Your search keyword '"Kapornai, K."' showing total 83 results

1. Film or mirror? The exploration of narratives during the road from recognition to recovery of addictive disorders

Author

Krupa, M., primary, Kiss, E., additional, and Kapornai, K., additional

Published

2022

2. Correction to: ESCAP CovCAP survey of heads of academic departments to assess the perceived initial (April/May 2020) impact of the COVID-19 pandemic on child and adolescent psychiatry services (European Child & Adolescent Psychiatry, (2021), 10.1007/s00787-020-01699-x)

Author

Revet, A. Hebebrand, J. Anagnostopoulos, D. Kehoe, L.A. Banaschewski, T. Bender, S. Csábi, G. Çuhadaroğlu, F. Dashi, E. Delorme, R. Radobuljac, M.D. Eliez, S. Krantz, M.F. Fricke, O. Gerstenberg, M. Giannopoulou, I. Graell, M. Kumperscak, H.G. Herpertz-Dahlmann, B. Huscsava, M. Kaess, M. Kapornai, K. Karwautz, A. Kresakova, D. Kölch, M. Kotsis, K. Lazaro, L. Moehler, E. Morón-Nozaleda, M.G. Özyurt, G. Pászthy, B. Podlipny, J. Purper-Ouakil, D. Remberk, B. Serdari, A. Stene, L.E. Thun-Hohenstein, L. Trebaticka, J. van West, D. Vitiello, B. Young, H. Yurteri, N. Zepf, F.D. Zielinska-Wieniawska, A. Zuddas, A. Klauser, P. COVID-19 Child Adolescent Psychiatry Consortium

Subjects

humanities

Abstract

In the original articles, the last four members’ of COVID-19 Child and Adolescent Psychiatry Consortium affiliation were incorrectly published. The correct affiliation are given below. Nihal Yurteri: Department of Child and Adolescent Psychiatry, Faculty of Medicine, Düzce University, Düzce, Turkey Florian Daniel Zepf: Department of Child and Adolescent Psychiatry, Psychosomatic Medicine and Psychotherapy, Jena University Hospital, Friedrich Schiller University Jena, Jena, Germany Anna Zielinska-Wieniawska: Department of Child and Adolescent Psychiatry, Medical University of Warsaw, Warsaw, Poland Alessandro Zuddas: Department of Biomedical Science and “G. Brotzu” Hospital Trust, Child and Adolescent Neuropsychiatry, University of Cagliari, Cagliari, Italy The original article has been corrected. © 2021, Springer-Verlag GmbH Germany, part of Springer Nature.

Published

2021

3. Psychophysiological responses to sadness in girls and boys with conduct disorder

Author

Oldenhof, H. Jansen, L. Ackermann, K. Baker, R. Batchelor, M. Baumann, S. Bernhard, A. Clanton, R. Dochnal, R. Fehlbaum, L.V. Fernandez-Rivas, A. Goergen, S. Gonzalez de Artaza-Lavesa, M. Gonzalez-Madruga, K. Gonzalez-Torres, M.A. Gundlach, M. Lotte van der Hoeven, M. Kalogerakis, Z. Kapornai, K. Kieser, M. Konsta, A. Martinelli, A. Pauli, R. Rogers, J. Smaragdi, A. Sesma-Pardo, E. Siklósi, R. Steppan, M. Tsiakoulia, F. Vermeiren, R. Vriends, N. Werner, M. Herpertz-Dahlmann, B. Kohls, G. De Brito, S. Konrad, K. Stadler, C. Fairchild, G. Freitag, C.M. Popma, A.

Abstract

General Scientific Summary: We investigated emotion processing in a large sample of boys and girls with a clinical diagnosis of conduct disorder (CD) to further the understanding of the underpinnings of antisocial behavior. We did not find support for the idea that children and adolescent with CD are physiologically unresponsive to sadness. Thus, although suggested by previous studies, children and adolescents with CD should not be perceived as “unemotional.” More studies are needed, however, to investigate whether this is specific for sadness or generalizes to other emotions. (PsycInfo Database Record (c) 2020 APA, all rights reserved) © 2020 American Psychological Association Reduced responsiveness to emotions is hypothesized to contribute to the development of conduct disorder (CD) in children and adolescents. Accordingly, blunted psychophysiological responses to emotions have been observed in boys with CD, but this has never been tested in girls. Therefore, this study compared psychophysiological responses to sadness in girls and boys with and without CD, and different clinical phenotypes of CD: with versus without limited prosocial emotions (LPE), and with versus without comorbid internalizing disorders (INT). Nine-hundred and 27 girls (427 CD, 500 controls) and 519 boys (266 CD, 253 controls) aged 9–18 years participated. Psychophysiological responses were measured while participants watched two validated sad film clips, specifically: heart rate (HR), respiratory sinus arrhythmia (RSA; indexing parasympathetic activity), preejection period (PEP; indexing sympathetic activity). Girls and boys with CD showed larger HR responses to sadness than controls. This effect was rendered nonsignificant, however, after controlling for covariates. We observed aberrant RSA responses to sadness in CD compared with controls. Similarly, we found a significant positive association between RSA responsivity and antisocial behavior when assessed dimensionally. The effects were very small, though. Results were similar for boys and girls. We found no evidence for emotional underresponsiveness in CD in the largest psychophysiological study to date in this field. More research is needed to explore whether this is specific to sadness or generalizes to other emotions. Furthermore, we recommend that studies on emotion processing in CD assess different physiological measures to help disentangle CD-related effects on sympathetic and parasympathetic activity. (PsycInfo Database Record (c) 2020 APA, all rights reserved) © 2020 American Psychological Association

Published

2020

4. Training for child and adolescent psychiatry in the twenty-first century

Author

Deschamps, P. Hebebrand, J. Jacobs, B. Robertson, P. Anagnostopoulos, D.C. Banaschewski, T. Birkle, S.M. Dubicka, B. Falissard, B. Giannopoulou, I. Hoekstra, P.J. Kaess, M. Kapornai, K. Klauser, P. Revet, A. Schröder, C.M. Seitz, J. Şeker, A. Signorini, G.

