Search

Your search keyword '"Sommer, Wolfgang H."' showing total 527 results
Start Over Author "Sommer, Wolfgang H."
527 results on '"Sommer, Wolfgang H."'

103. Increased network centrality of the anterior insula in early abstinence from alcohol.

Author

Bordier, Cecile, Weil, Georg, Bach, Patrick, Scuppa, Giulia, Nicolini, Carlo, Forcellini, Giulia, Pérez‐Ramirez, Ursula, Moratal, David, Canals, Santiago, Hoffmann, Sabine, Hermann, Derik, Vollstädt‐Klein, Sabine, Kiefer, Falk, Kirsch, Peter, Sommer, Wolfgang H., and Bifone, Angelo

Subjects
INSULAR cortex, TEMPERANCE, FUNCTIONAL magnetic resonance imaging, LARGE-scale brain networks, ALCOHOLISM, FUNCTIONAL connectivity
Abstract

Abnormal resting‐state functional connectivity, as measured by functional magnetic resonance imaging (MRI), has been reported in alcohol use disorders (AUD), but findings are so far inconsistent. Here, we exploited recent developments in graph‐theoretical analyses, enabling improved resolution and fine‐grained representation of brain networks, to investigate functional connectivity in 35 recently detoxified alcohol dependent patients versus 34 healthy controls. Specifically, we focused on the modular organization, that is, the presence of tightly connected substructures within a network, and on the identification of brain regions responsible for network integration using an unbiased approach based on a large‐scale network composed of more than 600 a priori defined nodes. We found significant reductions in global connectivity and region‐specific disruption in the network topology in patients compared with controls. Specifically, the basal brain and the insular–supramarginal cortices, which form tightly coupled modules in healthy subjects, were fragmented in patients. Further, patients showed a strong increase in the centrality of the anterior insula, which exhibited stronger connectivity to distal cortical regions and weaker connectivity to the posterior insula. Anterior insula centrality, a measure of the integrative role of a region, was significantly associated with increased risk of relapse. Exploratory analysis suggests partial recovery of modular structure and insular connectivity in patients after 2 weeks. These findings support the hypothesis that, at least during the early stages of abstinence, the anterior insula may drive exaggerated integration of interoceptive states in AUD patients with possible consequences for decision making and emotional states and that functional connectivity is dynamically changing during treatment. [ABSTRACT FROM AUTHOR]

Published
2022
Full Text
View/download PDF

104. Test–retest reliability of neural alcohol cue‐reactivity: Is there light at the end of the magnetic resonance imaging tube?

Author

Bach, Patrick, Reinhard, Iris, Koopmann, Anne, Bumb, Jan M., Sommer, Wolfgang H., Vollstädt‐Klein, Sabine, and Kiefer, Falk

Subjects
MAGNETIC resonance imaging, STATISTICAL reliability, ALCOHOL, INTRACLASS correlation
Abstract

Over the last decades, the assessment of alcohol cue‐reactivity gained popularity in addiction research, and efforts were undertaken to establish neural biomarkers. This attempt however depends on the reliability of cue‐induced brain activation. Thus, we assessed test–retest reliability of alcohol cue‐reactivity and its implications for imaging studies in addiction. We investigated test–retest reliability of alcohol cue‐induced brain activation in 144 alcohol‐dependent patients over 2 weeks. We computed established reliability estimates, such as intraclass correlation (ICC), Dice and Jaccard coefficients, for the three contrast conditions of interest: 'alcohol', 'neutral' and the 'alcohol versus neutral' difference contrast. We also investigated how test–retest reliability of the different contrasts affected the capacity to establishing associations with clinical data and determining effect size estimates. Whereas brain activation, indexed by the constituting contrast conditions 'alcohol' and 'neutral' separately, displayed overall moderate (ICC > 0.4) to good (ICC > 0.75) test–retest reliability in areas of the mesocorticolimbic system, the difference contrast 'alcohol versus neutral' showed poor overall reliability (ICC < 0.40), which was related to the intercorrelation between the constituting conditions. Data simulations and analyses of craving data confirmed that the low reliability of the difference contrast substantially limited the capacity to establish associations with clinical data and precisely estimate effect sizes. Future research on alcohol cue‐reactivity should be cautioned by the low reliability of the common 'alcohol versus neutral' difference contrast. We propose that this limitation can be overcome by using the constituent task conditions as an individual difference measure, when intending to longitudinally monitor brain responses. [ABSTRACT FROM AUTHOR]

Published
2022
Full Text
View/download PDF

108. Detecting alcohol-induced brain damage noninvasively using diffusion tensor imaging

Author

European Commission, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), German Research Foundation, European Research Council, De Santis, Silvia, Sommer, Wolfgang H., Canals, Santiago, European Commission, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), German Research Foundation, European Research Council, De Santis, Silvia, Sommer, Wolfgang H., and Canals, Santiago

Abstract

While alcohol’s detrimental effects on the brain are widely acknowledged, diagnostic markers for detection and monitoring alcohol-induced brain damage are lacking. A recent study showed that diffusion tensor imaging can be used to monitor this damage and characterized the progression of the observed changes into early abstinence. Here, we discuss the main findings of that study and highlight current technical limitations which, once addressed, can pave the way to the development of new powerful diagnostic markers for alcohol-induced brain damage.

Published
2019

109. Incubation of neural alcohol cue reactivity after withdrawal and its blockade by naltrexone

Author

German Research Foundation, European Commission, Bach, Patrick, Weil, Georg, Pompili, Enrico, Hoffmann, Sabine, Hermann, Derik, Vollstädt‐Klein, Sabine, Mann, Karl, Pérez-Ramírez, Úrsula, Moratal, David, Canals, Santiago, Dursun, Serdar M., Greenshaw, Andrew J., Kirsch, Peter, Kiefer, Falk, Sommer, Wolfgang H., German Research Foundation, European Commission, Bach, Patrick, Weil, Georg, Pompili, Enrico, Hoffmann, Sabine, Hermann, Derik, Vollstädt‐Klein, Sabine, Mann, Karl, Pérez-Ramírez, Úrsula, Moratal, David, Canals, Santiago, Dursun, Serdar M., Greenshaw, Andrew J., Kirsch, Peter, Kiefer, Falk, and Sommer, Wolfgang H.

Abstract

During the first weeks of abstinence, alcohol craving in patients may increase or “incubate.” We hypothesize that Naltrexone (NTX) blocks this incubation effect. Here, we compared NTX effects on neural alcohol cue reactivity (CR) over the first weeks of abstinence and on long‐term clinical outcomes to standard treatment. Male alcohol‐dependent patients (n = 55) and healthy controls (n = 35) were enrolled. Participants underwent baseline psychometric testing and functional magnetic resonance imaging (fMRI) assessment of mesolimbic alcohol CR. Patients participated in a standard treatment program with the option of adjuvant NTX. They received another scan after 2 weeks of treatment. We found higher CR in several brain regions in patients versus healthy controls. CR significantly increased over 2 weeks in the standard treatment group (n = 13) but not in the NTX group (n = 22). NTX significantly attenuated CR in the left putamen and reduced relapse risk to heavy drinking within 3 months of treatment. Additionally, increased CR in the left putamen and its course over time predicted both NTX response and relapse risk. Carrier status for the functional OPRM1 variant rs1799971:A > G was considered but had no effect on NTX efficacy. In conclusion, NTX was most effective in patients with high CR in the left putamen. While the results from our naturalistic study await further confirmation from prospective randomized trials, they support a potential role of neural CR as a biomarker in the development of precision medicine approaches with NTX.

