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单核苷酸变体 (SNVs) 定义了衰老加速 SAMP8 小鼠,这是一种老年病模型。

Single nucleotide variants (SNVs) define senescence-accelerated SAMP8 mice, a model of a geriatric condition.

机构信息

Brain and Mind Research Institute, University of Sydney, Camperdown, NSW, Australia.

出版信息

J Alzheimers Dis. 2013;36(2):349-63. doi: 10.3233/JAD-130089.

Abstract

One of the major challenges in neurodegenerative research is modeling systemic aging. Here, senescence-accelerated mice such as the multigenic SAMP8 (senescence accelerated prone 8) mice are useful as they are characterized by an early manifestation of senescence that includes a shortened lifespan and impaired brain and immune functions. While SAMP8 mice are widely used tools to address aging and neurodegenerative conditions such as Alzheimer's disease (AD), the underlying gene mutations are not known. To make the SAMP8 strain a more versatile and useful research tool, we performed exome sequencing, using SAMR1 (senescence accelerated mouse resistant 1) mice as controls. We identified 51 SNVs (single nucleotide variants) that discriminate SAMP8 from SAMR1 mice. Using the prediction tool Polyphen2, we were able to subdivide the SNVs into four categories: splice variants, probably damaging, possibly damaging, and benign. Of these genes, a significant fraction is predicted to be expressed in the brain. Our data present these genes for a more detailed analysis in aging and neurodegeneration studies. They underscore the usefulness of SAMP8 mice as an animal model to study fundamental mechanisms of both aging and the pathogenesis of AD.

摘要

神经退行性疾病研究的主要挑战之一是建立全身性衰老模型。在这里,多基因 SAMP8(衰老加速敏感 8)小鼠是有用的,因为它们的特征是衰老的早期表现,包括寿命缩短和大脑及免疫功能受损。虽然 SAMP8 小鼠是广泛用于研究衰老和神经退行性疾病(如阿尔茨海默病)的工具,但导致其衰老的潜在基因突变尚不清楚。为了使 SAMP8 品系成为一种更通用、更有用的研究工具,我们使用 SAMR1(衰老加速抵抗 1)小鼠作为对照进行外显子组测序。我们鉴定出 51 个可区分 SAMP8 和 SAMR1 小鼠的单核苷酸变异(SNVs)。使用 Polyphen2 预测工具,我们将这些 SNVs 细分为四类:剪接变异体、可能有害、可能有害和良性。这些基因中有很大一部分被预测在大脑中表达。我们的数据为衰老和神经退行性变研究中的这些基因提供了更详细的分析。它们强调了 SAMP8 小鼠作为研究衰老和 AD 发病机制的基础机制的动物模型的有用性。

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