H. Bensoussan
Institut de radioprotection et de sûreté nucléaire
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Featured researches published by H. Bensoussan.
Toxicology | 2009
H. Bensoussan; Line Grancolas; Bernadette Dhieux-Lestaevel; Olivia Delissen; Claire-Marie Vacher; Isabelle Dublineau; Philippe Voisin; Patrick Gourmelon; Mohammed Taouis; Philippe Lestaevel
Uranium is a heavy metal naturally present in the environment that may be chronically ingested by the population. Previous studies have shown that uranium is present in the brain and alters behaviour, notably locomotor activity, sensorimotor ability, sleep/wake cycle and the memory process, but also metabolism of neurotransmitters. The cholinergic system mediates many cognitive systems, including those disturbed after chronic exposure to uranium i.e., spatial memory, sleep/wake cycle and locomotor activity. The objective of this study was to assess whether these disorders follow uranium-induced alteration of the cholinergic system. In comparison with 40 control rats, 40 rats drank 40 mg/L uranyl nitrate for 1.5 or 9 months. Cortex and hippocampus were removed and gene expression and protein level were analysed to determine potential changes in cholinergic receptors and acetylcholine levels. The expression of genes showed various alterations in the two brain areas after short- and long-term exposure. Nevertheless, protein levels of the choline acetyltransferase enzyme (ChAT), the vesicular transporter of acetylcholine (VAChT) and the nicotinic receptor beta2 sub-unit (nAChRbeta2) were unmodified in all cases of the experiment and muscarinic receptor type 1 (m1AChR) protein level was disturbed only after 9 months of exposure in the cortex (-30%). Acetylcholine levels were unchanged in the hippocampus after 1.5 and 9 months, but were decreased in the cortex after 1.5 months only (-22%). Acetylcholinesterase (AChE) activity was also unchanged in the hippocampus but decreased in the cortex after 1.5 and 9 months (-16% and -18%, respectively). Taken together, these data indicate that the cholinergic system is a target of uranium exposure in a structure-dependent and time-dependent manner. These cholinergic alterations could participate in behavioural impairments.
Chemical Research in Toxicology | 2010
Caroline Rouas; H. Bensoussan; David Suhard; Christine Tessier; Line Grandcolas; François Rebiere; Isabelle Dublineau; Mohammed Taouis; Marc Pallardy; Philippe Lestaevel; Yann Gueguen
Uranium is naturally found in the environment, and its extensive use results in an increased risk of human exposure. Kidney cells have mainly been used as in vitro models to study effects of uranium exposure, and very little about the effects on other cell types is known. The aim of this study was to assess the impact of depleted uranium exposure at the cellular level in human kidney (HEK-293), liver (HepG2), and neuronal (IMR-32) cell lines. Cytotoxicity studies showed that these cell lines reacted in a roughly similar manner to depleted uranium exposure, responding at a cytotoxicity threshold of 300-500 μM. Uranium was localized in cells with secondary ion mass spectrometry technology. Results showed that uranium precipitates at subtoxic concentrations (>100 μM). With this approach, we were able for the first time to observe the soluble form of uranium in the cell at low concentrations (10-100 μM). Moreover, this technique allows us to localize it mainly in the nucleus. These innovative results raise the question of how uranium penetrates into cells and open new perspectives for studying the mechanisms of uranium chemical toxicity.
Comptes Rendus Biologies | 2011
Philippe Lestaevel; H. Bensoussan; Radjini Racine; Fabrice Airault; Patrick Gourmelon; Maâmar Souidi
Some heavy metals, or aluminium, could participate in the development of Alzheimer disease (AD). Depleted uranium (DU), another heavy metal, modulates the cholinergic system and the cholesterol metabolism in the brain of rats, but without neurological disorders. The aim of this study was to determine what happens in organisms exposed to DU that will/are developing the AD. This study was thus performed on a transgenic mouse model for human amyloid precursor protein (APP), the Tg2576 strain. The possible effects of DU through drinking water (20 mg/L) over an 8-month period were analyzed on acetylcholine and cholesterol metabolisms at gene level in the cerebral cortex. The mRNA levels of choline acetyl transferase (ChAT) vesicular acetylcholine transporter (VAChT) and ATP-binding cassette transporter A1 (ABC A1) decreased in control Tg2576 mice in comparison with wild-type mice (respectively -89%, -86% and -44%, p < 0.05). Chronic exposure of Tg2576 mice to DU increased mRNA levels of ChAT (+189%, p < 0.05), VAChT (+120%, p < 0.05) and ABC A1 (+52%, p < 0.05) compared to control Tg2576 mice. Overall, these modifications of acetylcholine and cholesterol metabolisms did not lead to increased disturbances that are specific of AD, suggesting that chronic DU exposure did not worsen the pathology in this experimental model.
Journal of Toxicological Sciences | 2013
Philippe Lestaevel; H. Bensoussan; B. Dhieux; Olivia Delissen; Claire-Marie Vacher; Isabelle Dublineau; Philippe Voisin; Mohammed Taouis
Journal of Molecular Neuroscience | 2014
Philippe Lestaevel; F. Airault; Radjini Racine; H. Bensoussan; B. Dhieux; Olivia Delissen; L. Manens; Jocelyne Aigueperse; Philippe Voisin; Maâmar Souidi
Toxicology Letters | 2010
Philippe Lestaevel; H. Bensoussan; B. Dhieux; Isabelle Dublineau; Philippe Voisin; Patrick Gourmelon
Toxicology | 2010
Philippe Lestaevel; E. Romero; B. Dhieux; H. Bensoussan; H. Berradi; Isabelle Dublineau; Philippe Voisin; Patrick Gourmelon
Toxicology | 2010
H. Bensoussan; Line Grandcolas; Bernadette Dhieux-Lestaevel; Olivia Delissen; Claire-Marie Vacher; Isabelle Dublineau; Philippe Voisin; Patrick Gourmelon; Mohammed Taouis; Philippe Lestaevel
Toxicology | 2010
Philippe Lestaevel; E. Romero; B. Dhieux; H. Bensoussan; H. Berradi; Isabelle Dublineau; Philippe Voisin; Patrick Gourmelon
Toxicology | 2010
H. Bensoussan; Line Grandcolas; Bernadette Dhieux-Lestaevel; Olivia Delissen; Claire-Marie Vacher; Isabelle Dublineau; Philippe Voisin; Patrick Gourmelon; Mohammed Taouis; Philippe Lestaevel