Published
2019

110. Microstructural white matter alterations in men with alcohol use disorder and rats with excessive alcohol consumption during early abstinence

Author

European Commission, Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Ministerio de Economía y Competitividad (España), Ministerio de Sanidad, Servicios Sociales e Igualdad (España), German Research Foundation, De Santis, Silvia, Bach, Patrick, Pérez-Cervera, Laura, Cosa-Linan, Alejandro, Weil, Georg, Vollstädt‐Klein, Sabine, Hermann, Derik, Kiefer, Falk, Kirsch, Peter, Ciccocioppo, Roberto, Sommer, Wolfgang H., Canals, Santiago, European Commission, Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Ministerio de Economía y Competitividad (España), Ministerio de Sanidad, Servicios Sociales e Igualdad (España), German Research Foundation, De Santis, Silvia, Bach, Patrick, Pérez-Cervera, Laura, Cosa-Linan, Alejandro, Weil, Georg, Vollstädt‐Klein, Sabine, Hermann, Derik, Kiefer, Falk, Kirsch, Peter, Ciccocioppo, Roberto, Sommer, Wolfgang H., and Canals, Santiago

Abstract

[Importance] Although the detrimental effects of alcohol on the brain are widely acknowledged, observed structural changes are highly heterogeneous, and diagnostic markers for characterizing alcohol-induced brain damage, especially in early abstinence, are lacking. This heterogeneity, likely contributed to by comorbidity factors in patients with alcohol use disorder (AUD), challenges a direct link of brain alterations to the pathophysiology of alcohol misuse. Translational studies in animal models may help bridge this causal gap., [Objective] To compare microstructural properties extracted using advanced diffusion tensor imaging (DTI) in the brains of patients with AUD and a well-controlled rat model of excessive alcohol consumption and monitor the progression of these properties during early abstinence., [Design, Setting, and Participants] This prospective observational study included 2 cohorts of hospitalized patients with AUD (n = 91) and Marchigian Sardinian alcohol-preferring (msP) rats (n = 27). In humans cross-sectional comparison were performed with control participants (healthy men [n = 36]) and longitudinal comparisons between different points after alcohol withdrawal. In rats, longitudinal comparisons were performed in alcohol-exposed (n = 27) and alcohol-naive msP rats (n = 9). Human data were collected from March 7, 2013, to August 3, 2016, and analyzed from June 14, 2017, to May 31, 2018; rat data were collected from January 15, 2017, to May 12, 2017, and analyzed from October 11, 2017, to May 28, 2018., [Main Outcomes and Measures] Fractional anisotropy and other DTI measures of white matter properties after long-term alcohol exposure and during early abstinence in both species and clinical and demographic variables and time of abstinence after discharge from hospital in patients., [Results] The analysis included 91 men with AUD (mean [SD] age, 46.1 [9.6] years) and 27 male rats in the AUD groups and 36 male controls (mean [SD] age, 41.7 [9.3] years) and 9 male control rats. Comparable DTI alterations were found between alcohol and control groups in both species, with a preferential involvement of the corpus callosum (fractional anisotropy Cohen d = −0.84 [P < .01] corrected in humans and Cohen d = −1.17 [P < .001] corrected in rats) and the fornix/fimbria (fractional anisotropy Cohen d = −0.92 [P < .001] corrected in humans and d = −1.24 [P < .001] corrected in rats). Changes in DTI were associated with preadmission consumption patterns in patients and progress in humans and rats during 6 weeks of abstinence. Mathematical modeling shows this process to be compatible with a sustained demyelination and/or a glial reaction., [Conclusions and Relevance] Using a translational DTI approach, comparable white matter alterations were found in patients with AUD and rats with long-term alcohol consumption. In humans and rats, a progression of DTI alterations into early abstinence (2-6 weeks) suggests an underlying process that evolves soon after cessation of alcohol use.

Published
2019

111. The SyBil-AA real-time fMRI neurofeedback study: protocol of a single-blind randomized controlled trial in alcohol use disorder

Author

Gerchen, Martin Fungisai, Kirsch, Martina, Bahs, Nathalie, Halli, Patrick, Gerhardt, Sarah, Schäfer, Axel, Sommer, Wolfgang H., Kiefer, Falk, and Kirsch, Peter

Subjects
Adult, Adolescent, lcsh:RC435-571, Functional magnetic resonance imaging, Prefrontal Cortex, Addiction, Cue-reactivity, Study Protocol, Young Adult, 610 Medical sciences Medicine, Clinical Protocols, lcsh:Psychiatry, Humans, Single-Blind Method, Aged, Auditory Cortex, Brain Mapping, Alcohol dependence, Middle Aged, Neurofeedback, Inferior frontal gyrus, Magnetic Resonance Imaging, Alcoholism, Treatment Outcome, Brain-computer interface, Ventral striatum, Follow-Up Studies
Abstract

Background Alcohol Use Disorder is a highly prevalent mental disorder which puts a severe burden on individuals, families, and society. The treatment of Alcohol Use Disorder is challenging and novel and innovative treatment approaches are needed to expand treatment options. A promising neuroscience-based intervention method that allows targeting cortical as well as subcortical brain processes is real-time functional magnetic resonance imaging neurofeedback. However, the efficacy of this technique as an add-on treatment of Alcohol Use Disorder in a clinical setting is hitherto unclear and will be assessed in the Systems Biology of Alcohol Addiction (SyBil-AA) neurofeedback study. Methods N = 100 patients with Alcohol Use Disorder will be randomized to 5 parallel groups in a single-blind fashion and receive real-time functional magnetic resonance imaging neurofeedback while they are presented pictures of alcoholic beverages. The groups will either downregulate the ventral striatum, upregulate the right inferior frontal gyrus, negatively modulate the connectivity between these regions, upregulate, or downregulate the auditory cortex as a control region. After receiving 3 sessions of neurofeedback training within a maximum of 2 weeks, participants will be followed up monthly for a period of 3 months and relapse rates will be assessed as the primary outcome measure. Discussion The results of this study will provide insights into the efficacy of real-time functional magnetic resonance imaging neurofeedback training in the treatment of Alcohol Use Disorder as well as in the involved brain systems. This might help to identify predictors of successful neurofeedback treatment which could potentially be useful in developing personalized treatment approaches. Trial registration The study was retrospectively registered in the German Clinical Trials Register (trial identifier: DRKS00010253 ; WHO Universal Trial Number (UTN): U1111–1181-4218) on May 10th, 2016.

