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2. European clinical guidelines for Tourette syndrome and other tic disorders—version 2.0. Part III: pharmacological treatment

Author

Roessner, Veit, Eichele, Heike, Stern, Jeremy S., Skov, Liselotte, Rizzo, Renata, Debes, Nanette Mol, Nagy, Péter, Cavanna, Andrea E., Termine, Cristiano, Ganos, Christos, Münchau, Alexander, Szejko, Natalia, Cath, Danielle, Müller-Vahl, Kirsten R., Verdellen, Cara, Hartmann, Andreas, Rothenberger, Aribert, Hoekstra, Pieter J., and Plessen, Kerstin J.

Published
2022
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3. Executive Control and Associated Brain Activity in Children With Familial High-Risk of Schizophrenia or Bipolar Disorder:A Danish Register-based Study

Author

Johnsen, Line Korsgaard, Larsen, Kit Melissa, Fuglsang, Søren Asp, van Themaat, Anna Hester Ver Loren, Baaré, William Frans Christiaan, Madsen, Kathrine Skak, Madsen, Kristoffer Hougaard, Hemager, Nicoline, Andreassen, Anna Krogh, Veddum, Lotte, Greve, Aja Neergaard, Nejad, Ayna Baladi, Burton, Birgitte Klee, Gregersen, Maja, Eichele, Heike, Lund, Torben E., Bliksted, Vibeke, Thorup, Anne Amalie Elgaard, Mors, Ole, Plessen, Kerstin Jessica, Nordentoft, Merete, Siebner, Hartwig Roman, Johnsen, Line Korsgaard, Larsen, Kit Melissa, Fuglsang, Søren Asp, van Themaat, Anna Hester Ver Loren, Baaré, William Frans Christiaan, Madsen, Kathrine Skak, Madsen, Kristoffer Hougaard, Hemager, Nicoline, Andreassen, Anna Krogh, Veddum, Lotte, Greve, Aja Neergaard, Nejad, Ayna Baladi, Burton, Birgitte Klee, Gregersen, Maja, Eichele, Heike, Lund, Torben E., Bliksted, Vibeke, Thorup, Anne Amalie Elgaard, Mors, Ole, Plessen, Kerstin Jessica, Nordentoft, Merete, and Siebner, Hartwig Roman

Abstract

Background and Hypotheses Impaired executive control is a potential prognostic and endophenotypic marker of schizophrenia (SZ) and bipolar disorder (BP). Assessing children with familial high-risk (FHR) of SZ or BP enables characterization of early risk markers and we hypothesize that they express impaired executive control as well as aberrant brain activation compared to population-based control (PBC) children. Study Design Using a flanker task, we examined executive control together with functional magnetic resonance imaging (fMRI) in 11- to 12-year-old children with FHR of SZ (FHR-SZ) or FHR of BP (FHR-BP) and PBC children as part of a register-based, prospective cohort-study; The Danish High Risk and Resilience study—VIA 11. Study Results We included 85 (44% female) FHR-SZ, 63 (52% female) FHR-BP and 98 (50% female) PBC in the analyses. Executive control effects, caused by the spatial visuomotor conflict, showed no differences between groups. Bayesian ANOVA of reaction time (RT) variability, quantified by the coefficient of variation (CVRT), revealed a group effect with similarly higher CVRT in FHR-BP and FHR-SZ compared to PBC (BF10 = 6.82). The fMRI analyses revealed no evidence for between-group differences in task-related brain activation. Post hoc analyses excluding children with psychiatric illness yielded same results. Conclusion FHR-SZ and FHR-BP at age 11–12 show intact ability to resolve a spatial visuomotor conflict and neural efficacy. The increased variability in RT may reflect difficulties in maintaining sustained attention. Since variability in RT was independent of existing psychiatric illness, it may reflect a potential endophenotypic marker of risk., BACKGROUND AND HYPOTHESES: Impaired executive control is a potential prognostic and endophenotypic marker of schizophrenia (SZ) and bipolar disorder (BP). Assessing children with familial high-risk (FHR) of SZ or BP enables characterization of early risk markers and we hypothesize that they express impaired executive control as well as aberrant brain activation compared to population-based control (PBC) children.STUDY DESIGN: Using a flanker task, we examined executive control together with functional magnetic resonance imaging (fMRI) in 11- to 12-year-old children with FHR of SZ (FHR-SZ) or FHR of BP (FHR-BP) and PBC children as part of a register-based, prospective cohort-study; The Danish High Risk and Resilience study-VIA 11.STUDY RESULTS: We included 85 (44% female) FHR-SZ, 63 (52% female) FHR-BP and 98 (50% female) PBC in the analyses. Executive control effects, caused by the spatial visuomotor conflict, showed no differences between groups. Bayesian ANOVA of reaction time (RT) variability, quantified by the coefficient of variation (CVRT), revealed a group effect with similarly higher CVRT in FHR-BP and FHR-SZ compared to PBC (BF10 = 6.82). The fMRI analyses revealed no evidence for between-group differences in task-related brain activation. Post hoc analyses excluding children with psychiatric illness yielded same results.CONCLUSION: FHR-SZ and FHR-BP at age 11-12 show intact ability to resolve a spatial visuomotor conflict and neural efficacy. The increased variability in RT may reflect difficulties in maintaining sustained attention. Since variability in RT was independent of existing psychiatric illness, it may reflect a potential endophenotypic marker of risk.

Published
2024

5. Sustained Attention and Interference Control Among 7-Year-Old Children With a Familial High Risk of Schizophrenia or Bipolar Disorder—A Nationwide Observational Cohort Study

Author

Burton, Birgitte Klee, Vangkilde, Signe, Petersen, Anders, Skovgaard, Lene Theil, Jepsen, Jens Richardt, Hemager, Nicoline, Christiani, Camilla Jerlang, Spang, Katrine Soeborg, Ellersgaard, Ditte, Greve, Aja, Gantriis, Ditte, Eichele, Heike, Mors, Ole, Nordentoft, Merete, Thorup, Anne Amalie Elgaard, and Plessen, Kerstin Jessica

Published
2018
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6. Executive Control and Associated Brain Activity in Children With Familial High-Risk of Schizophrenia or Bipolar Disorder: A Danish Register-based Study

Author

Johnsen, Line Korsgaard, primary, Larsen, Kit Melissa, additional, Fuglsang, Søren Asp, additional, Ver Loren van Themaat, Anna Hester, additional, Baaré, William Frans Christiaan, additional, Madsen, Kathrine Skak, additional, Madsen, Kristoffer Hougaard, additional, Hemager, Nicoline, additional, Andreassen, Anna Krogh, additional, Veddum, Lotte, additional, Greve, Aja Neergaard, additional, Nejad, Ayna Baladi, additional, Burton, Birgitte Klee, additional, Gregersen, Maja, additional, Eichele, Heike, additional, Lund, Torben E, additional, Bliksted, Vibeke, additional, Thorup, Anne Amalie Elgaard, additional, Mors, Ole, additional, Plessen, Kerstin Jessica, additional, Nordentoft, Merete, additional, and Siebner, Hartwig Roman, additional

Published
2023
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7. Executive Control and Associated Brain Activity in Children With Familial High-Risk of Schizophrenia or Bipolar Disorder: A Danish Register-based Study.

