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Dive into the research topics where Bruno Lebrun is active.

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Featured researches published by Bruno Lebrun.


Bioorganic & Medicinal Chemistry Letters | 2000

Syntheses of optically pure β-hydroxyaspartate derivatives as glutamate transporter blockers

Keiko Shimamoto; Yasushi Shigeri; Yoshimi Yasuda-Kamatani; Bruno Lebrun; Noboru Yumoto; Terumi Nakajima

DL-threo-beta-benzyloxyaspartate (DL-TBOA) is a non-transportable blocker of the glutamate transporters that serves as an indispensable tool for the investigation of the physiological roles of the transporters. To examine the precise interaction between a blocker and the transporters, we synthesized the optically pure isomers (L- and D-TBOA) and its erythro-isomers. L-TBOA is the most potent blocker for the human excitatory amino acid transporters (EAAT1-3), while D-TBOA revealed a difference in the pharmacophores between EAAT1 and EAAT3. We also synthesized the substituent variants (methyl or naphthylmethyl derivatives) of L-TBOA. The results obtained here suggest that bulky substituents are crucial for non-transportable blockers.


PLOS ONE | 2011

The Food-Contaminant Deoxynivalenol Modifies Eating by Targeting Anorexigenic Neurocircuitry

Clémence Girardet; Marion S. Bonnet; Rajae Jdir; Medhi Sadoud; Sylvie Thirion; Catherine Tardivel; Julien Roux; Bruno Lebrun; Nicolas Wanaverbecq; Lourdes Mounien; Jérôme Trouslard; André Jean; Michel Dallaporta; Jean-Denis Troadec

Physiological regulations of energy balance and body weight imply highly adaptive mechanisms which match caloric intake to caloric expenditure. In the central nervous system, the regulation of appetite relies on complex neurocircuitry which disturbance may alter energy balance and result in anorexia or obesity. Deoxynivalenol (DON), a trichothecene, is one of the most abundant mycotoxins found on contaminated cereals and its stability during processing and cooking explains its widespread presence in human food. DON has been implicated in acute and chronic illnesses in both humans and farm animals including weight loss. Here, we provide the first demonstration that DON reduced feeding behavior and modified satiation and satiety by interfering with central neuronal networks dedicated to food intake regulation. Moreover, our results strongly suggest that during intoxication, DON reaches the brain where it modifies anorexigenic balance. In view of the widespread human exposure to DON, the present results may lead to reconsider the potential consequences of chronic DON consumption on human eating disorders.


Toxicological Sciences | 2011

Central Inflammation and Sickness-Like Behavior Induced by the Food Contaminant Deoxynivalenol: A PGE2-Independent Mechanism

Clémence Girardet; Marion S. Bonnet; Rajae Jdir; Medhi Sadoud; Sylvie Thirion; Catherine Tardivel; Julien Roux; Bruno Lebrun; Lourdes Mounien; Jérôme Trouslard; André Jean; Michel Dallaporta; Jean-Denis Troadec

Deoxynivalenol (DON), one of the most abundant trichothecenes found on cereals, has been implicated in mycotoxicoses in both humans and farm animals. Low-dose toxicity is characterized by reduced weight gain, diminished nutritional efficiency, and immunologic effects. The levels and patterns of human food commodity contamination justify that DON consumption constitutes a public health issue. DON stability during processing and cooking explains its large presence in human food. We characterized here DON intoxication by showing that the toxin concomitantly affects feeding behavior, body temperature, and locomotor activity after both per os and central administration. Using c-Fos expression mapping, we identified the neuronal structures activated in response to DON and observed that the pattern of neuronal populations activated by the toxin resembled those induced by inflammatory signals. By real-time PCR, we report the first evidences for a DON-induced central inflammation, attested by the strong upregulation of interleukin-1β, interleukin-6, tumor necrosis factor-α, cyclooxygenase-2, and microsomal prostaglandin synthase-1 (mPGES-1) messenger RNA. However, silencing prostaglandins E2 signaling pathways using mPGES-1 knockout mice, which are resistant to cytokine-induced sickness behavior, did not modify the responses to the toxin. These results reveal that, despite strong similarities, behavioral changes observed after DON intoxication differ from classical sickness behavior evoked by inflammatory cytokines.