Published
2018

112. Addiction Research Consortium: Losing and regaining control over drug intake (ReCoDe)—From trajectories to mechanisms and interventions

Author

Heinz, Andreas, primary, Kiefer, Falk, additional, Smolka, Michael N., additional, Endrass, Tanja, additional, Beste, Christian, additional, Beck, Anne, additional, Liu, Shuyan, additional, Genauck, Alexander, additional, Romund, Lydia, additional, Banaschewski, Tobias, additional, Bermpohl, Felix, additional, Deserno, Lorenz, additional, Dolan, Raymond J., additional, Durstewitz, Daniel, additional, Ebner‐Priemer, Ulrich, additional, Flor, Herta, additional, Hansson, Anita C., additional, Heim, Christine, additional, Hermann, Derik, additional, Kiebel, Stefan, additional, Kirsch, Peter, additional, Kirschbaum, Clemens, additional, Koppe, Georgia, additional, Marxen, Michael, additional, Meyer‐Lindenberg, Andreas, additional, Nagel, Wolfgang E., additional, Noori, Hamid R., additional, Pilhatsch, Maximilian, additional, Priller, Josef, additional, Rietschel, Marcella, additional, Romanczuk‐Seiferth, Nina, additional, Schlagenhauf, Florian, additional, Sommer, Wolfgang H., additional, Stallkamp, Jan, additional, Ströhle, Andreas, additional, Stock, Ann‐Kathrin, additional, Winterer, Georg, additional, Winter, Christine, additional, Walter, Henrik, additional, Witt, Stephanie, additional, Vollstädt‐Klein, Sabine, additional, Rapp, Michael A., additional, Tost, Heike, additional, and Spanagel, Rainer, additional

Published
2019
Full Text
View/download PDF

114. Dysregulation of the histone demethylase KDM6B in alcohol dependence is associated with epigenetic regulation of inflammatory signaling pathways

Author

Johnstone, Andrea L., primary, Andrade, Nadja S., additional, Barbier, Estelle, additional, Khomtchouk, Bohdan B., additional, Rienas, Christopher A., additional, Lowe, Kenneth, additional, Van Booven, Derek J., additional, Domi, Esi, additional, Esanov, Rustam, additional, Vilca, Samara, additional, Tapocik, Jenica D., additional, Rodriguez, Keli, additional, Maryanski, Danielle, additional, Keogh, Michael Christopher, additional, Meinhardt, Marcus W., additional, Sommer, Wolfgang H., additional, Heilig, Markus, additional, Zeier, Zane, additional, and Wahlestedt, Claes, additional

Published
2019
Full Text
View/download PDF

115. Microstructural White Matter Alterations in Men With Alcohol Use Disorder and Rats With Excessive Alcohol Consumption During Early Abstinence

Author

De Santis, Silvia, primary, Bach, Patrick, additional, Pérez-Cervera, Laura, additional, Cosa-Linan, Alejandro, additional, Weil, Georg, additional, Vollstädt-Klein, Sabine, additional, Hermann, Derik, additional, Kiefer, Falk, additional, Kirsch, Peter, additional, Ciccocioppo, Roberto, additional, Sommer, Wolfgang H., additional, and Canals, Santiago, additional

Published
2019
Full Text
View/download PDF

117. Incubation of neural alcohol cue reactivity after withdrawal and its blockade by naltrexone

Author

Bach, Patrick, primary, Weil, Georg, additional, Pompili, Enrico, additional, Hoffmann, Sabine, additional, Hermann, Derik, additional, Vollstädt‐Klein, Sabine, additional, Mann, Karl, additional, Perez‐Ramirez, Ursula, additional, Moratal, David, additional, Canals, Santiago, additional, Dursun, Serdar M., additional, Greenshaw, Andrew J., additional, Kirsch, Peter, additional, Kiefer, Falk, additional, and Sommer, Wolfgang H., additional

Published
2019
Full Text
View/download PDF

120. Methylation of OPRL1 mediates the effect of psychosocial stress on binge drinking in adolescents

Author

Ruggeri, Barbara, Macare, Christine, Stopponi, Serena, Jia, Tianye, Carvalho, Fabiana M, Robert, Gabriel, Banaschewski, Tobias, Bokde, Arun L W, Bromberg, Uli, Büchel, Christian, Cattrell, Anna, Conrod, Patricia J, Desrivières, Sylvane, Flor, Herta, Frouin, Vincent, Gallinat, Jürgen, Garavan, Hugh, Gowland, Penny, Heinz, Andreas, Ittermann, Bernd, Martinot, Jean Luc, Martinot, Marie-Laure Paillère, Nees, Frauke, Papadopoulos-Orfanos, Dimitri, Paus, Tomáš, Poustka, Luise, Smolka, Michael N, Vetter, Nora C, Walter, Henrik, Whelan, Robert, Sommer, Wolfgang H, Bakalkin, Georgy, Ciccocioppo, Roberto, Schumann, Gunter, Ruggeri, Barbara, Macare, Christine, Stopponi, Serena, Jia, Tianye, Carvalho, Fabiana M, Robert, Gabriel, Banaschewski, Tobias, Bokde, Arun L W, Bromberg, Uli, Büchel, Christian, Cattrell, Anna, Conrod, Patricia J, Desrivières, Sylvane, Flor, Herta, Frouin, Vincent, Gallinat, Jürgen, Garavan, Hugh, Gowland, Penny, Heinz, Andreas, Ittermann, Bernd, Martinot, Jean Luc, Martinot, Marie-Laure Paillère, Nees, Frauke, Papadopoulos-Orfanos, Dimitri, Paus, Tomáš, Poustka, Luise, Smolka, Michael N, Vetter, Nora C, Walter, Henrik, Whelan, Robert, Sommer, Wolfgang H, Bakalkin, Georgy, Ciccocioppo, Roberto, and Schumann, Gunter

Abstract

BACKGROUND: Nociceptin is a key regulator linking environmental stress and alcohol drinking. In a genome-wide methylation analysis, we recently identified an association of a methylated region in the OPRL1 gene with alcohol-use disorders. METHODS: Here, we investigate the biological basis of this observation by analysing psychosocial stressors, methylation of the OPRL1 gene, brain response during reward anticipation and alcohol drinking in 660 fourteen-year-old adolescents of the IMAGEN study. We validate our findings in marchigian sardinian (msP) alcohol-preferring rats that are genetically selected for increased alcohol drinking and stress sensitivity. RESULTS: We found that low methylation levels in intron 1 of OPRL1 are associated with higher psychosocial stress and higher frequency of binge drinking, an effect mediated by OPRL1 methylation. In individuals with low methylation of OPRL1, frequency of binge drinking is associated with stronger BOLD response in the ventral striatum during reward anticipation. In msP rats, we found that stress results in increased alcohol intake and decreased methylation of OPRL1 in the nucleus accumbens. CONCLUSIONS: Our findings describe an epigenetic mechanism that helps to explain how psychosocial stress influences risky alcohol consumption and reward processing, thus contributing to the elucidation of biological mechanisms underlying risk for substance abuse.

