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Design and synthesis of [I-125]Pyricoxib: A novel I-125-labeled cyclooxygenase-2 (COX-2) inhibitors

机译:[I-125]吡咯昔布的设计与合成:新型I-125标记的环氧合酶2(COX-2)抑制剂

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Cyclooxygenase-2 (COX-2) is the key enzyme in the prostaglandin synthesis pathway which is involved in various pathophysiological conditions. The enzyme is membrane bound and located inside of the endoplasmic reticulum and nuclear membrane. Effective perfusion of inhibitors to the active site requires lipophilic drugs, which consequently display high unspecific background accumulation, for example, in fatty tissues. The objective of this work was the development of a small molecule radiolabeled with a long-lived iodine radioisotope to enable longer imaging times and better target-to-background ratios. A group of iodinated compounds (8-10) was synthesized and identified as selective COX-2 inhibitors (COX-2 IC50 = 0.85-13 mu M). Molecular docking results provided the theoretical support for the experimental COX-2 inhibition data. Furthermore, a novel I-125-containing trifluoro-pyrimidine compound ([I-125] Pyricoxib) was prepared via radioiododestannylation reaction as potent and selective COX-2 inhibitor. Radiosynthesis of [I-125] Pyricoxib was accomplished with innovative fluorous chemistry using fluorous chloroamine-T (F-CAT) as novel oxidizing agent in high radiochemical yields of 91 +/- 4%. (C) 2016 Elsevier Ltd. All rights reserved.
机译:环氧合酶-2(COX-2)是前列腺素合成途径中的关键酶,参与各种病理生理状况。该酶与膜结合并位于内质网和核膜内部。有效地将抑制剂灌注到活性位点需要亲脂性药物,因此其在脂肪组织中显示出很高的非特异性背景积累。这项工作的目的是开发一种放射性同位素并标记有长寿命碘放射性同位素的小分子,以实现更长的成像时间和更好的靶与背景比。合成了一组碘化化合物(8-10),并鉴定为选择性COX-2抑制剂(COX-2 IC50 = 0.85-13μM)。分子对接的结果为实验COX-2抑制数据提供了理论支持。此外,通过放射性碘去甲腺上腺素化反应制备了新型的含I-125的三氟嘧啶化合物([I-125]吡ox昔布)作为有效的和选择性的COX-2抑制剂。 [I-125]吡咯昔布的放射性合成是通过创新的氟化学方法完成的,该方法使用氟氯胺-T(F-CAT)作为新型氧化剂,放射化学产率高达91 +/- 4%。 (C)2016 Elsevier Ltd.保留所有权利。

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