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震颤和小脑退行性疾病中的攀缘纤维 - 浦肯野细胞突触病理学

Climbing fiber-Purkinje cell synaptic pathology in tremor and cerebellar degenerative diseases.

作者信息

Kuo Sheng-Han, Lin Chi-Ying, Wang Jie, Sims Peter A, Pan Ming-Kai, Liou Jyun-You, Lee Danielle, Tate William J, Kelly Geoffrey C, Louis Elan D, Faust Phyllis L

机构信息

Department of Neurology, College of Physicians and Surgeons, Columbia University, 650 West 168th Street, Room 305, New York, NY, 10032, USA.

Department of Neurology, Icahn School of Medicine at Mount Sinai, New York, NY, USA.

出版信息

Acta Neuropathol. 2017 Jan;133(1):121-138. doi: 10.1007/s00401-016-1626-1. Epub 2016 Oct 4.

Abstract

Changes in climbing fiber-Purkinje cell (CF-PC) synaptic connections have been found in the essential tremor (ET) cerebellum, and these changes are correlated with tremor severity. Whether these postmortem changes are specific to ET remains to be investigated. We assessed CF-PC synaptic pathology in the postmortem cerebellum across a range of degenerative movement disorders [10 Parkinson's disease (PD) cases, 10 multiple system atrophy (MSA) cases, 10 spinocerebellar ataxia type 1 (SCA1) cases, and 20 ET cases] and 25 controls. We observed differences in terms of CF pathological features across these disorders. Specifically, PD cases and ET cases both had more CFs extending into the parallel fiber (PF) territory, but ET cases had more complex branching and increased length of CFs in the PF territory along with decreased CF synaptic density compared to PD cases. MSA cases and SCA1 cases had the most severely reduced CF synaptic density and a marked paucity of CFs extending into the PF territory. Furthermore, CFs in a subset of MSA cases formed collateral branches parallel to the PC layer, a feature not seen in other diagnostic groups. Using unsupervised cluster analysis, the cases and controls could all be categorized into four clusters based on the CF pathology and features of PC pathology, including counts of PCs and their axonal torpedoes. ET cases and PD cases co-segregated into two clusters, whereas SCA1 cases and MSA cases formed another cluster, separate from the control cluster. Interestingly, the presence of resting tremor seemed to be the clinical feature that separated the cases into the two ET-PD clusters. In conclusion, our study demonstrates that these degenerative movement disorders seem to differ with respect to the pattern of CF synaptic pathology they exhibit. It remains to be determined how these differences contribute to the clinical presentations of these diseases.

摘要

在特发性震颤(ET)患者的小脑内,已发现攀缘纤维 - 浦肯野细胞(CF - PC)突触连接发生改变,且这些变化与震颤严重程度相关。这些死后变化是否为ET所特有仍有待研究。我们评估了一系列退行性运动障碍患者(10例帕金森病(PD)、10例多系统萎缩(MSA)、10例脊髓小脑共济失调1型(SCA1)和20例ET)以及25名对照者死后小脑的CF - PC突触病理情况。我们观察到这些疾病在CF病理特征方面存在差异。具体而言,PD患者和ET患者均有更多的CF延伸至平行纤维(PF)区域,但与PD患者相比,ET患者的CF在PF区域具有更复杂的分支和更长的长度,同时CF突触密度降低。MSA患者和SCA1患者的CF突触密度降低最为严重,且延伸至PF区域的CF明显稀少。此外,一部分MSA患者的CF形成了与浦肯野细胞层平行的侧支,这一特征在其他诊断组中未见。使用无监督聚类分析,根据CF病理和浦肯野细胞病理特征(包括浦肯野细胞计数及其轴突鱼雷),病例和对照均可分为四类。ET患者和PD患者共分为两类,而SCA1患者和MSA患者形成另一类,与对照类分开。有趣的是,静止性震颤的存在似乎是将病例分为两个ET - PD类别的临床特征。总之,我们的研究表明,这些退行性运动障碍在CF突触病理表现模式上似乎存在差异。这些差异如何导致这些疾病的临床表现仍有待确定。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/55b2/5481163/d7b0357ac7fe/nihms867890f1.jpg

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