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Polymorphic potential of SRF binding site of c-Fos gene promoter: in vitro study

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Author
Profantová, Barbora
Římal, VáclavORCiD Profile - 0000-0001-5680-9667WoS Profile - G-5488-2012Scopus Profile - 35318796900
Profant, VáclavORCiD Profile - 0000-0001-8161-305XWoS Profile - N-1199-2013Scopus Profile - 18635017200
Socha, OndřejORCiD Profile - 0000-0002-7218-9119WoS Profile - Q-9270-2017Scopus Profile - 56826174000
Barvík, IvanORCiD Profile - 0000-0002-0802-1346WoS Profile - G-8906-2014Scopus Profile - 16634588600
Štěpánková, HelenaORCiD Profile - 0000-0002-4051-2495WoS Profile - P-2352-2017Scopus Profile - 7003725998
Štěpánek, JosefORCiD Profile - 0000-0001-7307-2257WoS Profile - B-2309-2009Scopus Profile - 7102104693

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Publication date
2024
Published in
RSC Advances
Volume / Issue
14 (51)
ISBN / ISSN
ISSN: 2046-2069
ISBN / ISSN
eISSN: 2046-2069
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  • Faculty of Mathematics and Physics

This publication has a published version with DOI 10.1039/d4ra05897f

Abstract
Recently published in vivo observations have highlighted the presence of cruciform structures within the genome, suggesting their potential significance in the rapid recognition of the target sequence for transcription factor binding. In this in vitro study, we investigate the organization and stability of the sense (coding) strand within the Serum Response Element of the c-Fos gene promoter (c-Fos SRE), specifically focusing on segments spanning 12 to 36 nucleotides, centered around the CArG-box. Through a thorough examination of UV absorption patterns with varying temperatures, we identified the emergence of a remarkably stable structure, which we conclusively characterized as a hairpin using complementary (1)H NMR experiments. Our research decisively ruled out the formation of homoduplexes, as confirmed by supplementary fluorescence experiments. Utilizing molecular dynamics simulations with atomic distance constraints derived from NMR data, we explored the structural intricacies of the compact hairpin. Notably, the loop consisting of the six-membered A/T sequence demonstrated substantial stabilization through extensive stacking, non-canonical inter-base hydrogen bonding, and hydrophobic clustering of thymine methyl groups. These findings suggest the potential of the c-Fos SRE to adopt a cruciform structure (consisting of two opposing hairpins), potentially providing a topological recognition site for the SRF transcription factor under cellular conditions. Our results should inspire further biochemical and in vivo studies to explore the functional implications of these non-canonical DNA structures.
Keywords
serum response factor, chemical-shift prediction, box transcription factors, dot-t mismatches, MADS-box, cruciform structures, molecular dynamics, DNA hairpin, web server, NMR
Permanent link
https://hdl.handle.net/20.500.14178/2949
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WOS:001368282800001
SCOPUS:2-s2.0-85211491997
PUBMED:39628460
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Full text of this result is licensed under: Creative Commons Uveďte původ 3.0 Unported

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