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Imaging of cerebral α4β2* nicotinic acetylcholine receptors with (−)-18FFlubatine PET: Implementation of bolus plus constant infusion and sensitivity to acetylcholine in human brain

机译:(-)-18F氟丁胺PET对脑α4β2*烟碱型乙酰胆碱受体的成像:推注加恒定输注以及对人脑中乙酰胆碱的敏感性

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摘要

The positron emission tomography (PET) radioligand (−)-[18F]flubatine is specific to α4β2 nicotinic acetylcholine receptors (nAChRs) and has promise for future investigation of the acetylcholine system in neuropathologies such as Alzheimer's disease, schizophrenia, and substance use disorders. The two goals of this work were to develop a simplified method for α4β2 nAChR quantification with bolus plus constant infusion (B/I) (−)-[18F]flubatine administration, and to assess the radioligand's sensitivity to acetylcholine fluctuations in humans. Healthy human subjects were imaged following either bolus injection (n = 8) or B/I (n = 4) administration of (−)-[18F]flubatine. The metabolite-corrected input function in arterial blood was measured. Free-fraction corrected distribution volumes (VT/fP) were estimated with modeling and graphical analysis techniques. Next, sensitivity to acetylcholine was assessed in two ways: 1. A bolus injection paradigm with two scans (n = 6), baseline (scan 1) and physostigmine challenge (scan 2; 1.5 mg over 60 min beginning 5 min prior to radiotracer injection); 2. A single scan B/I paradigm (n = 7) lasting up to 240 min with 1.5 mg physostigmine administered over 60 min beginning at 125 min of radiotracer infusion. Changes in VT/fP were measured. Baseline VT/fP values were 33.8 ± 3.3 mL/cm3 in thalamus, 12.9 ± 1.6 mL/cm3 in cerebellum, and ranged from 9.8 to 12.5 mL/cm3 in other gray matter regions. The B/I paradigm with equilibrium analysis at 120 min yielded comparable VT/fP values with compartment modeling analysis of bolus data in extrathalamic gray matter regions (regional means <4% different). Changes in VT/fP following physostigmine administration were small and most pronounced in cortical regions, ranging from 0.8 to 4.6% in the two-scan paradigm and 2.8 to 6.5% with the B/I paradigm. These results demonstrate the use of B/I administration for accurate quantification of (−)-[18F]flubatine VT/fP in 120 min, and suggest possible sensitivity of (−)-[18F]flubatine binding to physostigmine-induced changes in acetylcholine levels.
机译:正电子发射断层扫描(PET)放射性配体(-)-[ 18 F]氟巴汀专用于 α 4 β< / mi> 2 * 烟碱型乙酰胆碱受体(nAChRs),并有望在神经病理学等领域进一步研究乙酰胆碱系统作为阿尔茨海默氏病,精神分裂症和物质使用障碍。这项工作的两个目标是为 α 4 β 2 nAChR定量与推注加恒定输注(B / I)(-)-[ 18 F]氟丁汀给药,并进行评估放射性配体对人类乙酰胆碱波动的敏感性。推注(-)-[ 18 F]氟丁汀后(n = 8)或B / I(n = 4),对健康的人类受试者进行成像。测量代谢物在动脉血中的输入功能。使用建模和图形分析技术估算自由分数校正的分布体积(VT / fP)。接下来,通过两种方式评估对乙酰胆碱的敏感性:1.推注注射范例,包括两次扫描(n = 6),基线(扫描1)和毒扁豆碱激发(扫描2;在注射放射性示踪剂前5分钟的60分钟内1.5 mg ); 2.一次单次扫描B / I范例(n = 7)持续长达240分钟,在放射性示踪剂注入125分钟后的60分钟内开始施用1.5 mg毒扁豆碱。测量VT / fP的变化。丘脑基线VT / fP值为33.8±3.3 mL / cm 3 ,小脑基线VT / fP值为12.9±1.6 mL / cm 3 ,范围为9.8至12.5 mL / cm <其他灰质区域中的sup> 3 。在丘脑外灰质区域(区域平均值相差<4%),在120分钟进行平衡分析的B / I范式产生了可比的VT / fP值,而该模型具有对推注数据进行隔室建模分析的结果。毒扁豆碱给药后VT / fP的变化很小,在皮质区域最为明显,两次扫描范式的变化范围为0.8至4.6%,而B / I范式的变化范围为2.8至6.5%。这些结果证明了B / I给药可在120分钟内准确定量(-)-[ 18 F]氟丁碱VT / fP,并暗示(-)-[ 18 F]氟巴汀与毒扁豆碱诱导的乙酰胆碱水平变化的结合。

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