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首页> 外文期刊>Annals of nuclear medicine >Preclinical and the first clinical studies on (11C)CHIBA-1001 for mapping alpha7 nicotinic receptors by positron emission tomography.
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Preclinical and the first clinical studies on (11C)CHIBA-1001 for mapping alpha7 nicotinic receptors by positron emission tomography.

机译:(11C)CHIBA-1001用于通过正电子发射断层扫描定位α7烟碱样受体的临床前和首次临床研究。

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OBJECTIVE: 4-[(11)C]methylphenyl 2,5-diazabicyclo[3.2.2]nonane-2-carboxylate ([(11)C]CHIBA-1001), a 4-methyl-substituted derivative of the selective alpha7 nicotinic acetylcholine receptor (alpha7 nAChR) partial agonist 4-bromophenyl 1,4 diazabicyclo[3.2.2]nonane-4-carboxylate (SSR180711), is a potential radioligand for mapping alpha7 nAChRs in the brain by positron emission tomography (PET). In this study, we performed preclinical and first clinical PET studies using [(11)C]CHIBA-1001 for imaging alpha7 nAChRs in the human brain. METHODS: [(11)C]CHIBA-1001 was synthesized by methylation of the tributylstannyl precursor with [(11)C]CH(3)I in a palladium-promoted Stille cross-coupling reaction. The radiation absorbed-dose of [(11)C]CHIBA-1001 in humans was calculated from distribution data in mice. The acute toxicity of CHIBA-1001 at a dose of 3.20 mg/kg body weight, which is more than 41,000-fold the clinical equivalent dose of [(11)C]CHIBA-1001, was evaluated. The mutagenicity of CHIBA-1001 was studied by a reverse mutation test in Salmonella typhimurium (Ames test). Metabolite analysis in the mouse brain was carried out by high-performance liquid chromatography. The first clinical PET imaging of alpha7 nAChRs with [(11)C]CHIBA-1001 in a normal volunteer was also performed. RESULTS: A suitable preparation method for [(11)C]CHIBA-1001 injection was established. The radiation absorbed-dose by [(11)C]CHIBA-1001 in humans was low enough for clinical use, and no acute toxicity or mutagenicity of CHIBA-1001 was found. Most radioactivity in the mouse brain was detected as an unchanged form, although peripherally [(11)C]CHIBA-1001 was degraded. We successfully performed brain imaging by PET with [(11)C]CHIBA-1001 in a normal volunteer. A 90-min dynamic scan showed a rapid accumulation and gradual washout of radioactivity in the brain. The highest distribution volume of [(11)C]CHIBA-1001 was found in the thalamus; however, regional differences in brain radioactivity were small. Peripherally, [(11)C]CHIBA-1001 was stable in humans: >80% of the radioactivity in plasma was detected as the unchanged form for 60 min. CONCLUSIONS: These results demonstrate that [(11)C]CHIBA-1001 is a suitable radioligand to use in clinical trials for imaging alpha7 nAChRs in the human brain, providing acceptable dosimetry and pharmacological safety at the dose required for adequate PET imaging.
机译:目的:4-[(11)C]甲基苯基2,5-二氮杂双环[3.2.2]壬烷-2-羧酸盐[[(11)C] CHIBA-1001),选择性α7烟碱的4-甲基取代衍生物乙酰胆碱受体(alpha7 nAChR)部分激动剂4-溴苯基1,4二氮杂双环[3.2.2]壬烷-4-羧酸酯(SSR180711)是一种潜在的放射性配体,可通过正电子发射断层扫描(PET)绘制大脑中的alpha7 nAChRs。在这项研究中,我们使用[(11)C] CHIBA-1001对人脑中的alpha7 nAChRs进行了成像前和首次临床PET研究。方法:[(11)C] CHIBA-1001是在钯促进的Stille交叉偶联反应中,将三丁基锡烷基前体与[(11)C] CH(3)I甲基化合成的。根据小鼠中的分布数据计算了[(11)C] CHIBA-1001在人体内的辐射吸收剂量。评估了3.20 mg / kg体重的CHIBA-1001的急性毒性,该毒性是[(11)C] CHIBA-1001临床等效剂量的41,000倍以上。在鼠伤寒沙门氏菌中通过反向突变试验(Ames试验)研究了CHIBA-1001的致突变性。小鼠大脑中的代谢物分析是通过高效液相色谱法进行的。还进行了在正常志愿者中用[(11)C] CHIBA-1001对alpha7 nAChRs的首次临床PET成像。结果:建立了适合[[11] C] CHIBA-1001注射剂的制备方法。 [(11)C] CHIBA-1001在人体中的辐射吸收剂量对于临床使用而言足够低,并且未发现CHIBA-1001的急性毒性或致突变性。尽管[[11] C] CHIBA-1001的外围细胞被降解,但在小鼠大脑中大多数放射性未检出。我们在正常志愿者中成功地通过PET与[(11)C] CHIBA-1001进行了脑成像。 90分钟的动态扫描显示了大脑中放射性的快速积累和逐渐清除。在丘脑中发现[(11)C] CHIBA-1001的分配量最高;但是,大脑放射性的区域差异很小。外围,[(11)C] CHIBA-1001在人类中稳定:在60分钟内检测到血浆中80%以上的放射性均保持不变。结论:这些结果表明,[(11)C] CHIBA-1001是适合在临床试验中用于对人脑中的alpha7 nAChRs进行成像的放射配体,以足够的PET成像所需的剂量提供了可接受的剂量学和药理学安全性。

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