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衰老神经元中雄性特异性行为和转录组变化。

Male-specific behavioral and transcriptomic changes in aging neurons.

作者信息

Weng Yifei, Murphy Coleen T

机构信息

Department of Molecular Biology, Princeton University, Princeton, NJ 08544, USA.

LSI Genomics, Princeton University, Princeton, NJ 08544, USA.

出版信息

iScience. 2024 May 8;27(6):109910. doi: 10.1016/j.isci.2024.109910. eCollection 2024 Jun 21.

Abstract

Aging is a complex biological process with sexually dimorphic aspects. Although cognitive aging of hermaphrodites has been studied, less is known about cognitive decline in males. We found that cognitive aging has both sex-shared and sex-dimorphic characteristics, and we identified neuron-specific age-associated sex-differential targets. In addition to sex-shared neuronal aging genes, males differentially downregulate mitochondrial metabolic genes and upregulate GPCR genes with age, while the X chromosome exhibits increased gene expression in hermaphrodites and altered dosage compensation complex expression with age, indicating possible X chromosome dysregulation that contributes to sexual dimorphism in cognitive aging. Finally, the sex-differentially expressed gene , an aspartic-type endopeptidase, regulates male cognitive aging but does not affect hermaphrodites' behaviors. These results suggest that males and hermaphrodites exhibit different age-related neuronal changes. This study will strengthen our understanding of sex-specific vulnerability and resilience and identify pathways to target with treatments that could benefit both sexes.

摘要

衰老 是一个具有性别差异特征的复杂生物学过程。尽管已经对雌雄同体的认知衰老进行了研究,但对于雄性的认知衰退了解较少。我们发现认知衰老具有性别共享和性别差异的特征,并且我们确定了神经元特异性的年龄相关性别差异靶点。除了性别共享的神经元衰老基因外,雄性随着年龄增长会差异性地下调线粒体代谢基因并上调GPCR基因,而X染色体在雌雄同体中表现出基因表达增加以及随着年龄增长剂量补偿复合体表达发生改变,这表明可能存在X染色体失调,其导致了认知衰老中的性别差异。最后,性别差异表达基因,一种天冬氨酸型内肽酶,调节雄性认知衰老,但不影响雌雄同体的行为。这些结果表明,雄性和雌雄同体表现出不同的与年龄相关的神经元变化。这项研究将加强我们对性别特异性易感性和恢复力的理解,并确定可通过治疗针对的途径,这些治疗可能对两性都有益。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f29/11111838/ba52747ae41b/fx1.jpg

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