Published

2020

5. Training for child and adolescent psychiatry in the twenty-first century

Author

Deschamps, P, Hebebrand, J, Jacobs, B, Robertson, P, Anagnostopoulos, DC, Banaschewski, T, Birkle, SM, Dubicka, B, Falissard, B, Giannopoulou, I, Hoekstra, PJ, Kaess, M, Kapornai, K, Klauser, P, Revet, A, Schroder, CM, Seitz, J, Seker, A, Signorini, G, Deschamps, P, Hebebrand, J, Jacobs, B, Robertson, P, Anagnostopoulos, DC, Banaschewski, T, Birkle, SM, Dubicka, B, Falissard, B, Giannopoulou, I, Hoekstra, PJ, Kaess, M, Kapornai, K, Klauser, P, Revet, A, Schroder, CM, Seitz, J, Seker, A, and Signorini, G

Published

2020

6. Association of the GABRD gene and childhood-onset mood disorders

Author

Feng, Y., Kapornai, K., Kiss, E., Tamás, Z., Mayer, L., Baji, I., Daróczi, G., Benák, I., Kothencné, V. O., Dombovári, E., Kaczvinszk, E., Besnyő, M., Gádoros, J., Székely, J., Kovacs, M., Vetró, Á., Kennedy, J. L., and Barr, C. L.

Published

2010

7. Relational Aggression in Adolescents with Conduct Disorder: Sex Differences and Behavioral Correlates

Author

Ackermann, K. Kirchner, M. Bernhard, A. Martinelli, A. Anomitri, C. Baker, R. Baumann, S. Dochnal, R. Fernandez-Rivas, A. Gonzalez-Madruga, K. Herpertz-Dahlmann, B. Hervas, A. Jansen, L. Kapornai, K. Kersten, L. Kohls, G. Limprecht, R. Lazaratou, H. McLaughlin, A. Oldenhof, H. Rogers, J.C. Siklósi, R. Smaragdi, A. Vivanco-Gonzalez, E. Stadler, C. Fairchild, G. Popma, A. De Brito, S.A. Konrad, K. Freitag, C.M.

Abstract

As most research on conduct disorder (CD) has been conducted on male participants, it has been suggested that female-specific symptoms may be underestimated based on current DSM-5 criteria. In particular, relational aggression, i.e. the hurtful, often indirect, manipulation of relationships with the intention of damaging the other’s social position, has been proposed as a characteristic of CD that is more common in females. In addition, sex-specific studies on correlates of relational aggressive behavior are lacking. Relational aggression may be strongly related to the correlates of proactive aggression, namely low affective empathy, and high levels of callous-unemotional (CU) traits and relational victimization. Thus, the present study investigated sex differences in relational aggression, and associations between relational aggression and correlates of proactive aggression in 662 adolescents with CD (403 females) and 849 typically-developing controls (568 females) aged 9–18 years (M = 14.74, SD = 2.34) from the European multi-site FemNAT-CD study. Females with CD showed significantly higher levels of relational aggression compared to males with CD, whereas no sex differences were seen in controls. Relational aggression was only partly related to correlates of proactive aggression in CD: Independent of sex, CU traits showed a positive association with relational aggression. In females only, cognitive, but not affective empathy, was negatively associated with relational aggression. Relational victimization was more strongly associated with relational aggression in males compared to females. Despite interesting sex specific correlates of relational aggression, effects are small and the potential clinical implications should be investigated in future studies. © 2019, Springer Science+Business Media, LLC, part of Springer Nature.

Published

2019

8. No evidence of association between a functional polymorphism in the MTHFR gene and childhood-onset mood disorders

Author

Dempster, E L, Kiss, E, Kapornai, K, Daróczy, G, Mayer, L, Baji, I, Tamas, Z, Gadoros, J, Kennedy, J L, Vetró, A, Kovacs, M, and Barr, C L

Published

2007

9. Maladaptive mood repair, atypical respiratory sinus arrhythmia, and risk of a recurrent major depressive episode among adolescents with prior major depression

Author

Kovacs, M., primary, Yaroslavsky, I., additional, Rottenberg, J., additional, George, C. J., additional, Kiss, E., additional, Halas, K., additional, Dochnal, R., additional, Benák, I., additional, Baji, I., additional, Vetró, A., additional, Makai, A., additional, and Kapornai, K., additional

Published

2016

10. Ruminative response style to depression and childhood onset major depression

Author

Kapornai, K., primary, Hegenbarth, N., additional, Halas, K., additional, Baji, I., additional, Kiss, E., additional, Vetró, A., additional, and Kovacs, M., additional

Published

2012

11. Cytokine Genes TNF, IL1A, IL1B, IL6, IL1RN and IL10, and Childhood-Onset Mood Disorders

Author

Misener, V.L., primary, Gomez, L., additional, Wigg, K.G., additional, Luca, P., additional, King, N., additional, Kiss, E., additional, Daróczi, G., additional, Kapornai, K., additional, Tamas, Z., additional, Mayer, L., additional, Gádoros, J., additional, Baji, I., additional, Kennedy, J.L., additional, Kovacs, M., additional, Vetró, Á., additional, and Barr, C.L., additional

Published

2008

12. The role of early developmental and familial factors in the development of selective mutism: A case-control study

Author

Kapornai, K., primary, Okros, S., additional, Kiss, E., additional, and Vetro, A., additional

Published

2007

13. Assessing quality of life: mother-child agreement in depressed and non-depressed Hungarian.

Author

Kiss E, Kapornai K, Baji I, Mayer L, and Vetró A

Abstract

PURPOSE: An important question in child psychiatry is the agreement between parents and children. We studied mother-child concordance about the quality of life of children (QoL). We hypothesized that mothers of depressed children rate lower QoL than children for themselves while mothers of non-depressed children rate better QoL; that inter-informant agreement is higher in the non-depressed sample; and finally that agreement increases with age of the child. METHODS: QoL of depressed children (N = 248, mean age 11.45 years, SD 2.02) were compared to that of non-depressed children (N = 1695, mean age 10.34 years, SD 2.19). QoL was examined by a 7 item questionnaire (ILK). RESULTS: Mothers of depressed children rated lower QoL than their children while mothers of nondepressed children rated higher QoL than their children. Agreement was low in both samples but higher in the controls. Inter-informant agreement was only influenced by depression. CONCLUSIONS: Our results show that mothers relate more serious negative effects to childhood depression than their children and rate less problems for their non-depressed children compared to self-reports. Mother-child agreement is negatively influenced by depression which further stresses the importance of obtaining reports from the child and at least one parent in order to understand the subjective experiences caused by the illness. [ABSTRACT FROM AUTHOR]

