Identification of Novel Domains within Sox-2 and Sox-11 Involved in Autoinhibition of DNA Binding and Partnership Specificity

Wiebe, Matthew S.; Nowling, Tamara K.; Rizzino, Angie

doi:10.1074/jbc.m212211200

Cited by 62 publications

(67 citation statements)

References 45 publications

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“…It was shown that both proteins cooperated with Oct-3, while only Sox11 could partner with Brn-2 to activate transcription. 26 Brn-2 is involved in the proliferation of melanoma cells and can, like cyclin D1, be induced by the WNT/Beta-catenin pathway. 27 In the murine system, it has been shown in primary and continuous cell cultures that neuron survival and neurite growth are dependent on Sox11.…”

Section: Discussionmentioning

confidence: 99%

Nuclear expression of the non–B-cell lineage Sox11 transcription factor identifies mantle cell lymphoma

Dictor²,

Jerkeman

et al. 2008

Blood

174

166

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Mantle cell lymphoma (MCL) is defined pathologically by the detection of CD20, CD5, and most importantly cyclin D1 (CCND1). Its distinction from other lymphomas is important for prognosis and appropriate therapy, but occasional cases may fail to express CCND1 and morphologic simulators may express CD20 and CD5 but not CD23. In this study, we show that the transcription factor Sox11 is specifically expressed in the nucleus of MCL compared with other lymphomas and benign lymphoid tissue. Although the role of Sox11 presently is not known in lymphocyte ontogeny, it is normally expressed in the developing central nervous system in the embryo and shows sequence homology with Sox4, a transcription factor crucial for B lymphopoiesis. Sox11 mRNA is increased in gliomas compared with healthy brain tissue, suggesting a role in malignant transformation and/or cell survival. Our novel finding of specific overexpression of Sox11 mRNA and nuclear protein in both cyclin D1-positive and -negative MCL may be useful for the diagnosis of MCL as a complement to cyclin D1 and also suggests a functional role for Sox11 in MCL. IntroductionB-cell lymphomas (BCLs) are divided into several subgroups depending on their morphologic and phenotypic properties, 1 and accurate diagnosis is necessary for prognosis and targeted therapy. Mantle cell lymphoma (MCL) accounts for 5% to 10% of BCLs and is characterized by overexpression of cyclin D1 (CCND1) due to the specific translocation t(11;14)(q13;q32), which brings the cyclin D1 (BCL1/CCND1) gene under the control of the immunoglobulin heavy chain enhancer. MCL may be distinguished from potential morphologic mimics, including chronic lymphocytic leukemia/small cell lymphoma (CLL), follicular lymphoma (FL), and marginal zone lymphoma (MZL) based on immunohistochemical staining (IHC) for CD5, CD23, and CD10. MCL and CLL both express CD5 but MCL, in contrast to CLL, generally lacks CD23 by immunohistochemistry. FL lacks both CD5 and CD23 but most often expresses CD10, whereas MZL is typically negative for all 3 antigens. Nevertheless, cases of CD23 Ϫ CLL occur and rare instances of CD5 ϩ MZL have been described. Follicular dendritic cell networks are characteristically expanded in MCL, but this occurs also in FL and MZL. CCND1 overexpression is thus the hallmark of MCL even though approximately 10% of MCLs lack CCND1 expression and may be misdiagnosed by overreliance on CCND1 IHC. 2,3 For these reasons, fluorescence in situ hybridization (FISH) targeting the specific translocation probably affords the most sensitive detection of MCL, although it is not widely performed and the results may be more easily affected by technical factors than modern IHC. Thus, specific markers that can aid in stratification and diagnosis of lymphomas in general and MCL in particular would be of major interest.In this study, we demonstrate that the transcription factor Sox11 is specifically up-regulated in MCL and distinguishes MCL from other B-cell lymphomas. Sox11 belongs to the Sox gene family and is mapped to chrom...

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Section: Discussionmentioning

confidence: 99%

Nuclear expression of the non–B-cell lineage Sox11 transcription factor identifies mantle cell lymphoma

Dictor²,

Jerkeman

et al. 2008

Blood

174

166

View full text Add to dashboard Cite

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“…Similarly, the sequences bound by Sox9 dimers found in the enhancers of genes associated with chondrocyte development, e.g. those for collagens, deviate considerably from the Sox consensus binding (Wiebe et al, 2003), Sox2 (Tomioka et al, 2002), Utf1 (Nishimoto et al, 1999), nestin (Nes) (Tanaka et al, 2004). In contrast to the heterodimers, the Sox9 dimer-binding sequences deviate from the Sox consensus in both sites (Bernard et al, 2003;Bridgewater et al, 2003;Dy et al, 2012;Han and Lefebvre, 2008;Sock et al, 2003).…”

Section: Mechanism Of Action: Sox Proteins Complex With Partner Factorsmentioning

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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“…Sox11 but not Sox2 stimulated the reporter construct in transfection experiments, but only Sox2 was capable of binding to the putative binding site as judged by the EMSA. The authors suggested that there is a domain in the Sox11 protein that has a capability of autoinhibiting its ability to bind DNA in vitro and to activate gene expression in vivo (41). This suggestion may also explain the results we obtained with the Optimedin promoter.…”

Section: Discussionmentioning

confidence: 60%

“…Sox2, Sox11, and Brn1 cDNAs were cloned into the pCMV5 expression vector (41,42) and were kindly provided by Drs. A. Rizzino (University of Nebraska) and D. Robbins (University of Michigan), respectively.…”

Section: Methodsmentioning

confidence: 99%