Author

Johnsen, Line Korsgaard, Larsen, Kit Melissa, Fuglsang, Søren Asp, Themaat, Anna Hester Ver Loren van, Baaré, William Frans Christiaan, Madsen, Kathrine Skak, Madsen, Kristoffer Hougaard, Hemager, Nicoline, Andreassen, Anna Krogh, Veddum, Lotte, Greve, Aja Neergaard, Nejad, Ayna Baladi, Burton, Birgitte Klee, Gregersen, Maja, Eichele, Heike, Lund, Torben E, Bliksted, Vibeke, Thorup, Anne Amalie Elgaard, Mors, Ole, and Plessen, Kerstin Jessica

Subjects
BRAIN physiology, SCHIZOPHRENIA risk factors, GENETICS of bipolar disorder, GENETICS of schizophrenia, BIPOLAR disorder, RISK assessment, TASK performance, RESEARCH funding, EXECUTIVE function, LONGITUDINAL method, ANALYSIS of variance, COMPARATIVE studies, SPACE perception, COGNITION, DISEASE risk factors, CHILDREN
Abstract

Background and Hypotheses Impaired executive control is a potential prognostic and endophenotypic marker of schizophrenia (SZ) and bipolar disorder (BP). Assessing children with familial high-risk (FHR) of SZ or BP enables characterization of early risk markers and we hypothesize that they express impaired executive control as well as aberrant brain activation compared to population-based control (PBC) children. Study Design Using a flanker task, we examined executive control together with functional magnetic resonance imaging (fMRI) in 11- to 12-year-old children with FHR of SZ (FHR-SZ) or FHR of BP (FHR-BP) and PBC children as part of a register-based, prospective cohort-study; The Danish High Risk and Resilience study—VIA 11. Study Results We included 85 (44% female) FHR-SZ, 63 (52% female) FHR-BP and 98 (50% female) PBC in the analyses. Executive control effects, caused by the spatial visuomotor conflict, showed no differences between groups. Bayesian ANOVA of reaction time (RT) variability, quantified by the coefficient of variation (CVRT), revealed a group effect with similarly higher CVRT in FHR-BP and FHR-SZ compared to PBC (BF10 = 6.82). The fMRI analyses revealed no evidence for between-group differences in task-related brain activation. Post hoc analyses excluding children with psychiatric illness yielded same results. Conclusion FHR-SZ and FHR-BP at age 11–12 show intact ability to resolve a spatial visuomotor conflict and neural efficacy. The increased variability in RT may reflect difficulties in maintaining sustained attention. Since variability in RT was independent of existing psychiatric illness, it may reflect a potential endophenotypic marker of risk. [ABSTRACT FROM AUTHOR]

Published
2024
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9. Executive Control and Associated Brain Activity in Children With Familial High-Risk of Schizophrenia or Bipolar Disorder:A Danish Register-based Study

Author

Johnsen, Line Korsgaard, Larsen, Kit Melissa, Fuglsang, Søren Asp, Ver Loren van Themaat, Anna Hester, Baaré, William Frans Christiaan, Madsen, Kathrine Skak, Madsen, Kristoffer Hougaard, Hemager, Nicoline, Andreassen, Anna Krogh, Veddum, Lotte, Greve, Aja Neergaard, Nejad, Ayna Baladi, Burton, Birgitte Klee, Gregersen, Maja, Eichele, Heike, Lund, Torben E, Bliksted, Vibeke, Thorup, Anne Amalie Elgaard, Mors, Ole, Plessen, Kerstin Jessica, Nordentoft, Merete, Siebner, Hartwig Roman, Johnsen, Line Korsgaard, Larsen, Kit Melissa, Fuglsang, Søren Asp, Ver Loren van Themaat, Anna Hester, Baaré, William Frans Christiaan, Madsen, Kathrine Skak, Madsen, Kristoffer Hougaard, Hemager, Nicoline, Andreassen, Anna Krogh, Veddum, Lotte, Greve, Aja Neergaard, Nejad, Ayna Baladi, Burton, Birgitte Klee, Gregersen, Maja, Eichele, Heike, Lund, Torben E, Bliksted, Vibeke, Thorup, Anne Amalie Elgaard, Mors, Ole, Plessen, Kerstin Jessica, Nordentoft, Merete, and Siebner, Hartwig Roman

Abstract

Background and Hypotheses: Impaired executive control is a potential prognostic and endophenotypic marker of schizophrenia (SZ) and bipolar disorder (BP). Assessing children with familial high-risk (FHR) of SZ or BP enables characterization of early risk markers and we hypothesize that they express impaired executive control as well as aberrant brain activation compared to population-based control (PBC) children. Study Design: Using a flanker task, we examined executive control together with functional magnetic resonance imaging (fMRI) in 11- to 12-year-old children with FHR of SZ (FHR-SZ) or FHR of BP (FHR-BP) and PBC children as part of a register-based, prospective cohort-study; The Danish High Risk and Resilience study—VIA 11. Study Results: We included 85 (44% female) FHR-SZ, 63 (52% female) FHR-BP and 98 (50% female) PBC in the analyses. Executive control effects, caused by the spatial visuomotor conflict, showed no differences between groups. Bayesian ANOVA of reaction time (RT) variability, quantified by the coefficient of variation (CVRT), revealed a group effect with similarly higher CVRT in FHR-BP and FHR-SZ compared to PBC (BF10 = 6.82). The fMRI analyses revealed no evidence for between-group differences in task-related brain activation. Post hoc analyses excluding children with psychiatric illness yielded same results. Conclusion: FHR-SZ and FHR-BP at age 11–12 show intact ability to resolve a spatial visuomotor conflict and neural efficacy. The increased variability in RT may reflect difficulties in maintaining sustained attention. Since variability in RT was independent of existing psychiatric illness, it may reflect a potential endophenotypic marker of risk.

Published
2023

10. Rectal sensitivity correlated with gastrointestinal-mediated glucose disposal, but not the incretin effect

Author

Meling, Sondre, Tjora, Erling, Eichele, Heike, Nedergaard, Rasmus B., Knop, Filip K., Ejskjaer, Niels, Carlsen, Siri, Njølstad, Pål R., Brock, Christina, Søfteland, Eirik, Meling, Sondre, Tjora, Erling, Eichele, Heike, Nedergaard, Rasmus B., Knop, Filip K., Ejskjaer, Niels, Carlsen, Siri, Njølstad, Pål R., Brock, Christina, and Søfteland, Eirik

Abstract

Objective: The mechanisms behind the diminished incretin effect in type 2 diabetes are uncertain, but impaired vagal transmission has been suggested. We aimed to investigate the association between the incretin effect and autonomic neuropathy, and the degree of dysglycaemia and duration of diabetes. Design and Methods: For a cross-sectional study, we included participants with either longstanding type 2 diabetes, recent onset, untreated diabetes and controls without diabetes matched for age, sex and body mass index. Autonomic nerve function was assessed with cardiovascular reflex tests, heart rate variability and sudomotor function. Visceral afferent nerves in the gut were tested performing rapid rectal balloon distention. An oral glucose tolerance test and an intravenous isoglycaemic glucose infusion were performed to calculate the incretin effect and gastrointestinal-mediated glucose disposal (GIGD). Results: Sixty-five participants were recruited. Participants with diabetes had rectal hyposensitivity for earliest sensation (3.7 ± 1.1 kPa in longstanding, 4.0 ± 1.3 in early), compared to controls (3.0 ± 0.9 kPa), p =.005. Rectal hyposensitivity for earliest sensation was not associated with the incretin effect (rho = −0.204, p =.106), but an association was found with GIGD (rho −0.341, p =.005). Incretin effect and GIGD were correlated with all glucose values, HbA1c and duration of diabetes. Conclusions: Rectal hyposensitivity was uncovered in both longstanding and early type 2 diabetes, and was not associated with the incretin effect, but with GIGD, implying a potential link between visceral neuropathy and gastrointestinal handling of glucose. Both the incretin effect and GIGD were associated with the degree of dysglycaemia and the duration of diabetes. Previously Published: Some of the data have previously been published and presented as a poster on the American Diabetes Association 83rd Scientific Sessions: Meling et al; 1658-P: Rectal Hyposensitivity, a Pot

Published
2023

11. Rectal sensitivity correlated with gastrointestinal‐mediated glucose disposal, but not the incretin effect.

Author

Meling, Sondre, Tjora, Erling, Eichele, Heike, Nedergaard, Rasmus B., Knop, Filip K., Ejskjaer, Niels, Carlsen, Siri, Njølstad, Pål R., Brock, Christina, and Søfteland, Eirik

Subjects
TYPE 2 diabetes, GLUCOSE, GLUCOSE tolerance tests, BODY mass index, GESTATIONAL diabetes, DYSAUTONOMIA, HEART beat
Abstract