Published

2009

14. Insomnia and hypersomnia associated with depressive phenomenology and comorbidity in childhood depression.

Author

Liu X, Buysse DJ, Gentzler AL, Kiss E, Mayer L, Kapornai K, Vetró A, and Kovacs M

Published

2007

15. Mutation screen and association analysis of the glucocorticoid receptor gene NR3C1 in childhoodonset mood disorders COMDPlease cite this article as follows: Mill J, Wigg K, Burcescu I, Vetró Á, Kiss E, Kapornai K, Tamás Z, Baji I, Gádoros J, Kennedy JL, Kovacs M, Barr CL, The International Consortium for ChildhoodOnset Mood Disorders. 2009. Mutation screen and association analysis of the glucocorticoid receptor gene NR3C1 in childhoodonset mood disorders COMD. Am J Med Genet Part B 150B:866–873.

Author

Mill, J., Wigg, K., Burcescu, I., Vetró, Á., Kiss, E., Kapornai, K., Tamás, Z., Baji, I., Gádoros, J., Kennedy, J.L., Kovacs, M., and Barr, C.L.

Abstract

Depressive disorders are highly heterogeneous psychiatric disorders involving deficits to cognitive, psychomotor, and emotional processing. Considerable evidence links disruption to the hypothalamic–pituitary–adrenal HPA axis to the etiology of depression, with specific deficits reported in glucocorticoid receptor GRmediated negative feedback. Given the role of GRmediated negative feedback in mediating response to stress, and the clear link between stress and depression, it is plausible that polymorphisms in the GR gene NR3C1 act to increase susceptibility. Maternal behavior in rats epigenetically alters a NGF1A transcription factor bindingsite in the promoter region of the GR gene, providing a mechanism by which environmental cues can regulate GR expression and thus response to stress. The analogous region of the human GR gene NR3C1 has not been studied, but it is possible that polymorphisms in this region may alter the binding of transcription factors known to regulate GR expression. In this study, we have performed bioinformatic analyses on the promoter region of NR3C1to identify conserved promoter sequences and predicted transcription factor binding sites. These regions were screened with denaturing highperformance liquid chromatography DHPLC and direct resequencing, and several novel polymorphic variants were identified. We genotyped nine polymorphisms across NR3C1in a large sample of Hungarian nuclear families ascertained through affected probands with a diagnosis of childhoodonset mood disorders COMD. Singlemarker analysis provided little evidence for an association of this gene with COMD, but multimarker analysis across a region of high linkage disequilibrium revealed modest evidence for the biased transmission of several haplotypes. © 2008 WileyLiss, Inc.

Published

2009

16. Association study of the adrenergic receptors and childhood‐onset mood disorders in Hungarian families

Author

Burcescu, I., Wigg, K., Gomez, L., King, N., Vetró, Á., Kiss, E., Kapornai, K., Gádoros, J., Kennedy, J.L., Kovacs, M., and Barr, C.L.

Abstract

The adrenergic system has been implicated in the etiology of depression based on a number of lines of evidence, particularly, the mechanism of some classes of antidepressants which increase the synaptic levels of norepinephrine. Further, several genome scans for mood disorders, both unipolar and bipolar, have indicated linkage to the chromosomal regions of 5q23–q33.3, 8p12–p11.2, 4p16, and 10q24–q26, the location of the adrenergic receptors α1B (ADRA1B), β3 (ADRB3), α2C (ADRA2C), α2A (ADRA2A), and β1 (ADRB1). In this manuscript, we report on the relationship of the adrenergic receptors and depression using a family based association approach and 189 families (223 affected children) with childhood‐onset mood disorder (COMD) collected in Hungary. We found no significant evidence for an association with any of the 24 markers, in total, tested across these genes using single marker analysis or haplotypes of markers across these genes. The results in the present sample indicate that these nine genes are unlikely to be major susceptibility genes contributing to COMD. © 2006 Wiley‐Liss, Inc.

Published

2006

17. Mutation-screen and association analysis of the glucocorticoid receptor gene (NR3C1) in childhood-onset mood disorders (COMD)

Author

Jonathan Mill, Wigg, Karen, Burcescu, Irina, Vetro, Agnes, Kiss, E., Kapornai, K., Tamas, Zsuzsa, Baji, Ildi, Gadoros, Julia, Kennedy, James, Kovacs, Maria, and Barr, Cathy

18. ESCAP CovCAP survey of heads of academic departments to assess the perceived initial (April/May 2020) impact of the COVID-19 pandemic on child and adolescent psychiatry services

Author

Revet, Alexis, Hebebrand, Johannes, Anagnostopoulos, Dimitris, Kehoe, Laura A., Banaschewski, Tobias, Bender, Stephan, Csábi, Györgyi, Çuhadaroğlu, Füsun, Dashi, Elona, Delorme, Richard, Radobuljac, Maja Drobnic, Eliez, Stephan, Krantz, Mette Falkenberg, Fricke, Oliver, Gerstenberg, Miriam, Giannopoulou, Ioanna, Graell, Montserrat, Kumperscak, Hojka Gregoric, Herpertz-Dahlmann, Beate, Huscsava, Mercedes, Kaess, Michael, Kapornai, Krisztina, Karwautz, Andreas, Kresakova, Dominika, Kölch, Michael, Kotsis, Konstantinos, Lazaro, Luisa, Moehler, Eva, Morón-Nozaleda, M. Goretti, Özyurt, Gonca, Pászthy, Bea, Podlipny, Jiri, Purper-Ouakil, Diane, Remberk, Barbara, Serdari, Aspasia, Stene, Lise Eilin, Thun-Hohenstein, Leonhard, Trebaticka, Jana, van West, Dirk, Vitiello, Benedetto, Young, Héloïse, Yurteri, Nihal, Zepf, Florian Daniel, Zielinska-Wieniawska, Anna, Zuddas, Alessandro, Klauser, Paul, COVID-19 Child and Adolescent Psychiatry Consortium, Banaschewski, T., Bender, S., Csábi, G., Çuhadaroğlu, F., Dashi, E., Delorme, R., Radobuljac, M.D., Eliez, S., Krantz, M.F., Fricke, O., Gerstenberg, M., Giannopoulou, I., Graell, M., Kumperscak, H.G., Herpertz-Dahlmann, B., Huscsava, M., Kaess, M., Kapornai, K., Karwautz, A., Kresakova, D., Kölch, M., Kotsis, K., Lazaro, L., Moehler, E., Morón-Nozaleda, M.G., Özyurt, G., Pászthy, B., Podlipny, J., Purper-Ouakil, D., Remberk, B., Serdari, A., Stene, L.E., Thun-Hohenstein, L., Trebaticka, J., van West, D., Vitiello, B., Young, H., Yurteri, N., Zepf, F.D., Zielinska-Wieniawska, A., and Zuddas, A.

