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Open AccessJournal ArticleDOI

Analysis of the murine All-1 gene reveals conserved domains with human ALL-1 and identifies a motif shared with DNA methyltransferases

TLDR
The cloning, sequencing, and mapping of the mouse homolog of ALL-1 are described and it is reported that All-1 resides in the proximal portion of mouse chromosome 9 and is a candidate for a mutation that results in skeletal transformations during embryonic development.
Abstract
A series of translocation break points found in a subset of human acute leukemias have one of the breaks on human chromosome 11q23. This region has recently been cloned and a large gene, ALL-1, with homology to the Drosophila trithorax gene has been identified. This paper describes the cloning, sequencing, and mapping of the mouse homolog of ALL-1. We have found a motif present in All-1 that shows homology to the zinc-binding domain of DNA (cytosine-5) methyltransferases (EC 2.1.1.63). Sequence analysis of the murine All-1 gene has identified distinct regions of homology with the human ALL-1 gene; these highly conserved domains may define regions of functional significance in mammals. In addition, we have identified alternatively spliced forms of All-1 within one of the zinc-finger domains, suggesting that there may be different targets and/or functions for All-1 proteins. Finally, we report that All-1 resides in the proximal portion of mouse chromosome 9 and is a candidate for a mutation that results in skeletal transformations during embryonic development.

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Journal ArticleDOI

DNA methyltransferase Dnmt1 associates with histone deacetylase activity.

TL;DR: A transcriptional repression domain in Dnmt1 is identified that functions, at least partly, by recruiting histone deacetylase activity and shows homology to the repressor domain of the trithorax-related protein HRX (also known as MLL and ALL-1).
Journal ArticleDOI

Altered Hox expression and segmental identity in Mll -mutant mice

TL;DR: Mll is required for proper segment identity in mammals, displays haplo-insufficiency, and positively regulates Hox gene expression.
Journal ArticleDOI

Recombinant Human DNA (Cytosine-5) Methyltransferase I. EXPRESSION, PURIFICATION, AND COMPARISON OF DE NOVO AND MAINTENANCE METHYLATION

TL;DR: Results show that, in addition to maintenance methylation, human DNMT1 may also carry out de novo and non-CG methyltransferase activities in vivo, and formed covalent complexes with substrates containing 5-fluoro-CNG, indicating that substrate specificity extended beyond the canonical CG dinucleotide.
Journal ArticleDOI

The secretory phospholipase A2 gene is a candidate for the Mom1 locus, a major modifier of ApcMin-induced intestinal neoplasia

TL;DR: The results indicate that Pla2s acts as a novel gene that modifies polyp number by altering the cellular microenvironment within the intestinal crypt within Min mice, suggesting that Mom1 susceptible strains are most likely null for PlA2s activity.
Journal ArticleDOI

Dnmt3a binds deacetylases and is recruited by a sequence-specific repressor to silence transcription

TL;DR: It is shown that Dnmt3a associates with RP58, a DNA‐binding transcriptional repressor protein found at transcriptionally silent heterochromatin that acts as a co‐repressor for RP58 in a manner that does not require its de novo methyltransferase activity.
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