Objective: The mechanisms behind the diminished incretin effect in type 2 diabetes are uncertain, but impaired vagal transmission has been suggested. We aimed to investigate the association between the incretin effect and autonomic neuropathy, and the degree of dysglycaemia and duration of diabetes. Design and Methods: For a cross‐sectional study, we included participants with either longstanding type 2 diabetes, recent onset, untreated diabetes and controls without diabetes matched for age, sex and body mass index. Autonomic nerve function was assessed with cardiovascular reflex tests, heart rate variability and sudomotor function. Visceral afferent nerves in the gut were tested performing rapid rectal balloon distention. An oral glucose tolerance test and an intravenous isoglycaemic glucose infusion were performed to calculate the incretin effect and gastrointestinal‐mediated glucose disposal (GIGD). Results: Sixty‐five participants were recruited. Participants with diabetes had rectal hyposensitivity for earliest sensation (3.7 ± 1.1 kPa in longstanding, 4.0 ± 1.3 in early), compared to controls (3.0 ± 0.9 kPa), p =.005. Rectal hyposensitivity for earliest sensation was not associated with the incretin effect (rho = −0.204, p =.106), but an association was found with GIGD (rho −0.341, p =.005). Incretin effect and GIGD were correlated with all glucose values, HbA1c and duration of diabetes. Conclusions: Rectal hyposensitivity was uncovered in both longstanding and early type 2 diabetes, and was not associated with the incretin effect, but with GIGD, implying a potential link between visceral neuropathy and gastrointestinal handling of glucose. Both the incretin effect and GIGD were associated with the degree of dysglycaemia and the duration of diabetes. Previously Published: Some of the data have previously been published and presented as a poster on the American Diabetes Association 83rd Scientific Sessions: Meling et al; 1658‐P: Rectal Hyposensitivity, a Potential Marker of Enteric Autonomic Nerve Dysfunction, Is Significantly Associated with Gastrointestinally Mediated Glucose Disposal in Persons with Type 2 Diabetes. Diabetes 20 June 2023; 72 (Supplement_1): 1658–P. https://doi.org/10.2337/db23‐1658‐P. [ABSTRACT FROM AUTHOR]

Published
2024
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13. Reduced error signalling in medication-naive children with ADHD: associations with behavioural variability and post-error adaptations

Author

Plessen, Kerstin J., Allen, Elena A., Eichele, Heike, van Wageningen, Heidi, Hovik, Marie Farstad, Sorensen, Lin, Worren, Marius Kalsas, Hugdahl, Kenneth, and Eichele, Tom

Subjects
Drug therapy, Observations, Methods, Drug interactions -- Observations, Behavioral assessment -- Methods, Attention deficit hyperactivity disorder -- Drug therapy, Attention-deficit hyperactivity disorder -- Drug therapy
Abstract

Introduction Attention-deficit/hyperactivity disorder (ADHD) is the most frequent disorder in child and adolescent mental health services, affecting 3%-5% of children. (1) Several pathways and processes have been identified in the [...], Background: We examined the blood-oxygen level-dependent (BOLD) activation in brain regions that signal errors and their association with intraindividual behavioural variability and adaptation to errors in children with attention-deficit/hyperactivity disorder (ADHD). Methods: We acquired functional MRI data during a Flanker task in medication-naive children with ADHD and healthy controls aged 8-12 years and analyzed the data using independent component analysis. For components corresponding to performance monitoring networks, we compared activations across groups and conditions and correlated them with reaction times (RT). Additionally, we analyzed post-error adaptations in behaviour and motor component activations. Results: We included 25 children with ADHD and 29 controls in our analysis. Children with ADHD displayed reduced activation to errors in cingulo-opercular regions and higher RT variability, but no differences of interference control. Larger BOLD amplitude to error trials significantly predicted reduced RT variability across all participants. Neither group showed evidence of post-error response slowing; however, post-error adaptation in motor networks was significantly reduced in children with ADHD. This adaptation was inversely related to activation of the right-lateralized ventral attention network (VAN) on error trials and to task-driven connectivity between the cingulo-opercular system and the VAN. Limitations: Our study was limited by the modest sample size and imperfect matching across groups. Conclusion: Our findings show a deficit in cingulo-opercular activation in children with ADHD that could relate to reduced signalling for errors. Moreover, the reduced orienting of the VAN signal may mediate deficient post- error motor adaptions. Pinpointing general performance monitoring problems to specific brain regions and operations in error processing may help to guide the targets of future treatments for ADHD.

Published
2016
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14. Interference control and associated brain activity in children with familial high-risk of schizophrenia or bipolar disorder – A Danish register-based study

Author

Johnsen, Line Korsgaard, primary, Larsen, Kit Melissa, additional, Asp Fuglsang, Søren, additional, Ver Loren van Themaat, Anna Hester, additional, Baaré, William Frans Christiaan, additional, Madsen, Kathrine Skak, additional, Madsen, Kristoffer Hougaard, additional, Hemager, Nicoline, additional, Andreassen, Anna Krogh, additional, Veddum, Lotte, additional, Greve, Aja Neergaard, additional, Nejad, Ayna Baladi, additional, Burton, Birgitte Klee, additional, Gregersen, Maja, additional, Eichele, Heike, additional, Lund, Torben E., additional, Bliksted, Vibeke, additional, Thorup, Anne Amalie Elgaard, additional, Mors, Ole, additional, Plessen, Kerstin Jessica, additional, Nordentoft, Merete, additional, and Siebner, Hartwig Roman, additional

Published
2022
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15. Enhancing neuroimaging genetics through meta-analysis for Tourette syndrome (ENIGMA-TS)

Author

Paschou, Peristera, Jin, Yin, Müller-Vahl, Kirsten, Möller, Harald E., Rizzo, Renata, Hoekstra, Pieter J., Roessner, Veit, Mol Debes, Nanette, Worbe, Yulia, Hartmann, Andreas, Mir, Pablo, Cath, Danielle, Neuner, Irene, Eichele, Heike, Zhang, ChenCheng, Lewandowska, Katarzyna, Munchau, Alexander, Verrel, Julius, Musil, Richard, Silk, Tim J., Hanlon, Colleen A., Bihun, Emily D., Brandt, Valerie, Dietrich, Andrea, Forde, Natalie, Ganos, Christos, Greene, Deanna J., Chu, Chunguang, Grothe, Michel J., Hershey, Tamara, Janik, Piotr, Koller, Jonathan M., Martin-Rodriguez, Juan Francisco, Müller, Karsten, Palmucci, Stefano, Prato, Adriana, Ramkiran, Shukti, Saia, Federica, Szejko, Natalia, Torrecuso, Renzo, Tumer, Zeynep, Uhlmann, Anne, Veselinović, Tanja, Wolańczyk, Tomasz, Zouki, Jade-Jocelyne, Jain, Pritesh, Topaloudi, Apostolia, Kaka, Mary, Yang, Zhiyu, Drineas, Petros, Thomopoulos, Sophia I., White, Tonya, Veltman, Dick J., Schmaal, Lianne, Stein, Dan J., Buitelaar, Jan, Franke, Barbara, van den Heuvel, Odile, Jahanshad, Neda, Thompson, Paul M., Black, Kevin J., ENIGMA-TS Working Group, Anatomy and neurosciences, Psychiatry, Amsterdam Neuroscience - Brain Imaging, Amsterdam Neuroscience - Mood, Anxiety, Psychosis, Stress & Sleep, Amsterdam Neuroscience - Compulsivity, Impulsivity & Attention, Amsterdam Neuroscience - Neurodegeneration, Clinical Cognitive Neuropsychiatry Research Program (CCNP), National Institute of Mental Health (US), National Science Foundation (US), Innovative Medicines Initiative, National Institutes of Health (US), Universidad de Sevilla, Lundbeck Foundation, Dagmar Marshall Foundation, Bøhmske Foundation, Hansen Memorial Foundation, Queen Louise’s Children’s Hospital Foundation, King Christian X’s Foundation, and Child and Adolescent Psychiatry / Psychology

Subjects
Psychiatry and Mental health, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], brain MRI, neuroimaging, SDG 3 - Good Health and Well-being, Brain MRI, Tourette syndrome, Genetics, ENIGMA, Neuroimaging, genetics, ddc:610
Abstract