Published
2018
Full Text
View/download PDF

121. Oxytocin Reduces Alcohol Cue-Reactivity in Alcohol-Dependent Rats and Humans

Author

Hansson, Anita C., Koopmann, Anne, Uhrig, Stefanie, Buhler, Sina, Domi, Esi, Kiessling, Eva, Ciccocioppo, Roberto, Froemke, Robert C., Grinevich, Valery, Kiefer, Falk, Sommer, Wolfgang H., Vollstaedt-Klein, Sabine, Spanagel, Rainer, Hansson, Anita C., Koopmann, Anne, Uhrig, Stefanie, Buhler, Sina, Domi, Esi, Kiessling, Eva, Ciccocioppo, Roberto, Froemke, Robert C., Grinevich, Valery, Kiefer, Falk, Sommer, Wolfgang H., Vollstaedt-Klein, Sabine, and Spanagel, Rainer

Abstract

Approved pharmacological treatments for alcohol use disorder are limited in their effectiveness, and new drugs that can easily be translated into the clinic are warranted. One of those candidates is oxytocin because of its interaction with several alcohol-induced effects. Alcoholdependent rats as well as post-mortem brains of human alcoholics and controls were analyzed for the expression of the oxytocin system by qRT-PCR, in situ hybridizaton, receptor autoradiography ([(125)l]OVTA binding), and immunohistochemistry. Alcohol self administration and cue-induced reinstatement behavior was measured after intracerebroventicular injection of 10 nM oxytocin in dependent rats. Here we show a pronounced upregulation of oxytocin receptors in brain tissues of alcohol dependent rats and deceased alcoholics, primarily in frontal and striatal areas. This upregulation stems most likely from reduced oxytocin expression in hypothalamic nuclei. Pharmacological validaton showed that oxytocin reduced cue-induced reinstatement response in dependent rats-an effect that was not observed in nondependent rats. Finally, a clinical pilot study (German clinical trial number DRKS00009253) using functional magnetic resonance imaging in heavy social male drinkers showed that intranasal oxytocin (24 IU) decreased neural cue-reactivity in brain networks similar to those detected in dependent rats and humans with increased oxytocin receptor expression. These studies suggest that oxytocin might be used as an anticraving medication and thus may positvely affect treatment outcomes in alcoholics., Funding Agencies|Bundesministerium fur Bildung und Forschung [FKZ: 01ZX1311A, 01 EE 1406 C]; Deutsche Forschungsgemeinschaft [SFB1134, DFG HA6102/1-1]; European Unions Horizon research and innovation program [668863]

Published
2018
Full Text
View/download PDF

122. Multi-modal imaging biomarkers

Author

Cosa, Alejandro, Moreno, Andrea, Pacheco Torres, Jesús, Ciccocioppo, Roberto, Hyytiä, Petri, Sommer, Wolfgang H, Moratal, David, Canals, Santiago, Ministerio de Economía y Competitividad (España), European Commission, and Ministerio de Ciencia e Innovación (España)

Subjects
Classification algorithms, Alcohol Drinking, Ethanol, Narcotic Antagonists, Brain, Central Nervous System Depressants, Magnetic Resonance Imaging, Naltrexone, Rats, Multi-modal MRI, TECNOLOGIA ELECTRONICA, Alcoholism, Disease Models, Animal, Alcohol use disorders, Machine learning, Animals, Rat, Longitudinal Studies
Abstract

Robust neuroimaging markers of neuropsychiatric disorders have proven difficult to obtain. In alcohol use disorders, profound brain structural deficits can be found in severe alcoholic patients, but the heterogeneity of unimodal MRI measurements has so far precluded the identification of selective biomarkers, especially for early diagnosis. In the present work we used a combination of multiple MRI modalities to provide comprehensive and insightful descriptions of brain tissue microstructure. We performed a longitudinal experiment using Marchigian–Sardinian (msP) rats, an established model of chronic excessive alcohol consumption, and acquired multi-modal images before and after 1 month of alcohol consumption (6.8 ± 1.4 g/kg/day, mean ± SD), as well as after 1 week of abstinence with or without concomitant treatment with the antirelapse opioid antagonist naltrexone (2.5 mg/kg/day). We found remarkable sensitivity and selectivity to accurately classify brains affected by alcohol even after the relative short exposure period. One month drinking was enough to imprint a highly specific signature of alcohol consumption. Brain alterations were regionally specific and affected both gray and white matter and persisted into the early abstinence state without any detectable recovery. Interestingly, naltrexone treatment during early abstinence resulted in subtle brain changes that could be distinguished from non-treated abstinent brains, suggesting the existence of an intermediate state associated with brain recovery from alcohol exposure induced by medication. The presented framework is a promising tool for the development of biomarkers for clinical diagnosis of alcohol use disorders, with capacity to further inform about its progression and response to treatment., Supported by grants from the Spanish MINECO to S.C. (BFU2015-64380-C2-1-R and PIM2010ERN-00679 as part of the Era-Net NEURON TRANSALC) and from the EU Horizon 2020 Program 668863-SyBil-AA grant, and to D.M. including FEDER funds under grant TEC2012-33778 and BFU2015-64380-C2-2-R. A.M. holds a studentship from the University of Edinburgh. The Instituto de Neurociencias is ‘Centre of Excellence Severo Ochoa’.

Published
2017
Full Text
View/download PDF

123. Aberrant insular cortex connectivity in abstinent alcohol-dependent rats is reversed by dopamine D3 receptor blockade.

Author

Scuppa, Giulia, Tambalo, Stefano, Pfarr, Simone, Sommer, Wolfgang H., and Bifone, Angelo

Subjects
INSULAR cortex, DOPAMINE receptors, ALCOHOLISM, INDEPENDENT component analysis, NEURAL circuitry, RESEARCH, LIMBIC system, NEURAL pathways, BASAL ganglia, ANIMAL experimentation, RESEARCH methodology, CELL receptors, FUNCTIONAL connectivity, ISOQUINOLINE, ORGANIC compounds, MAGNETIC resonance imaging, MEDICAL cooperation, EVALUATION research, RATS, COMPARATIVE studies, REWARD (Psychology), RESEARCH funding, DRINKING behavior, NEUROLOGIC examination, CEREBRAL cortex, DOPAMINE antagonists, PHARMACODYNAMICS
Abstract

A few studies have reported aberrant functional connectivity in alcoholic patients, but the specific neural circuits involved remain unknown. Moreover, it is unclear whether these alterations can be reversed upon treatment. Here, we used functional MRI to study resting state connectivity in rats following chronic intermittent exposure to ethanol. Further, we evaluated the effects of SB-277011-a, a selective dopamine D3 receptor antagonist, known to decrease ethanol consumption. Alcohol-dependent and control rats (N = 13/14 per group), 3 weeks into abstinence, were administered SB-277011-a or vehicle before fMRI sessions. Resting state connectivity networks were extracted by independent component analysis. A dual-regression analysis was performed using independent component maps as spatial regressors, and the effects of alcohol history and treatment on connectivity were assessed. A history of alcohol dependence caused widespread reduction of the internal coherence of components. Weaker correlation was also found between the insula cortex (IC) and cingulate cortices, key constituents of the salience network. Similarly, reduced connectivity was observed between a component comprising the anterior insular cortex, together with the caudate putamen (CPu-AntIns), and the posterior part of the IC. On the other hand, postdependent rats showed strengthened connectivity between salience and reward networks. In particular, higher connectivity was observed between insula and nucleus accumbens, between the ventral tegmental area and the cingulate cortex and between the VTA and CPu-AntIns. Interestingly, aberrant connectivity in postdependent rats was partially restored by acute administration of SB-277011-a, which, conversely, had no significant effects in naïve rats. [ABSTRACT FROM AUTHOR]