Subjects

Telepsychiatry, Adolescent, Adolescent Psychiatry, COVID-19, Child, Humans, Pandemics, Psychiatry, Surveys and Questionnaires, Telemedicine/methods, United Nations, Child and adolescent psychiatry, Europe, 05 social sciences, Medizin, Original Contribution, General Medicine, 030227 psychiatry, 03 medical and health sciences, Psychiatry and Mental health, 0302 clinical medicine, Pediatrics, Perinatology and Child Health, Developmental and Educational Psychology, 0501 psychology and cognitive sciences, Pediatrics, Perinatology, and Child Health, 050104 developmental & child psychology

Abstract

In April 2020, the European Society for Child and Adolescent Psychiatry (ESCAP) Research Academy and the ESCAP Board launched the first of three scheduled surveys to evaluate the impact of the coronavirus disease 2019 (COVID-19) pandemic on child and adolescent psychiatry (CAP) services in Europe and to assess the abilities of CAP centers to meet the new challenges brought on by the crisis. The survey was a self-report questionnaire, using a multistage process, which was sent to 168 heads of academic CAP services in 24 European countries. Eighty-two responses (56 complete) from 20 countries, representing the subjective judgement of heads of CAP centers, were received between mid-April and mid-May 2020. Most respondents judged the impact of the crisis on the mental health of their patients as medium (52%) or strong (33%). A large majority of CAP services reported no COVID-19 positive cases among their inpatients and most respondents declared no or limited sick leaves in their team due to COVID-19. Outpatient, daycare, and inpatient units experienced closures or reductions in the number of treated patients throughout Europe. In addition, a lower referral rate was observed in most countries. Respondents considered that they were well equipped to handle COVID-19 patients despite a lack of protective equipment. Telemedicine was adopted by almost every team despite its sparse use prior to the crisis. Overall, these first results were surprisingly homogeneous, showing a substantially reduced patient load and a moderate effect of the COVID-19 crisis on psychopathology. The effect on the organization of CAP services appears profound. COVID-19 crisis has accelerated the adoption of new technologies, including telepsychiatry. Supplementary Information The online version contains supplementary material available at 10.1007/s00787-020-01699-x.

Published

2022

19. The effect of psychological and behavioral problems on the quality of life of children and adolescents based on self-reports and proxy reports.

Author

Kiss E, de Oliveira OR, Wittmann E, Herczegh Z, and Kapornai K

Subjects

Humans, Male, Female, Adolescent, Child, Surveys and Questionnaires, Self Report, Problem Behavior psychology, Parents psychology, Sex Factors, Age Factors, Quality of Life psychology, Proxy psychology

Abstract

Purpose: Investigations of the quality of life (QoL) of young people have shown that psychological and behavioral problems are associated with lower subjective well-being. The QoL ratings of children and adolescents based on self-reports and proxy reports are significantly different. The aim of the present study was to examine youth self-reported and parent proxy-reported QoL and investigate the effects of age, gender and psychological/behavioral symptoms on the QoL reports of youth. We hypothesized that self-reported emotional and anxiety problems influence self-reported QoL, while proxy-reported behavioral problems influence proxy reports of QoL., Methods: The sample consisted of 284 parent-child pairs. Youths were between the ages of 11 and 18 years, the mean age was 14.3 (SD 2.1) years, and 35.6% were males. The Inventory of Life Quality (ILK) scale was used to measure QoL, and the Strengths and Difficulties Questionnaire was used to assess psychological and behavioral problems., Results: Males had higher self-reported QoL than females, and younger children had better QoL than older children. Emotional peer problems and hyperactivity reported by youth and hyperactivity and conduct problems reported by parents predicted youth self-rated ILK. Only parent-reported psychological/behavioral problems predicted proxy-rated ILK., Conclusion: The evaluation of QoL of children and adolescents should involve both self and proxy reports in order to capture the effects of various psychological/behavioral symptoms and the perspectives of both youth and parents., (© 2024. The Author(s).)

Published

2024

20. Short-Term Blood Pressure Variability among Young Adults at High or Low Risk for Depression.

Author

Nyárády BB, Vértes M, Dósa E, Yang X, George CJ, Kiss E, Baji I, Kapornai K, and Kovacs M

Abstract

Background: Depression has been shown to have adverse effects on blood pressure (BP) and is associated with high blood pressure variability (BPV). In turn, high short-term BPV has been related to eventual cardiovascular risk. But it is not clear how early in adulthood the detrimental effects of depression on BPV may be discerned, if being at high risk for depression also compromises BPV, and whether the clinical features of depression moderate its adverse effects. We investigated these three issues among young adults using an office-like setting. Methods: In total, 218 subjects with a history of childhood-onset major depressive episodes (probands), 206 never-depressed full biological siblings of the probands (high-risk siblings), and 166 emotionally healthy unrelated controls received a psychiatric evaluation and three standardized-sitting BP measurements 5 min apart. Short-term BPV was defined as the maximum difference between measures (range) for each case. The statistical methods included analyses of variance/covariance, chi-square tests, and multiple regression. Results: Systolic and diastolic BP decreased over consecutive measurements ( p < 0.001). After controlling for age, the probands, siblings, and controls did not differ significantly in terms of BPV. However, the number of lifetime depressive episodes did predict the diastolic BP range ( p = 0.005): probands with the highest number of depressive episodes had the largest short-term diastolic BPV. Conclusions: On a group level, the adverse effects on BPV of having experienced or being at high risk for depression are not yet evident during young adulthood. However, the number of major depressive episodes, which is an index of lifetime depression burden, predicts higher BPV. Thus, BPV monitoring for young adults with clinical depression histories could be part of an early intervention program to reduce the risk of eventual cardiovascular disease.

