Phosphorylation of
            <i>Sox9</i>
            is required for neural crest delamination and is regulated downstream of BMP and canonical Wnt signaling

Liu, Jessica Aijia; Wu, Ming‐Hoi; Yan, Carol H.; Chau, Bolton K.H.; So, Henry B.; Ng, Alvis; Chan, Alan K. L.; Cheah, Kathryn S.E.; Briscoe, James; Cheung, Martin

doi:10.1073/pnas.1211747110

Cited by 82 publications

(93 citation statements)

References 30 publications

(44 reference statements)

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“…Interestingly Snail2 has been also shown to transcriptionally repress cadherin-6B, which belongs to type II classical cadherins in chick cranial and trunk NC cells during delamination . The action of Snail2 is supported by interaction with Sox9, another transcription factor, which upon phosphorylation, induced by BMP and canonical Wnt signaling, binds directly Snail2 and promotes EMT of chick trunk NC (Cheung and Briscoe, 2003;Liu et al, 2013). Furthermore, canonical Wnt signaling is also thought to be involved in EMT by transcriptional and post-transcriptional regulation of Snail2 (Vallin et al, 2001;Yook et al, 2006).…”

Section: Loss Of Epithelial Polarity and Modulation Of Cell Adhesionmentioning

confidence: 99%

Controlled levels of canonical Wnt signaling are required for neural crest migration

Maj

Künneke

Loresch

et al. 2016

Developmental Biology

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Section: Loss Of Epithelial Polarity and Modulation Of Cell Adhesionmentioning

confidence: 99%

Controlled levels of canonical Wnt signaling are required for neural crest migration

Maj

Künneke

Loresch

et al. 2016

Developmental Biology

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“…Sry and Sox9 are phosphorylated by protein kinase A (PKA), which enhances their DNA-binding activity (Malki et al, 2010). This phosphorylation of Sox9 also leads to its translocation into the nucleus in cells of the testis (Malki et al, 2010), and is essential in neural crest (NC) cells for the Sox9-Snail interaction that promotes NC delamination (Liu et al, 2013). The functional relevance of sumoylation has been best demonstrated for SoxE proteins in NC development.…”

Section: Sox Protein Structurementioning

confidence: 99%

“…Sry and Sox9 are phosphorylated by protein kinase A (PKA), which enhances their DNA-binding activity (Malki et al, 2010). This phosphorylation of Sox9 also leads to its translocation into the nucleus in cells of the testis (Malki et al, 2010), and is essential in neural crest (NC) cells for the Sox9-Snail interaction that promotes NC delamination (Liu et al, 2013 miR-145 expression is highly upregulated during the differentiation of human embryonic stem cells (ESCs). miR-145 directly targets 3Ј UTRs (untranslated regions) of the mRNAs of Sox2 and other 'core pluripotency factors', and promotes differentiation into mesoderm and ectoderm lineages (Xu et al, 2009b).…”

mentioning

confidence: 99%

Sox proteins: regulators of cell fate specification and differentiation

2013

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SummarySox transcription factors play widespread roles during development; however, their versatile functions have a relatively simple basis: the binding of a Sox protein alone to DNA does not elicit transcriptional activation or repression, but requires binding of a partner transcription factor to an adjacent site on the DNA. Thus, the activity of a Sox protein is dependent upon the identity of its partner factor and the context of the DNA sequence to which it binds. In this Primer, we provide an mechanistic overview of how Sox family proteins function, as a paradigm for transcriptional regulation of development involving multi-transcription factor complexes, and we discuss how Sox factors can thus regulate diverse processes during development. Key words: HMG domain, Partner factors, Transcriptional regulation, Stem cells, Cell lineage specification IntroductionAn emerging view of transcriptional regulation in developmental processes is that transcription factor complexes, rather than single transcription factors, play a major role (Reményi et al., 2004;Verger and Duterque-Coquillaud, 2002). This idea has been pioneered, most rigorously tested and studied in a variety of developmental contexts in the case of Sox (SRY-related HMG-box) family proteins. Sox family proteins are a conserved group of transcriptional regulators (see Box 1) defined by the presence of a highly conserved highmobility group (HMG) domain that mediates DNA binding. This domain was first identified in Sry, a crucial factor involved in mammalian male sex determination (Gubbay et al., 1990;Sinclair et al., 1990). Multiple other Sox proteins have subsequently been identified and analysed. Vertebrate genomes contain ~20 Sox family members with highly divergent developmental functions, as was indicated by the initial analyses of Sox expression in embryos (Collignon et al., 1996;Uwanogho et al., 1995). Although Sox proteins are also conserved in invertebrate lineages and exert analogous regulatory functions (Phochanukul and Russell, 2010), we here confine our discussion to the vertebrate Sox family members. In this Primer, we first outline the structure and molecular activities of Sox proteins, before discussing their roles during vertebrate development. In particular, the action and function of Sox proteins will be overviewed as a paradigm for transcriptional regulation mediated by a family of transcription factors. Sox protein structureSox proteins can bind to ATTGTT or related sequence motifs through their HMG domain, which consists of three α helices (Badis et al., 2009;Kondoh and Kamachi, 2010). This binding is established by the interaction of the HMG domain with the minor groove of the DNA, which widens the minor groove and causes DNA to bend towards the major groove (Reményi et al., 2003). It is speculated that DNA bending itself may contribute to the regulatory functions of Sox proteins (Pevny and Lovell-Badge, 1997), but this has not been proved experimentally. Sox proteins are classified into groups A-H, depending on the amino acid sequ...

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“…This is accomplished through direct interaction with a pair of E-box sites located in the vicinity of the Kozak consensus sequence. An important partner of Snai1/2 during the process of EMT is the transcription factor Sox9, which when phosphorylated physically interacts with Snai1/2 to drive EMT (Cheung and Briscoe, 2003;Liu et al, 2013b).…”

Section: Transcriptional Control Of the Neural Crest Emt Programmentioning

confidence: 99%

Establishing neural crest identity: a gene regulatory recipe

2015

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The neural crest is a stem/progenitor cell population that contributes to a wide variety of derivatives, including sensory and autonomic ganglia, cartilage and bone of the face and pigment cells of the skin. Unique to vertebrate embryos, it has served as an excellent model system for the study of cell behavior and identity owing to its multipotency, motility and ability to form a broad array of cell types. Neural crest development is thought to be controlled by a suite of transcriptional and epigenetic inputs arranged hierarchically in a gene regulatory network. Here, we examine neural crest development from a gene regulatory perspective and discuss how the underlying genetic circuitry results in the features that define this unique cell population.

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Phosphorylation of Sox9 is required for neural crest delamination and is regulated downstream of BMP and canonical Wnt signaling

Cited by 82 publications

References 30 publications

Controlled levels of canonical Wnt signaling are required for neural crest migration

Controlled levels of canonical Wnt signaling are required for neural crest migration

Sox proteins: regulators of cell fate specification and differentiation

Establishing neural crest identity: a gene regulatory recipe

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