Tourette syndrome (TS) is characterized by multiple motor and vocal tics, and high-comorbidity rates with other neuropsychiatric disorders. Obsessive compulsive disorder (OCD), attention deficit hyperactivity disorder (ADHD), autism spectrum disorders (ASDs), major depressive disorder (MDD), and anxiety disorders (AXDs) are among the most prevalent TS comorbidities. To date, studies on TS brain structure and function have been limited in size with efforts mostly fragmented. This leads to low-statistical power, discordant results due to differences in approaches, and hinders the ability to stratify patients according to clinical parameters and investigate comorbidity patterns. Here, we present the scientific premise, perspectives, and key goals that have motivated the establishment of the Enhancing Neuroimaging Genetics through Meta-Analysis for TS (ENIGMA-TS) working group. The ENIGMA-TS working group is an international collaborative effort bringing together a large network of investigators who aim to understand brain structure and function in TS and dissect the underlying neurobiology that leads to observed comorbidity patterns and clinical heterogeneity. Previously collected TS neuroimaging data will be analyzed jointly and integrated with TS genomic data, as well as equivalently large and already existing studies of highly comorbid OCD, ADHD, ASD, MDD, and AXD. Our work highlights the power of collaborative efforts and transdiagnostic approaches, and points to the existence of different TS subtypes. ENIGMA-TS will offer large-scale, high-powered studies that will lead to important insights toward understanding brain structure and function and genetic effects in TS and related disorders, and the identification of biomarkers that could help inform improved clinical practice., This work was supported by NIMH grant no. 1R01MH126213 and NSF IIS grant no. 1715202 to PP, the Innovative Medicines Initiative 2 Joint Undertaking (grant no. 777394) to NF, the NIH (grant nos. R01MH118217 and K01MH104592) to DG, the NIH (grant nos. R01MH126213, R01MH116147, and P41EB015922) to NJ, the VI-PPIT-US from the University of Seville (grant no. USE-18817-A) to JM-R, the Lundbeck Foundation, the Dagmar Marshall Foundation, the Bøhmske Foundation, the Carpenter Jørgen Holm, and wife Elisa born Hansen Memorial Foundation, the Queen Louise’s Children’s Hospital Foundation, and the King Christian X Foundation to NM, the NIH (grant nos. R01MH126213, R01MH116147, and P41EB015922) to PT and ST.

Published
2022
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16. ENIGMA-TS: a worldwide platform for collaboration on the study of Tourette Syndrome genetics and neuroimaging

Author

Paschou, Peristera, Jin, Yin, Müller-Vahl, Kirsten, Möller, Harald, Rizzo, Renata, Hoekstra, Pieter, Roessner, Veit, Mol Debes, Nanette, Worbe, Yulia, Hartmann, Andreas, Mir, Pablo, Cath, Danielle, Neuner, Irene, Eichele, Heike, Zhang, Chencheng, Szamburska-Lewandowska, Katarzyna, Muenchau, Alexander, Verrel, Julius, Musil, Richard, Silk, Tim, Hanlon, Colleen, Bihun, Emily, Brandt, Valerie, Dietrick, Andrea, Forde, Natalie, Ganos, Christos, Greene, Deanna, Chunguang, Chu, Grothe, Michel, Hershey, Tamara, Janik, Piotr, Koller, Jonathan, Rodriguez, Juan Francisco Martin, Mueller, Karsten, Palmucci, Stefano, Prato, Adriana, Ramkiran, Shukti, Saia, Federica, Szejko, Natalia, Torrecuso, Renzo, Tumer, Zeynep, Uhlmann, Anne, Veselinovic, Tanja, Wolanczyk, Tomasz, Zouki, Jace, Jain, Pritesh, Topaloudi, Apostolia, Kaka, Mary, Yang, Zhiyu, Drineas, Petros, Thomopoulos, Sophia, White, Tonya, Veltman, Dick, Schmaal, Lianne, Stein, Dan, Franke, Barbara, van den Heuvel, Odile, Jahanshad, Neda, Thompson, Paul, and Black, Kevin

Published
2022

17. Post-error adjustment among children aged 7 years with a familial high risk of schizophrenia or bipolar disorder:A population-based cohort study

Author

Burton, Birgitte Klee, Petersen, Anders, Eichele, Heike, Hemager, Nicoline, Spang, Katrine S., Ellersgaard, Ditte, Christiani, Camilla Jerlang, Greve, Aja, Gantriis, Ditte, Jepsen, Jens Richardt M., Mors, Ole, Nordentoft, Merete, Thorup, Anne A.E., Plessen, Kerstin Jessica, Vangkilde, Signe, Burton, Birgitte Klee, Petersen, Anders, Eichele, Heike, Hemager, Nicoline, Spang, Katrine S., Ellersgaard, Ditte, Christiani, Camilla Jerlang, Greve, Aja, Gantriis, Ditte, Jepsen, Jens Richardt M., Mors, Ole, Nordentoft, Merete, Thorup, Anne A.E., Plessen, Kerstin Jessica, and Vangkilde, Signe

Abstract

The cognitive control system matures gradually with age and shows age-related sex differences. To gain knowledge concerning error adaptation in familial high-risk groups, investigating error adaptation among the offspring of parents with severe mental disorders is important and may contribute to the understanding of cognitive functioning in at-risk individuals. We identified an observational cohort through Danish registries and measured error adaptation using an Eriksen flanker paradigm. We tested 497 7-year-old children with a familial high risk of schizophrenia (N = 192) or bipolar disorder (N = 116) for deficits in error adaptation compared with a control group (N = 189). We investigated whether error adaptation differed between high-risk groups compared with controls and sex differences in the adaptation to errors, irrespective of high-risk status. Overall, children exhibited post-error slowing (PES), but the slowing of responses did not translate to significant improvements in accuracy. No differences were detected between either high-risk group compared with the controls. Boys showed less PES and PES after incongruent trials than girls. Our results suggest that familial high risk of severe mental disorders does not influence error adaptation at this early stage of cognitive control development. Error adaptation behavior at age 7 years shows specific sex differences.

Published
2022

18. Enhancing neuroimaging genetics through meta-analysis for Tourette syndrome (ENIGMA-TS):A worldwide platform for collaboration

Author

Paschou, Peristera, Jin, Yin, Müller-Vahl, Kirsten, Möller, Harald E., Rizzo, Renata, Hoekstra, Pieter J., Roessner, Veit, Debes, Nanette Mol, Worbe, Yulia, Hartmann, Andreas, Mir, Pablo, Cath, Danielle, Neuner, Irene, Eichele, Heike, Zhang, Chencheng, Lewandowska, Katarzyna, Munchau, Alexander, Verrel, Julius, Musil, Richard, Silk, Tim J., Hanlon, Colleen A., Bihun, Emily D., Brandt, Valerie, Dietrich, Andrea, Forde, Natalie, Ganos, Christos, Greene, Deanna J., Chu, Chunguang, Grothe, Michel J, Hershey, Tamara, Janik, Piotr, Koller, Jonathan M., Martin-Rodriguez, Juan Francisco, Müller, Karsten, Palmucci, Stefano, Prato, Adriana, Ramkiran, Shukti, Saia, Federica, Szejko, Natalia, Torrecuso, Renzo, Tumer, Zeynep, Uhlmann, Anne, Veselinovic, Tanja, Wolańczyk, Tomasz, Zouki, Jade Jocelyne, Jain, Pritesh, Topaloudi, Apostolia, Kaka, Mary, Yang, Zhiyu, Drineas, Petros, Thomopoulos, Sophia I., White, Tonya, Veltman, Dick J, Schmaal, Lianne, Stein, Dan J, Buitelaar, Jan, Franke, Barbara, van den Heuvel, Odile, Jahanshad, Neda, Thompson, Paul M., Black, Kevin J., Paschou, Peristera, Jin, Yin, Müller-Vahl, Kirsten, Möller, Harald E., Rizzo, Renata, Hoekstra, Pieter J., Roessner, Veit, Debes, Nanette Mol, Worbe, Yulia, Hartmann, Andreas, Mir, Pablo, Cath, Danielle, Neuner, Irene, Eichele, Heike, Zhang, Chencheng, Lewandowska, Katarzyna, Munchau, Alexander, Verrel, Julius, Musil, Richard, Silk, Tim J., Hanlon, Colleen A., Bihun, Emily D., Brandt, Valerie, Dietrich, Andrea, Forde, Natalie, Ganos, Christos, Greene, Deanna J., Chu, Chunguang, Grothe, Michel J, Hershey, Tamara, Janik, Piotr, Koller, Jonathan M., Martin-Rodriguez, Juan Francisco, Müller, Karsten, Palmucci, Stefano, Prato, Adriana, Ramkiran, Shukti, Saia, Federica, Szejko, Natalia, Torrecuso, Renzo, Tumer, Zeynep, Uhlmann, Anne, Veselinovic, Tanja, Wolańczyk, Tomasz, Zouki, Jade Jocelyne, Jain, Pritesh, Topaloudi, Apostolia, Kaka, Mary, Yang, Zhiyu, Drineas, Petros, Thomopoulos, Sophia I., White, Tonya, Veltman, Dick J, Schmaal, Lianne, Stein, Dan J, Buitelaar, Jan, Franke, Barbara, van den Heuvel, Odile, Jahanshad, Neda, Thompson, Paul M., and Black, Kevin J.

