Literature DB >> 8756673

Surprising deficiency of CENP-B binding sites in African green monkey alpha-satellite DNA: implications for CENP-B function at centromeres.

I G Goldberg1, H Sawhney, A F Pluta, P E Warburton, W C Earnshaw.   

Abstract

Centromeres of mammalian chromosomes are rich in repetitive DNAs that are packaged into specialized nucleoprotein structures called heterochromatin. In humans, the major centromeric repetitive DNA, alpha-satellite DNA, has been extensively sequenced and shown to contain binding sites for CENP-B, an 80-kDa centromeric autoantigen. The present report reveals that African green monkey (AGM) cells, which contain extensive alpha-satellite arrays at centromeres, appear to lack the well-characterized CENP-B binding site (the CENP-B box). We show that AGM cells express a functional CENP-B homolog that binds to the CENP-B box and is recognized by several independent anti-CENP-B antibodies. However, three independent assays fail to reveal CENP-B binding sites in AGM DNA. Methods used include a gel mobility shift competition assay using purified AGM alpha-satellite, a novel kinetic electrophoretic mobility shift assay competition protocol using bulk genomic DNA, and bulk sequencing of 76 AGM alpha-satellite monomers. Immunofluorescence studies reveal the presence of significant levels of CENP-B antigen dispersed diffusely throughout the nuclei of interphase cells. These experiments reveal a paradox. CENP-B is highly conserved among mammals, yet its DNA binding site is conserved in human and mouse genomes but not in the AGM genome. One interpretation of these findings is that the role of CENP-B may be in the maintenance and/or organization of centromeric satellite DNA arrays rather than a more direct involvement in centromere structure.

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Year:  1996        PMID: 8756673      PMCID: PMC231516          DOI: 10.1128/MCB.16.9.5156

Source DB:  PubMed          Journal:  Mol Cell Biol        ISSN: 0270-7306            Impact factor:   4.272


  61 in total

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3.  Purification of a human centromere antigen (CENP-B) and application of DNA immunoprecipitation to quantitative assay for anti-CENP-B antibodies.

Authors:  Y Muro; H Masumoto; T Okazaki; M Ohashi
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Authors:  K F Sullivan; C A Glass
Journal:  Chromosoma       Date:  1991-07       Impact factor: 4.316

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Authors:  C A Cooke; D P Bazett-Jones; W C Earnshaw; J B Rattner
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8.  Identification of a subdomain of CENP-B that is necessary and sufficient for localization to the human centromere.

Authors:  A F Pluta; N Saitoh; I Goldberg; W C Earnshaw
Journal:  J Cell Biol       Date:  1992-03       Impact factor: 10.539

9.  A human centromere protein, CENP-B, has a DNA binding domain containing four potential alpha helices at the NH2 terminus, which is separable from dimerizing activity.

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Journal:  J Cell Biol       Date:  1992-12       Impact factor: 10.539

10.  Centromere protein B assembles human centromeric alpha-satellite DNA at the 17-bp sequence, CENP-B box.

Authors:  Y Muro; H Masumoto; K Yoda; N Nozaki; M Ohashi; T Okazaki
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  26 in total

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Review 6.  Using human artificial chromosomes to study centromere assembly and function.

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7.  Uterine dysfunction and genetic modifiers in centromere protein B-deficient mice.

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8.  Fission yeast homologs of human CENP-B have redundant functions affecting cell growth and chromosome segregation.

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9.  Interspersed centromeric element with a CENP-B box-like motif in Chironomus pallidivittatus.

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10.  The C-terminal domain of CENP-C displays multiple and critical functions for mammalian centromere formation.

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