Published
2020
Full Text
View/download PDF

124. Efficacy and safety of sodium oxybate in alcohol-dependent patients with a very high drinking risk level

Author

van den Brink, Wim, primary, Addolorato, Giovanni, additional, Aubin, Henri-Jean, additional, Benyamina, Amine, additional, Caputo, Fabio, additional, Dematteis, Maurice, additional, Gual, Antoni, additional, Lesch, Otto-Michael, additional, Mann, Karl, additional, Maremmani, Icro, additional, Nutt, David, additional, Paille, François, additional, Perney, Pascal, additional, Rehm, Jürgen, additional, Reynaud, Michel, additional, Simon, Nicolas, additional, Söderpalm, Bo, additional, Sommer, Wolfgang H., additional, Walter, Henriette, additional, and Spanagel, Rainer, additional

Published
2018
Full Text
View/download PDF

125. Choice for Drug or Natural Reward Engages Largely Overlapping Neuronal Ensembles in the Infralimbic Prefrontal Cortex

Author

Pfarr, Simone, primary, Schaaf, Laura, additional, Reinert, Janine K., additional, Paul, Elisabeth, additional, Herrmannsdörfer, Frank, additional, Roßmanith, Martin, additional, Kuner, Thomas, additional, Hansson, Anita C., additional, Spanagel, Rainer, additional, Körber, Christoph, additional, and Sommer, Wolfgang H., additional

Published
2018
Full Text
View/download PDF

127. Multi-modal MRI classifiers identify excessive alcohol consumption and treatment effects in the brain

Author

Universitat Politècnica de València. Departamento de Ingeniería Electrónica - Departament d'Enginyeria Electrònica, Ministerio de Ciencia e Innovación, European Commission, Ministerio de Economía y Competitividad, University of Edinburgh, Cosa, Alejandro, Moreno, Andrea, Pacheco-Torres, Jesús, Ciccocioppo, Roberto, Hyytiä, Petri, Sommer, Wolfgang H., Moratal, David, Canals, Santiago, Universitat Politècnica de València. Departamento de Ingeniería Electrónica - Departament d'Enginyeria Electrònica, Ministerio de Ciencia e Innovación, European Commission, Ministerio de Economía y Competitividad, University of Edinburgh, Cosa, Alejandro, Moreno, Andrea, Pacheco-Torres, Jesús, Ciccocioppo, Roberto, Hyytiä, Petri, Sommer, Wolfgang H., Moratal, David, and Canals, Santiago

Abstract

[EN] Robust neuroimaging markers of neuropsychiatric disorders have proven difficult to obtain. In alcohol use disorders, profound brain structural deficits can be found in severe alcoholic patients, but the heterogeneity of unimodal MRI measurements has so far precluded the identification of selective biomarkers, especially for early diagnosis. In the present work we used a combination of multiple MRI modalities to provide comprehensive and insightful descriptions of brain tissue microstructure. We performed a longitudinal experiment using Marchigian¿Sardinian (msP) rats, an established model of chronic excessive alcohol consumption, and acquired multi¿modal images before and after 1¿month of alcohol consumption (6.8¿±¿1.4¿g/kg/day, mean¿±¿SD), as well as after 1¿week of abstinence with or without concomitant treatment with the antirelapse opioid antagonist naltrexone (2.5¿mg/kg/day). We found remarkable sensitivity and selectivity to accurately classify brains affected by alcohol even after the relative short exposure period. One month drinking was enough to imprint a highly specific signature of alcohol consumption. Brain alterations were regionally specific and affected both gray and white matter and persisted into the early abstinence state without any detectable recovery. Interestingly, naltrexone treatment during early abstinence resulted in subtle brain changes that could be distinguished from non¿treated abstinent brains, suggesting the existence of an intermediate state associated with brain recovery from alcohol exposure induced by medication. The presented framework is a promising tool for the development of biomarkers for clinical diagnosis of alcohol use disorders, with capacity to further inform about its progression and response to treatment.

Published
2017

128. Genetic Contribution to Alcohol Dependence: Investigation of a Heterogeneous German Sample of Individuals with Alcohol Dependence, Chronic Alcoholic Pancreatitis, and Alcohol-Related Cirrhosis

Author

Treutlein, Jens, Frank, Josef, Streit, Fabian, Reinbold, Celine S., Juraeva, Dilafruz, Degenhardt, Franziska, Rietschel, Liz, Witt, Stephanie H., Forstner, Andreas J., Ridinger, Monika, Strohmaier, Jana, Wodarz, Norbert, Dukal, Helene, Foo, Jerome C., Hoffmann, Per, Herms, Stefan, Heilmann-Heimbach, Stefanie, Soyka, Michael, Maier, Wolfgang, Gaebel, Wolfgang, Dahmen, Norbert, Scherbaum, Norbert, Mueller-Myhsok, Bertram, Lucae, Susanne, Ising, Marcus, Stickel, Felix, Berg, Thomas, Roggenbuck, Ulla, Joeckel, Karl-Heinz, Scholz, Henrike, Zimmermann, Ulrich S., Buch, Stephan, Sommer, Wolfgang H., Spanagel, Rainer, Brors, Benedikt, Cichon, Sven, Mann, Karl, Kiefer, Falk, Hampe, Jochen, Rosendahl, Jonas, Noethen, Markus M., Rietschel, Marcella, Treutlein, Jens, Frank, Josef, Streit, Fabian, Reinbold, Celine S., Juraeva, Dilafruz, Degenhardt, Franziska, Rietschel, Liz, Witt, Stephanie H., Forstner, Andreas J., Ridinger, Monika, Strohmaier, Jana, Wodarz, Norbert, Dukal, Helene, Foo, Jerome C., Hoffmann, Per, Herms, Stefan, Heilmann-Heimbach, Stefanie, Soyka, Michael, Maier, Wolfgang, Gaebel, Wolfgang, Dahmen, Norbert, Scherbaum, Norbert, Mueller-Myhsok, Bertram, Lucae, Susanne, Ising, Marcus, Stickel, Felix, Berg, Thomas, Roggenbuck, Ulla, Joeckel, Karl-Heinz, Scholz, Henrike, Zimmermann, Ulrich S., Buch, Stephan, Sommer, Wolfgang H., Spanagel, Rainer, Brors, Benedikt, Cichon, Sven, Mann, Karl, Kiefer, Falk, Hampe, Jochen, Rosendahl, Jonas, Noethen, Markus M., and Rietschel, Marcella

Abstract

The present study investigated the genetic contribution to alcohol dependence (AD) using genome-wide association data from three German samples. These comprised patients with: (i) AD; (ii) chronic alcoholic pancreatitis (ACP); and (iii) alcohol-related liver cirrhosis (ALC). Single marker, gene-based, and pathway analyses were conducted. A significant association was detected for the ADH1B locus in a gene-based approach (p(uncorrected) = 1.2 x 10(-6); p(corrected) = 0.020). This was driven by the AD subsample. No association with ADH1B was found in the combined ACP + ALC sample. On first inspection, this seems surprising, since ADH1B is a robustly replicated risk gene for AD and may therefore be expected to be associated also with subgroups of AD patients. The negative finding in the ACP + ALC sample, however, may reflect genetic stratification as well as random fluctuation of allele frequencies in the cases and controls, demonstrating the importance of large samples in which the phenotype is well assessed.

