Kawakami Ito, Iseki Eizo, Kasanuki Koji, Minegishi Michiko, Sato Kiyoshi, Hino Hiroyuki, Shibuya Katsuhiko, Fujisawa Kohshiro, Higashi Shinji, Akiyama Haruhiko, Furuta Akiko, Takanashi Masashi, Li Yuanzhe, Hattori Nobutaka, Mitsuyama Yoshio, Arai Heii
PET/CT Dementia Research Center, Juntendo Tokyo Koto Geriatric Medical Center, Juntendo University School of Medicine, 3-3-20 Shinsuna, Koto-ku, Tokyo 136-0075, Japan; Yokohama Hoyu Hospital, Psychiatry, Yokohama 241-0812, Japan; Dementia Research Project, Tokyo Metropolitan Institute of Medical Science, Tokyo 156-8506, Japan.
PET/CT Dementia Research Center, Juntendo Tokyo Koto Geriatric Medical Center, Juntendo University School of Medicine, 3-3-20 Shinsuna, Koto-ku, Tokyo 136-0075, Japan; Department of Psychiatry, Juntendo University School of Medicine, Tokyo 113-8421, Japan.
J Neurol Sci. 2016 Aug 15;367:349-55. doi: 10.1016/j.jns.2016.06.013. Epub 2016 Jun 7.
Clinical phenotypes of hereditary diffuse leukoencephalopathy with spheroids (HDLS), a familial progressive neurodegenerative disorder affecting the white matter of the brain, are heterogenous and may include behavioral and personality changes, memory impairment, parkinsonism, seizure, and spasticity. Thus, HDLS is frequently unrecognized and misdiagnosed. Heterozygous mutations located within the kinase domain of the gene encoding the colony-stimulating factor 1 receptor (CSF1R), a cell surface receptor with key roles in development and innate immunity, have been shown in HDLS. These different gene mutations may be related to the various clinical phenotypes. We report here a newly identified family with HDLS harboring a mutation in the CSF1R gene. We examined clinical and neuropathological features in three members of this family. These patients presented with affective incontinence, memory impairment, and executive dysfunction at onset, and revealed nonfluent aphasia, parkinsonism, and seizure as the disease progressed. We identified a novel CSF1R splice site mutation (c.2442+2T>C) in intron 18 for two of the patients. MRI of these patients revealed progressive, frontotemporal-predominant, confluent leukoencephalopathy. We also observed severe myelin loss, axonal degeneration, and abundant axonal spheroids, astrocytes, and microglia in the cerebral white matter, consistent with HDLS neuropathological features. Additionally, we identified atypical neuropathological findings for HDLS, including neuronal loss and gliosis with ballooned neurons and central chromatolysis in the frontal cortex and hippocampus. This report provides further evidence for the clinical and neuropathological heterogeneity of HDLS.
遗传性球形细胞白质营养不良(HDLS)是一种影响大脑白质的家族性进行性神经退行性疾病,其临床表型具有异质性,可能包括行为和性格改变、记忆障碍、帕金森综合征、癫痫和痉挛。因此,HDLS常常未被识别和误诊。在HDLS中已发现位于编码集落刺激因子1受体(CSF1R)的基因激酶结构域内的杂合突变,CSF1R是一种在发育和先天免疫中起关键作用的细胞表面受体。这些不同的基因突变可能与各种临床表型有关。我们在此报告一个新发现的患有HDLS的家族,该家族携带CSF1R基因突变。我们检查了这个家族三名成员的临床和神经病理学特征。这些患者起病时表现为情感失禁、记忆障碍和执行功能障碍,随着疾病进展出现非流利性失语、帕金森综合征和癫痫。我们在两名患者的第18内含子中鉴定出一种新的CSF1R剪接位点突变(c.2442+2T>C)。这些患者的MRI显示进行性、以额颞叶为主的融合性白质脑病。我们还在脑白质中观察到严重的髓鞘丢失、轴突变性以及大量轴突球状体、星形胶质细胞和小胶质细胞,这与HDLS的神经病理学特征一致。此外,我们还发现了HDLS的非典型神经病理学表现,包括额叶皮质和海马体中的神经元丢失以及伴有气球样神经元和中央染色质溶解的胶质增生。本报告为HDLS的临床和神经病理学异质性提供了进一步的证据。
