Detrimental effects of ethanol and its metabolite acetaldehyde, on first trimester human placental cell turnover and function.

Detrimental effects of ethanol and its metabolite acetaldehyde, on first trimester human placental cell turnover and function.

Fetal alcohol spectrum disorder (FASD) describes developmental issues from high maternal alcohol intake, which commonly results in fetal growth restriction and long term morbidity. We aimed to investigate the effect of alcohol and acetaldehyde, on the first trimester placenta, the period essential f...

Full description

Bibliographic Details
Main Authors: Sylvia Lui, Rebecca L Jones, Nathalie J Robinson, Susan L Greenwood, John D Aplin, Clare L Tower
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3913587?pdf=render
id doaj-de99283e9bfc4d2b88c849cf869b9cc9
record_format Article
spelling doaj-de99283e9bfc4d2b88c849cf869b9cc92020-11-24T21:16:58ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0192e8732810.1371/journal.pone.0087328Detrimental effects of ethanol and its metabolite acetaldehyde, on first trimester human placental cell turnover and function.Sylvia LuiRebecca L JonesNathalie J RobinsonSusan L GreenwoodJohn D AplinClare L TowerFetal alcohol spectrum disorder (FASD) describes developmental issues from high maternal alcohol intake, which commonly results in fetal growth restriction and long term morbidity. We aimed to investigate the effect of alcohol and acetaldehyde, on the first trimester placenta, the period essential for normal fetal organogenesis. Normal invasion and establishment of the placenta during this time are essential for sustaining fetal viability to term. We hypothesise that alcohol (ethanol) and acetaldehyde have detrimental effects on cytotrophoblast invasion, turnover and placental function. Taurine is an important amino acid for neuronal and physiological development, and so, its uptake was assayed in cells and placental explants exposed to alcohol or acetaldehyde. First trimester villous explants and BeWo cells were treated with 0, 10, 20, 40 mM ethanol or 0, 10, 20, 40 µM acetaldehyde. The invasive capacity of SGHPL4, a first trimester extravillous cytotrophoblast cell line, was unaffected by ethanol or acetaldehyde (p>0.05; N = 6). The cells in-cycle were estimated using immunostaining for Ki67. Proliferating trophoblast cells treated with ethanol were decreased in both experiments (explants: 40% at 20 mM and 40 mM, p<0.05, N = 8-9) (cell line: 5% at 20 mM and 40 mM, p<0.05, N = 6). Acetaldehyde also reduced Ki67-positive cells in both experiments (explants at 40 µM p<0.05; N = 6) (cell line at 10 µM and 40 µM; p<0.05; N = 7). Only in the cell line at 20 µM acetaldehyde demonstrated increased apoptosis (p<0.05; N = 6). Alcohol inhibited taurine transport in BeWo cells at 10 mM and 40 mM (p<0.05; N = 6), and in placenta at 40 mM (p<0.05; N = 7). Acetaldehyde did not affect taurine transport in either model (P<0.05; N = 6). Interestingly, system A amino acid transport in placental explants was increased at 10 µM and 40 µM acetaldehyde exposure (p<0.05; N = 6). Our results demonstrate that exposure to both genotoxins may contribute to the pathogenesis of FASD by reducing placental growth. Alcohol also reduces the transport of taurine, which is vital for developmental neurogenesis.http://europepmc.org/articles/PMC3913587?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Sylvia Lui
Rebecca L Jones
Nathalie J Robinson
Susan L Greenwood
John D Aplin
Clare L Tower
spellingShingle Sylvia Lui
Rebecca L Jones
Nathalie J Robinson
Susan L Greenwood
John D Aplin
Clare L Tower
Detrimental effects of ethanol and its metabolite acetaldehyde, on first trimester human placental cell turnover and function.
PLoS ONE
author_facet Sylvia Lui
Rebecca L Jones
Nathalie J Robinson
Susan L Greenwood
John D Aplin
Clare L Tower
author_sort Sylvia Lui
