Molecular basis of neurodegeneration in a mouse model of Polr3-related disease.

IF 6.4 1区 生物学 Q1 BIOLOGY
eLife Pub Date : 2024-11-05 DOI:10.7554/eLife.95314
Robyn D Moir, Emilio Merheb, Violeta Chitu, E Richard Stanley, Ian M Willis
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引用次数: 0

Abstract

Pathogenic variants in subunits of RNA polymerase (Pol) III cause a spectrum of Polr3-related neurodegenerative diseases including 4H leukodystrophy. Disease onset occurs from infancy to early adulthood and is associated with a variable range and severity of neurological and non-neurological features. The molecular basis of Polr3-related disease pathogenesis is unknown. We developed a postnatal whole-body mouse model expressing pathogenic Polr3a mutations to examine the molecular mechanisms by which reduced Pol III transcription results primarily in central nervous system phenotypes. Polr3a mutant mice exhibit behavioral deficits, cerebral pathology and exocrine pancreatic atrophy. Transcriptome and immunohistochemistry analyses of cerebra during disease progression show a reduction in most Pol III transcripts, induction of innate immune and integrated stress responses and cell-type-specific gene expression changes reflecting neuron and oligodendrocyte loss and microglial activation. Earlier in the disease when integrated stress and innate immune responses are minimally induced, mature tRNA sequencing revealed a global reduction in tRNA levels and an altered tRNA profile but no changes in other Pol III transcripts. Thus, changes in the size and/or composition of the tRNA pool have a causal role in disease initiation. Our findings reveal different tissue- and brain region-specific sensitivities to a defect in Pol III transcription.

Polr3 相关疾病小鼠模型神经退行性变的分子基础
RNA 聚合酶(Pol)III 亚基的致病变体会导致一系列与 Polr3 相关的神经退行性疾病,包括 4H 白营养不良症。疾病的发病期从婴儿期到成年早期不等,并伴有不同范围和严重程度的神经和非神经特征。Polr3 相关疾病发病机制的分子基础尚不清楚。我们开发了一种表达致病性 Polr3a 突变的出生后全身小鼠模型,以研究 Pol III 转录减少主要导致中枢神经系统表型的分子机制。Polr3a 突变小鼠表现出行为缺陷、脑病理学和胰腺外分泌萎缩。对疾病进展过程中大脑的转录组和免疫组化分析表明,大多数 Pol III 转录物减少,先天性免疫和综合应激反应诱导,细胞类型特异性基因表达发生变化,反映出神经元和少突胶质细胞丢失以及小胶质细胞活化。在疾病早期,综合应激反应和先天性免疫反应诱导程度较低时,成熟 tRNA 测序显示 tRNA 水平全面下降,tRNA 配置发生改变,但其他 Pol III 转录本没有变化。因此,tRNA池的大小和/或组成的变化在疾病的发生中起着因果作用。我们的研究结果揭示了不同组织和脑区对 Pol III 转录缺陷的不同敏感性。
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来源期刊
eLife
eLife BIOLOGY-
CiteScore
12.90
自引率
3.90%
发文量
3122
审稿时长
17 weeks
期刊介绍: eLife is a distinguished, not-for-profit, peer-reviewed open access scientific journal that specializes in the fields of biomedical and life sciences. eLife is known for its selective publication process, which includes a variety of article types such as: Research Articles: Detailed reports of original research findings. Short Reports: Concise presentations of significant findings that do not warrant a full-length research article. Tools and Resources: Descriptions of new tools, technologies, or resources that facilitate scientific research. Research Advances: Brief reports on significant scientific advancements that have immediate implications for the field. Scientific Correspondence: Short communications that comment on or provide additional information related to published articles. Review Articles: Comprehensive overviews of a specific topic or field within the life sciences.
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