dysfunction and weight loss. Recently our laboratory found that acrolein is expressed in large amounts in cancer cells. Furthermore, our laboratory has developed a prodrug that can be activated selectively by the reaction with acrolein of cancer cells. Herein, this author attempted to deliver a sialyltransferase inhibitor selectively to the cancer cells by using the [3+2] cycloaddition of azide and acrolein. A prodrug was synthesized by conjugating the hydroxyl group of the sialyltransferase inhibitor with 2, 6-diisopropylphenyl azide via a carbonyl linker. The prodrug reacts with endogenous to give a diazo compound, which subsequently cleave the linker and release of the sialyltransferase inhibitor only in cancer cells.

現在までの達成度 (区分)
現在までの達成度 (区分)

2: おおむね順調に進展している

理由

We have succeeded in finding a specific cancer targeting method, that is, targeting acrolein expressed by cancer cells by [3+2] cycloaddition of azide and acrolein.
With the targeting system, a prodrug composed of a sialyltransferase inhibitor with 2, 6-diisopropylphenyl azide could be able to release the inhibitor to cancer cells via endogenous acrolein. Therefore, we think the system can succeefully inhibit tumors in vivo.

今後の研究の推進方策

In the next step, administration of the prodrug to A549 (lung cancer) and B16F10 (mouse-derived malignant melanoma) cells to reduce fsialic acid on the cancer cells surface will be examined. After that, experiments using a mouse model to examine whether the prodrug can efficiently inhibit tumor growth while reducing the side effects will proceed.

次年度使用額が生じた理由

For purchasing animals for experiments

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公開日: 2023-12-25  

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