Literature DB >> 12714687

What do human micronuclei contain?

Hannu Norppa1, Ghita C-M Falck.   

Abstract

As micronuclei (MN) derive from chromosomal fragments and whole chromosomes lagging behind in anaphase, the MN assay can be used to show both clastogenic and aneugenic effects. The distinction between these phenomena is important, since the exposure studied often induces only one type of MN. This particularly concerns the use of MN as a biomarker of genotoxic exposure and effects, where differences in MN frequencies between exposed subjects and referents are expected to be small. A specific analysis of the induced type of MN may considerably improve the sensitivity of detecting the exposure effect. MN harbouring chromosomes can be distinguished from those harbouring acentric fragments by the presence of a centromere. The proportion of centromere-positive MN in human lymphocytes increases with age, which primarily reflects an age-dependent micronucleation of the X and Y chromosomes. The X chromosome especially tends to lag behind in female lymphocyte anaphase, being micronucleated more efficiently than autosomes. There is some evidence for an enhanced prevalence of fragments from chromosome 9 in spontaneous human lymphocyte MN and from chromosomes 1, 9 or 16 in MN induced in vitro by some clastogens; the breakage appears to occur in the heterochromatic block of these chromosomes. Although there are indications that centromere identification can improve the detection of clastogenic effects in humans in vivo, smokers have not shown an increase in centromere-negative MN in their cultured lymphocytes, although smoking is known to produce chromosomal aberrations. This may suggest that fragment-containing MN and chromosomal aberrations cover partly different phenomena. Understanding the mechanistic origin and contents of MN is essential for the proper use of this cytogenetic end-point in biomarker studies, genotoxicity testing and risk assessment.

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Year:  2003        PMID: 12714687     DOI: 10.1093/mutage/18.3.221

Source DB:  PubMed          Journal:  Mutagenesis        ISSN: 0267-8357            Impact factor:   3.000


  76 in total

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Authors:  Corentin Laulier; Anita Cheng; Nick Huang; Jeremy M Stark
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2.  Micronuclei levels in peripheral blood lymphocytes as a potential biomarker for pancreatic cancer risk.

Authors:  Ping Chang; Yanan Li; Donghui Li
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3.  Resolution of anaphase bridges in cancer cells.

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4.  Micronuclei in lymphocytes from currently active uranium miners.

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Review 5.  Current status of biodosimetry based on standard cytogenetic methods.

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Journal:  Radiat Environ Biophys       Date:  2010-07-09       Impact factor: 1.925

6.  Nucleoplasmic bridges and tailed nuclei are signatures of radiation exposure in Oreochromis mossambicus using erythrocyte micronucleus cytome assay (EMNCA).

Authors:  S Anbumani; Mary N Mohankumar
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7.  Complementarity of standard cytogenetic assays.

Authors:  Slavka Ibrulj; Sanin Haverić; Anja Haverić
Journal:  Bosn J Basic Med Sci       Date:  2008-02       Impact factor: 3.363

Review 8.  Sizing up the nucleus: nuclear shape, size and nuclear-envelope assembly.

Authors:  Micah Webster; Keren L Witkin; Orna Cohen-Fix
Journal:  J Cell Sci       Date:  2009-05-15       Impact factor: 5.285

9.  Mechanisms leading to the formation of micronuclei containing sex chromosomes differ with age.

Authors:  Kimberly H Jones; Timothy P York; Colleen Jackson-Cook
Journal:  Mutat Res       Date:  2012-05-18       Impact factor: 2.433

10.  Assessment of individual susceptibility to baseline DNA and cytogenetic damage in a healthy Turkish population: evaluation with lifestyle factors.

Authors:  Ela Kadioglu; Neslihan Aygun Kocabas; Gonca Cakmak Demircigil; Erdem Coskun; Eren Ozcagli; Emre Durmaz; Bensu Karahalil; Sema Burgaz; Semra Sardas
Journal:  Genet Test Mol Biomarkers       Date:  2012-08-20
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