title Detrimental effects of ethanol and its metabolite acetaldehyde, on first trimester human placental cell turnover and function.
title_short Detrimental effects of ethanol and its metabolite acetaldehyde, on first trimester human placental cell turnover and function.
title_full Detrimental effects of ethanol and its metabolite acetaldehyde, on first trimester human placental cell turnover and function.
title_fullStr Detrimental effects of ethanol and its metabolite acetaldehyde, on first trimester human placental cell turnover and function.
title_full_unstemmed Detrimental effects of ethanol and its metabolite acetaldehyde, on first trimester human placental cell turnover and function.
title_sort detrimental effects of ethanol and its metabolite acetaldehyde, on first trimester human placental cell turnover and function.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description Fetal alcohol spectrum disorder (FASD) describes developmental issues from high maternal alcohol intake, which commonly results in fetal growth restriction and long term morbidity. We aimed to investigate the effect of alcohol and acetaldehyde, on the first trimester placenta, the period essential for normal fetal organogenesis. Normal invasion and establishment of the placenta during this time are essential for sustaining fetal viability to term. We hypothesise that alcohol (ethanol) and acetaldehyde have detrimental effects on cytotrophoblast invasion, turnover and placental function. Taurine is an important amino acid for neuronal and physiological development, and so, its uptake was assayed in cells and placental explants exposed to alcohol or acetaldehyde. First trimester villous explants and BeWo cells were treated with 0, 10, 20, 40 mM ethanol or 0, 10, 20, 40 µM acetaldehyde. The invasive capacity of SGHPL4, a first trimester extravillous cytotrophoblast cell line, was unaffected by ethanol or acetaldehyde (p>0.05; N = 6). The cells in-cycle were estimated using immunostaining for Ki67. Proliferating trophoblast cells treated with ethanol were decreased in both experiments (explants: 40% at 20 mM and 40 mM, p<0.05, N = 8-9) (cell line: 5% at 20 mM and 40 mM, p<0.05, N = 6). Acetaldehyde also reduced Ki67-positive cells in both experiments (explants at 40 µM p<0.05; N = 6) (cell line at 10 µM and 40 µM; p<0.05; N = 7). Only in the cell line at 20 µM acetaldehyde demonstrated increased apoptosis (p<0.05; N = 6). Alcohol inhibited taurine transport in BeWo cells at 10 mM and 40 mM (p<0.05; N = 6), and in placenta at 40 mM (p<0.05; N = 7). Acetaldehyde did not affect taurine transport in either model (P<0.05; N = 6). Interestingly, system A amino acid transport in placental explants was increased at 10 µM and 40 µM acetaldehyde exposure (p<0.05; N = 6). Our results demonstrate that exposure to both genotoxins may contribute to the pathogenesis of FASD by reducing placental growth. Alcohol also reduces the transport of taurine, which is vital for developmental neurogenesis.
url http://europepmc.org/articles/PMC3913587?pdf=render
work_keys_str_mv AT sylvialui detrimentaleffectsofethanolanditsmetaboliteacetaldehydeonfirsttrimesterhumanplacentalcellturnoverandfunction
AT rebeccaljones detrimentaleffectsofethanolanditsmetaboliteacetaldehydeonfirsttrimesterhumanplacentalcellturnoverandfunction
AT nathaliejrobinson detrimentaleffectsofethanolanditsmetaboliteacetaldehydeonfirsttrimesterhumanplacentalcellturnoverandfunction
AT susanlgreenwood detrimentaleffectsofethanolanditsmetaboliteacetaldehydeonfirsttrimesterhumanplacentalcellturnoverandfunction
AT johndaplin detrimentaleffectsofethanolanditsmetaboliteacetaldehydeonfirsttrimesterhumanplacentalcellturnoverandfunction
AT clareltower detrimentaleffectsofethanolanditsmetaboliteacetaldehydeonfirsttrimesterhumanplacentalcellturnoverandfunction
_version_ 1726015041481736192

Similar Items