Role of clonal inflammatory microglia in histiocytosis-associated neurodegeneration.

IF 14.7 1区医学 Q1 NEUROSCIENCES

Neuron Pub Date : 2025-04-02 Epub Date: 2025-03-12 DOI:10.1016/j.neuron.2025.02.007

Rocio Vicario, Stamatina Fragkogianni, Maria Pokrovskii, Carina Meyer, Estibaliz Lopez-Rodrigo, Yang Hu, Masato Ogishi, Araitz Alberdi, Ann Baako, Oyku Ay, Isabelle Plu, Véronique Sazdovitch, Sebastien Heritier, Fleur Cohen-Aubart, Natalia Shor, Makoto Miyara, Florence Nguyen-Khac, Agnes Viale, Ahmed Idbaih, Zahir Amoura, Marc K Rosenblum, Haochen Zhang, Elias-Ramzey Karnoub, Palash Sashittal, Akhil Jakatdar, Christine A Iacobuzio-Donahue, Omar Abdel-Wahab, Viviane Tabar, Nicholas D Socci, Olivier Elemento, Eli L Diamond, Bertrand Boisson, Jean-Laurent Casanova, Danielle Seilhean, Julien Haroche, Jean Donadieu, Frederic Geissmann

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引用次数: 0

Abstract

Langerhans cell histiocytosis (LCH) and Erdheim-Chester disease (ECD) are clonal myeloid disorders associated with mitogen-activated protein (MAP)-kinase-activating mutations and an increased risk of neurodegeneration. We found microglial mutant clones in LCH and ECD patients, whether or not they presented with clinical symptoms of neurodegeneration, associated with microgliosis, astrocytosis, and neuronal loss, predominantly in the rhombencephalon gray nuclei. Neurological symptoms were associated with PU.1⁺ clone size (p = 0.0003) in patients with the longest evolution of the disease, indicating a phase of subclinical incipient neurodegeneration. Genetic barcoding analysis suggests that clones may originate from definitive or yolk sac hematopoiesis, depending on the patients. In a mouse model, disease topography was attributable to a local clonal proliferative advantage, and microglia depletion by a CSF1R-inhibitor limited neuronal loss and improved survival. These studies characterize a neurodegenerative disease associated with clonal proliferation of inflammatory microglia. The long preclinical stage represents a therapeutic window before irreversible neuronal depletion.

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克隆炎性小胶质细胞在组织细胞增生症相关神经变性中的作用

朗格汉斯细胞组织细胞增多症（LCH）和厄德海姆-切斯特病（ECD）是与丝裂原活化蛋白（MAP）激酶激活突变和神经变性风险增加相关的克隆性髓系疾病。我们在LCH和ECD患者中发现了小胶质细胞突变克隆，无论他们是否表现出神经变性的临床症状，与小胶质细胞增多、星形细胞增多和神经元丢失相关，主要发生在菱形脑灰色核。在病程发展最久的患者中，神经系统症状与PU.1+克隆大小相关（p = 0.0003），表明处于亚临床早期神经变性阶段。基因条形码分析表明，克隆可能来源于最终的或卵黄囊造血，这取决于患者。在小鼠模型中，疾病地形归因于局部克隆增殖优势，csf1r抑制剂引起的小胶质细胞耗损限制了神经元损失并提高了生存率。这些研究表征了一种与炎性小胶质细胞克隆性增殖相关的神经退行性疾病。漫长的临床前阶段代表了不可逆神经元耗竭之前的治疗窗口期。

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

Neuron 医学-神经科学

CiteScore

24.50

自引率

3.10%

发文量

382

审稿时长

1 months

期刊介绍： Established as a highly influential journal in neuroscience, Neuron is widely relied upon in the field. The editors adopt interdisciplinary strategies, integrating biophysical, cellular, developmental, and molecular approaches alongside a systems approach to sensory, motor, and higher-order cognitive functions. Serving as a premier intellectual forum, Neuron holds a prominent position in the entire neuroscience community.