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增殖停滞在正常及克雅氏病病原体(CJ)感染的大鼠中隔神经元中诱导神经元分化和先天免疫反应。

Proliferative arrest induces neuronal differentiation and innate immune responses in normal and Creutzfeldt-Jakob Disease agent (CJ) infected rat septal neurons.

作者信息

Pagano Nathan, Perez Gerard Aguilar, Garcia-Milian Rolando, Manuelidis Laura

机构信息

Yale University Medical School, 333 Cedar Street, Room FMB11, New Haven CT 06510.

出版信息

bioRxiv. 2025 Feb 3:2024.07.26.605349. doi: 10.1101/2024.07.26.605349.

DOI:10.1101/2024.07.26.605349
PMID:39131355
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11312452/
Abstract

Rat post-mitotic septal neurons, engineered to proliferate and arrest under physiological conditions can be maintained for weeks without cytotoxic effects. Nine independent cDNA libraries were made to follow arrest-induced neural differentiation and innate immune responses in normal uninfected and CJ agent infected septal neurons for weeks. CJ infection created a non-productive latent (CJ-) and a productive (CJ+) high infectivity model (10 logs/gm). Arrest of normal uninfected cells upregulated a plethora of anti-proliferative transcripts and known neuronal differentiation transcripts (e.g., Agtr2, Neuregulin-1, GDF6, SFRP4 and Prnp). Notably, many activated IFN innate immune genes were simultaneously upregulated (e.g., OAS1, RTP4, ISG20, GTB4, CD80, cytokines, chemokines and complement) along with clusterin (CLU) that binds misfolded proteins. Arrest of latently infected CJ- cells induced even more profound global transcript differences. CJ+ cells markedly downregulated the anti-proliferative controls seen in arrested normal cells. CJ+ infection also suppressed neuronal differentiation transcripts, including Prnp which is essential for CJ agent infection. Additionally, IFN and cytokine/chemokine pathways were also strongly enhanced. Analysis of the 342 CJ+ unique transcripts revealed additional innate immune and anti-viral-linked transcripts, e.g., Il17, ISG15, and RSAD2 (viperin). These data show: 1) innate immune transcripts are produced by normal neurons during differentiation; 2) CJ infection enhances and expands anti-viral responses; 3) non-productive latent infection can epigenetically imprint many proliferative pathways to thwart complete arrest. Consequently, human blood and intestinal myeloid peripheral cells that are latently infected (silent) for many years may be stimulated in vitro to produce CJ+ linked diagnostic transcripts.

摘要

经过基因工程改造后能在生理条件下增殖和停滞的大鼠有丝分裂后间隔神经元,可以维持数周而无细胞毒性作用。制备了9个独立的cDNA文库,用于追踪正常未感染和感染克雅氏病(CJ)病原体的间隔神经元中,停滞诱导的神经分化和固有免疫反应长达数周。CJ感染产生了一种非增殖性潜伏(CJ-)和一种增殖性(CJ+)高感染性模型(10个对数/克)。正常未感染细胞的停滞上调了大量抗增殖转录本和已知的神经分化转录本(如Agtr2、神经调节蛋白-1、生长分化因子6、分泌型卷曲相关蛋白4和朊蛋白)。值得注意的是,许多激活的干扰素固有免疫基因同时上调(如2'-5'-寡腺苷酸合成酶1、RTP4、干扰素刺激基因20、GTB4、CD80、细胞因子、趋化因子和补体),同时还有与错误折叠蛋白结合的簇集蛋白(CLU)。潜伏感染的CJ-细胞的停滞诱导了更深刻的全局转录差异。CJ+细胞显著下调了在停滞的正常细胞中所见的抗增殖调控因子。CJ+感染还抑制了神经分化转录本,包括对CJ病原体感染至关重要的朊蛋白。此外,干扰素和细胞因子/趋化因子途径也被强烈增强。对342个CJ+独特转录本的分析揭示了额外的固有免疫和抗病毒相关转录本,如白细胞介素17、ISG-15和RSAD2(蝰蛇毒素)。这些数据表明:1)正常神经元在分化过程中产生固有免疫转录本;2)CJ感染增强并扩大抗病毒反应;3)非增殖性潜伏感染可在表观遗传上印记许多增殖途径以阻止完全停滞。因此,多年来潜伏感染(无症状)的人类血液和肠道髓样外周细胞可能在体外被刺激产生与CJ+相关的诊断转录本。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3512/11828568/031d1c553b4e/nihpp-2024.07.26.605349v3-f0009.jpg
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https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3512/11828568/15e92a4b305e/nihpp-2024.07.26.605349v3-f0006.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3512/11828568/a42a6f29d205/nihpp-2024.07.26.605349v3-f0007.jpg
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https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3512/11828568/031d1c553b4e/nihpp-2024.07.26.605349v3-f0009.jpg

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