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Use of a Novel High-Resolution Magnetic Resonance Neurography Protocol to Detect Abnormal Dorsal Root Ganglia in Sjögren Patients With Neuropathic Pain

机译:新型高分辨率磁共振神经成像协议在干燥性神经性疼痛干燥患者中检测背根神经节异常

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摘要

The diagnosis and treatment of patients with Sjögren syndrome (SS) with neuropathic pain pose several challenges. Patients with SS may experience unorthodox patterns of burning pain not conforming to a traditional “stocking-and-glove” distribution, which can affect the face, torso, and proximal extremities. This distribution of neuropathic pain may reflect mechanisms targeting the proximal-most element of the peripheral nervous system—the dorsal root ganglia (DRG). Skin biopsy can diagnose such a small-fiber neuropathy and is a surrogate marker of DRG neuronal cell loss. However, SS patients have been reported who have similar patterns of proximal neuropathic pain, despite having normal skin biopsy studies. In such cases, DRGs may be targeted by mechanisms not associated with neuronal cell loss. Therefore, alternative approaches are warranted to help characterize abnormal DRGs in SS patients with proximal neuropathic pain.We performed a systematic review of the literature to define the frequency and spectrum of SS peripheral neuropathies, and to better understand the attribution of SS neuropathic pain to peripheral neuropathies. We found that the frequency of SS neuropathic pain exceeded the prevalence of peripheral neuropathies, and that painful peripheral neuropathies occurred less frequently than neuropathies not always associated with pain. We developed a novel magnetic resonance neurography (MRN) protocol to evaluate DRG abnormalities. Ten SS patients with proximal neuropathic pain were evaluated by this MRN protocol, as well as by punch skin biopsies evaluating for intraepidermal nerve fiber density (IENFD) of unmyelinated nerves. Five patients had radiographic evidence of DRG abnormalities. Patients with MRN DRG abnormalities had increased IENFD of unmyelinated nerves compared to patients without MRN DRG abnormalities (30.2 [interquartile range, 4.4] fibers/mm vs. 11.0 [4.1] fibers/mm, respectively; p = 0.03). Two of these 5 SS patients whose neuropathic pain resolved with intravenous immunoglobulin (IVIg) therapy had improvement of MRN DRG abnormalities.We have developed a novel MRN protocol that can detect DRG abnormalities in SS patients with neuropathic pain who do not have markers of peripheral neuropathy. We found that SS patients with MRN DRG abnormalities had statistically significant, increased IENFD on skin biopsy studies, which may suggest a relationship between trophic mediators and neuropathic pain. Given that our literature review has demonstrated that many SS neuropathic pain patients do not have a neuropathy, our findings suggest an important niche for this MRN DRG technique in the evaluation of broader subsets of SS neuropathic pain patients who may not have underlying neuropathies. The improvement of MRN DRG abnormalities in patients with IVIg-induced remission of neuropathic pain suggests that our MRN protocol may be capturing reversible, immune-mediated mechanisms targeting the DRG.
机译:患有神经性疼痛的Sjögren综合征(SS)患者的诊断和治疗提出了一些挑战。患有SS的患者可能会经历非常规的烧灼痛模式,这不符合传统的“袜套”分布,会影响面部,躯干和四肢。神经性疼痛的这种分布可能反映了针对周围神经系统的最近端元件-背根神经节(DRG)的机制。皮肤活检可以诊断出这种小纤维神经病变,并且是DRG神经元细胞丢失的替代标志。然而,据报道,尽管皮肤活检研究正常,但SS患者的近端神经性疼痛模式相似。在这种情况下,DRG可以通过与神经元细胞丢失无关的机制来靶向。因此,有必要采取其他方法来帮助特征性SS患者伴有近端神经性疼痛的异常DRGs。神经病。我们发现SS神经性疼痛的发生率超过了周围神经病变的患病率,并且与并非总是与疼痛相关的神经病变相比,疼痛性周围神经病变的发生频率更低。我们开发了一种新颖的磁共振神经成像(MRN)协议来评估DRG异常。通过此MRN方案以及通过穿孔皮肤活检评估十名近端神经性疼痛的SS患者,以评估无髓神经的表皮内神经纤维密度(IENFD)。 5例患者有影像学检查表明DRG异常。与无MRN DRG异常的患者相比,具有MRN DRG异常的患者的无髓神经IENFD升高(分别为30.2 [四分位间距,4.4]纤维/毫米与11.0 [4.1]纤维/毫米; p = 0.03)。在5例经静脉免疫球蛋白(IVIg)治疗可缓解神经性疼痛的SS患者中,有2例改善了MRN DRG异常。我们开发了一种新的MRN方案,可以检测没有周围神经病变标志物的神经性疼痛SS患者的DRG异常。我们发现,在皮肤活检研究中,具有MRN DRG异常的SS患者在统计学上显着增加,IENFD升高,这可能表明营养介质和神经性疼痛之间存在关联。鉴于我们的文献综述表明许多SS神经性疼痛患者没有神经病变,因此我们的发现表明,这种MRN DRG技术在评估可能没有潜在神经病变的SS神经性疼痛患者的更广泛亚群中具有重要的市场地位。 IVIg诱导的神经性疼痛缓解患者MRN DRG异常的改善表明,我们的MRN方案可能正在捕获针对DRG的可逆的,免疫介导的机制。

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