| Literature DB >> 26823482 |
Bi-He Cai1, Chung-Faye Chao2, Hwang-Chi Lin3, Hua-Ying Huang2, Reiji Kannagi4, Jang-Yi Chen5.
Abstract
The canonical core sequence of the p53 response element, CATG, has a two-base A/T gap. Previously, we found that p53 can also activate a non-canonical four-base A/T gap CATATG core sequence. In this study, we investigated the possible number of A/T bases used by p53 and showed that a six-base A/T gap CATATATG core sequence was the maximum A/T gap in the p53 response element that could be upregulated by p53 and p63. Canonical and non-canonical p53 response elements also have three-base flanking sequences. A/T bases could be substituted by G/C bases, including CACACG and CGTGTG, but not CGCGCG. We found that the SV40 promoter with functional six- and two-base A/T gap core sequences could be activated by TAp63γ and that TAp63γ could upregulate SV40 small and large T antigens expression in COS7 cells. We also found that the distal region of PUMA promoter with functional two six-base A/T gap core sequences could be activated by TAp63γ in 293T cells. These new findings could provide novel rules for the non-canonical p53 family response element and could extend the entire p53 family regulation network.Entities:
Keywords: flanking sequence; non-canonical; p53; p63; response element
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Year: 2016 PMID: 26823482 PMCID: PMC4892394 DOI: 10.1093/jb/mvw005
Source DB: PubMed Journal: J Biochem ISSN: 0021-924X Impact factor: 3.387