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在大鼠周围神经病变模型中,疼痛与情感障碍之间缺乏直接因果关系的证据。

Evidence for lack of direct causality between pain and affective disturbances in a rat peripheral neuropathy model.

机构信息

Life and Health Sciences Research Institute, School of Health Sciences, University of Minho, Braga, Portugal.

ICVS/3B's - PT Government Associate Laboratory, Braga, Portugal.

出版信息

Genes Brain Behav. 2019 Jul;18(6):e12542. doi: 10.1111/gbb.12542. Epub 2018 Dec 26.

DOI:10.1111/gbb.12542
PMID:30488664
Abstract

Chronic pain is frequently accompanied by the manifestation of emotional disturbances and cognitive deficits. While a causality relation between pain and emotional/cognitive disturbances is generally assumed, several observations suggest a temporal dissociation and independent mechanisms. We therefore studied Sprague-Dawley rats that presented a natural resistance to pain manifestation in a neuropathy model (spared nerve injury [SNI]) and compared their performance in a battery of behavioral paradigms-anxiety, depression and fear memory-with animals that presented a pain phenotype. Afterward, we performed an extensive volumetric analysis across prefrontal, orbitofrontal and insular cortical areas. The majority of SNI animals manifested mechanical allodynia (low threshold [LT]), but 13% were similar to Sham controls (high threshold [HT]). Readouts of spontaneous hypersensivity (paw flinches) were also significantly reduced in HT and correlated with allodynia. To increase the specificity of our findings, we segregated the SNI animals in those with left (SNI-L) and right (SNI-R) lesions and the lack of association between pain and behavior still remains. Left-lesioned animals, independent of the LT or HT phenotype, presented increased anxiety-like behaviors and decreased well-being. In contrast, we found that the insular cortex (agranular division) was significantly smaller in HT than in LT. To conclude, pain and emotional disturbances observed following nerve injury are to some extent segregated phenomena. Also, HT and LT SNI presented differences in insular volumes, an area vastly implicated in pain perception, suggesting a supraspinal involvement in the manifestation of these phenotypes.

摘要

慢性疼痛常伴有情绪障碍和认知缺陷的表现。虽然普遍认为疼痛与情绪/认知障碍之间存在因果关系,但有几项观察结果表明存在时间上的分离和独立的机制。因此,我们研究了在神经病变模型( spared nerve injury [SNI])中表现出对疼痛表现天然抵抗力的 Sprague-Dawley 大鼠,并比较了它们在一系列行为范式中的表现——焦虑、抑郁和恐惧记忆——与表现出疼痛表型的动物。之后,我们对前额叶、眶额皮质和岛叶皮质区域进行了广泛的体积分析。大多数 SNI 动物表现出机械性痛觉过敏(低阈值 [LT]),但 13%的动物与 Sham 对照组相似(高阈值 [HT])。HT 动物的自发性过敏(爪子抽搐)读数也显著降低,并与痛觉过敏相关。为了提高我们发现的特异性,我们将 SNI 动物分为左侧(SNI-L)和右侧(SNI-R)损伤组,疼痛与行为之间仍然没有关联。无论 LT 或 HT 表型如何,左损伤动物都表现出焦虑样行为增加和幸福感降低。相比之下,我们发现 HT 组的岛叶皮质(无颗粒区)明显小于 LT 组。总之,神经损伤后观察到的疼痛和情绪障碍在某种程度上是分离的现象。此外,HT 和 LT SNI 在岛叶体积上存在差异,而岛叶在疼痛感知中广泛涉及,这表明在这些表型的表现中存在脊髓以上的参与。

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