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首页> 外文期刊>NeuroImage >Quantification of opioid receptor availability following spontaneous epileptic seizures: Correction of [11C]diprenorphine PET data for the partial-volume effect
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Quantification of opioid receptor availability following spontaneous epileptic seizures: Correction of [11C]diprenorphine PET data for the partial-volume effect

机译:自发性癫痫发作后阿片受体可用量的量化:[11C] diprenorphine PET数据对部分量效应的校正

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摘要

Previous positron emission tomography (PET) studies in refractory temporal lobe epilepsy (TLE) using the non-selective opioid receptor antagonist [11C]diprenorphine (DPN) did not detect any changes in mesial temporal structures, despite known involvement of the hippocampus in seizure generation. Normal binding in smaller hippocampi is suggestive of increased receptor concentration in the remaining grey matter. Correction for partial-volume effect (PVE) has not been used in previous DPN PET studies. Here, we present PVE-corrected DPN-PET data quantifying post-ictal and interictal opioid receptor availability in humans with mTLE.Eight paired datasets of post-ictal and interictal DPN PET scans and eleven test/retest control datasets were available from a previously published study on opioid receptor changes in TLE following seizures (Hammers et al., 2007a). Five of the eight participants with TLE had documented hippocampal sclerosis. Data were re-analyzed using regions of interest and a novel PVE correction method (structural functional synergistic-resolution recovery (SFS-RR); (Shidahara et al., 2012)). Data were denoised, followed by application of SFS-RR, with anatomical information derived via precise anatomical segmentation of the participants' MRI (MAPER; (Heckemann et al., 2010)). [11C]diprenorphine volume-of-distribution (VT) was quantified in six regions of interest.Post-ictal increases were observed in the ipsilateral fusiform gyri and lateral temporal pole. A novel finding was a post-ictal increase in [11C]DPN VT relative to the interictal state in the ipsilateral parahippocampal gyrus, not observed in uncorrected datasets. As for voxel-based (SPM) analyses, correction for global VT values was essential in order to demonstrate focal post-ictal increases in [11C]DPN VT.This study provides further direct human in vivo evidence for changes in opioid receptor availability in TLE following seizures, including changes that were not evident without PVE correction. Denoising, resolution recovery and precise anatomical segmentation can extract valuable information from PET studies that would be missed with conventional post-processing procedures.
机译:先前使用非选择性阿片受体拮抗剂[11C]双戊北啡(DPN)进行的难治性颞叶癫痫(TLE)的正电子发射断层扫描(PET)研究,尽管已知海马体参与了癫痫发作的发生,但并未发现中颞叶结构的任何变化。在较小的海马体中正常结合提示剩余灰质中受体浓度增加。以前的DPN PET研究中尚未使用对部分体积效应(PVE)的校正。在这里,我们介绍了PVE校正的DPN-PET数据,量化了患有mTLE的人的发作后和发作间阿片受体的可用性。八对成对的发作后和发作间DPN PET扫描数据以及十一个测试/重测对照数据集可从先前发表的文献中获得癫痫发作后阿片类药物受体变化的研究(Hammers等,2007a)。 TLE的八名参与者中有五名记录了海马硬化。使用感兴趣区域和新型PVE校正方法(结构功能协同分辨率恢复(SFS-RR);(Shidahara等人,2012))重新分析数据。对数据进行去噪,然后应用SFS-RR,并通过参与者MRI的精确解剖分割(MAPER;(Heckemann等,2010))获得解剖信息。 [11C] diprenorphine的分布体积(VT)在六个感兴趣的区域进行了量化。在同侧梭状回和侧面颞极观察到发作后增加。一个新发现是[11C] DPN VT相对于同侧海马旁回的发作间期增加,在未经校正的数据集中未观察到。至于基于体素(SPM)的分析,校正整体VT值对于证明[11C] DPN VT局部发作后局部增加是至关重要的。这项研究为TLE中阿片样物质受体可用性的变化提供了进一步的直接体内证据。癫痫发作后的变化,包括未经PVE校正就不明显的变化。去噪,分辨率恢复和精确的解剖分割可以从PET研究中提取有价值的信息,而传统的后处理程序可能会丢失这些信息。

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