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PET 在脑小血管病评估中的附加价值。

The Additional Value of PET in the Assessment of Cerebral Small Vessel Disease.

机构信息

Max Planck Institute for Metabolism Research, Cologne, Germany

出版信息

J Nucl Med. 2018 Nov;59(11):1660-1664. doi: 10.2967/jnumed.118.214270. Epub 2018 Jun 29.

Abstract

The diagnosis of cerebral small vessel disease (SVD) is difficult because there is no consensus on clinical criteria, and therefore imaging is important for diagnosis. Most patients undergo brain imaging by CT, which is able to detect ischemic strokes, hemorrhages, and brain atrophy and may also indicate white matter changes. MRI remains the key neuroimaging modality and is preferred to CT in vascular cognitive impairment (VCI) because it has higher sensitivity and specificity for detecting pathologic changes. These modalities for imaging morphology permit detection of vascular lesions traditionally attributed to VCI in subcortical areas of the brain, single infarction or lacunes in strategic areas (thalamus or angular gyrus), or large cortical-subcortical lesions reaching a critical threshold of tissue loss. In SVD, multiple punctuate or confluent lesions can be seen in the white matter by MRI and were called leukoaraiosis. Another major neuroimaging finding of SVD in VCI are microhemorrhages. However, whereas CT and MRI are able to detect morphologic lesions, these modalities cannot determine functional consequences of the underlying pathologic changes. PET can support the clinical diagnosis by visualizing cerebral functions in typically affected brain regions. In SVD, F-FDG PET can clearly differentiate scattered areas of focal cortical and subcortical hypometabolism that differ from the typical metabolic pattern seen in Alzheimer dementia (AD) with marked hypometabolism affecting the association areas. Additional PET tracers can further support the diagnosis of a type of dementia and also yield information on the underlying pathophysiology.

摘要

脑小血管病 (SVD) 的诊断较为困难,因为目前尚无临床标准的共识,因此影像学检查对于诊断十分重要。大多数患者接受 CT 脑部成像检查,CT 可检测到缺血性卒、出血和脑萎缩,也可能提示白质改变。MRI 仍然是关键的神经影像学方式,并且在血管性认知障碍 (VCI) 中优于 CT,因为它对检测病理性改变具有更高的敏感性和特异性。这些形态学成像方式可用于检测传统上归因于脑皮质下区域 VCI 的血管病变,包括单一梗死或腔隙性梗死(丘脑或角回),或达到临界组织丢失阈值的大皮质下病变。在 SVD 中,MRI 可在白质中检测到多发点状或融合性病变,被称为脑白质疏松症。SVD 在 VCI 中的另一个主要神经影像学发现是微出血。然而,CT 和 MRI 能够检测形态学病变,但这些方式无法确定潜在病理变化的功能后果。PET 可通过可视化典型受累脑区的脑功能来支持临床诊断。在 SVD 中,18F-FDG PET 可清晰区分散在的局灶性皮质和皮质下代谢减低区,这些区域与阿尔茨海默病(AD)中典型的代谢模式不同,AD 表现为明显的代谢减低影响联合区。其他 PET 示踪剂可进一步支持痴呆类型的诊断,并提供潜在病理生理学的信息。

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