Chia Nan University of Pharmacy & Science Institutional Repository:Item 310902800/33574
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    CNU IR > Pharmacy and Science > 2017 >  Item 310902800/33574
    Please use this identifier to cite or link to this item: https://ir.cnu.edu.tw/handle/310902800/33574


    Title: Enhancing the Yield of 10-HydroxycamptothecinGlucuronide Prodrug.
    Authors: 陳國輝
    邱沛芳
    Contributors: 藥學系
    Date: 2017
    Issue Date: 2022-01-25 14:45:14 (UTC+8)
    Abstract: For chemotherapy, many chemotherapy target rapidly proliferating cells, these therapies might act at cell cycle. So the drug has not tumor specificity, it will cause severe side effects. In order to increase the tumor targeting, we accord to the strategy of prodrug. We design and synthesize glucuronide prodrug of 10-hydroxycamptothecin. Make the anti-tumor drug, 10-hydroxycamptothecin, conjugate with β-D-glucuronic acid to improve drug’s tumor specific and water solubility. Then, 10-hydroxycamptothecin connect conjugate with β-D-glucuronic acid via a self-immolative 3-methylpiperazine benzyl ether linker. The linker improve the prodrug affinity for β-glucuronidase. However, the benzyl ether linkage is nonpolar groups, which reduce water solubility, then will increase cytotoxity to normal cell. In order to improve solubility of prodrug. We created the 3-methylpiperazine group on benzyl ether, it is tertiary amine which will improve water solubility and reduce the prodrug impermeability to normal cell. When the spacer including the 3-methylpiperazine group on benzyl ether, it is more bulk group than benzyl ether, this benzyl group conduction with the 10-hydorxycamptothecin have poor yield. For solving this problem, the spacer conjugate the 2-amino-5-hydroxybenzaldehyde first, then conduction with tricyclic ketone to form 10-hydorxycamptothecin.
    Relation: 2017 第十一屆嘉南藥理大學藥理學院師生研究成果發表會,起迄日:2017/05/02-2017/05/04
    Appears in Collections:[Pharmacy and Science] 2017
    [Dept. of Pharmacy] Proceedings

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