Abstract

Tourette syndrome (TS) is characterized by multiple motor and vocal tics, and high-comorbidity rates with other neuropsychiatric disorders. Obsessive compulsive disorder (OCD), attention deficit hyperactivity disorder (ADHD), autism spectrum disorders (ASDs), major depressive disorder (MDD), and anxiety disorders (AXDs) are among the most prevalent TS comorbidities. To date, studies on TS brain structure and function have been limited in size with efforts mostly fragmented. This leads to low-statistical power, discordant results due to differences in approaches, and hinders the ability to stratify patients according to clinical parameters and investigate comorbidity patterns. Here, we present the scientific premise, perspectives, and key goals that have motivated the establishment of the Enhancing Neuroimaging Genetics through Meta-Analysis for TS (ENIGMA-TS) working group. The ENIGMA-TS working group is an international collaborative effort bringing together a large network of investigators who aim to understand brain structure and function in TS and dissect the underlying neurobiology that leads to observed comorbidity patterns and clinical heterogeneity. Previously collected TS neuroimaging data will be analyzed jointly and integrated with TS genomic data, as well as equivalently large and already existing studies of highly comorbid OCD, ADHD, ASD, MDD, and AXD. Our work highlights the power of collaborative efforts and transdiagnostic approaches, and points to the existence of different TS subtypes. ENIGMA-TS will offer large-scale, high-powered studies that will lead to important insights toward understanding brain structure and function and genetic effects in TS and related disorders, and the identification of biomarkers that could help inform improved clinical practice.

Published
2022

19. Enhancing neuroimaging genetics through meta-analysis for Tourette syndrome (ENIGMA-TS): A worldwide platform for collaboration

Author

National Institute of Mental Health (US), National Science Foundation (US), Innovative Medicines Initiative, National Institutes of Health (US), Universidad de Sevilla, Lundbeck Foundation, Dagmar Marshall Foundation, Bohemia Fund, Jeff Hansen Memorial Foundation, Queen Louise's Children's Hospital Foundation, King Christian X’s Foundation, Paschou, Peristera, Jin, Yin, Müller-Vahl, Kirsten R., Möller, Harald E., Rizzo, Renata, Hoekstra, Pieter J., Roessner, Veit, Mol Debes, Nanette, Worbe, Yulia, Hartmann, Andreas, Mir, Pablo, Cath, Danielle, Neuner, Irene, Eichele, Heike, Zhang, Chencheng, Lewandowska, Katarzyna, Münchau, Alexander, Verrel, Julius, Musil, Richard, Silk, Tim J., Hanlon, Colleen A., Bihun, Emily D., Brandt, Valerie, Dietrich, Andrea, Forde, Natalie, Ganos, Christos, Greene, Deanna J., Chu, Chunguang, Grothe, Michel J., Hershey, Tamara, Janik, Piotr, Koller, Jonathan M., Martín-Rodríguez, Juan Francisco, Müller, Karsten, Palmucci, Stefano, Prato, Adriana, Ramkiran, Shukti, Saia, Federica, Szejko, Natalia, Torrecuso, Renzo, Tumer, Zeynep, Uhlmann, Anne, Veselinovic, Tanja, Wolańczyk, Tomasz, Zouki, Jade Jocelyne, Jain, Pritesh, Topaloudi, Apostolia, Kaka, Mary, Yang, Zhiyu, Drineas, Petros, Thomopoulos, Sophia I., White, Tonya, Veltman, Dick J., Schmaal, Lianne, Stein, Dan J., Buitelaar, Jan, Franke, Barbara, Heuvel, Odile van den, Jahanshad, Neda, Thompson, Paul M., Black, Kevin J., National Institute of Mental Health (US), National Science Foundation (US), Innovative Medicines Initiative, National Institutes of Health (US), Universidad de Sevilla, Lundbeck Foundation, Dagmar Marshall Foundation, Bohemia Fund, Jeff Hansen Memorial Foundation, Queen Louise's Children's Hospital Foundation, King Christian X’s Foundation, Paschou, Peristera, Jin, Yin, Müller-Vahl, Kirsten R., Möller, Harald E., Rizzo, Renata, Hoekstra, Pieter J., Roessner, Veit, Mol Debes, Nanette, Worbe, Yulia, Hartmann, Andreas, Mir, Pablo, Cath, Danielle, Neuner, Irene, Eichele, Heike, Zhang, Chencheng, Lewandowska, Katarzyna, Münchau, Alexander, Verrel, Julius, Musil, Richard, Silk, Tim J., Hanlon, Colleen A., Bihun, Emily D., Brandt, Valerie, Dietrich, Andrea, Forde, Natalie, Ganos, Christos, Greene, Deanna J., Chu, Chunguang, Grothe, Michel J., Hershey, Tamara, Janik, Piotr, Koller, Jonathan M., Martín-Rodríguez, Juan Francisco, Müller, Karsten, Palmucci, Stefano, Prato, Adriana, Ramkiran, Shukti, Saia, Federica, Szejko, Natalia, Torrecuso, Renzo, Tumer, Zeynep, Uhlmann, Anne, Veselinovic, Tanja, Wolańczyk, Tomasz, Zouki, Jade Jocelyne, Jain, Pritesh, Topaloudi, Apostolia, Kaka, Mary, Yang, Zhiyu, Drineas, Petros, Thomopoulos, Sophia I., White, Tonya, Veltman, Dick J., Schmaal, Lianne, Stein, Dan J., Buitelaar, Jan, Franke, Barbara, Heuvel, Odile van den, Jahanshad, Neda, Thompson, Paul M., and Black, Kevin J.

Abstract

Tourette syndrome (TS) is characterized by multiple motor and vocal tics, and high-comorbidity rates with other neuropsychiatric disorders. Obsessive compulsive disorder (OCD), attention deficit hyperactivity disorder (ADHD), autism spectrum disorders (ASDs), major depressive disorder (MDD), and anxiety disorders (AXDs) are among the most prevalent TS comorbidities. To date, studies on TS brain structure and function have been limited in size with efforts mostly fragmented. This leads to low-statistical power, discordant results due to differences in approaches, and hinders the ability to stratify patients according to clinical parameters and investigate comorbidity patterns. Here, we present the scientific premise, perspectives, and key goals that have motivated the establishment of the Enhancing Neuroimaging Genetics through Meta-Analysis for TS (ENIGMA-TS) working group. The ENIGMA-TS working group is an international collaborative effort bringing together a large network of investigators who aim to understand brain structure and function in TS and dissect the underlying neurobiology that leads to observed comorbidity patterns and clinical heterogeneity. Previously collected TS neuroimaging data will be analyzed jointly and integrated with TS genomic data, as well as equivalently large and already existing studies of highly comorbid OCD, ADHD, ASD, MDD, and AXD. Our work highlights the power of collaborative efforts and transdiagnostic approaches, and points to the existence of different TS subtypes. ENIGMA-TS will offer large-scale, high-powered studies that will lead to important insights toward understanding brain structure and function and genetic effects in TS and related disorders, and the identification of biomarkers that could help inform improved clinical practice.

Published
2022

20. European clinical guidelines for Tourette syndrome and other tic disorders - version 2.0. Part III:pharmacological treatment

Author

Roessner, Veit, Eichele, Heike, Stern, Jeremy S, Skov, Liselotte, Rizzo, Renata, Debes, Nanette Mol, Nagy, Peter, Cavanna, Andrea E, Termine, Cristiano, Ganos, Christos, Münchau, Alexander, Szejko, Natalia, Cath, Danielle, Müller-Vahl, Kirsten R., Verdellen, Cara, Hartmann, Andreas, Rothenberger, Aribert, Hoekstra, Pieter J, Plessen, Kerstin J., Roessner, Veit, Eichele, Heike, Stern, Jeremy S, Skov, Liselotte, Rizzo, Renata, Debes, Nanette Mol, Nagy, Peter, Cavanna, Andrea E, Termine, Cristiano, Ganos, Christos, Münchau, Alexander, Szejko, Natalia, Cath, Danielle, Müller-Vahl, Kirsten R., Verdellen, Cara, Hartmann, Andreas, Rothenberger, Aribert, Hoekstra, Pieter J, and Plessen, Kerstin J.

