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Identification of Estrogen Receptor-Related Receptor Gamma as a Direct Transcriptional Target of Angiogenin
Author(s) -
Jian Ang,
Jinghao Sheng,
Kairan Lai,
Saisai Wei,
Xiangwei Gao
Publication year - 2013
Publication title -
plos one
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.99
H-Index - 332
ISSN - 1932-6203
DOI - 10.1371/journal.pone.0071487
Subject(s) - gene knockdown , angiogenin , chromatin immunoprecipitation , repressor , nuclear receptor , estrogen receptor , microbiology and biotechnology , biology , receptor , cell growth , transcription factor , transcriptional regulation , estrogen receptor beta , cancer research , gene expression , promoter , gene , cancer , breast cancer , angiogenesis , genetics
Nuclear translocation of angiogenin (ANG) is essential for the proliferation of its target cells. ANG promotes rRNA synthesis, while whether it regulates mRNA transcription remains unknown. Using the chromatin immunoprecipitation method, we have identified 12 ANG-binding sequences. One of these sequences lies in the estrogen receptor-related receptor gamma (ERRγ) gene which we designated as ANG-Binding Sequence within ERRγ (ABSE). ABSE exhibited ANG-dependent repressor activity in the luciferase reporter system. Down-regulation of ANG increased ERRγ expression, and active gene marker level at the ABSE region. The expression levels of ERRγ targets genes, p21 WAF/CIP and p27 KIP1 , and the occupation of ERRγ on their promoter regions were increased in ANG-deficient cells accordingly. Furthermore, knockdown of ERRγ promoted the proliferation rate in ANG-deficient breast cancer cells. Finally, immunohistochemistry staining showed negative correlation between ANG and ERRγ in breast cancer tissue. Altogether, our study provides evidence that nuclear ANG directly binds to the ABSE of ERRγ gene and inhibits ERRγ transcription to promote breast cancer cell proliferation.

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