Direct regulation of E-cadherin by targeted histone methylation of TALE-SET fusion protein in cancer cells = TALE-SET 재조합 단백질의 targeted histone methylation에 의한 E-Cadherin의 발현 조절

Cited 19 time in scopus
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Title
Direct regulation of E-cadherin by targeted histone methylation of TALE-SET fusion protein in cancer cells = TALE-SET 재조합 단백질의 targeted histone methylation에 의한 E-Cadherin의 발현 조절
Author(s)
Hyun Soo ChoJeong Gu Kang; Jae Hye Lee; Jeong Ju Lee; Seong Kook Jeon; Jeong Heon KoDae Soo KimKun Hyang ParkYong Sam KimNam-Soon Kim
Bibliographic Citation
Oncotarget, vol. 6, no. 27, pp. 23837-23844
Publication Year
2015
Abstract
TALE-nuclease chimeras (TALENs) can bind to and cleave specific genomic loci and, are used to engineer gene knockouts and additions. Recently, instead of using the FokI domain, epigenetically active domains, such as TET1 and LSD1, have been combined with TAL effector domains to regulate targeted gene expression via DNA and histone demethylation. However, studies of histone methylation in the TALE system have not been performed. Therefore, in this study, we established a novel targeted regulation system with a TAL effector domain and a histone methylation domain. To construct a TALE-methylation fusion protein, we combined a TAL effector domain containing an E-Box region to act as a Snail binding site and the SET domain of EHMT 2 to allow for histone methylation. The constructed TALE-SET module (TSET) repressed the expression of E-cadherin via by increasing H3K9 dimethylation. Moreover, the cells that overexpressed TSET showed increased cell migration and invasion. This is the first phenotype-based study of targeted histone methylation by the TALE module, and this new system can be applied in new cancer therapies to reduce side effects.
Keyword
CancerHistone methylationMigrationTALEN
ISSN
1949-2553
Publisher
Impact Journals
DOI
http://dx.doi.org/10.18632/oncotarget.4340
Type
Article
Appears in Collections:
Division of Research on National Challenges > Stem Cell Convergenece Research Center > 1. Journal Articles
Synthetic Biology and Bioengineering Research Institute > Genome Editing Research Center > 1. Journal Articles
Division of Biomedical Research > Rare Disease Research Center > 1. Journal Articles
Division of Bio Technology Innovation > Core Research Facility & Analysis Center > 1. Journal Articles
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