FEBS Letters | 2001

A new class of scorpion toxin binding sites related to an A-type K+ channel: pharmacological characterization and localization in rat brain.

Hélène Vacher; Régine Romi-Lebrun; Christiane Mourre; Bruno Lebrun; Saïd Kourrich; Frédérique Masmejean; Terumi Nakajima; Christian Legros; Marcel Crest; Pierre E. Bougis; Marie-France Martin-Eauclaire

A new scorpion toxin (3751.8 Da) was isolated from the Buthus martensi venom, sequenced and chemically synthesized (sBmTX3). The A‐type current of striatum neurons in culture completely disappeared when 1 μM sBmTX3 was applied (K d=54 nM), whereas the sustained K+ current was unaffected. 125I‐sBmTX3 specifically bound to rat brain synaptosomes (maximum binding=14 fmol mg−1 of protein, K d=0.21 nM). A panel of toxins yet described as specific ligands for K+ channels were unable to compete with 125I‐sBmTX3. A high density of 125I‐sBmTX3 binding sites was found in the striatum, hippocampus, superior colliculus, and cerebellum in the adult rat brain.


Neuropharmacology | 2009

Depolarization-induced release of endocannabinoids by murine dorsal motor nucleus of the vagus nerve neurons differentially regulates inhibitory and excitatory neurotransmission

Julien Roux; Nicolas Wanaverbecq; André Jean; Bruno Lebrun; Jérôme Trouslard

Numerous studies, focused on the hypothalamus, have recently implicated endocannabinoids (EC) as orexigenic factors in the central control of food intake. However, the EC system is also highly expressed in the hindbrain autonomic integrator of food intake regulation, i.e. the dorsal vagal complex (DVC). Previous studies have shown that exogenous cannabinoids, by acting on cannabinoid 1 receptor (CB1R), suppress GABAergic and glutamatergic neuronal transmission in adult rat dorsal motor nucleus of the vagus nerve (DMNV), the principal efferent compartment of the DVC. However, no endogenous release of EC has been demonstrated in DVC to date. Using patch-clamp techniques on mouse coronal brainstem slices, we confirmed that both inhibitory and excitatory neurotransmission were depressed by WIN 55,212-2, a CB1R agonist. We demonstrated that DMNV neurons exhibited a rapid and reversible depolarization-induced suppression of electrically evoked GABAergic IPSCs (eIPSCs), classically known as DSI (depolarization-induced suppression of inhibition), while spontaneous or miniature IPSCs activity remained unaltered. Further, no depolarization-induced suppression of glutamatergic eEPSCs (DSE) occurred. Our results indicate that DSI was blocked by SR141716A (Rimonabant), a selective CB1R antagonist, and was dependent on calcium elevation in DMNV neurons, suggesting a release of EC in the DVC. Moreover, the analysis of the paired-pulse ratio, of the coefficient of variation and of the failure rate of eIPSCs support the fact that EC-mediated suppression of GABAergic inhibition takes place at the presynaptic level. These results show for the first time that DMNV neurons release EC in an activity-dependent manner, which in turn differentially regulates their inhibitory and excitatory synaptic inputs.


