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C. Andrianopoulos

Researcher at University of Patras

Publications -  8
Citations -  128

C. Andrianopoulos is an academic researcher from University of Patras. The author has contributed to research in topics: Micronucleus test & Micronucleus. The author has an hindex of 7, co-authored 8 publications receiving 124 citations.

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Spontaneous and spindle poison-induced micronuclei and chromosome non-disjunction in cytokinesis-blocked lymphocytes from two age groups of women

TL;DR: It was confirmed that age increases micronucleus frequency and non-disjunction of chromosomes X and 8 also increased with age, chromosome X being the more sensitive.
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Induction of micronuclei and sister chromatid exchange in mouse splenocytes after exposure to the butadiene metabolite 3, 4-epoxy-1-butene

TL;DR: The genotoxic effects of EB were studied by estimating micronuclei (MN) and sister chromatid exchange (SCE) frequencies in stimulated mouse splenocytes and a weak aneugenic effect was found as well.
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Micronucleus induction in somatic cells of mice as evaluated after 1,3-butadiene inhalation

TL;DR: BD was found to be clastogenic by inducing increased micronucleus frequencies in both cell compartments and also to induce cytotoxicity at the highest level of exposure and in mouse splenocytes, BD has also shown a weak aneugenic effect at a short time interval after the exposure.
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Aneugenic potential of the nitrogen mustard analogues melphalan, chlorambucil and p-N,N-bis(2-chloroethyl)aminophenylacetic acid in cell cultures in vitro

TL;DR: The carcinogenicity of nitrogen mustard analogues studied may be attributed not only to their activity to trigger gene mutation and chromosome breakage, but also to their aneugenic potential.
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Genotoxicity of hydrochlorothiazide in cultured human lymphocytes. I. Evaluation of chromosome delay and chromosome breakage.

TL;DR: Evaluated genotoxicity of HCTZ in cultured human lymphocytes using the Cytokinesis Blocked Micronucleus (CBMN) assay indicates that HCTz produces micronuclei in culturedhuman lymphocytes by a mechanism that involves chromosome delay and to a lesser extent through chromosome breakage.