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Genome-wide profiling of DNA methyltransferases in mammalian cells

Authors :
Vavouri, Tanya
Peinado, Miguel A
Vavouri, T ( Tanya )
Peinado, M A ( Miguel A )
Manzo, Massimiliano
Ambrosi, Christina
Baubec, Tuncay; https://orcid.org/0000-0001-8474-6587
Vavouri, Tanya
Peinado, Miguel A
Vavouri, T ( Tanya )
Peinado, M A ( Miguel A )
Manzo, Massimiliano
Ambrosi, Christina
Baubec, Tuncay; https://orcid.org/0000-0001-8474-6587
Source :
Manzo, Massimiliano; Ambrosi, Christina; Baubec, Tuncay (2018). Genome-wide profiling of DNA methyltransferases in mammalian cells. In: Vavouri, Tanya; Peinado, Miguel A. CpG Islands. Berlin, Germany: Springer, 157-174.
Publication Year :
2018

Abstract

Chromatin immunoprecipitation followed by high-throughput sequencing (ChIP-seq) is currently the method of choice to determine binding sites of chromatin-associated factors in a genome-wide manner. Here, we describe a method to investigate the binding preferences of mammalian DNA methyltransferases (DNMT) based on ChIP-seq using biotin-tagging. Stringent ChIP of DNMT proteins based on the strong interaction between biotin and avidin circumvents limitations arising from low antibody specificity and ensures reproducible enrichment. DNMT-bound DNA fragments are ligated to sequencing adaptors, amplified and sequenced on a high-throughput sequencing instrument. Bioinformatic analysis gives valuable information about the binding preferences of DNMTs genome-wide and around promoter regions. This method is unconventional due to the use of genetically engineered cells; however, it allows specific and reliable determination of DNMT binding.

Details

Database :
OAIster
Journal :
Manzo, Massimiliano; Ambrosi, Christina; Baubec, Tuncay (2018). Genome-wide profiling of DNA methyltransferases in mammalian cells. In: Vavouri, Tanya; Peinado, Miguel A. CpG Islands. Berlin, Germany: Springer, 157-174.
Notes :
English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1415665756
Document Type :
Electronic Resource