Literature DB >> 1551672

Characterization of centromere arrangements and test for random distribution in G0, G1, S, G2, G1, and early S' phase in human lymphocytes.

R Weimer1, T Haaf, J Krüger, M Poot, M Schmid.   

Abstract

The arrangement of centromeres, cluster formation and association with the nucleolus and the nuclear membrane were characterized in human lymphocytes during the course of interphase in a cell-phase-dependent manner. We evaluated 3,893 cell nuclei categorized by five parameters. The centromeres were visualized by means of indirect immunofluorescent labeling with anti-centromere antibodies (ACA) contained in serum of patients with CREST syndrome. The cell nuclei were classified as G0, G1, S, G2, G1' and early S' phase by comparing microscopically identified groups of cell nuclei with flow cytometric determination of cell cycle stage of synchronized and unsynchronized lymphocyte cell cultures. Based on a discrimination analysis, a program was devised that calculated the probability for any cell nucleus belonging to the G0, G1, S, G2, G1' and early S' phase using only two microscopic parameters. Various characteristics were determined in the G0, S, and G2 stages. A transition stage to S phase within G1 was detected. This stage shows centromere arrangements not repeated in later cell cycles and which develop from the dissolution of centromere clusters in the periphery of the nucleus during G0 and G1. S phase exhibits various non-random centromere arrangements and associations of centromeres with the nucleolus. G1' and early S' phase of the second cell cycle display no characteristic centromere arrangement. The duplication of centromeres in G2 is asynchronous in two phases. For all cell phases a test for random distribution of the centromeres in the cell nucleus was performed. There is a distinct tendency for centromeres to be in a peripheral position during G0 and G1; this tendency becomes weaker in S phase. Although the visual impression is a seemingly random distribution of centromeres in G2 and G1', statistical analysis still demonstrates a significant deviation from random distribution in favor of a peripheral location. Only the early S phase of the second cell cycle shows no significant deviation from a random distribution.

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Year:  1992        PMID: 1551672     DOI: 10.1007/bf02265296

Source DB:  PubMed          Journal:  Hum Genet        ISSN: 0340-6717            Impact factor:   4.132


  23 in total

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Authors:  C L Rieder
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Review 5.  Arrangement of chromatin in the nucleus.

Authors:  D E Comings
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6.  Telomere and centromere association tendencies in the human male metaphase complement.

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Journal:  Hum Genet       Date:  1980       Impact factor: 4.132

7.  Human anticentromere antibodies: distribution, characterization of antigens, and effect on microtubule organization.

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8.  Autoantibody to centromere (kinetochore) in scleroderma sera.

Authors:  Y Moroi; C Peebles; M J Fritzler; J Steigerwald; E M Tan
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10.  Kinetochore structure, duplication, and distribution in mammalian cells: analysis by human autoantibodies from scleroderma patients.

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  20 in total

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Review 3.  Transcription and ncRNAs: at the cent(rome)re of kinetochore assembly and maintenance.

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7.  Data-Driven Polymer Model for Mechanistic Exploration of Diploid Genome Organization.

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9.  Nuclear organization of centromeric domains is not perturbed by inhibition of histone deacetylases.

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10.  Three-dimensional analysis of the arrangement of compact chromatin in the nucleus of G0 rat lymphocytes.

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