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Titlebook: Stress Responses; Methods and Protocol Christine M. Oslowski Book 2015 Springer Science+Business Media New York 2015 cellular pathways.cell

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Book 2015ular stresses in select diseases. In addition, this book reviews the crosstalk between different stress pathways, stress responses during ageing, and targeting stress for regenerative medicine. Written in the highly successful .Methods of Molecular Biology. series format, chapters include introducti
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Visualizing the Spatiotemporal Dynamics of DNA Damage in Budding Yeastion of DNA double-strand breaks (DSBs) relative to the nuclear envelope. The second part describes how to quantify the co-localization of DNA DSBs with nuclear pore clusters, or other nuclear subcompartments. The final protocols describe methods for the quantification of locus mobility over time.
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Methods for Studying microRNA Functions During Stressrological disorders. Intriguingly, many phenotypes of microRNA deficiencies are subdued in normal condition but manifested apparently upon stress. Here, we outline experimental methods to monitor the level, targets, and activity of microRNAs as the first few steps to characterize how microRNA functions are altered upon stress.
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Methods for Studying ER Stress and UPR Markers in Human Cellsed proteins in the ER lumen which is sensed by three ER-resident transmembrane proteins, PERK, ATF6, and IRE1. Their activation by such ER stress affects the unfolded protein response, which consists of a shutoff of protein translation and at the same time the switching-on of specific transcription
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Immunofluorescence-Based Methods to Monitor DNA End Resection (e.g., DNA replication stress) and exogenous insults (e.g., ionizing radiation). DSBs are principally repaired by one of two major pathways: nonhomologous end joining (NHEJ) or homologous recombination (HR). NHEJ is an error-prone process that can occur in all phases of the cell cycle, while HR is
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Visualizing the Spatiotemporal Dynamics of DNA Damage in Budding Yeast Three microscopic techniques can be used to study the spatiotemporal dynamics of DNA damage. In the first part we describe how we determine the position of DNA double-strand breaks (DSBs) relative to the nuclear envelope. The second part describes how to quantify the co-localization of DNA DSBs wit
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