Published

2024

21. Self-Harm in Children and Adolescents Who Presented at Emergency Units During the COVID-19 Pandemic: An International Retrospective Cohort Study.

Author

Wong BH, Cross S, Zavaleta-Ramírez P, Bauda I, Hoffman P, Ibeziako P, Nussbaum L, Berger GE, Hassanian-Moghaddam H, Kapornai K, Mehdi T, Tolmac J, Barrett E, Romaniuk L, Davico C, Moghraby OS, Ostrauskaite G, Chakrabarti S, Carucci S, Sofi G, Hussain H, Lloyd ASK, McNicholas F, Meadowcroft B, Rao M, Csábi G, Gatica-Bahamonde G, Öğütlü H, Skouta E, Elvins R, Boege I, Dahanayake DMA, Anderluh M, Chandradasa M, Girela-Serrano BM, Uccella S, Stevanovic D, Lamberti M, Piercey A, Nagy P, Mehta VS, Rohanachandra Y, Li J, Tufan AE, Mirza H, Rozali F, Baig BJ, Noor IM, Fujita S, Gholami N, Hangül Z, Vasileva A, Salucci K, Bilaç Ö, Yektaş Ç, Cansız MA, Aksu GG, Babatunde S, Youssef F, Al-Huseini S, Kılıçaslan F, Kutuk MO, Pilecka I, Bakolis I, and Ougrin D

Subjects

Child, Humans, Female, Adolescent, Male, Pandemics, Retrospective Studies, Emergency Service, Hospital, COVID-19 epidemiology, Self-Injurious Behavior epidemiology, Self-Injurious Behavior psychology

Abstract

Objective: To compare psychiatric emergencies and self-harm at emergency departments (EDs) 1 year into the pandemic, to early pandemic and pre-pandemic, and to examine the changes in the characteristics of self-harm presentations., Method: This retrospective cohort study expanded on the Pandemic-Related Emergency Psychiatric Presentations (PREP-kids) study. Routine record data in March to April of 2019, 2020, and 2021 from 62 EDs in 25 countries were included. ED presentations made by children and adolescents for any mental health reasons were analyzed., Results: Altogether, 8,174 psychiatric presentations were recorded (63.5% female; mean [SD] age, 14.3 [2.6] years), 3,742 of which were self-harm presentations. Rate of psychiatric ED presentations in March to April 2021 was twice as high as in March to April 2020 (incidence rate ratio [IRR], 1.93; 95% CI, 1.60-2.33), and 50% higher than in March to April 2019 (IRR, 1.51; 95% CI, 1.25-1.81). Rate of self-harm presentations doubled between March to April 2020 and March to April 2021 (IRR, 1.98; 95% CI, 1.68-2.34), and was overall 1.7 times higher than in March to April 2019 (IRR, 1.70; 95% CI, 1.44-2.00). Comparing self-harm characteristics in March to April 2021 with March to April 2019, self-harm contributed to a higher proportion of all psychiatric presentations (odds ratio [OR], 1.30; 95% CI, 1.05-1.62), whereas female representation in self-harm presentations doubled (OR, 1.98; 95% CI, 1.45-2.72) and follow-up appointments were offered 4 times as often (OR, 4.46; 95% CI, 2.32-8.58)., Conclusion: Increased pediatric ED visits for both self-harm and psychiatric reasons were observed, suggesting potential deterioration in child mental health. Self-harm in girls possibly increased and needs to be prioritized. Clinical services should continue using follow-up appointments to support discharge from EDs., Diversity & Inclusion Statement: One or more of the authors of this paper self-identifies as a member of one or more historically underrepresented racial and/or ethnic groups in science. We actively worked to promote inclusion of historically underrepresented racial and/or ethnic groups in science in our author group. While citing references scientifically relevant for this work, we also actively worked to promote inclusion of historically underrepresented racial and/or ethnic groups in science in our reference list. The author list of this paper includes contributors from the location and/or community where the research was conducted who participated in the data collection, design, analysis, and/or interpretation of the work., (Copyright © 2023 American Academy of Child and Adolescent Psychiatry. Published by Elsevier Inc. All rights reserved.)

Published

2023

22. Metabolic syndrome among young adults at high and low familial risk for depression.

Author

Daches S, Vértes M, Matthews K, Dósa E, Kiss E, Baji I, Kapornai K, George CJ, and Kovacs M

Subjects

Humans, Depression epidemiology, Genetic Predisposition to Disease, Risk Factors, Phenotype, Metabolic Syndrome epidemiology, Metabolic Syndrome genetics

Abstract

Background: Our study examined whether the early-onset depression phenotype among young adults (probands) is associated with the metabolic syndrome (MetS) and its components, and if MetS characterizes unaffected but high-risk siblings of probands., Methods: We studied three groups of young adults ( M age = 25 years, s.d. = 3.84 years): probands with histories of childhood onset depression - i.e. early-onset phenotype - ( n = 293), their unaffected siblings (high-risk siblings, n = 273), and healthy controls ( n = 171). Participants completed a full psychiatric interview, physical and laboratory assessments, and self-rating scales. MetS was defined using the criteria of the Expert Panel on Detection, Evaluation, and Treatment of High Blood Cholesterol in Adults ()., Results: Early-onset depression phenotype and being a high-risk sibling were associated with higher MetS composite scores relative to that of controls, but did not differ from one another. With regard to MetS components: Probands and siblings had similarly larger waist circumference and lower HDL than did controls, while siblings and controls had lower triglyceride levels than did probands but did not differ from one another. Groups did not differ on glucose levels and SBP., Conclusions: Our study extends the literature on the association between MetS and depression and underscores the importance of depression phenotypes: failure to account for the clinical heterogeneity of depression may partly underlie the inconsistent findings regarding its relation to MetS. The results also suggest that, in depression-prone populations, MetS may predate and possibly function as a risk factor for eventual depression.