Published
2017

129. Multi-modal MRI classifiers identify excessive alcohol consumption and treatment effects in the brain

Author

Ministerio de Economía y Competitividad (España), European Commission, Ministerio de Ciencia e Innovación (España), Cosa-Linan, Alejandro, Moreno, Andrea, Pacheco-Torres, Jesús, Ciccocioppo, Roberto, Hyytiä, Petri, Sommer, Wolfgang H., Moratal, David, Canals, Santiago, Ministerio de Economía y Competitividad (España), European Commission, Ministerio de Ciencia e Innovación (España), Cosa-Linan, Alejandro, Moreno, Andrea, Pacheco-Torres, Jesús, Ciccocioppo, Roberto, Hyytiä, Petri, Sommer, Wolfgang H., Moratal, David, and Canals, Santiago

Abstract

Robust neuroimaging markers of neuropsychiatric disorders have proven difficult to obtain. In alcohol use disorders, profound brain structural deficits can be found in severe alcoholic patients, but the heterogeneity of unimodal MRI measurements has so far precluded the identification of selective biomarkers, especially for early diagnosis. In the present work we used a combination of multiple MRI modalities to provide comprehensive and insightful descriptions of brain tissue microstructure. We performed a longitudinal experiment using Marchigian–Sardinian (msP) rats, an established model of chronic excessive alcohol consumption, and acquired multi-modal images before and after 1 month of alcohol consumption (6.8 ± 1.4 g/kg/day, mean ± SD), as well as after 1 week of abstinence with or without concomitant treatment with the antirelapse opioid antagonist naltrexone (2.5 mg/kg/day). We found remarkable sensitivity and selectivity to accurately classify brains affected by alcohol even after the relative short exposure period. One month drinking was enough to imprint a highly specific signature of alcohol consumption. Brain alterations were regionally specific and affected both gray and white matter and persisted into the early abstinence state without any detectable recovery. Interestingly, naltrexone treatment during early abstinence resulted in subtle brain changes that could be distinguished from non-treated abstinent brains, suggesting the existence of an intermediate state associated with brain recovery from alcohol exposure induced by medication. The presented framework is a promising tool for the development of biomarkers for clinical diagnosis of alcohol use disorders, with capacity to further inform about its progression and response to treatment.

Published
2017

131. Oxytocin Reduces Alcohol Cue-Reactivity in Alcohol-Dependent Rats and Humans

Author

Hansson, Anita C, primary, Koopmann, Anne, additional, Uhrig, Stefanie, additional, Bühler, Sina, additional, Domi, Esi, additional, Kiessling, Eva, additional, Ciccocioppo, Roberto, additional, Froemke, Robert C, additional, Grinevich, Valery, additional, Kiefer, Falk, additional, Sommer, Wolfgang H, additional, Vollstädt-Klein, Sabine, additional, and Spanagel, Rainer, additional

Published
2017
Full Text
View/download PDF

134. mRNA GPR162 changes are associated with decreased food intake in rat, and its human genetic variants with impairments in glucose homeostasis in two Swedish cohorts

Author

Caruso, Vanni, Sreedharan, Smitha, Carlini, Valeria P., Jacobsson, Josefin A., Haitina, Tatjana, Hammer, Joanna, Stephansson, Olga, Crona, Filip, Sommer, Wolfgang H., Risérus, Ulf, Lannfelt, Lars, Marcus, Claude, Heilig, Markus, de Barioglio, Susana R., Fredriksson, Robert, Schiöth, Helgi B., Caruso, Vanni, Sreedharan, Smitha, Carlini, Valeria P., Jacobsson, Josefin A., Haitina, Tatjana, Hammer, Joanna, Stephansson, Olga, Crona, Filip, Sommer, Wolfgang H., Risérus, Ulf, Lannfelt, Lars, Marcus, Claude, Heilig, Markus, de Barioglio, Susana R., Fredriksson, Robert, and Schiöth, Helgi B.

Abstract

G protein-coupled receptors (GPCRs) are a class of integral membrane proteins mediating intercellular interactions of fundamental physiological importance for survival including regulation of food intake, blood pressure, and hormonal sensing signaling, among other roles. Homeostatic alterations in the physiological status of GPCRs are often associated with underlying causes of disease, and to date, several orphan GPCRs are still uncharacterized. Findings from our previous study demonstrate that the Rhodopsin family protein GPR162 is widely expressed in GABAergic as well as other neurons within the mouse hippocampus, whereas extensive expression is observed in hypothalamus, amygdala, and ventral tegmental area, regions strictly interconnected and involved in the regulation of energy homeostasis and hedonic feeding. In this study, we provide a further anatomical characterization of GPR162 in mouse brain via in situ hybridization as well as detailed mRNA expression in a panel of rat tissues complementing a specie-specific mapping of the receptor. We also provide an attempt to demonstrate a functional implication of GPR162 in food intake-related behavior via antisense knockdown studies. Furthermore, we performed human genetic studies in which for the first time, variants of the GPR162 gene were associated with impairments in glucose homeostasis.

Published
2016
Full Text
View/download PDF

135. Differential Roles for L-Type Calcium Channel Subtypes in Alcohol Dependence

Author

Uhrig, Stefanie, primary, Vandael, David, additional, Marcantoni, Andrea, additional, Dedic, Nina, additional, Bilbao, Ainhoa, additional, Vogt, Miriam A, additional, Hirth, Natalie, additional, Broccoli, Laura, additional, Bernardi, Rick E, additional, Schönig, Kai, additional, Gass, Peter, additional, Bartsch, Dusan, additional, Spanagel, Rainer, additional, Deussing, Jan M, additional, Sommer, Wolfgang H, additional, Carbone, Emilio, additional, and Hansson, Anita C, additional

Published
2016
Full Text
View/download PDF

136. Low μ-Opioid Receptor Status in Alcohol Dependence Identified by Combined Positron Emission Tomography and Post-Mortem Brain Analysis

Author

Hermann, Derik, primary, Hirth, Natalie, additional, Reimold, Matthias, additional, Batra, Anil, additional, Smolka, Michael N, additional, Hoffmann, Sabine, additional, Kiefer, Falk, additional, Noori, Hamid R, additional, Sommer, Wolfgang H, additional, Reischl, Gerald, additional, la Fougère, Christian, additional, Mann, Karl, additional, Spanagel, Rainer, additional, and Hansson, Anita C, additional

Published
2016
Full Text
View/download PDF

138. mRNA GPR162 changes are associated with decreased food intake in rat, and its human genetic variants with impairments in glucose homeostasis in two Swedish cohorts

Author

Caruso, Vanni, primary, Sreedharan, Smitha, additional, Carlini, Valeria P., additional, Jacobsson, Josefin A., additional, Haitina, Tatjana, additional, Hammer, Joanna, additional, Stephansson, Olga, additional, Crona, Filip, additional, Sommer, Wolfgang H., additional, Risérus, Ulf, additional, Lannfelt, Lars, additional, Marcus, Claude, additional, Heilig, Markus, additional, de Barioglio, Susana R., additional, Fredriksson, Robert, additional, and Schiöth, Helgi B., additional

Published
2016
Full Text
View/download PDF

139. Association of Protein Phosphatase PPM1G With Alcohol Use Disorder and Brain Activity During Behavioral Control in a Genome-Wide Methylation Analysis

