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Titlebook: Cell Cycle Checkpoints; Methods and Protocol Willis X. Li Book 2011 Springer Science+Business Media, LLC 2011 DNA damage checkpoints.apopto

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楼主: COAX
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Analyzing DNA Replication Dynamics of Genotoxin-Treated Cells Using Velocity Sedimentation,ransduction pathways negatively regulate the initiation of DNA synthesis at unfired origins of replication, a process termed the ‘S-phase checkpoint’ or the ‘intra-S-phase checkpoint’. Additionally, many DNA lesions pose physical barriers to replication forks and therefore inhibit DNA synthesis dire
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A Human Cell Extract-Based Assay for the Activation of ATM and ATR Checkpoint Kinases,f DNA damage. In this chapter, we describe an in vitro biochemical assay to study the activation of ATM and ATR by double-stranded DNA breaks (DSBs) (Shiotani and Zou, 2009, .., 547–58). In this assay, DNA fragments with different structural features are used to activate ATM and ATR in human cell ex
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Using , S2 Cells to Measure S phase-Coupled Protein Destruction via Flow Cytometry,he destruction of several key cell cycle regulatory proteins during S phase is coupled directly to DNA replication. These proteins harbor a motif called a PIP degron that mediates binding to chromatin bound PCNA at replication forks and recruits the CRL4. E3 ubiquitin ligase. These interactions comp
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Indirect Immunofluorescence for Monitoring Spindle Assembly and Disassembly in Yeast,assembly status and position of the mitotic spindle, as well as cytoplasmic microtubules, can be monitored easily using indirect immunofluorescence with antibodies against tubulin. A detailed protocol is described for . that involves the fixation of actively growing cells, removal of the cell wall b
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Detecting Recruitment of DNA Damage Response Factors Through the eChIP Approach,DNA lesions whose repair mechanisms remain largely unclear. Uncovering proteins involved in the processing of ICLs and understand how they interact with the damaged DNA in vivo is crucial for the understanding of DNA interstrand crosslink repair processes. Moreover, the presence of an ICL during S p
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Late Medieval and Renaissance Europeto kill checkpoint mutants preferentially over wild-type. The differential use of wild-type and checkpoint mutants has the potential to identify molecules that act in a genotype-specific manner to eradicate checkpoint mutant tissues when combined with radiation, while sparing wild-type tissues.
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