Published

2023

23. Psychophysiological responses to sadness in girls and boys with conduct disorder.

Author

Oldenhof H, Jansen L, Ackermann K, Baker R, Batchelor M, Baumann S, Bernhard A, Clanton R, Dochnal R, Fehlbaum LV, Fernandez-Rivas A, Goergen S, Gonzalez de Artaza-Lavesa M, Gonzalez-Madruga K, Gonzalez-Torres MA, Gundlach M, Lotte van der Hoeven M, Kalogerakis Z, Kapornai K, Kieser M, Konsta A, Martinelli A, Pauli R, Rogers J, Smaragdi A, Sesma-Pardo E, Siklósi R, Steppan M, Tsiakoulia F, Vermeiren R, Vriends N, Werner M, Herpertz-Dahlmann B, Kohls G, De Brito S, Konrad K, Stadler C, Fairchild G, Freitag CM, and Popma A

Subjects

Adolescent, Antisocial Personality Disorder, Emotions physiology, Humans, Sadness, Conduct Disorder, Respiratory Sinus Arrhythmia physiology

Abstract

Reduced responsiveness to emotions is hypothesized to contribute to the development of conduct disorder (CD) in children and adolescents. Accordingly, blunted psychophysiological responses to emotions have been observed in boys with CD, but this has never been tested in girls. Therefore, this study compared psychophysiological responses to sadness in girls and boys with and without CD, and different clinical phenotypes of CD: with versus without limited prosocial emotions (LPE), and with versus without comorbid internalizing disorders (INT). Nine-hundred and 27 girls (427 CD, 500 controls) and 519 boys (266 CD, 253 controls) aged 9-18 years participated. Psychophysiological responses were measured while participants watched two validated sad film clips, specifically: heart rate (HR), respiratory sinus arrhythmia (RSA; indexing parasympathetic activity), preejection period (PEP; indexing sympathetic activity). Girls and boys with CD showed larger HR responses to sadness than controls. This effect was rendered nonsignificant, however, after controlling for covariates. We observed aberrant RSA responses to sadness in CD compared with controls. Similarly, we found a significant positive association between RSA responsivity and antisocial behavior when assessed dimensionally. The effects were very small, though. Results were similar for boys and girls. We found no evidence for emotional underresponsiveness in CD in the largest psychophysiological study to date in this field. More research is needed to explore whether this is specific to sadness or generalizes to other emotions. Furthermore, we recommend that studies on emotion processing in CD assess different physiological measures to help disentangle CD-related effects on sympathetic and parasympathetic activity. (PsycInfo Database Record (c) 2022 APA, all rights reserved).

Published

2022

24. Potential effects of Covid-19 on training in CAP: the balance after a year.

Author

Deschamps P, Bailey S, Dubicka B, Hansen AS, Hebebrand J, Jacobs B, Kapornai K, Klauser P, Kumperscak HG, Revet A, Seker A, Schroder C, and Schumann T

Subjects

Humans, Adolescent Psychiatry education, COVID-19, Child Psychiatry education

Published

2021

25. Childhood-onset depression and arterial stiffness in young adulthood.

Author

Barinas-Mitchell E, Yang X, Matthews KA, Columbus ML, George CJ, Dósa E, Kiss E, Kapornai K, Evans R, and Kovacs M

Subjects

Adult, Child, Depression epidemiology, Humans, Pulse Wave Analysis, Young Adult, Cardiovascular Diseases epidemiology, Depressive Disorder, Major, Vascular Stiffness

Abstract

Objectives: The literature on childhood-onset depression and future compromised vascular function is suggestive but limited. The objective of this study was to determine if arterial stiffness, a predictor of future cardiovascular disease (CVD), measured in young adulthood, is associated with childhood-onset depression., Methods: Cardiometabolic risk factors and pulse wave velocity (PWV), a measure of arterial stiffness, were cross-sectionally assessed in young adults with a history of childhood-onset depression (clinical diagnosis of major depressive episode or dysthymic disorder; N = 294 probands; initially recruited via child mental health facilities across Hungary; mean age of first depressive episode = 10.4 years), their never-depressed full biological siblings (N = 269), and never-depressed controls (N = 169). The mean ages of probands, siblings, and controls at the PWV visit were 25.6, 25.0, and 21.7 years, respectively, and 8.8% of the probands were in a current depressive episode., Results: Controlling for age, sex, age*sex, education, and family clusters, PWV (m/s) did not statistically differ across the groups (probands = 7.01; siblings = 6.98; controls = 6.81). However, after adjusting for key covariates, there were several across-group differences in CVD risk factors: compared to controls, probands and siblings had higher diastolic blood pressure and lower high-density lipoprotein cholesterol, probands had higher triglycerides, and siblings had higher body mass index (all p < 0.05)., Conclusion: We found limited evidence of an association between a history of childhood-onset depression and young adulthood arterial stiffness. However, our findings of elevated cardiovascular risk factors in those with childhood-onset depression suggest that pediatric depression may predispose to increased CVD risk later in life and warrants further investigation., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

26. [Psychometric properties of the Hungarian Adult Attachment Scale].

Author

Őri D, Kapornai K, Baji I, and Kiss E

Subjects

Adult, Factor Analysis, Statistical, Humans, Hungary, Psychometrics, Reproducibility of Results, Surveys and Questionnaires, Young Adult, Depressive Disorder, Major

Abstract

Background and Purpose: The revised Adult Attachment Scale (AAS) developed by N. L. Collins is a widely used questionnaire to measure adult attachment. However, its psychometric properties have not been investigated in Hungary. We aimed to confirm the key psychometric properties of the Hungarian version of the AAS focusing on reliability indices on a population that consis-ted of depressed and non-depressed young adults., Methods: The AAS is a self-report questionnaire, in which two different dimensional evaluating systems are possible: the original (close, depend, and anxiety) and the alternative scoring system (anxiety, avoidance). Our study population consisted of young adults with a history of major depression (n = 264, median age = 25.7 years) and their never-depressed biological siblings (n = 244, median age = 24.0)., Results: The internal consistency of close, anxiety, and avoidance scales were satisfactory (Cronbach-α >0.7). The consistency of the depend scale was slightly lower than expected (Cronbach-α = 0.62). Test-retest reliability was good for all of the scales, it ranged from 0.73 to 0.78 after 14 months of follow-up period. The scale showed good discrimination as tested by the differences of close and anxiety attachment dimensions between the groups (p<0.01). More-over, we were able to differentiate the currently dep-res-sed subjects based on these attachment dimensions. Explo-ra-tory and confirmatory factor analyses were conducted, and a bifactor solution proved optimal model fit., Conclusion: The three dimensions of the AAS has not been confirmed. However, the close and anxiety scales of AAS were found to be adequate. Our results also indicate that attachment features correlate with major depressive episodes in adulthood.

