Bisphenol-A induces cell cycle delay and alters centrosome and spindle microtubular organization in oocytes during meiosis

doi:10.1093/molehr/gah179

Mol. Hum. Reprod. Advance Access published online on May 6, 2005
Molecular Human Reproduction, doi:10.1093/molehr/gah179

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Molecular Human Reproduction © The Author 2005. Published by Oxford University Press on behalf of the European Society of Human Reproduction and Embryology. All rights reserved. For Permissions, please email: journals.permissions@oupjournals.org
Received February 28, 2005
Revised April 6, 2005
Accepted April 10, 2005

Article

Bisphenol-A induces cell cycle delay and alters centrosome and spindle microtubular organization in oocytes during meiosis

A. Can ¹^*, O. Semiz ², and O. Cinar ³

¹ Laboratory for Reproductive Cell Science, Department of Histology-Embryology, Ankara University School of Medicine, Ankara, 06100,, Turkey Ankara University Biotechnology Institute, Besevler, Ankara, 06500, Turkey
² Sakarya University School of Health, Esentepe Campus, Sakarya 54187, Turkey
³ Laboratory for Reproductive Cell Science, Department of Histology-Embryology, Ankara University School of Medicine, Ankara, 06100,, Turkey

^* To whom correspondence should be addressed.
A. Can, E-mail: alpcan{at}medicine.ankara.edu.tr

Abstract

Bisphenol-A (BPA) is a widely used environmental estrogen-likechemical that has a weak estrogenic activity. This study aimedto test the potential inhibitory effects of BPA on meiotic cellcycle progression, centrosomes and spindle integrity in mousecumulus-oocyte complexes (COCs). They were exposed to BPA (10-30µM; 2.3-6.8 ppb) during meiosis-I and the formation ofmetaphase-II (M-II) spindle. Exposure to BPA during meiosis-Icaused a dose-dependent retardation/inhibition of cell cycleprogression; 74 and 61% of cells reached metaphase-I (M-I) inthe presence of 10 and 30 µM BPA, respectively, (81% incontrols, P<0.001). A more striking delay was noted whenoocytes were exposed to BPA during the formation of M-II spindle,i.e. 61 and 41% of cells (94% in controls, P<0.001) reachedM-II while the remaining cells remained at M-I. Depending ondose, both (i) loosening and elongation of meiotic spindlesand (ii) compaction and dispersion of pericentriolar material(PCM) were noted in all samples, all of which resulted in aseries of spindle abnormalities. Interestingly, no chromosomewas detected in the first polar body after the 10 and 30 µMBPA treatments. When the cells were freed from BPA exposureat 10 and 30 µM, 70 and 61%, of the cells succeeded inreaching M-II (93% in controls, P<0.001), respectively. Inconclusion, one mode of action of BPA is a moderately severeyet reversible delay in the meiotic cell cycle, possibly bya mechanism that degrades centrosomal proteins and thus perturbsthe spindle microtubule organization and chromosome segregation.

Keywords: bisphenol-A; centrosome abnormality; meiotic spindle; oocyte; pericentrin.

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