Discovery of MLL1 binding units, their localization to CpG Islands, and their potential function in mitotic chromatin

Bina, Minou; Wyss, Phillip; Novorolsky, Elise; Zulkelfi, Noorfatin; Xue, Jing; Price, R. Aden; Fay, Matthew; Gutmann, Zach; Fogler, Brian D.; Wang, Daidong

doi:10.1186/1471-2164-14-927

Cited by 17 publications

(27 citation statements)

References 86 publications

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“…The MLL1 morphemes consist of the following sequences: CGCG, CGACG/CGTCG; CGCCG/CGGCG; CGCGCG; CGTGCG/CGCACG; CGCCCG/CGGGCG; CGGACG/CGTCCG; CGTACG; complementary sequences are shown in 5′ to 3’ direction. These sequences are interchangeably referred to as MLL1 sites, binding units, or morphemes: the smallest “words” in DNA that selectively bind MLL1 . In a DNA segment, morpheme occurrences may overlap at CG producing a short or a long block of consecutive morphemes.…”

Section: Resultsmentioning

confidence: 99%

“…For example: DNA compaction may enforce rules for structural features that would facilitate nucleosome formation . Creation and maintenance of open chromatin structures may involve specific DNA sequence elements spread in promoters as well is exons of genes . Regulation of gene expression may favor dual‐use for codons "duons", sequences that would simultaneously specify a codon for amino acids and transcription factor recognition sites .…”

Section: Discussionmentioning

confidence: 99%

“…MLL1 contributes to the regulation of several genes in the four human HOX loci , which contain 39 genes with major roles in the development of the central nervous system, axial skeleton, gastrointestinal and urogenital tracts . Several genes in these loci include overlaps of the various MLL1 morphemes . Furthermore, the genes that encode HOXD13 and HOXA13 include tracts of repeated GGC/CCG, produced from overlapping morphemes (Figures and ); Significantly, expansion of these repeats causes limb malformations, synpolydactyly, and hand‐foot‐genital syndrome …”

Section: Discussionmentioning

confidence: 99%

“…At the onset of mitosis, MLL1 associates with gene promoters in a manner favoring genes that were highly transcribed during interphase . The MLL1 morphemes in CGIs have been implicated in gene bookmarking events by serving as Trithorax Response Elements (TREs) in the human chromosomes . Furthermore, MLL1 is the central component in multiprotein complexes that catalyze trimethylation of lysine 4 in histone H3 producing H3K4me3, marks that create chromatin structures that could support or be poised for transcription .…”

Section: Introductionmentioning

confidence: 99%

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Impact of the MLL1 morphemes on codon utilization and preservation in CpG Islands

Bina

Wyss

2015

Biopolymers

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Previous studies have shown that Mixed Lineage Leukemia 1 (MLL1 or MLL) binds a group of CpG-rich motifs known as morphemes. To examine whether occurrences of MLL1 morphemes in genomic DNA may influence codon utilization, we analyzed the frequency of various 9-mers in human cDNAs and in total human genomic DNA. We uncovered preferential utilization of GGC for Gly, GCG for Ala, CCG for Pro, and TCG for Ser, in coding sequences (CDSs) that included MLL1 morphemes. We also examined weighted occurrences of CDS 9-mers in a 30-base window that moved along each human chromosome. In plots, we observed peaks with fluctuating intensities. High intensity peaks appeared within promoter and exons localized in CpG islands, encompassing sequences that included MLL1 morphemes. High intensity peaks included CCG/GGC repeats, whose expansion may cause neurological disorders and congenital malformations. Such repeats are generated from overlap of a morpheme (CGCCG/CGGCG), which depending on reading frame and orientation would produce runs of Ala, Gly, or Pro in proteins. Overall, our results point to a role for morpheme occurrences on synonymous codon utilization in human genomic DNA and indicate that regulatory instructions are dispersed not only in promoters but also in exons of human genes.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Impact of the MLL1 morphemes on codon utilization and preservation in CpG Islands

Bina

Wyss

2015

Biopolymers

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“…On the other hand, and this need not conflict with the idea just mentioned, MLL1 may play a more widespread role in global H3K4 methylation than is generally suggested. 69,70 An ongoing concern for drug discovery efforts involving high-throughput screening of large compound collections are promiscuous inhibitors or nuisance compounds, 71,72 which by various mechanisms, such as chemical assay interference 73 or compound aggregation-based effects, 74 show up repeatedly, across multiple target classes, as false-positive hits. 75 A different but related concern is that hit compounds exhibit leadlike properties; that is, they have physical and chemical properties suitable for the downstream analytical and chemical modification procedures employed in the further steps of drug development.…”

Section: Discussionmentioning

confidence: 99%

Development and Use of Assay Conditions Suited to Screening for and Profiling of SET-Domain-Targeted Inhibitors of the MLL/SET1 Family of Lysine Methyltransferases

Ferry

Smith

Denney

et al. 2015

ASSAY and Drug Development Technologies

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Methylation of histone H3 lysine-4 (H3K4) is an important, regulatory, epigenetic post-translational modification associated with actively transcribed genes. In humans, the principal mediators of this modification are part of the MLL/SET1 family of methyltransferases, which comprises six members, MLLs1-4 and SET1A/SET1B. Aberrations in the structure, expression, and regulation of these enzymes are implicated in various disease states, making them important potential targets for drug discovery, particularly for oncology indications. The MLL/SET1 family members are most enzymatically active when part of a ''core complex,'' the catalytic SET-domain-containing subunits bound to a subcomplex consisting of the proteins WDR5, RbBP5, Ash2L and a homodimer of DPY-30 (WRAD 2 ). The necessity of MLL/SET1 members to bind WRAD 2 for full activity is the basis of a particular drug development strategy, which seeks to disrupt the interaction between the MLL/SET1 subunits and WDR5. This strategy is not without its theoretical and practical drawbacks, some of which relate to the ease with which complexes of Escherichia coli-expressed MLL/SET1 and WRAD 2 fall apart. As an alternative strategy, we explore ways to stabilize the complex, focusing on the use of an excess of WRAD 2 to drive the binding equilibria toward complex formation while maintaining low concentrations of the catalytic subunits. The purpose of this approach is to seek inhibitors that bind the SET domain, an approach proven successful with the related, but inherently more stable, enhancer of zeste homolog 2 (EZH2) complex.

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Polycomb and Trithorax factors in transcriptional and epigenetic regulation

Lau¹,

So²

2015

Epigenetic Gene Expression and Regulation

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Discovery of MLL1 binding units, their localization to CpG Islands, and their potential function in mitotic chromatin

Cited by 17 publications

References 86 publications

Impact of the MLL1 morphemes on codon utilization and preservation in CpG Islands

Impact of the MLL1 morphemes on codon utilization and preservation in CpG Islands

Development and Use of Assay Conditions Suited to Screening for and Profiling of SET-Domain-Targeted Inhibitors of the MLL/SET1 Family of Lysine Methyltransferases

Polycomb and Trithorax factors in transcriptional and epigenetic regulation

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