Abstract

In 2011, the European Society for the Study of Tourette Syndrome (ESSTS) published the first European guidelines for Tourette Syndrome (TS). We now present an update of the part on pharmacological treatment, based on a review of new literature with special attention to other evidence-based guidelines, meta-analyses, and randomized double-blinded studies. Moreover, our revision took into consideration results of a recent survey on treatment preferences conducted among ESSTS experts. The first preference should be given to psychoeducation and to behavioral approaches, as it strengthens the patients' self-regulatory control and thus his/her autonomy. Because behavioral approaches are not effective, available, or feasible in all patients, in a substantial number of patients pharmacological treatment is indicated, alone or in combination with behavioral therapy. The largest amount of evidence supports the use of dopamine blocking agents, preferably aripiprazole because of a more favorable profile of adverse events than first- and second-generation antipsychotics. Other agents that can be considered include tiapride, risperidone, and especially in case of co-existing attention deficit hyperactivity disorder (ADHD), clonidine and guanfacine. This view is supported by the results of our survey on medication preference among members of ESSTS, in which aripiprazole was indicated as the drug of first choice both in children and adults. In treatment resistant cases, treatment with agents with either a limited evidence base or risk of extrapyramidal adverse effects might be considered, including pimozide, haloperidol, topiramate, cannabis-based agents, and botulinum toxin injections. Overall, treatment of TS should be individualized, and decisions based on the patient's needs and preferences, presence of co-existing conditions, latest scientific findings as well as on the physician's preferences, experience, and local regulatory requirements.

Published
2022

23. Post-error adjustment among children aged 7 years with a familial high risk of schizophrenia or bipolar disorder: A population-based cohort study.

Author

Burton, Birgitte Klee, Petersen, Anders, Eichele, Heike, Hemager, Nicoline, Spang, Katrine S., Ellersgaard, Ditte, Christiani, Camilla Jerlang, Greve, Aja, Gantriis, Ditte, Jepsen, Jens Richardt M., Mors, Ole, Nordentoft, Merete, Thorup, Anne AE, Plessen, Kerstin Jessica, and Vangkilde, Signe

Subjects
BIPOLAR disorder, SCHIZOPHRENIA, CONTROL (Psychology), COGNITIVE ability, MENTAL illness
Abstract

The cognitive control system matures gradually with age and shows age-related sex differences. To gain knowledge concerning error adaptation in familial high-risk groups, investigating error adaptation among the offspring of parents with severe mental disorders is important and may contribute to the understanding of cognitive functioning in at-risk individuals. We identified an observational cohort through Danish registries and measured error adaptation using an Eriksen flanker paradigm. We tested 497 7-year-old children with a familial high risk of schizophrenia (N = 192) or bipolar disorder (N = 116) for deficits in error adaptation compared with a control group (N = 189). We investigated whether error adaptation differed between high-risk groups compared with controls and sex differences in the adaptation to errors, irrespective of high-risk status. Overall, children exhibited post-error slowing (PES), but the slowing of responses did not translate to significant improvements in accuracy. No differences were detected between either high-risk group compared with the controls. Boys showed less PES and PES after incongruent trials than girls. Our results suggest that familial high risk of severe mental disorders does not influence error adaptation at this early stage of cognitive control development. Error adaptation behavior at age 7 years shows specific sex differences. [ABSTRACT FROM AUTHOR]

Published
2022
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24. European clinical guidelines for Tourette syndrome and other tic disorders—version 2.0. Part III: pharmacological treatment

Author

Roessner, Veit, primary, Eichele, Heike, additional, Stern, Jeremy S., additional, Skov, Liselotte, additional, Rizzo, Renata, additional, Debes, Nanette Mol, additional, Nagy, Péter, additional, Cavanna, Andrea E., additional, Termine, Cristiano, additional, Ganos, Christos, additional, Münchau, Alexander, additional, Szejko, Natalia, additional, Cath, Danielle, additional, Müller-Vahl, Kirsten R., additional, Verdellen, Cara, additional, Hartmann, Andreas, additional, Rothenberger, Aribert, additional, Hoekstra, Pieter J., additional, and Plessen, Kerstin J., additional

Published
2021
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25. Post-error adjustment among children aged 7 years with a familial high risk of schizophrenia or bipolar disorder: A population-based cohort study

Author

Burton, Birgitte Klee, primary, Petersen, Anders, additional, Eichele, Heike, additional, Hemager, Nicoline, additional, Spang, Katrine S., additional, Ellersgaard, Ditte, additional, Christiani, Camilla Jerlang, additional, Greve, Aja, additional, Gantriis, Ditte, additional, Jepsen, Jens Richardt M., additional, Mors, Ole, additional, Nordentoft, Merete, additional, Thorup, Anne AE, additional, Plessen, Kerstin Jessica, additional, and Vangkilde, Signe, additional

Published
2021
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28. Lower Cardiac Vagal Activity Predicts Self-Reported Difficulties With Emotion Regulation in Adolescents With ADHD

Author

Kvadsheim, Elisabet, Fasmer, Ole Bernt, Osnes, Berge, Koenig, Julian, Adolfsdottir, Steinunn, Eichele, Heike, Plessen, Kerstin Jessica, Sørensen, Lin, Kvadsheim, Elisabet, Fasmer, Ole Bernt, Osnes, Berge, Koenig, Julian, Adolfsdottir, Steinunn, Eichele, Heike, Plessen, Kerstin Jessica, and Sørensen, Lin

Abstract

Objective: To investigate the relation between cardiac vagal activity (CVA), a measure of autonomic nervous system (ANS) flexibility, and self-reported emotion regulation (ER) difficulties in adolescents with attention-deficit/hyperactivity disorder (ADHD) and controls. Methods: The sample comprised 11–17-year-old adolescents with ADHD (n=34) and controls (n = 33). Multiple linear regression analyses investigated the relation between CVA, as indexed by high frequency heart rate variability (HF-HRV), and ER difficulties as assessed by the Difficulties in Emotion Regulation Scale (DERS). Supplemental analyses were performed in ADHD and control groups separately. Analyses assessed effects of body mass index (BMI), physical activity levels, and HF peak as a surrogate of respiration on CVA. Results: Lower CVA was associated with ER difficulties, and specifically with limited access to effective ER strategies. When investigating the relation between CVA and ER in the ADHD and control groups separately, there was a tendency of lower CVA predicting limited access to effective ER strategies in the ADHD group, and not in the control group. Conclusion: The results suggest that lower CVA, i.e., reduced ANS flexibility, in adolescents with ADHD and controls is associated with self-reported ER difficulties, and specifically with limited access to effective ER strategies. There was a tendency for lower CVA to predict limited ER strategies only in the adolescents with ADHD and not controls.

Published
2020

29. Event-related electroencephalographic responses in children at familial high risk for schizophrenia or bipolar disorder: a single-site EEG sub-study of the Danish High Risk and Resilience Study-VIA 11

Author

Ver Loren van Themaat, Anna, primary, Larsen, Kit Melissa, additional, Oranje, Bob, additional, Johnsen, Line Korsgaard, additional, Tomasevic, Leo, additional, Baare, William Frans Christiaan, additional, Nejad, Ayna Baladi, additional, Eichele, Heike, additional, Thorup, Anne Amalie Elgaard, additional, Nordentoft, Merete, additional, Plessen, Kerstin Jessica, additional, and Siebner, Hartwig Roman, additional

Published
2019
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32. Sustained Attention and Interference Control Among 7-Year-Old Children With a Familial High Risk of Schizophrenia or Bipolar Disorder:A Nationwide Observational Cohort Study

Author

Burton, Birgitte Klee, Vangkilde, Signe, Petersen, Anders, Skovgaard, Lene Theil, Jepsen, Jens Richardt, Hemager, Nicoline, Christiani, Camilla Jerlang, Spang, Katrine Soeborg, Ellersgaard, Ditte, Greve, Aja, Gantriis, Ditte, Eichele, Heike, Mors, Ole, Nordentoft, Merete, Thorup, Anne Amalie Elgaard, Plessen, Kerstin Jessica, Burton, Birgitte Klee, Vangkilde, Signe, Petersen, Anders, Skovgaard, Lene Theil, Jepsen, Jens Richardt, Hemager, Nicoline, Christiani, Camilla Jerlang, Spang, Katrine Soeborg, Ellersgaard, Ditte, Greve, Aja, Gantriis, Ditte, Eichele, Heike, Mors, Ole, Nordentoft, Merete, Thorup, Anne Amalie Elgaard, and Plessen, Kerstin Jessica

Abstract

Background: Given the partially shared genetic liability between schizophrenia and bipolar disorder, we aimed to assess whether 7-year-old children with a familial high risk of schizophrenia or bipolar disorder display specific deficits of sustained attention and interference control compared with each other and with control children. Methods: An observational cohort was identified through Danish registries and consisted of 522 children 7 years of age with no, one, or two parents with a diagnosis of schizophrenia or bipolar disorder. Control subjects were matched based on age, sex, and municipality. Sustained attention and interference control were assessed using Conners’ Continuous Performance Test II and a modified Eriksen flanker task. Assessors were blinded to group membership of participants. The effect of higher genetic loading was not considered in the statistical models owing to low numbers. Results: At 7 years of age, children with a familial high risk of schizophrenia displayed deficits of sustained attention and subtle deficits in interference control compared with control children and children with a familial high risk of bipolar disorder. Children with a familial high risk of bipolar disorder displayed similar abilities of sustained attention and interference control as control children except in terms of a lower accuracy. Conclusions: Our findings suggest distinct neurodevelopmental characteristics in middle childhood of sustained attention and interference control for children of parents with schizophrenia or bipolar disorder.

