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  • [Bioconjug Chem.] 전립선 암에 대한 특이성 다기능 형광 억제제의 합성 및 평가Synthesis and Evaluation of Multifunctional Fluorescent Inhibitors with Synergistic Interaction of PSMA and Hypoxia for Prostate Cancer.

    전북대 / 권영도, 오정미, 김희권*

  • 출처
    Bioconjug Chem.
  • 등재일
    2018 Nov 28. doi: 10.1021/acs.bioconjchem.8b00767.
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    Abstract
    Prostate cancer is one of the most common cancers in the world. It is widely known that prostate-specific membrane antigen (PSMA) is highly expressed in prostate cancer, and hypoxia is a common characteristic of many solid tumors, including prostate cancer. In this study, we designed multifunctional fluorescent inhibitors to target PSMA and tumor hypoxia in order to increase the tumor uptake of inhibitors. Novel PSMA inhibitors were prepared using lysine as the backbone to connect three different functional groups: the glutamate-urea-lysine (GUL) structure for inhibiting PSMA, 2-nitroimidazole for the hypoxia-sensitive moiety, and a near-infrared fluorophore (sulfo-Cyanine 5.5). According to the in vitro PSMA binding assay, novel fluorescent inhibitors were demonstrated to have nanomolar binding affinities. Multifunctional inhibitor 2 with one 2-nitroimidazole had a similar inhibitory activity to inhibitor 1 that did not contain the hypoxia targeting moiety, but multifunctional inhibitor 3 with two 2-nitroimidazoles showed lower inhibitory activity than inhibitor 1 due to the bulky structure of the hypoxia-sensitive group. However, in vivo optical imaging and ex vivo biodistribution studies indicated that both multifunctional inhibitors 2 and 3 had higher accumulation in tumors than inhibitor 1 due to a synergistic combination of PSMA and hypoxia targeting moieties. These observations suggest that this novel multifunctional strategy might be a promising approach to improve the diagnosis and therapy of prostate cancer.

     

    Kwon YD, Oh JM, La MT, Chung HJ, Lee SJ, Chun S, Lee SH, Jeong BH, Kim HK.

  • 편집위원

    본 연구는 전립선암의 근적외선 형광영상을 위하여 근적외선 형광염료(sulfo-Cyanine 5.5), 전립선암의 PSMA 억제제(the glutamate-urealysine, GUL) 및 종양 hypoxia 표적물질(2-nitroimidazole)이 연결된 다기능성 억제제를 개발한 연구로, 다양한 종양의 영상 및 치료연구에 활용될 가능성을 기대하게 한다.

    2019-02-22 17:49:13

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