Literature DB >> 17785538

Computational identification and functional validation of regulatory motifs in cartilage-expressed genes.

Sherri R Davies1, Li-Wei Chang, Debabrata Patra, Xiaoyun Xing, Karen Posey, Jacqueline Hecht, Gary D Stormo, Linda J Sandell.   

Abstract

Chondrocyte gene regulation is important for the generation and maintenance of cartilage tissues. Several regulatory factors have been identified that play a role in chondrogenesis, including the positive transacting factors of the SOX family such as SOX9, SOX5, and SOX6, as well as negative transacting factors such as C/EBP and delta EF1. However, a complete understanding of the intricate regulatory network that governs the tissue-specific expression of cartilage genes is not yet available. We have taken a computational approach to identify cis-regulatory, transcription factor (TF) binding motifs in a set of cartilage characteristic genes to better define the transcriptional regulatory networks that regulate chondrogenesis. Our computational methods have identified several TFs, whose binding profiles are available in the TRANSFAC database, as important to chondrogenesis. In addition, a cartilage-specific SOX-binding profile was constructed and used to identify both known, and novel, functional paired SOX-binding motifs in chondrocyte genes. Using DNA pattern-recognition algorithms, we have also identified cis-regulatory elements for unknown TFs. We have validated our computational predictions through mutational analyses in cell transfection experiments. One novel regulatory motif, N1, found at high frequency in the COL2A1 promoter, was found to bind to chondrocyte nuclear proteins. Mutational analyses suggest that this motif binds a repressive factor that regulates basal levels of the COL2A1 promoter.

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Year:  2007        PMID: 17785538      PMCID: PMC1987341          DOI: 10.1101/gr.6224007

Source DB:  PubMed          Journal:  Genome Res        ISSN: 1088-9051            Impact factor:   9.043


  60 in total

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4.  A predictive model for regulatory sequences directing liver-specific transcription.

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5.  L-Sox5, Sox6 and Sox9 control essential steps of the chondrocyte differentiation pathway.

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7.  Human-mouse genome comparisons to locate regulatory sites.

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8.  SOX9 binds DNA, activates transcription, and coexpresses with type II collagen during chondrogenesis in the mouse.

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  18 in total

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3.  CaMKII plays a part in the chondrogenesis of bone marrow-derived mesenchymal stem cells.

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7.  Exuberant expression of chemokine genes by adult human articular chondrocytes in response to IL-1beta.

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8.  Computational design and application of endogenous promoters for transcriptionally targeted gene therapy for rheumatoid arthritis.

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