Published

2021

27. [Telemental health service in child and adolescent psychiatry].

Author

Kiss E, Kakuszi S, and Kapornai K

Subjects

Adolescent, Adolescent Psychiatry, Child, Humans, Hungary, Child Psychiatry, Mental Disorders diagnosis, Mental Disorders therapy, Mental Health Services, Telemedicine

Abstract

Introduction: Even though mental disorders present significant health burden worldwide, most patients with mental disorders do not receive adequate healthcare. The possibility of telemental health service came into prominence in Hungary due to the restriciton of face-to-face doctor-patient meetings. The present review, based on the last 20 years' scientific literature, aims to summarize the feasability, efficacy and effectivity of telemedicine services in child and adolescent psychiatry., Method: A review by Gloff et al (17) summarized telepsychiatry service in children and adolescents before 2015. A literature search was generated in order to summarize current knowledge based on 3 international databases (Pubmed, Cochrane Database of Systematic Reviews és Web of Science) for scientific publi - cations after 2015. Search words were telemental health, children, adolescent, and telepsychiatry., Results: International literature showed similar feasability, efficacy and effectivity of evidence based diagnostic and therapeutic methods in tele- child and adolescent psychiatry as in face-to-face services., Conclusion: The application of telemedicine in child and adolescent psychiatry is internationally accepted, feasible and effective. Its widespread use in Hungary would require a professional protocol which specifies the conditions and advices of telemental health services in this age group.

Published

2021

28. [Long-term follow-up of childhood-onset depression - comorbidity, suicidal behavior and prognosis in adulthood].

Author

Kiss E, Baji I, Kellner A, Mayer L, and Kapornai K

Subjects

Adolescent, Adult, Age of Onset, Anxiety Disorders complications, Anxiety Disorders diagnosis, Anxiety Disorders psychology, Child, Comorbidity, Depression complications, Depressive Disorder, Major complications, Female, Follow-Up Studies, Humans, Male, Prognosis, Risk Factors, Young Adult, Depression diagnosis, Depression psychology, Depressive Disorder, Major diagnosis, Depressive Disorder, Major psychology, Suicide psychology

Abstract

Introduction: Several long-term follow-up studies investigate the progression of adolescent onset major depressive disorder but much less explore short and long-term consequences and prognosis into adulthood of childhood- onset depression. The aim of the present study is to follow childhood-onset depression, lifetime comorbid psychiatric disorders and suicidal behavior into adulthood., Methods: Subjects (N=166) were 25.95+2.42 years old on average, 54.2% were women. Follow-up period lasted for a mean of 14.74+1.31 years. Psychiatric diagnosis was assessed by a DSM-IV based semi-structured interview. Subjects reported on 4 stages of suicidal behavior as one of the symptoms of depressive disorder., Results: The onset of the first depressive episode was at the mean age of 10.17+2.34 years. 40,4% of the sample had only 1 episode while recurrent depressive episode presented in 32.5% above 18 years of age. Lifetime comorbid psychiatric disorders were present in more than 1/3 of the sample. The most frequent lifetime comorbidity was anxiety (42.4%), and specific phobia among anxiety disorders. Lifetime attention deficit-hyperactivity disorder and oppositional/conduct disorder were also frequent (25.9% and 16.9%, respectively). Suicidal behavior was not present life-time in 19.1% of the sample. Thoughts of death and thoughts of suicide were quite frequent (80.8% and 69.5%, respectively), specific plans and suicidal attempt were more frequent in girls (plan:female vs male 53.9% vs 38.4%, attempt: 33.3% vs 9.6%) during follow-up., Conclusion: About one-third of childhood-onset depression had recurrence above 18 years of age, which is lower than the recurrence rate for adolescent onset depression. A high rate of lifetime comorbidity was found between depression and anxiety disorders. The assessment of the actual level of suicidal behavior is important in the prevention of selfdestructive behavior.

Published

2020

29. Training for child and adolescent psychiatry in the twenty-first century.

Author

Deschamps P, Hebebrand J, Jacobs B, Robertson P, Anagnostopoulos DC, Banaschewski T, Birkle SM, Dubicka B, Falissard B, Giannopoulou I, Hoekstra PJ, Kaess M, Kapornai K, Klauser P, Revet A, Schröder CM, Seitz J, Şeker A, and Signorini G

Subjects

Adolescent, Adolescent Psychiatry trends, Child, Child Psychiatry trends, Health Workforce, Humans, Specialization trends, Adolescent Psychiatry education, Child Psychiatry education, Forecasting, Mental Health Services trends

Published

2020

30. ["Risk factors of childhood depression" research grant - past, present, future].

Author

Kapornai K, Baji I, Benák I, Dochnal R, Dósa E, Kiss E, Merkely B, Prohászka Z, Szabados E, Varga A, Vetró Á, and Kovács M

Subjects

Biomedical Research organization & administration, Child, Humans, Longitudinal Studies, Risk Factors, Universities organization & administration, Biomedical Research economics, Depression etiology, Depressive Disorder, Major etiology, Financing, Organized trends

Abstract

The authors summarize the last 10 years of an ongoing collaborative study between the Universities of Szeged and Pittsburgh on early onset major depression. First, the "Risk factors of childhood depression" grant is presented briefly as an initial research study in which the subjects of the current studies were recruited. This is a prominently large clinical sample in the field of child psychiatry even on an international level. In addition to the follow-up of the prognosis of the disorder, recent studies continue to explore the early onset depression in two directions. On the one hand, two studies investigate the role of biobehavioral inflexibility markers in the development of major depression ("Biobehavioral inflexibility and risk for juvenile-onset depression" and "Biobehavioral inflexibility and risk for juvenile-onset depression - renewal grant"). On the other hand, the authors would like to have a better understanding of the possible relationship between the major depression and cardiovascular diseases ("Pediatric depression and subsequent cardiac risk factors: a longitudinal study"). The most significant aims of the three studies will be demonstrated, as well as how the studies were prepared and organized along with the already existing experience concerning research management and involvement of new collaborating partners and experts.

