Transcription factor Sp1
Template:Short description Template:Cs1 config Template:Infobox gene Transcription factor Sp1, also known as specificity protein 1* is a protein that in humans is encoded by the SP1 gene.[1]
Function
The protein encoded by this gene is a zinc finger transcription factor that binds to GC-rich motifs of many promoters. The encoded protein is involved in many cellular processes, including cell differentiation, cell growth, apoptosis, immune responses, response to DNA damage, and chromatin remodeling. post-translational modifications such as phosphorylation, acetylation, O-GlcNAcylation, and proteolytic processing significantly affect the activity of this protein, which can be an activator or a repressor.[1]
In the SV40 virus, Sp1 binds to the GC boxes in the regulatory sequence of the genome.
Structure
SP1 belongs to the Sp/KLF family of transcription factors. The protein is 785 amino acids long, with a molecular weight of 81 kDa. The SP1 transcription factor contains two glutamine-rich activation domains at its N-terminus that are believed to be necessary for promoter trans-activation.[2] SP1 most notably contains three zinc finger protein motifs at its C-terminus, by which it binds directly to DNA and allows for interaction of the protein with other transcriptional regulators. Its zinc fingers are of the Cys2/His2 type and bind the consensus sequence 5'-(G/T)GGGCGG(G/A)(G/A)(C/T)-3' (GC box element). Some 12,000 SP-1 binding sites are found in the human genome.[3]
Applications
Sp1 has been used as a control protein to compare with when studying the increase or decrease of the aryl hydrocarbon receptor and/or the estrogen receptor, since it binds to both and generally remains at a relatively constant level.[4]
Recently, a putative promoter region in FTMT, and positive regulators {SP1, cAMP response element-binding protein (CREB), and Ying Yang 1 (YY1)] and negative regulators [GATA2, forkhead box protein A1 (FoxA1), and CCAAT enhancer-binding protein b (C/EBPb)] of FTMT transcription have been identified (Guaraldo et al, 2016).The effect of DFP on the DNA-binding activity of these regulators to the FTMT promoter was examined using chromatin immunoprecipitation (ChIP) assay. Among the regulators, only SP1 displayed significantly increased DNA- binding activity following DFP treatment in a dose-dependent manner. SP1 knockdown by siRNA abolished the DFP-induced increase in the mRNA levels of FTMT, indicating SP1-mediated regulation of FTMT expression in the presence of DFP. Treatment with Deferiprone increased the expression of cytoplasmic and nuclear SP1 with predominant localization in the nucleus.[5]
Inhibitors
Plicamycin, an antineoplastic antibiotic produced by Streptomyces plicatus, and Withaferin A, a steroidal lactone from Withania somnifera plant are known to inhibit Sp1 transcription factor.[6][7]
miR-375-5p microRNA significantly decreased expression of SP1 and YAP1 in colorectal cancer cells. SP1 and YAP1 mRNAs are direct targets of miR-375-5p.[8]
Interactions
Transcription factor Sp1 has been shown to interact with: Template:Div col
- AATF,[9]
- CEBPB,[10][11]
- COL1A1,[12]
- E2F1,[13][14][15]
- FOSL1,[16]
- GABPA,[17]
- HDAC1,[9][18][19][20]
- HDAC2,[19][20][21]
- HMGA1,[11]
- HCFC1,[22][23]
- HTT,[24]
- KLF6,[25]
- MEF2C,[26]
- MEF2D,[27]
- MSX1,[28]
- Myogenin,[29]
- POU2F1,[22][30]
- PPP1R13L,[31]
- PSMC5,[32][33]
- PML,[34]
- RELA,[35][36]
- SMAD3,[37][38]
- SUMO1,[32]
- SF1,[39]
- TAL1,[40]
- UBC.[32]
- WRN,[41]
- DDX3X
References
Further reading
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External links
Template:PDB Gallery Template:Transcription factors Template:NLM content
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