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  4. TOR1 Gene Regulates Genome Stability in Mismatch Repair Defected Cells during Chronological Aging in Saccharomyces cerevisiae
 
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TOR1 Gene Regulates Genome Stability in Mismatch Repair Defected Cells during Chronological Aging in Saccharomyces cerevisiae

Date Issued
2014
Date
2014
Author(s)
Chang, Jia-Ci
URI
http://ntur.lib.ntu.edu.tw//handle/246246/262465
Abstract
Mismatch repair (MMR) is a DNA repair system which is critical for the maintenance of genome stability. Defects in mismatch repair have been linked to colorectal and sporadic cancers. Calorie restriction (CR) has been shown to extend life span and increases stress resistance via TOR/SCH9 and RAS signaling pathways in various organisms. We have found that CR containing 0.5% glucose compared to normal treatment (2.0% glucose) can extend life span and promote HOM3 gene stability in MMR-defected cells during aging process in yeast previously. Here, we demonstrate tor1∆ can mimic CR condition and extend life span of msh2∆ and msh3∆ mutants with low mutation frequency. We also found the levels of reactive oxygen species (ROS) were significantly increased during aging and tor1∆ dramatically reduced the levels of ROS. However, tor1∆ could not completely reverse mutation rates in msh2∆msh3∆ mutants. According to these, we believe TOR1 gene can only partially regulates genome stability in MMR defected cells during aging. Whether RAS also affects the genome stability in MMR defected cells during aging needs to be further investigated.
Subjects
老化
錯誤配對修復系統
TOR1
酵母菌
熱量限制
SDGs

[SDGs]SDG3

Type
thesis
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ntu-103-R01641010-1.pdf

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(MD5):233799ffb33668710291d940385cce5e

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