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Cell cycle-specific measurement of γH2AX and apoptosis after genotoxic stress by flow cytometry

The presented method or slightly modified versions have been devised to study specific treatment responses and side effects of various anti-cancer treatments as used in clinical oncology. It enables a quantitative and longitudinal analysis of the DNA damage response after genotoxic stress, as induce...

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Bibliographic Details
Main Authors: Lopez Perez, Ramon (Author) , Münz, Franziska (Author) , Kroschke, Jonas (Author) , Brauer, Jannek (Author) , Nicolay, Nils (Author) , Huber, Peter E. (Author)
Format: Article (Journal) Video
Language:English
Published: 9/01/2019
In: JoVE. Video journal
Year: 2019, Issue: 151, Pages: ?
ISSN:1940-087X
DOI:10.3791/59968
Subjects:
Film
Online Access:Verlag, Volltext: https://doi.org/10.3791/59968
Verlag, Volltext: https://www.jove.com/video/59968/cell-cycle-specific-measurement-h2ax-apoptosis-after-genotoxic-stress
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Author Notes:Ramon Lopez Perez, Franziska Münz, Jonas Kroschke, Jannek Brauer, Nils H. Nicolay, Peter E. Huber
Description
Summary:The presented method or slightly modified versions have been devised to study specific treatment responses and side effects of various anti-cancer treatments as used in clinical oncology. It enables a quantitative and longitudinal analysis of the DNA damage response after genotoxic stress, as induced by radiotherapy and a multitude of anti-cancer drugs. The method covers all stages of the DNA damage response, providing endpoints for induction and repair of DNA double-strand breaks (DSBs), cell cycle arrest and cell death by apoptosis in case of repair failure. Combining these measurements provides information about cell cycle-dependent treatment effects and thus allows an in-depth study of the interplay between cellular proliferation and coping mechanisms against DNA damage. As the effect of many cancer therapeutics including chemotherapeutic agents and ionizing radiation is limited to or strongly varies according to specific cell cycle phases, correlative analyses rely on a robust and feasible method to assess the treatment effects on the DNA in a cell cycle-specific manner. This is not possible with single-endpoint assays and an important advantage of the presented method. The method is not restricted to any particular cell line and has been thoroughly tested in a multitude of tumor and normal tissue cell lines. It can be widely applied as a comprehensive genotoxicity assay in many fields of oncology besides radio-oncology, including environmental risk factor assessment, drug screening and evaluation of genetic instability in tumor cells.
Item Description:Enthält auch eine Versuchsbeschreibung in Textform
Gesehen am 02.12.2019
Wissenschaftlicher Film. Deutschland. 2019
Physical Description:Online Resource
ISSN:1940-087X
DOI:10.3791/59968

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