Mechanisms of Ageing and Development | 2012

Effects of aging and caloric restriction on brainstem satiety center signals in rats

Emmanuel Moyse; Karine Bédard; Stéphanie Segura; Stéphanie Mahaut; Catherine Tardivel; Guylaine Ferland; Bruno Lebrun; Pierrette Gaudreau

Age-related increases of body weight and adiposity, indicating dysregulation of food intake/energy expenditure, can be prevented in rodents by long-term 40% caloric restriction. The dorsal vagal complex (DVC), the brainstem center mediating the satiety reflex, has recently emerged as a determinant effector of long-term feeding adaptation. To study the effects of aging and caloric restriction on satiety circuits, leptin and brain-derived neurotrophic factor (BDNF) signaling systems were studied in 2- and 19-month-old ad libitum-fed (AL) and 19-month-old calorie-restricted (CR) rats. Age-induced hyperleptinemia in AL rats was correlated with elevated DVC BDNF immunoreactive concentrations and satiety threshold stability, suggesting functional desensitization of the DVC to these signals. To better understand this phenomenon, mRNA levels of receptor and post-receptor signaling effectors were measured by real-time RT-PCR. Aging selectively increased BDNF receptors and suppressor of cytokine signaling-3 (SOCS-3) mRNA levels. Caloric restriction prevented age-related increases of serum leptin, DVC BDNF and SOCS-3 mRNA levels, but not those of BDNF receptors. In CR rats, prevention of leptin resistance-promoting SOCS-3 induction was also observed at the protein level. This study suggests that leptin post-receptor targets and BDNF signaling play a role in the establishment of age-related DVC dysfunction.


Journal of Neuroscience Methods | 1993

A new configuration for voltage clamp of axons used to demonstrate nerve conduction blockade by a 2,5-disubstituted pyrrolidine

Daniel Cattaert; Bruno Lebrun

An original voltage-clamp technique on axons from crayfish Procambarus clarkii is described in this paper. Its advantages are: a fast dissection leading to the availability of several fibers of different diameters (10-500 microns) that may contain different ion channels; and use of a double-electrode voltage clamp on a chosen fiber with good clamping characteristics (short time clamp and good space clamp, small leak conductance). Because of the absence of exogenous lipidic phase in the superfusion chamber, this technique appears particularly suited to studying how liposoluble neurotoxins affect nerve conduction. This method has been successfully applied to test the effect of a synthetic derivative (2-(1non-8enyl)-5(1non-8enyl)pyrrolidine (Pyr 9)) of ant venom alkaloids from Monomorium species on nerve conduction. We present here evidence of a strong blocking effect on inward current involved in spike conduction. The resting potential of the treated axons did not change and it appears that only the inward current was affected.


Biochemical Journal | 1997

A four-disulphide-bridged toxin, with high affinity towards voltage-gated K+ channels, isolated from Heterometrus spinnifer (Scorpionidae) venom.

Bruno Lebrun; Régine Romi-Lebrun; Marie-France Martin-Eauclaire; Akikazu Yasuda; Masaji Ishiguro; Yoshiaki Oyama; Olaf Pongs; Terumi Nakajima


Biochemistry | 1997

Purification, Characterization, and Synthesis of Three Novel Toxins from the Chinese Scorpion Buthus martensi, Which Act on K+ Channels

Régine Romi-Lebrun; Bruno Lebrun; Marie-France Martin-Eauclaire; Masaji Ishiguro; Pierre Escoubas; Fang Qi Wu; Miki Hisada; Olaf Pongs; Terumi Nakajima


Journal of Biological Chemistry | 1997

New β-Hydroxyaspartate Derivatives Are Competitive Blockers for the Bovine Glutamate/Aspartate Transporter

Bruno Lebrun; Masahiro Sakaitani; Keiko Shimamoto; Yoshimi Yasuda-Kamatani; Terumi Nakajima

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Terumi Nakajima

Japanese Ministry of International Trade and Industry

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André Jean

Centre national de la recherche scientifique

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Julien Roux

Centre national de la recherche scientifique

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Régine Romi-Lebrun

French Alternative Energies and Atomic Energy Commission

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Catherine Tardivel

Centre national de la recherche scientifique

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Jérôme Trouslard

Centre national de la recherche scientifique

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Marion S. Bonnet

Centre national de la recherche scientifique

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Medhi Sadoud

Centre national de la recherche scientifique

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Rajae Jdir

Centre national de la recherche scientifique

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Bruno Bariohay

Institut national de la recherche agronomique

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