Deciphering glial contributions to CSF1R-related disorder via single-nuclear transcriptomic profiling: a case study.

IF 6.2 2区 医学 Q1 NEUROSCIENCES
Jie Pan, Jaume Fores-Martos, Claire Delpirou Nouh, Tanner D Jensen, Kristen Vallejo, Romain Cayrol, Saman Ahmadian, Euan A Ashley, Michael D Greicius, Inma Cobos
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引用次数: 0

Abstract

CSF1R-related disorder (CSF1R-RD) is a neurodegenerative condition that predominantly affects white matter due to genetic alterations in the CSF1R gene, which is expressed by microglia. We studied an elderly man with a hereditary, progressive dementing disorder of unclear etiology. Standard genetic testing for leukodystrophy and other neurodegenerative conditions was negative. Brain autopsy revealed classic features of adult-onset leukoencephalopathy with axonal spheroids and pigmented glia (ALSP), including confluent white matter degeneration with axonal spheroids and pigmented glial cells in the affected white matter, consistent with CSF1R-RD. Subsequent long-read sequencing identified a novel deletion in CSF1R that was not detectable with short-read exome sequencing. To gain insight into potential mechanisms underlying white matter degeneration in CSF1R-RD, we studied multiple brain regions exhibiting varying degrees of white matter pathology. We found decreased CSF1R transcript and protein across brain regions, including intact white matter. Single nuclear RNA sequencing (snRNAseq) identified two disease-associated microglial cell states: lipid-laden microglia (expressing GPNMB, ATG7, LGALS1, LGALS3) and inflammatory microglia (expressing IL2RA, ATP2C1, FCGBP, VSIR, SESN3), along with a small population of CD44+ peripheral monocyte-derived macrophages exhibiting migratory and phagocytic signatures. GPNMB+ lipid-laden microglia with ameboid morphology represented the end-stage disease microglia state. Disease-associated oligodendrocytes exhibited cell stress signatures and dysregulated apoptosis-related genes. Disease-associated oligodendrocyte precursor cells (OPCs) displayed a failure in their differentiation into mature myelin-forming oligodendrocytes, as evidenced by upregulated LRP1, PDGFRA, SOX5, NFIA, and downregulated NKX2-2, NKX6.2, SOX4, SOX8, TCF7L2, YY1, ZNF488. Overall, our findings highlight microglia-oligodendroglia crosstalk in demyelination, with CSF1R dysfunction promoting phagocytic and inflammatory microglia states, an arrest in OPC differentiation, and oligodendrocyte depletion.

通过单核转录组分析破译神经胶质对 CSF1R 相关疾病的贡献:一项案例研究。
CSF1R相关障碍(CSF1R-RD)是一种神经退行性疾病,主要影响白质,原因是小胶质细胞表达的CSF1R基因发生了遗传改变。我们研究了一名病因不明的遗传性进行性痴呆症老人。白质营养不良症和其他神经退行性疾病的标准基因检测结果均为阴性。脑部解剖发现了成人型白质脑病伴轴索球体和色素性胶质细胞(ALSP)的典型特征,包括受累白质中伴有轴索球体和色素性胶质细胞的融合性白质变性,与CSF1R-RD一致。随后的长线程测序发现了CSF1R中的一个新缺失,而短线程外显子测序无法检测到该缺失。为了深入了解CSF1R-RD白质变性的潜在机制,我们对表现出不同程度白质病变的多个脑区进行了研究。我们发现包括完整白质在内的各个脑区的 CSF1R 转录物和蛋白质都有所减少。单核 RNA 测序(snRNAseq)确定了两种与疾病相关的小胶质细胞状态:脂质增生性小胶质细胞(表达 GPNMB、ATG7、LGALS1、LGALS3)和炎症性小胶质细胞(表达 IL2RA、ATP2C1、FCGBP、VSIR、SESN3),以及一小部分 CD44+ 外周单核细胞源性巨噬细胞,它们表现出迁移和吞噬特征。GPNMB+脂质包涵的小胶质细胞具有小鼠形态,代表了疾病晚期的小胶质细胞状态。疾病相关的少突胶质细胞表现出细胞应激特征和凋亡相关基因失调。疾病相关的少突胶质细胞前体细胞(OPCs)未能分化为成熟的髓鞘形成少突胶质细胞,表现为 LRP1、PDGFRA、SOX5、NFIA 上调,NKX2-2、NKX6.2、SOX4、SOX8、TCF7L2、YY1、ZNF488 下调。总之,我们的研究结果突显了小胶质细胞-少突胶质细胞在脱髓鞘过程中的相互影响,CSF1R功能障碍会促进小胶质细胞的吞噬和炎症状态、OPC分化停滞以及少突胶质细胞耗竭。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Acta Neuropathologica Communications
Acta Neuropathologica Communications Medicine-Pathology and Forensic Medicine
CiteScore
11.20
自引率
2.80%
发文量
162
审稿时长
8 weeks
期刊介绍: "Acta Neuropathologica Communications (ANC)" is a peer-reviewed journal that specializes in the rapid publication of research articles focused on the mechanisms underlying neurological diseases. The journal emphasizes the use of molecular, cellular, and morphological techniques applied to experimental or human tissues to investigate the pathogenesis of neurological disorders. ANC is committed to a fast-track publication process, aiming to publish accepted manuscripts within two months of submission. This expedited timeline is designed to ensure that the latest findings in neuroscience and pathology are disseminated quickly to the scientific community, fostering rapid advancements in the field of neurology and neuroscience. The journal's focus on cutting-edge research and its swift publication schedule make it a valuable resource for researchers, clinicians, and other professionals interested in the study and treatment of neurological conditions.
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