Published
2018

33. Electrophysiological Correlates of Performance Monitoring in Children with Tourette Syndrome. A developmental perspective

Author

Eichele, Heike

Abstract

Tourette syndrome (TS) is a neuropsychiatric disorder with childhood onset, characterized by chronic motor and vocal tics. Typically, tic symptoms attenuate during adolescence in parallel with the emerging self-regulatory control during brain development. The voluntary control over thought and action provides the ability to withhold unwanted behaviour and an association between cognitive control and tic control has been suggested. This attenuation of tic symptoms also suggests that neuroplasticity may play an important role in this process. The work discussed herein is centred on how compensatory mechanisms may affect dysfunctional neurocognitive processes, specifically performance monitoring deficits in children and adolescents with TS. In paper I, we have summarized current knowledge on neural plasticity in children and adolescence with TS. To present the current understanding of dysfunctional neurocognitive processes seen in functional magnetic resonance imaging and possible compensatory effects seen in anatomical magnetic resonance imaging in TS, we conducted an overview of data from studies comparing children with TS to healthy peers. In order to assess the importance of possible adaptive effects in paediatric TS, we reviewed with special attention to covariation with tic severity. The summary revealed differences in brain regions representing the tic origin along with deviations in other regions that might represent activity-dependent activation that help to modulate tic severity in TS compared with controls. Age, comorbidity with other developmental disorders, especially with attention deficit/hyperactivity disorder (ADHD), medication use, and intelligence were identified as factors that potentially influence the development of adaptive changes. Comparative analyses or meta-analytic approaches are thus far difficult due to inherent differences in study-design, magnetic resonance imaging techniques for acquisition, and analysis of primary data. The paper highlights the importance of studying cognitive control and adaptive effects in TS, while also revealing the scarcity of studies with longitudinal design and other modalities, as e.g. electrophysiology. The two next papers are based on the electrophysiological data collected to better understand the origins of cognitive control and performance monitoring deficits in TS. The main aim of paper II was to test an established experimental setup of performance monitoring in order to identify if behavioural and electrophysiological performance monitoring differences occur in children with TS when compared to controls and a contrast group with children with ADHD at the age of 8-12 years. We employed event-related potentials (ERP) in order to monitor stimulus-related and response-related components elicited during a flanker task. The main findings of this investigation indicate that the children with TS and children with ADHD and healthy controls behaviourally performed much the same regarding reaction times, accuracy and response variability when controlling for covariates. However, when not controlling for relevant covariates, children with TS and children with ADHD performed on a slightly lower level. ERP results showed higher amplitudes of an early P3 component of the stimulus-locked potentials in ensemble averages and in separate trial outcomes, as well as a slightly higher positive complex before the motor response, likely reflecting a late P3 in children with TS when compared to controls and children with ADHD. We interpreted the differences as mainly caused by heightened attentional resource allocation during stimulus evaluation. Groups did not differ in post-response components. These findings thus suggest that children with TS may employ additional attentional resources as a compensatory mechanism to maintain equal behavioural performance. While paper II focused on disentangling the role of sub-processes of performance monitoring in children with TS, paper III was more focused on the developmental changes in performance monitoring which might help the understanding of tic regulation and attenuation over time in children and adolescents with TS. To this end, we compared task performance and ERP components from the first assessment with a follow-up ERP study administered on average 4.5 years later in the same population using regression models. The results from this investigation indicated that cognitive measures of children with TS approached the values found in controls at the second assessment while differences between children with ADHD and controls largely persisted. ERP measures related to orienting and sustained attention, that developed earlier in children with TS compared with controls at the first assessment converged with maturation and correlated with worst-ever tic scores. In summary, the research described in this thesis contributes to the further understanding of electrophysiological correlates of performance monitoring in children with Tourette syndrome in several ways. In paper I, we found the current literature to implicate dysfunctional neurocognitive processes and possible compensatory effects in children with TS. The use of a neurocognitive model of performance monitoring in paper II suggested heightened orienting and/or attention requirements during stimulus evaluation as a compensatory mechanism to maintain equal behavioural performance. The developmental approach in paper III allowed us to find evidence of converging cognitive and electrophysiological measures over time in children with TS when compared with controls as well as correlation between ERPs and worst-ever tic scores. The main results from each of the papers presented continue to implicate compensatory self-regulation mechanisms during early adolescence, probably facilitating tic suppression. Correlations between ERP amplitudes and tic scores also support this notion.

Published
2017

35. Suboptimal decision making by children with ADHD in the face of risk:Poor risk adjustment and delay aversion rather than general proneness to taking risks

Author

Sørensen, Lin, Sonuga-Barke, Edmund, Eichele, Heike, van Wageningen, Heidi, Wollschlaeger, Daniel, Plessen, Kerstin Jessica, Sørensen, Lin, Sonuga-Barke, Edmund, Eichele, Heike, van Wageningen, Heidi, Wollschlaeger, Daniel, and Plessen, Kerstin Jessica

Abstract

Objective: Suboptimal decision making in the face of risk (DMR) in children with attention-deficit hyperactivity disorder (ADHD) may be mediated by deficits in a number of different neuropsychological processes. We investigated DMR in children with ADHD using the Cambridge Gambling Task (CGT) to distinguish difficulties in adjusting to changing probabilities of choice outcomes (so-called risk adjustment) from general risk proneness, and to distinguish these 2 processes from delay aversion (the tendency to choose the least delayed option) and impairments in the ability to reflect on choice options. Based on previous research, we predicted that suboptimal performance on this task in children with ADHD would be primarily relate to problems with risk adjustment and delay aversion rather than general risk proneness. Method: Drug naïve children with ADHD (n = 36), 8 to 12 years, and an age-matched group of typically developing children (n = 34) performed the CGT. Results: As predicted, children with ADHD were not more prone to making risky choices (i.e., risk proneness). However, they had difficulty adjusting to changing risk levels and were more delay aversive-with these 2 effects being correlated. Conclusions: Our findings add to the growing body of evidence that children with ADHD do not favor risk taking per se when performing gambling tasks, but rather may lack the cognitive skills or motivational style to appraise changing patterns of risk effectively.

Published
2017

36. Development of Performance and ERPs in a Flanker Task in Children and Adolescents with Tourette Syndrome-A Follow-Up Study

Author

Eichele, Heike, Eichele, Tom, Marquardt, Lynn, Adolfsdottir, Steinunn, Hugdahl, Kenneth, Sørensen, Lin, Plessen, Kerstin J, Eichele, Heike, Eichele, Tom, Marquardt, Lynn, Adolfsdottir, Steinunn, Hugdahl, Kenneth, Sørensen, Lin, and Plessen, Kerstin J

Abstract

Background: Tourette Syndrome (TS) is a neurodevelopmental disorder with childhood-onset, with a typical decline in tic severity, as well as an increasing ability to suppress tics in late childhood and adolescence. These processes develop in parallel with general improvement of self-regulatory abilities, and performance monitoring during this age-span. Hence, changes in performance monitoring over time might provide insight into the regulation of tics in children and adolescents with TS. Method: We measured reaction time, reaction time variability, accuracy, and event-related potentials (ERP) in 17 children with TS, including 10 children with comorbid Attention-Deficit/Hyperactivity Disorder (ADHD), 24 children with ADHD, and 29 typically developing children, using a modified Eriksen Flanker task in two testing sessions administered on average 4.5 years apart. We then compared task performance, as well as ERP components across groups, and over time using regression models. Results: Task performance improved in all groups with age, and behavioral differences between children with TS and controls diminished at second assessment, while differences between controls and children with ADHD largely persisted. In terms of ERP, the early P3 developed earlier in children with TS compared with controls at the first assessment, but trajectories converged with maturation. ERP component amplitudes correlated with worst-ever tic scores. Conclusions: Merging trajectories between children with TS and controls are consistent with the development of compensatory self-regulation mechanisms during early adolescence, probably facilitating tic suppression, in contrast to children with ADHD. Correlations between ERP amplitudes and tic scores also support this notion.

