2005
DOI: 10.1038/emm.2005.33
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Identification of a putative transactivation domain in human Nanog

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Cited by 41 publications
(35 citation statements)
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“…When fused to the DNA-binding domain of Gal4, both N-and C-terminal domains show trans-activator function [23], but the activity of the C-terminal domain is much higher (at least seven times) than the N-terminal domain [23]. Similar analysis on human Nanog protein reveals that only the C-terminal domain has transcriptional activity [24], suggesting that the C-terminal domain is functionally dominant. The prominent feature of the C-terminal domain is the presence of a 10 pentapeptide repeat (WR), each starting with a tryptophan (W).…”
Section: Nanog Is a Unique Homeobox Transcription Factormentioning
confidence: 89%
“…When fused to the DNA-binding domain of Gal4, both N-and C-terminal domains show trans-activator function [23], but the activity of the C-terminal domain is much higher (at least seven times) than the N-terminal domain [23]. Similar analysis on human Nanog protein reveals that only the C-terminal domain has transcriptional activity [24], suggesting that the C-terminal domain is functionally dominant. The prominent feature of the C-terminal domain is the presence of a 10 pentapeptide repeat (WR), each starting with a tryptophan (W).…”
Section: Nanog Is a Unique Homeobox Transcription Factormentioning
confidence: 89%
“…Transactivation activity of NANOG can be mediated via the C-terminal WR and CD2 domains (Supplemental Fig. 6A; Pan and Pei 2003;Oh et al 2005). We hypothesized that the recruitment of the transactivation domains to major satellite repeats could underlie the open PCH organization typical of ESCs.…”
Section: The Nanog Transactivation Domain Is Critical For Heterochrommentioning
confidence: 99%
“…Murine and human Nanog were described as 3-domain proteins containing a homeodomain (HD), a serine enriched N-terminal, and a C-terminal transactivator domain containing several tryptophan repeats [40,41]. The tryptophan repeats were shown to be crucial for dimerization, proliferation, the maintenance of Nanog-dependent cell selfrenewal, and for binding of Nac1 [42][43][44].…”
Section: Divergence Of Nanog Proteins In Different Species and Relatimentioning
confidence: 99%