Literature DB >> 26863565

Genome-wide Mapping of Drug-DNA Interactions in Cells with COSMIC (Crosslinking of Small Molecules to Isolate Chromatin).

Graham S Erwin1, Matthew P Grieshop1, Devesh Bhimsaria2, Asuka Eguchi3, José A Rodríguez-Martínez1, Aseem Z Ansari4.   

Abstract

The genome is the target of some of the most effective chemotherapeutics, but most of these drugs lack DNA sequence specificity, which leads to dose-limiting toxicity and many adverse side effects. Targeting the genome with sequence-specific small molecules may enable molecules with increased therapeutic index and fewer off-target effects. N-methylpyrrole/N-methylimidazole polyamides are molecules that can be rationally designed to target specific DNA sequences with exquisite precision. And unlike most natural transcription factors, polyamides can bind to methylated and chromatinized DNA without a loss in affinity. The sequence specificity of polyamides has been extensively studied in vitro with cognate site identification (CSI) and with traditional biochemical and biophysical approaches, but the study of polyamide binding to genomic targets in cells remains elusive. Here we report a method, the crosslinking of small molecules to isolate chromatin (COSMIC), that identifies polyamide binding sites across the genome. COSMIC is similar to chromatin immunoprecipitation (ChIP), but differs in two important ways: (1) a photocrosslinker is employed to enable selective, temporally-controlled capture of polyamide binding events, and (2) the biotin affinity handle is used to purify polyamide-DNA conjugates under semi-denaturing conditions to decrease DNA that is non-covalently bound. COSMIC is a general strategy that can be used to reveal the genome-wide binding events of polyamides and other genome-targeting chemotherapeutic agents.

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Year:  2016        PMID: 26863565      PMCID: PMC4781686          DOI: 10.3791/53510

Source DB:  PubMed          Journal:  J Vis Exp        ISSN: 1940-087X            Impact factor:   1.355


  68 in total

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3.  Mapping polyamide-DNA interactions in human cells reveals a new design strategy for effective targeting of genomic sites.

Authors:  Graham S Erwin; Devesh Bhimsaria; Asuka Eguchi; Aseem Z Ansari
Journal:  Angew Chem Int Ed Engl       Date:  2014-07-27       Impact factor: 15.336

4.  Base-catalyzed reversal of a psoralen-DNA cross-link.

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Journal:  Biochemistry       Date:  1988-07-12       Impact factor: 3.162

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Authors:  Ganesh N Pandian; Ken-ichi Shinohara; Akimichi Ohtsuki; Yusuke Nakano; Minoshima Masafumi; Toshikazu Bando; Hiroki Nagase; Yasuhiro Yamada; Akira Watanabe; Naohiro Terada; Shinsuke Sato; Hironobu Morinaga; Hiroshi Sugiyama
Journal:  Chembiochem       Date:  2011-10-28       Impact factor: 3.164

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Journal:  Proc Natl Acad Sci U S A       Date:  2014-06-13       Impact factor: 11.205

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Journal:  Chem Biol       Date:  2000-03

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Authors:  V Jackson
Journal:  Methods       Date:  1999-02       Impact factor: 3.608

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Authors:  Karl E Hauschild; James S Stover; Dale L Boger; Aseem Z Ansari
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Authors:  Peter V Kharchenko; Michael Y Tolstorukov; Peter J Park
Journal:  Nat Biotechnol       Date:  2008-11-16       Impact factor: 54.908

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  1 in total

1.  Estimating genome-wide off-target effects for pyrrole-imidazole polyamide binding by a pathway-based expression profiling approach.

Authors:  Jason Lin; Sakthisri Krishnamurthy; Hiroyuki Yoda; Yoshinao Shinozaki; Takayoshi Watanabe; Nobuko Koshikawa; Atsushi Takatori; Paul Horton; Hiroki Nagase
Journal:  PLoS One       Date:  2019-04-09       Impact factor: 3.240

  1 in total

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