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含氟磷酸二酯酶10A(PDE10A)抑制剂的合成以及F-18标记的PDE10A PET示踪剂在啮齿动物和非人灵长类动物中的体内评估。

Synthesis of Fluorine-Containing Phosphodiesterase 10A (PDE10A) Inhibitors and the In Vivo Evaluation of F-18 Labeled PDE10A PET Tracers in Rodent and Nonhuman Primate.

作者信息

Li Junfeng, Zhang Xiang, Jin Hongjun, Fan Jinda, Flores Hubert, Perlmutter Joel S, Tu Zhude

机构信息

Department of Radiology and ‡Department of Neurology, Washington University School of Medicine , St. Louis, Missouri 63110, United States.

出版信息

J Med Chem. 2015 Nov 12;58(21):8584-600. doi: 10.1021/acs.jmedchem.5b01205. Epub 2015 Oct 15.

Abstract

A series of fluorine-containing PDE10A inhibitors were designed and synthesized to improve the metabolic stability of [(11)C]MP-10. Twenty of the 22 new analogues had high potency and selectivity for PDE10A: 18a-j, 19d-j, 20a-b, and 21b had IC50 values <5 nM for PDE10A. Seven F-18 labeled compounds [(18)F]18a-e, [(18)F]18g, and [(18)F]20a were radiosynthesized by (18)F-introduction onto the quinoline rather than the pyrazole moiety of the MP-10 pharmacophore and performed in vivo evaluation. Biodistribution studies in rats showed ~2-fold higher activity in the PDE10A-enriched striatum than nontarget brain regions; this ratio increased from 5 to 30 min postinjection, particularly for [(18)F]18a-d and [(18)F]20a. MicroPET studies of [(18)F]18d and [(18)F]20a in nonhuman primates provided clear visualization of striatum with suitable equilibrium kinetics and favorable metabolic stability. These results suggest this strategy may identify a (18)F-labeled PET tracer for quantifying the levels of PDE10A in patients with CNS disorders including Huntington's disease and schizophrenia.

摘要

设计并合成了一系列含氟的PDE10A抑制剂,以提高[(11)C]MP-10的代谢稳定性。22种新类似物中的20种对PDE10A具有高效力和选择性:18a-j、19d-j、20a-b和21b对PDE10A的IC50值<5 nM。通过将(18)F引入到MP-10药效团的喹啉而非吡唑部分,放射合成了7种F-18标记的化合物[(18)F]18a-e、[(18)F]18g和[(18)F]20a,并进行了体内评价。大鼠体内分布研究表明,富含PDE10A的纹状体中的活性比非靶脑区高约2倍;该比值在注射后5至30分钟增加,特别是对于[(18)F]18a-d和[(18)F]20a。对[(18)F]18d和[(18)F]20a在非人灵长类动物中的MicroPET研究显示,纹状体具有清晰的可视化效果,具有合适的平衡动力学和良好的代谢稳定性。这些结果表明,该策略可能鉴定出一种(18)F标记的PET示踪剂,用于定量患有包括亨廷顿舞蹈病和精神分裂症在内的中枢神经系统疾病患者的PDE10A水平。

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