Author

Ruggeri, Barbara, Nymberg, Charlotte, Vuoksimaa, Eero, Lourdusamy, Anbarasu, Wong, Cybele P., Carvalho, Fabiana M., Jia, Tianye, Cattrell, Anna, Macare, Christine, Banaschewski, Tobias, Barker, Gareth J., Bokde, Arun L. W., Bromberg, Uli, Buechel, Christian, Conrad, Patricia J., Fauth-Buehler, Mira, Flor, Herta, Frouin, Vincent, Gallinat, Juergen, Garavan, Hugh, Gowland, Penny, Heinz, Andreas, Ittermann, Bernd, Martinot, Jean-Luc, Nees, Frauke, Pausova, Zdenka, Paus, Tomas, Rietschel, Marcella, Robbins, Trevor, Smolka, Michael N., Spanagel, Rainer, Bakalkin, Georgy, Mill, Jonathan, Sommer, Wolfgang H., Rose, Richard J., Yan, Jia, Aliey, Fazil, Dick, Danielle, Kaprio, Jaakko, Desrivieres, Sylvane, Schumann, Gunter, Ruggeri, Barbara, Nymberg, Charlotte, Vuoksimaa, Eero, Lourdusamy, Anbarasu, Wong, Cybele P., Carvalho, Fabiana M., Jia, Tianye, Cattrell, Anna, Macare, Christine, Banaschewski, Tobias, Barker, Gareth J., Bokde, Arun L. W., Bromberg, Uli, Buechel, Christian, Conrad, Patricia J., Fauth-Buehler, Mira, Flor, Herta, Frouin, Vincent, Gallinat, Juergen, Garavan, Hugh, Gowland, Penny, Heinz, Andreas, Ittermann, Bernd, Martinot, Jean-Luc, Nees, Frauke, Pausova, Zdenka, Paus, Tomas, Rietschel, Marcella, Robbins, Trevor, Smolka, Michael N., Spanagel, Rainer, Bakalkin, Georgy, Mill, Jonathan, Sommer, Wolfgang H., Rose, Richard J., Yan, Jia, Aliey, Fazil, Dick, Danielle, Kaprio, Jaakko, Desrivieres, Sylvane, and Schumann, Gunter

Abstract

Objective: The genetic component of alcohol use disorder is substantial, but monozygotic twin discordance indicates a role for nonheritable differences that could be mediated by epigenetics. Despite growing evidence associating epigenetics and psychiatric disorders, it is unclear how epigenetics, particularly DNA methylation, relate to brain function and behavior, including drinking behavior. Method: The authors carried out a genome-wide analysis of DNA methylation of 18 monozygotic twin pairs discordant for alcohol use disorder and validated differentially methylated regions. After validation, the authors characterized these differentially methylated regions using personality trait assessment and functional MRI in a sample of 499 adolescents. Results: Hypermethylation in the 3'-protein-phosphatase-1G (PPM1G) gene locus was associated with alcohol use disorder. The authors found association of PPM1G hypermethylation with early escalation of alcohol use and increased impulsiveness. They also observed association of PPM1G hypermethylation with increased blood-oxygen-level-dependent response in the right subthalamic nucleus during an impulsiveness task. Conclusions: Overall, the authors provide first evidence for an epigenetic marker associated with alcohol consumption and its underlying neurobehavioral phenotype.

Published
2015
Full Text
View/download PDF

140. XRCC5 as a Risk Gene for Alcohol Dependence: Evidence from a Genome-Wide Gene-Set-Based Analysis and Follow-up Studies in Drosophila and Humans

Author

Juraeva, Dilafruz, Treutlein, Jens, Scholz, Henrike, Frank, Josef, Degenhardt, Franziska, Cichon, Sven, Ridinger, Monika, Mattheisen, Manuel, Witt, Stephanie H., Lang, Maren, Sommer, Wolfgang H., Hoffmann, Per, Herms, Stefan, Wodarz, Norbert, Soyka, Michael, Zill, Peter, Maier, Wolfgang, Juenger, Elisabeth, Gaebel, Wolfgang, Dahmen, Norbert, Scherbaum, Norbert, Schmael, Christine, Steffens, Michael, Lucae, Susanne, Ising, Marcus, Smolka, Michael N., Zimmermann, Ulrich S., Mueller-Myhsok, Bertram, Noethen, Markus M., Mann, Karl, Kiefer, Falk, Spanagel, Rainer, Brors, Benedikt, Rietschel, Marcella, Juraeva, Dilafruz, Treutlein, Jens, Scholz, Henrike, Frank, Josef, Degenhardt, Franziska, Cichon, Sven, Ridinger, Monika, Mattheisen, Manuel, Witt, Stephanie H., Lang, Maren, Sommer, Wolfgang H., Hoffmann, Per, Herms, Stefan, Wodarz, Norbert, Soyka, Michael, Zill, Peter, Maier, Wolfgang, Juenger, Elisabeth, Gaebel, Wolfgang, Dahmen, Norbert, Scherbaum, Norbert, Schmael, Christine, Steffens, Michael, Lucae, Susanne, Ising, Marcus, Smolka, Michael N., Zimmermann, Ulrich S., Mueller-Myhsok, Bertram, Noethen, Markus M., Mann, Karl, Kiefer, Falk, Spanagel, Rainer, Brors, Benedikt, and Rietschel, Marcella

Abstract

Genetic factors have as large role as environmental factors in the etiology of alcohol dependence (AD). Although genome-wide association studies (GWAS) enable systematic searches for loci not hitherto implicated in the etiology of AD, many true findings may be missed owing to correction for multiple testing. The aim of the present study was to circumvent this limitation by searching for biological system-level differences, and then following up these findings in humans and animals. Gene-set-based analysis of GWAS data from 1333 cases and 2168 controls identified 19 significantly associated gene-sets, of which 5 could be replicated in an independent sample. Clustered in these gene-sets were novel and previously identified susceptibility genes. The most frequently present gene, ie in 6 out of 19 gene-sets, was X-ray repair complementing defective repair in Chinese hamster cells 5 (XRCC5). Previous human and animal studies have implicated XRCC5 in alcohol sensitivity. This phenotype is inversely correlated with the development of AD, presumably as more alcohol is required to achieve the desired effects. In the present study, the functional role of XRCC5 in AD was further validated in animals and humans. Drosophila mutants with reduced function of Ku80-the homolog of mammalian XRCC5-due to RNAi silencing showed reduced sensitivity to ethanol. In humans with free access to intravenous ethanol self-administration in the laboratory, the maximum achieved blood alcohol concentration was influenced in an allele-dose-dependent manner by genetic variation in XRCC5. In conclusion, our convergent approach identified new candidates and generated independent evidence for the involvement of XRCC5 in alcohol dependence.

