Literature DB >> 28668129

What Combined Measurements From Structures and Imaging Tell Us About DNA Damage Responses.

Chris A Brosey1, Zamal Ahmed1, Susan P Lees-Miller2, John A Tainer3.   

Abstract

DNA damage outcomes depend upon the efficiency and fidelity of DNA damage responses (DDRs) for different cells and damage. As such, DDRs represent tightly regulated prototypical systems for linking nanoscale biomolecular structure and assembly to the biology of genomic regulation and cell signaling. However, the dynamic and multifunctional nature of DDR assemblies can render elusive the correlation between the structures of DDR factors and specific biological disruptions to the DDR when these structures are altered. In this chapter, we discuss concepts and strategies for combining structural, biophysical, and imaging techniques to investigate DDR recognition and regulation, and thus bridge sequence-level structural biochemistry to quantitative biological outcomes visualized in cells. We focus on representative DDR responses from PARP/PARG/AIF damage signaling in DNA single-strand break repair and nonhomologous end joining complexes in double-strand break repair. Methods with exemplary experimental results are considered with a focus on strategies for probing flexibility, conformational changes, and assembly processes that shape a predictive understanding of DDR mechanisms in a cellular context. Integration of structural and imaging measurements promises to provide foundational knowledge to rationally control and optimize DNA damage outcomes for synthetic lethality and for immune activation with resulting insights for biology and cancer interventions.
© 2017 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  Apoptosis; Cancer Genome; DNA damage response; DNA double-strand breaks; Excision repair; Genome instability; Homologous recombination; Molecular mimicry; Nonhomologous end joining; Replication; Small-angle X-ray scattering; Super-resolution imaging; Transcription

Mesh:

Substances:

Year:  2017        PMID: 28668129      PMCID: PMC5549440          DOI: 10.1016/bs.mie.2017.04.005

Source DB:  PubMed          Journal:  Methods Enzymol        ISSN: 0076-6879            Impact factor:   1.600


  167 in total

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5.  XLF and APLF bind Ku80 at two remote sites to ensure DNA repair by non-homologous end joining.

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