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Murine adult neural progenitor cells alter their proliferativebehavior and gene expression after the activation of Toll-like-receptor3

机译:小鼠成年神经祖细胞改变其增殖Toll样受体激活后的行为和基因表达3

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摘要

Viral infections during pregnancy significantly increase the risk for psychological pathologies like schizophrenia in the offspring. One of the main morphological hallmarks of schizophrenia is a reduced size of the hippocampus. Since new neurons are produced in this particular brain compartment throughout life, it might be possible that low neurogenesis levels triggered by a maternal viral infection contribute to developmental deficits of the hippocampus. We injected polyinosinic:polycytidylic acid (Poly I:C) in pregnant C57Bl/6 mice to stimulate an anti-viral response through TLR3 and examined gene expressions in the neuronal progenitor cells (NPCs) of the offspring at different ages. Additionally, we treated adult NPC lines with Poly I:C to investigate its direct effect. We could show for the first time that TLR3 and its downstream effector molecule IRF3 are expressed in adult NPCs. Poly I:C treatment in vitro and in vivo led to the regulation of proliferation and genes involved in antiviral response, migration, and survival. These findings indicate that NPCs of the fetus are able to react towards an in utero immune response, and thus, changes in the neuronal stem cell pool can contribute to the development of neurological diseases likeschizophrenia.
机译:怀孕期间的病毒感染会大大增加后代发生精神分裂症等心理疾病的风险。精神分裂症的主要形态学特征之一是海马体大小减少。由于整个一生都会在这个特定的大脑隔室中产生新的神经元,因此由母体病毒感染触发的低神经发生水平可能导致海马的发育缺陷。我们在怀孕的C57Bl / 6小鼠中注射了多肌苷酸:聚胞苷酸(Poly I:C)以通过TLR3刺激抗病毒反应,并检查了不同年龄后代的神经元祖细胞(NPC)中的基因表达。此外,我们用Poly I:C处理了成年NPC品系,以研究其直接作用。我们可以首次证明TLR3及其下游效应分子IRF3在成年NPC中表达。在体外和体内,Poly I:C治疗导致了调控增殖和涉及抗病毒反应,迁移和存活的基因的调控。这些发现表明,胎儿的NPC能够对子宫内免疫反应做出反应,因此,神经元干细胞池的变化可以促进神经系统疾病的发展,例如精神分裂症。

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