OCT4 and SOX2 transcription factors
From Proteopedia
(Difference between revisions)
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size='340' side='right' caption='Caption for this structure' scene=''> | size='340' side='right' caption='Caption for this structure' scene=''> | ||
- | + | =Introduction= | |
Oct4 and Sox2 are two transcription factors (TFs) involved in various roles in murine and primate cells, mainly related to the maintenance of pluripotency and self-renewal properties in embryonic stem cells. These two factors, encoded by the ''POU5F1'' (POU Class 5 Homeobox 1) and ''SOX2'' (SRY-Box Transcription Factor 2) genes, respectively, serve as repprogramming TFs and occupy the same target genes in vivo <ref>PMID:16153702</ref><ref>PMID:18555785</ref>, forming the complex OCT4-SOX2, which is the main way in which they act, although they are not obligate heterodimers in solution. | Oct4 and Sox2 are two transcription factors (TFs) involved in various roles in murine and primate cells, mainly related to the maintenance of pluripotency and self-renewal properties in embryonic stem cells. These two factors, encoded by the ''POU5F1'' (POU Class 5 Homeobox 1) and ''SOX2'' (SRY-Box Transcription Factor 2) genes, respectively, serve as repprogramming TFs and occupy the same target genes in vivo <ref>PMID:16153702</ref><ref>PMID:18555785</ref>, forming the complex OCT4-SOX2, which is the main way in which they act, although they are not obligate heterodimers in solution. | ||
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OCT3/4 in ES cells | OCT3/4 in ES cells | ||
- | + | =The OCT4-SOX2 mechanism in the nucleosome= | |
The nucleosome is the chromatin basic unit, composed of a 147 pb DNA segment wrapped around 8 histone proteins. It is a convention that the sites in which a DNA major groove is pointed to the nucleosome core are called "superhelix location" (SHL). The SHL are enumerated from 0 to ±7, having 0 as the nucleosome main axis, known as "dyad". The OCT4-SOX2 binds in the SHL-6 site (Fig 1) and both of them act in the DNA removal from the core histones [ref1]. OCT4 has a bipartite DNA binding domain (DBD) comprised of a POU-specific (POUS) and POU-homeo-domain (POUHD) separated by 17-residues (Fig 2) and SOX2 has a high-mobility group (HMG) domain (Fig 2) [refs 1, 8]. The OCT4-POUS and SOX2-HMG DBDs engage major and minor grooves, respectively [ref1]. The DNA remains attached and straightened around the OCT4 site but is detached around the SOX2 motif [ref1]. | The nucleosome is the chromatin basic unit, composed of a 147 pb DNA segment wrapped around 8 histone proteins. It is a convention that the sites in which a DNA major groove is pointed to the nucleosome core are called "superhelix location" (SHL). The SHL are enumerated from 0 to ±7, having 0 as the nucleosome main axis, known as "dyad". The OCT4-SOX2 binds in the SHL-6 site (Fig 1) and both of them act in the DNA removal from the core histones [ref1]. OCT4 has a bipartite DNA binding domain (DBD) comprised of a POU-specific (POUS) and POU-homeo-domain (POUHD) separated by 17-residues (Fig 2) and SOX2 has a high-mobility group (HMG) domain (Fig 2) [refs 1, 8]. The OCT4-POUS and SOX2-HMG DBDs engage major and minor grooves, respectively [ref1]. The DNA remains attached and straightened around the OCT4 site but is detached around the SOX2 motif [ref1]. | ||
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Movie 1 - Extracted from the Supplementary Materials for the article '''Mechanisms of OCT4-SOX2 motif readout on nucleosomes''' (Alicia K. Michael et al., 2020). OCT4-SOX2 binding at SHL-6 removes DNA from the histone core. A morph video modelling the structural change induced in the nucleosome upon OCT4-SOX2 binding at SHL-6. Morph is between the DNA of the NCP-SHL-6 and OCT4-SOX2-NCP-SHL-6 models. | Movie 1 - Extracted from the Supplementary Materials for the article '''Mechanisms of OCT4-SOX2 motif readout on nucleosomes''' (Alicia K. Michael et al., 2020). OCT4-SOX2 binding at SHL-6 removes DNA from the histone core. A morph video modelling the structural change induced in the nucleosome upon OCT4-SOX2 binding at SHL-6. Morph is between the DNA of the NCP-SHL-6 and OCT4-SOX2-NCP-SHL-6 models. | ||
- | = | + | =OCT4 and SOX2 Embryonic Expression= |
'''OCT4''' | '''OCT4''' | ||
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- | + | =Gatekeeper for Embryonic Stem Cell Pluripotency= | |
The pluripotent identity is ruled by transcriptional factor such as Oct4 and Sox2, that act as key pluripotency regulators among the mammals [rev oct4]. Oct4 keeps the undifferentiated cells from becoming trophoblast or endoderm [rev oct4] and Sox2 is critical in the formation of pluripotent epiblast cells [artg sox2]. The forced expression of Oct4 in Sox2-null mouse embryonic stem cells can rescue the pluripotency, indicating that the role of Sox2 in maintaining the pluripotent state of embryonic stem cells is primarily to sustain a sufficient level of Oct4 expression [ artigo sox2 - 2,13]. Oct4 and Sox2 cooperate to keep the pluripotency of embryonic stem cells by co-occupying a large number of enhancers and/or promoters and regulating the expression levels of their target genes [ref artigo sox2]. They activate the transcription of genes involved in the self renewal of embryonic stem cells [ref revisao oct4]. Besides, they bind themselves to the promoters of their own genes activating them [revisao oct4]. | The pluripotent identity is ruled by transcriptional factor such as Oct4 and Sox2, that act as key pluripotency regulators among the mammals [rev oct4]. Oct4 keeps the undifferentiated cells from becoming trophoblast or endoderm [rev oct4] and Sox2 is critical in the formation of pluripotent epiblast cells [artg sox2]. The forced expression of Oct4 in Sox2-null mouse embryonic stem cells can rescue the pluripotency, indicating that the role of Sox2 in maintaining the pluripotent state of embryonic stem cells is primarily to sustain a sufficient level of Oct4 expression [ artigo sox2 - 2,13]. Oct4 and Sox2 cooperate to keep the pluripotency of embryonic stem cells by co-occupying a large number of enhancers and/or promoters and regulating the expression levels of their target genes [ref artigo sox2]. They activate the transcription of genes involved in the self renewal of embryonic stem cells [ref revisao oct4]. Besides, they bind themselves to the promoters of their own genes activating them [revisao oct4]. | ||
- | + | =iPSC/Yamanaka factors= | |
- | + | =OCT4/SOX2 and Tumorigenicity= | |
- | + | =Related Diseases= | |
- | + | =References= | |
<references/> | <references/> |
Revision as of 12:02, 17 June 2020
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