Published
2015

141. Brain activation induced by voluntary alcohol and saccharin drinking in rats assessed with manganese-enhanced magnetic resonance imaging

Author

Academy of Finland, European Commission, Federal Ministry of Education and Research (Germany), Ministerio de Ciencia e Innovación (España), Dudek, Mateusz, Abo-Ramadan, Usama, Hermann, Derik, Brown, Matthew, Canals, Santiago, Sommer, Wolfgang H., Hyytiä, Petri, Academy of Finland, European Commission, Federal Ministry of Education and Research (Germany), Ministerio de Ciencia e Innovación (España), Dudek, Mateusz, Abo-Ramadan, Usama, Hermann, Derik, Brown, Matthew, Canals, Santiago, Sommer, Wolfgang H., and Hyytiä, Petri

Abstract

The neuroanatomical and neurochemical basis of alcohol reward has been studied extensively, but global alterations of neural activity in reward circuits during chronic alcohol use remain poorly described. Here, we measured brain activity changes produced by long-term voluntary alcohol drinking in the alcohol-preferring AA (Alko alcohol) rats using manganese-enhanced magnetic resonance imaging (MEMRI). MEMRI is based on the ability of paramagnetic manganese ions to accumulate in excitable neurons and thereby enhance the T1-weighted signal in activated brain areas. Following 6 weeks of voluntary alcohol drinking, AA rats were allowed to drink alcohol for an additional week, during which they were administered manganese chloride (MnCl2 ) with subcutaneous osmotic minipumps before MEMRI. A second group with an identical alcohol drinking history received MnCl2 during the abstinence week following alcohol drinking. For comparing alcohol with a natural reinforcer, MEMRI was also performed in saccharin-drinking rats. A water-drinking group receiving MnCl2 served as a control. We found that alcohol drinking increased brain activity extensively in cortical and subcortical areas, including the mesocorticolimbic and nigrostriatal dopamine pathways and their afferents. Remarkably similar activation maps were seen after saccharin ingestion. Particularly in the prelimbic cortex, ventral hippocampus and subthalamic nucleus, activation persisted into early abstinence. These data show that voluntary alcohol recruits an extensive network that includes the ascending dopamine systems and their afferent connections, and that this network is largely shared with saccharin reward. The regions displaying persistent alterations after alcohol drinking could participate in brain networks underlying alcohol seeking and relapse.

Published
2015

142. Dynorphin and κ-Opioid Receptor Dysregulation in the Dopaminergic Reward System of Human Alcoholics.

Author

Bazov, Igor, Sarkisyan, Daniil, Kononenko, Olga, Watanabe, Hiroyuki, Yakovleva, Tatiana, Hansson, Anita C., Sommer, Wolfgang H., Spanagel, Rainer, and Bakalkin, Georgy

Abstract

Molecular changes induced by excessive alcohol consumption may underlie formation of dysphoric state during acute and protracted alcohol withdrawal which leads to craving and relapse. A main molecular addiction hypothesis is that the upregulation of the dynorphin (DYN)/κ-opioid receptor (KOR) system in the nucleus accumbens (NAc) of alcohol-dependent individuals causes the imbalance in activity of D1- and D2 dopamine receptor (DR) expressing neural circuits that results in dysphoria. We here analyzed post-mortem NAc samples of human alcoholics to assess changes in prodynorphin (PDYN) and KOR (OPRK1) gene expression and co-expression (transcriptionally coordinated) patterns. To address alterations in D1- and D2-receptor circuits, we studied the regulatory interactions between these pathways and the DYN/KOR system. No significant differences in PDYN and OPRK1 gene expression levels between alcoholics and controls were evident. However, PDYN and OPRK1 showed transcriptionally coordinated pattern that was significantly different between alcoholics and controls. A downregulation of DRD1 but not DRD2 expression was seen in alcoholics. Expression of DRD1 and DRD2 strongly correlated with that of PDYN and OPRK1 suggesting high levels of transcriptional coordination between these gene clusters. The differences in expression and co-expression patterns were not due to the decline in neuronal proportion in alcoholic brain and thereby represent transcriptional phenomena. Dysregulation of DYN/KOR system and dopamine signaling through both alterations in co-expression patterns of opioid genes and decreased DRD1 gene expression may contribute to imbalance in the activity of D1- and D2-containing pathways which may lead to the negative affective state in human alcoholics. [ABSTRACT FROM AUTHOR]

Published
2018
Full Text
View/download PDF

143. Speaker 3: Sabine Vollstädt-Klein, Germany

Author

Sabine, Vollstädt-Klein, Helmut, Nakovics, Martina, Kirsch, Sommer, Wolfgang H., Karl, Mann, and Falk, Kiefer

Subjects
Abstracts, Speaker Abstracts
Published
2016

145. A common functional allele of the Nogo receptor gene, reticulon 4 receptor (RTN4R), is associated with sporadic amyotrophic lateral sclerosis in a French population

Author

Amy, Maïté, primary, Staehlin, Oliver, additional, René, Frédérique, additional, Blasco, Hélène, additional, Marouillat, Sylviane, additional, Daoud, Hussein, additional, Vourc’h, Patrick, additional, Gordon, Paul H., additional, Camu, William, additional, Corcia, Philippe, additional, Loeffler, Jean-Philippe, additional, Palkovits, Miklós, additional, Sommer, Wolfgang H., additional, and Andres, Christian R., additional

Published
2015
Full Text
View/download PDF

148. Early rearing history influences oxytocin receptor epigenetic regulation in rhesus macaques.

Author

Baker, Maggie, Lindell, Stephen G., Driscoll, Carlos A., Zhifeng Zhou, Qiaoping Yuan, Schwandt, Melanie L., Miller-Crews, Isaac, Simpson, Elizabeth A., Paukner, Annika, Ferrari, Pier Francesco, Sindhu, Ravi Kumar, Razaqyar, Muslima, Sommer, Wolfgang H., Lopez, Juan F., Thompson, Robert C., Goldman, David, Heilig, Markus, Higley, J. Dee, Suomi, Stephen J., and Barr, Christina S.

Subjects
OXYTOCIN receptors, RHESUS monkeys, EPIGENETICS, MATERNAL deprivation in animals, SINGLE nucleotide polymorphisms, PARENTAL behavior in animals, PHYSIOLOGY, MAMMALS
Abstract

Adaptations to stress can occur through epigenetic processes and may be a conduit for informing offspring of environmental challenge. We employed ChIP-sequencing for H3K4me3 to examine effects of early maternal deprivation (peer-rearing, PR) in archived rhesus macaque hippocampal samples (male, n = 13). Focusing on genes with roles in stress response and behavior, we assessed the effects of rearing on H3K4me3 binding by ANOVA. We found decreased H3K4me3 binding at genes critical to behavioral stress response, the most robust being the oxytocin receptor gene OXTR, for which we observed a corresponding decrease in RNA expression. Based on this finding, we performed behavioral analyses to determine whether a gain-of-function nonsynonymous OXTR SNP interacted with early stress to influence relevant behavioral stress reactivity phenotypes (n = 194), revealing that this SNP partially rescued the PR phenotype. PR infants exhibited higher levels of separation anxiety and arousal in response to social separation, but infants carrying the alternative OXTR allele did not exhibit as great a separation response. These data indicate that the oxytocin system is involved in social-separation response and suggest that epigenetic down-modulation of OXTR could contribute to behavioral differences observed in PR animals. Epigenetic changes at OXTR may represent predictive adaptive responses that could impart readiness to respond to environmental challenge or maintain proximity to a caregiver but also contribute to behavioral pathology. Our data also demonstrate that OXTR polymorphism can permit animals to partially overcome the detrimental effects of early maternal deprivation, which could have translational implications for human psychiatric disorders. [ABSTRACT FROM AUTHOR]

Published
2017
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results