Published
2017

38. Reduced error signalling in medication-naive children with ADHD:associations with behavioural variability and post-error adaptations

Author

Plessen, Kerstin J, Allen, Elena A, Eichele, Heike, van Wageningen, Heidi, Høvik, Marie Farstad, Sørensen, Lin, Worren, Marius Kalsås, Hugdahl, Kenneth, Eichele, Tom, Plessen, Kerstin J, Allen, Elena A, Eichele, Heike, van Wageningen, Heidi, Høvik, Marie Farstad, Sørensen, Lin, Worren, Marius Kalsås, Hugdahl, Kenneth, and Eichele, Tom

Abstract

BACKGROUND: We examined the blood-oxygen level-dependent (BOLD) activation in brain regions that signal errors and their association with intraindividual behavioural variability and adaptation to errors in children with attention-deficit/hyperactivity disorder (ADHD).METHODS: We acquired functional MRI data during a Flanker task in medication-naive children with ADHD and healthy controls aged 8-12 years and analyzed the data using independent component analysis. For components corresponding to performance monitoring networks, we compared activations across groups and conditions and correlated them with reaction times (RT). Additionally, we analyzed post-error adaptations in behaviour and motor component activations.RESULTS: We included 25 children with ADHD and 29 controls in our analysis. Children with ADHD displayed reduced activation to errors in cingulo-opercular regions and higher RT variability, but no differences of interference control. Larger BOLD amplitude to error trials significantly predicted reduced RT variability across all participants. Neither group showed evidence of post-error response slowing; however, post-error adaptation in motor networks was significantly reduced in children with ADHD. This adaptation was inversely related to activation of the right-lateralized ventral attention network (VAN) on error trials and to task-driven connectivity between the cingulo-opercular system and the VAN.LIMITATIONS: Our study was limited by the modest sample size and imperfect matching across groups.CONCLUSION: Our findings show a deficit in cingulo-opercular activation in children with ADHD that could relate to reduced signalling for errors. Moreover, the reduced orienting of the VAN signal may mediate deficient post-error motor adaptions. Pinpointing general performance monitoring problems to specific brain regions and operations in error processing may help to guide the targets of future treatments for ADHD.

Published
2016

39. Performance Monitoring in Medication-Naïve Children with Tourette Syndrome

Author

Eichele, Heike, Eichele, Tom, Bjelland, Ingvar, Høvik, Marie F, Sørensen, Lin, van Wageningen, Heidi, Worren, Marius Kalsås, Hugdahl, Kenneth, Plessen, Kerstin J, Eichele, Heike, Eichele, Tom, Bjelland, Ingvar, Høvik, Marie F, Sørensen, Lin, van Wageningen, Heidi, Worren, Marius Kalsås, Hugdahl, Kenneth, and Plessen, Kerstin J

Abstract

BACKGROUND: Tourette syndrome (TS) is a childhood-onset neurodevelopmental disorder and its impact on cognitive development needs further study. Evidence from neuropsychological, neuroimaging and electrophysiological studies suggests that the decline in tic severity and the ability to suppress tics relate to the development of self-regulatory functions in late childhood and adolescence. Hence, tasks measuring performance monitoring might provide insight into the regulation of tics in children with TS.METHOD: Twenty-five children with TS, including 14 with comorbid Attention-deficit/ hyperactivity disorder (ADHD), 39 children with ADHD and 35 typically developing children aged 8-12 years were tested with a modified Eriksen-Flanker task during a 34-channel electroencephalography (EEG) recording. Task performance, as well as stimulus-locked and response-locked event-related potentials (ERP) were analyzed and compared across groups.RESULTS: Participants did not differ in their behavioral performance. Children with TS showed higher amplitudes of an early P3 component of the stimulus-locked ERPs in ensemble averages and in separate trial outcomes, suggesting heightened orienting and/or attention during stimulus evaluation. In response-locked averages, children with TS had a slightly higher positive complex before the motor response, likely also reflecting a late P3. Groups did not differ in post-response components, particularly in the error-related negativity (ERN) and error-related positivity (Pe).CONCLUSIONS: These findings suggest that children with TS may employ additional attentional resources as a compensatory mechanism to maintain equal behavioral performance.

Published
2016

41. Neural plasticity in functional and anatomical MRI studies of children with Tourette syndrome

Author

Eichele, Heike, Plessen, Kerstin J, Eichele, Heike, and Plessen, Kerstin J

Abstract

Background: Tourette syndrome (TS) is a neuropsychiatric disorder with childhood onset characterized by chronic motor and vocal tics. The typical clinical course of an attenuation of symptoms during adolescence in parallel with the emerging self-regulatory control during development suggests that plastic processes may play an important role in the development of tic symptoms. Methods: We conducted a systematic search to identify existing imaging studies (both anatomical and functional magnetic resonance imaging [fMRI]) in young persons under the age of 19 years with TS. Results: The final search resulted in 13 original studies, which were reviewed with a focus on findings suggesting adaptive processes (using fMRI) and plasticity (using anatomical MRI). Differences in brain activation compared to healthy controls during tasks that require overriding of prepotent responses help to understand compensatory pathways in children with TS. Along with alterations in regions putatively representing the origin of tics, deviations in several other regions most likely represent an activity-dependent neural plasticity that help to modulate tic severity, such as the prefrontal cortex, but also in the corpus callosum and the limbic system. Discussion: Factors that potentially influence the development of adaptive changes in the brain of children with TS are age, comorbidity with other developmental disorders, medication use, IQ along with study-design or MRI techniques for acquisition, and analysis of data. The most prominent limitation of all studies is their cross-sectional design. Longitudinal studies extending to younger age groups and to children at risk for developing TS hopefully will confirm findings of neural plasticity in future investigations.

Published
2012

42. Go/NoGo performance in boys with Tourette syndrome

Author

Eichele, Heike, Eichele, Tom, Hammar, Asa, Freyberger, Harald J, Hugdahl, Kenneth, Plessen, Kerstin J, Eichele, Heike, Eichele, Tom, Hammar, Asa, Freyberger, Harald J, Hugdahl, Kenneth, and Plessen, Kerstin J

Abstract

This study compared performance and performance monitoring in 19 boys with Tourette syndrome (TS) (12.64 years, +/- 2.05) and 19 age-matched controls (13.16 years, +/- 2.29) using a Go/NoGo task. The results indicated similar performance accuracy in the TS group and the control group. TS participants showed slower correct responses than the control group, whereas error response times were not different between the groups. The results are discussed with reference to inhibitory adaptive effects that may be employed by TS participants to maintain high accuracy at the cost of overall slower performance. These effects may be suspended prior to errors.

Published
2010

48. Mal-adaptation of event-related EEG responses preceding performance errors.

Author

Eichele H, Juvodden HT, Ullsperger M, and Eichele T

Abstract

Recent EEG and fMRI evidence suggests that behavioral errors are foreshadowed by systematic changes in brain activity preceding the outcome by seconds. In order to further characterize this type of error precursor activity, we investigated single-trial event-related EEG activity from 70 participants performing a modified Eriksen flanker task, in particular focusing on the trial-by-trial dynamics of a fronto-central independent component that previously has been associated with error and feedback processing. The stimulus-locked peaks in the N2 and P3 latency range in the event-related averages showed expected compatibility and error-related modulations. In addition, a small pre-stimulus negative slow wave was present at erroneous trials. Significant error-preceding activity was found in local stimulus sequences with decreased conflict in the form of less negativity at the N2 latency (310-350 ms) accumulating across five trials before errors; concomitantly response times were speeding across trials. These results illustrate that error-preceding activity in event-related EEG is associated with the performance monitoring system and we conclude that the dynamics of performance monitoring contribute to the generation of error-prone states in addition to the more remote and indirect effects in ongoing activity such as posterior alpha power in EEG and default mode drifts in fMRI.

Published
2010
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