Literature DB >> 28623092

CtIP/Ctp1/Sae2, molecular form fit for function.

Sara N Andres1, R Scott Williams2.   

Abstract

Vertebrate CtIP, and its fission yeast (Ctp1), budding yeast (Sae2) and plant (Com1) orthologs have emerged as key regulatory molecules in cellular responses to DNA double strand breaks (DSBs). By modulating the nucleolytic 5'-3' resection activity of the Mre11/Rad50/Nbs1 (MRN) DSB repair processing and signaling complex, CtIP/Ctp1/Sae2/Com1 is integral to the channeling of DNA double strand breaks through DSB repair by homologous recombination (HR). Nearly two decades since its discovery, emerging new data are defining the molecular underpinnings for CtIP DSB repair regulatory activities. CtIP homologs are largely intrinsically unstructured proteins comprised of expanded regions of low complexity sequence, rather than defined folded domains typical of DNA damage metabolizing enzymes and nucleases. A compact structurally conserved N-terminus forms a functionally critical tetrameric helical dimer of dimers (THDD) region that bridges CtIP oligomers, and is flexibly appended to a conserved C-terminal Sae2-homology DNA binding and DSB repair pathway choice regulatory hub which influences nucleolytic activities of the MRN core nuclease complex. The emerging evidence from structural, biophysical, and biological studies converges on CtIP having functional roles in DSB repair that include: 1) dynamic DNA strand coordination through direct DNA binding and DNA bridging activities, 2) MRN nuclease complex cofactor functions that direct MRN endonucleolytic cleavage of protein-blocked DSB ends and 3) acting as a protein binding hub targeted by the cell cycle regulatory apparatus, which influences CtIP expression and activity via layers of post-translational modifications, protein-protein interactions and DNA binding. Published by Elsevier B.V.

Entities:  

Keywords:  CtIP/Ctp1/Sae2; DNA bridging; Homologous recombination; Intrinsically disordered proteins; Resection

Mesh:

Substances:

Year:  2017        PMID: 28623092      PMCID: PMC5543718          DOI: 10.1016/j.dnarep.2017.06.013

Source DB:  PubMed          Journal:  DNA Repair (Amst)        ISSN: 1568-7856


  109 in total

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Authors:  R Scott Williams; Jessica S Williams; John A Tainer
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Authors:  Lorraine S Symington
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7.  Molecular characterization of the role of the Schizosaccharomyces pombe nip1+/ctp1+ gene in DNA double-strand break repair in association with the Mre11-Rad50-Nbs1 complex.

Authors:  Yufuko Akamatsu; Yasuto Murayama; Takatomi Yamada; Tomofumi Nakazaki; Yasuhiro Tsutsui; Kunihiro Ohta; Hiroshi Iwasaki
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Review 8.  An Overview of the Molecular Mechanisms of Recombinational DNA Repair.

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Authors:  Josep V Forment; Stephen P Jackson; Luca Pellegrini
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10.  Mre11 regulates CtIP-dependent double-strand break repair by interaction with CDK2.

Authors:  Jeffrey Buis; Trina Stoneham; Elizabeth Spehalski; David O Ferguson
Journal:  Nat Struct Mol Biol       Date:  2012-01-08       Impact factor: 15.369

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  17 in total

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Authors:  Hannah L Klein; Giedrė Bačinskaja; Jun Che; Anais Cheblal; Rajula Elango; Anastasiya Epshtein; Devon M Fitzgerald; Belén Gómez-González; Sharik R Khan; Sandeep Kumar; Bryan A Leland; Léa Marie; Qian Mei; Judith Miné-Hattab; Alicja Piotrowska; Erica J Polleys; Christopher D Putnam; Elina A Radchenko; Anissia Ait Saada; Cynthia J Sakofsky; Eun Yong Shim; Mathew Stracy; Jun Xia; Zhenxin Yan; Yi Yin; Andrés Aguilera; Juan Lucas Argueso; Catherine H Freudenreich; Susan M Gasser; Dmitry A Gordenin; James E Haber; Grzegorz Ira; Sue Jinks-Robertson; Megan C King; Richard D Kolodner; Andrei Kuzminov; Sarah Ae Lambert; Sang Eun Lee; Kyle M Miller; Sergei M Mirkin; Thomas D Petes; Susan M Rosenberg; Rodney Rothstein; Lorraine S Symington; Pawel Zawadzki; Nayun Kim; Michael Lisby; Anna Malkova
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6.  Intrinsically disordered regions regulate both catalytic and non-catalytic activities of the MutLα mismatch repair complex.

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8.  CtIP is essential for telomere replication.

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Review 9.  Functional and structural insights into the MRX/MRN complex, a key player in recognition and repair of DNA double-strand breaks.

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Review 10.  A Review of the Recent Advances Made with SIRT6 and its Implications on Aging Related Processes, Major Human Diseases, and Possible Therapeutic Targets.

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