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衰老小鼠肝脏中短期和长期热量限制效应的基因组分析

Genomic profiling of short- and long-term caloric restriction effects in the liver of aging mice.

作者信息

Cao S X, Dhahbi J M, Mote P L, Spindler S R

机构信息

Department of Biochemistry, University of California, Riverside, CA 92521, USA.

出版信息

Proc Natl Acad Sci U S A. 2001 Sep 11;98(19):10630-5. doi: 10.1073/pnas.191313598. Epub 2001 Sep 4.

Abstract

We present genome-wide microarray expression analysis of 11,000 genes in an aging potentially mitotic tissue, the liver. This organ has a major impact on health and homeostasis during aging. The effects of life- and health-span-extending caloric restriction (CR) on gene expression among young and old mice and between long-term CR (LT-CR) and short-term CR (ST-CR) were examined. This experimental design allowed us to accurately distinguish the effects of aging from those of CR on gene expression. Aging was accompanied by changes in gene expression associated with increased inflammation, cellular stress, and fibrosis, and reduced capacity for apoptosis, xenobiotic metabolism, normal cell-cycling, and DNA replication. LT-CR and just 4 weeks of ST-CR reversed the majority of these changes. LT-CR produced in young mice a pattern of gene expression that is a subset of the changes found in old LT-CR mice. It is possible that the early changes in gene expression, which extend into old age, are key to the life- and health-span-extending effects of CR. Further, ST-CR substantially shifted the "normo-aging" genomic profile of old control mice toward the "slow-aging" profile associated with LT-CR. Therefore, many of the genomic effects of CR are established rapidly. Thus, expression profiling should prove useful in quickly identifying CR- mimetic drugs and treatments.

摘要

我们展示了对肝脏这一潜在有丝分裂衰老组织中的11000个基因进行的全基因组微阵列表达分析。该器官在衰老过程中对健康和体内平衡有着重大影响。我们研究了延长寿命和健康寿命的热量限制(CR)对年轻和年老小鼠之间以及长期CR(LT-CR)和短期CR(ST-CR)之间基因表达的影响。这种实验设计使我们能够准确区分衰老和CR对基因表达的影响。衰老伴随着与炎症增加、细胞应激和纤维化相关的基因表达变化,以及细胞凋亡、异生物代谢、正常细胞周期和DNA复制能力的降低。LT-CR和仅4周的ST-CR逆转了这些变化中的大部分。LT-CR在年轻小鼠中产生的基因表达模式是老年LT-CR小鼠中发现的变化的一个子集。有可能延伸至老年的基因表达早期变化是CR延长寿命和健康寿命作用的关键。此外,ST-CR使老年对照小鼠的“正常衰老”基因组图谱显著向与LT-CR相关的“缓慢衰老”图谱转变。因此,CR的许多基因组效应迅速确立。因此,表达谱分析在快速识别CR模拟药物和治疗方法方面应该会很有用。

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