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Brain Morphological Signatures for Chronic Pain

机译:慢性疼痛的脑形态特征

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摘要

Chronic pain can be understood not only as an altered functional state, but also as a consequence of neuronal plasticity. Here we use in vivo structural MRI to compare global, local, and architectural changes in gray matter properties in patients suffering from chronic back pain (CBP), complex regional pain syndrome (CRPS) and knee osteoarthritis (OA), relative to healthy controls. We find that different chronic pain types exhibit unique anatomical ‘brain signatures’. Only the CBP group showed altered whole-brain gray matter volume, while regional gray matter density was distinct for each group. Voxel-wise comparison of gray matter density showed that the impact on the extent of chronicity of pain was localized to a common set of regions across all conditions. When gray matter density was examined for large regions approximating Brodmann areas, it exhibited unique large-scale distributed networks for each group. We derived a barcode, summarized by a single index of within-subject co-variation of gray matter density, which enabled classification of individual brains to their conditions with high accuracy. This index also enabled calculating time constants and asymptotic amplitudes for an exponential increase in brain re-organization with pain chronicity, and showed that brain reorganization with pain chronicity was 6 times slower and twice as large in CBP in comparison to CRPS. The results show an exuberance of brain anatomical reorganization peculiar to each condition and as such reflecting the unique maladaptive physiology of different types of chronic pain.
机译:慢性疼痛不仅可以理解为功能状态的改变,还可以理解为神经元可塑性的结果。在这里,我们使用体内结构MRI来比较与健康对照相比患有慢性背痛(CBP),复杂区域疼痛综合征(CRPS)和膝骨关节炎(OA)的患者的灰质性质的整体,局部和结构变化。我们发现,不同的慢性疼痛类型表现出独特的解剖学“大脑特征”。仅CBP组显示全脑灰质体积改变,而各组区域灰质密度不同。灰质密度的Voxel方式比较显示,在所有情况下,对疼痛慢性程度的影响均局限于一组共同的区域。当检查接近布罗德曼地区的大区域的灰质密度时,对于每组,它都表现出独特的大规模分布式网络。我们得出了一个条形码,该条形码由灰质密度的受试者内部协变的单个索引概括,该条形码使单个大脑能够根据其状况进行高精度分类。该指数还可以计算时间常数和渐近振幅,以使疼痛慢性病的大脑重组呈指数增长,并且显示与疼痛慢性病有关的脑重组比CRPS慢6倍,是CBP的两倍。结果显示,每种情况都具有丰富的大脑解剖结构重组,因此反映了不同类型的慢性疼痛的独特适应不良生理。

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