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蓝斑核的新奇样激活可防止人类前缠结tau蛋白的有害影响,而应激诱导的激活则会使其影响恶化。

Novelty-like activation of locus coeruleus protects against deleterious human pretangle tau effects while stress-inducing activation worsens its effects.

作者信息

Omoluabi Tamunotonye, Torraville Sarah E, Maziar Aida, Ghosh Abhinaba, Power Kyron D, Reinhardt Camila, Harley Carolyn W, Yuan Qi

机构信息

Division of Biomedical Sciences, Faculty of Medicine Memorial University St. John's Newfoundland and Labrador Canada.

Department of Psychology, Faculty of Science Memorial University St. John's Newfoundland and Labrador Canada.

出版信息

Alzheimers Dement (N Y). 2021 Dec 31;7(1):e12231. doi: 10.1002/trc2.12231. eCollection 2021.

Abstract

The earliest abnormality associated with Alzheimer's disease (AD) is the presence of persistently phosphorylated pretangle tau in locus coeruleus (LC) neurons. LC neuron numbers and fiber density are positive predictors of cognition prior to death. Using an animal model of LC pretangle tau, we ask if LC activity patterns influence the sequelae of pretangle tau. We seeded LC neurons with a pretangle human tau gene. We provided daily novelty- or stress-associated optogenetic activation patterns to LC neurons for 6 weeks in mid-adulthood and, subsequently, probed cognitive and anatomical changes. Prior LC phasic stimulation prevented spatial and olfactory discrimination deficits and preserved LC axonal density. A stress-associated activation pattern increased indices of anxiety and depression, did not improve cognition, and worsened LC neuronal health. These results argue that variations in environmental experiences associated with differing LC activity patterns may account for individual susceptibility to development of AD in humans.

摘要

与阿尔茨海默病(AD)相关的最早异常是蓝斑(LC)神经元中持续磷酸化的前缠结tau蛋白的存在。LC神经元数量和纤维密度是死亡前认知的阳性预测指标。使用LC前缠结tau蛋白的动物模型,我们探究LC活动模式是否会影响前缠结tau蛋白的后遗症。我们将人前缠结tau基因导入LC神经元。在成年中期,我们每天为LC神经元提供与新奇或应激相关的光遗传学激活模式,持续6周,随后探究认知和解剖学变化。先前的LC相位刺激可预防空间和嗅觉辨别缺陷,并保留LC轴突密度。与应激相关的激活模式增加了焦虑和抑郁指数,没有改善认知,反而恶化了LC神经元健康。这些结果表明,与不同LC活动模式相关的环境经历差异可能解释了人类个体对AD发展的易感性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1b61/8719346/32b5b9016539/TRC2-7-e12231-g001.jpg

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