Published

2020

31. Emotion Regulation Among Adolescents With Pediatric Depression As a Function of Anxiety Comorbidity.

Author

Dochnal R, Vetró Á, Kiss E, Baji I, Lefkovics E, Bylsma LM, Yaroslavsky I, Rottenberg J, Kovacs M, and Kapornai K

Abstract

Background: Both depression and anxiety (two of the most common internalizing psychopathologies among youths) are associated with difficulties in emotion regulation (ER). Little is known about whether anxiety as a comorbid condition has an effect on the habitual use of different ER strategies in youngsters with depression histories. We aimed 1) to compare ER in adolescents with histories of childhood onset major depressive disorder (MDD) with and without comorbid anxiety and 2) to examine whether certain ER response clusters (Cognitive, Social, and Behavioral/Physical) characterize comorbid children and adolescents. Methods: We analyzed data on 217 youth (11-18 years old) with depression history: 85 subjects with lifetime anxiety comorbidity (comorbid group) and 132 without lifetime anxiety (non-comorbid group). Psychiatric diagnosis was established by a comprehensive Diagnostic and Statistical Manual of Mental Disorders (DSM) IV-based diagnostic procedure. ER strategies were examined via the self-rated "Feelings and Me" Child version questionnaire (FAM-C). Results: The comorbid group used maladaptive ER strategies significantly more frequently than the non-comorbid youngsters. The Behavioral/Physical and Social ER skills, especially those reflecting social withdrawal and self-harm, were responsible for the higher maladaptive scores. Limitations: Because our study is a cross-sectional analysis, we have no information about the development or the onset of maladaptive ER strategies. Therefore, we were unable to examine whether maladaptive ER was a risk factor or a consequence of the internalizing psychopathology and comorbidity. Conclusions: Comorbid anxiety worsens the impaired use of ER strategies in depression-prone youths. Further longitudinal research is needed to explore the causal role of dysfunctional ER in the development of internalizing psychopathology., (Copyright © 2019 Dochnal, Vetró, Kiss, Baji, Lefkovics, Bylsma, Yaroslavsky, Rottenberg, Kovacs and Kapornai.)

Published

2019

32. Relational Aggression in Adolescents with Conduct Disorder: Sex Differences and Behavioral Correlates.

Author

Ackermann K, Kirchner M, Bernhard A, Martinelli A, Anomitri C, Baker R, Baumann S, Dochnal R, Fernandez-Rivas A, Gonzalez-Madruga K, Herpertz-Dahlmann B, Hervas A, Jansen L, Kapornai K, Kersten L, Kohls G, Limprecht R, Lazaratou H, McLaughlin A, Oldenhof H, Rogers JC, Siklósi R, Smaragdi A, Vivanco-Gonzalez E, Stadler C, Fairchild G, Popma A, De Brito SA, Konrad K, and Freitag CM

Subjects

Adolescent, Child, Female, Humans, Male, Adolescent Behavior physiology, Aggression physiology, Child Behavior physiology, Conduct Disorder physiopathology, Empathy physiology, Interpersonal Relations, Sex Characteristics, Social Behavior

Abstract

As most research on conduct disorder (CD) has been conducted on male participants, it has been suggested that female-specific symptoms may be underestimated based on current DSM-5 criteria. In particular, relational aggression, i.e. the hurtful, often indirect, manipulation of relationships with the intention of damaging the other's social position, has been proposed as a characteristic of CD that is more common in females. In addition, sex-specific studies on correlates of relational aggressive behavior are lacking. Relational aggression may be strongly related to the correlates of proactive aggression, namely low affective empathy, and high levels of callous-unemotional (CU) traits and relational victimization. Thus, the present study investigated sex differences in relational aggression, and associations between relational aggression and correlates of proactive aggression in 662 adolescents with CD (403 females) and 849 typically-developing controls (568 females) aged 9-18 years (M = 14.74, SD = 2.34) from the European multi-site FemNAT-CD study. Females with CD showed significantly higher levels of relational aggression compared to males with CD, whereas no sex differences were seen in controls. Relational aggression was only partly related to correlates of proactive aggression in CD: Independent of sex, CU traits showed a positive association with relational aggression. In females only, cognitive, but not affective empathy, was negatively associated with relational aggression. Relational victimization was more strongly associated with relational aggression in males compared to females. Despite interesting sex specific correlates of relational aggression, effects are small and the potential clinical implications should be investigated in future studies.

Published

2019

33. Autonomic correlates of lifetime suicidal thoughts and behaviors among adolescents with a history of depression.

Author

Yang X, Daches S, George CJ, Kiss E, Kapornai K, Baji I, and Kovacs M

Subjects

Adolescent, Adult, Child, Depressive Disorder complications, Female, Humans, Male, Respiratory Sinus Arrhythmia, Stress, Psychological physiopathology, Young Adult, Autonomic Nervous System, Depressive Disorder psychology, Suicidal Ideation

Abstract

Suicidal thoughts and behaviors (STBs) have been associated with emotion dysregulation and atypical responses to affective and stressful stimuli. To investigate the psychophysiology involved, we measured changes in respiratory sinus arrhythmia (RSA) and cardiac pre-ejection period (PEP; indexing parasympathetic and sympathetic functioning, respectively) in response to stressful- and sadness-eliciting laboratory probes. Our sample included adolescents with a history of depression and STBs (n = 177), adolescents with a history of depression but no history of STBs (n = 47), and healthy controls (n = 175). The outcome of interest was the most severe form of clinician-rated STBs across the subject's lifetime. In partial support of our hypotheses, during the stressful task, adolescents with a history of depression and STBs did not evidence the RSA decrease that was exhibited by controls and displayed greater PEP shortening compared to ever-depressed adolescents with no lifetime STBs. No group differences were found in either RSA or PEP reactivity to the sadness-eliciting stimulus. As expected, severity of STBs was positively correlated with the extent of PEP shortening during the stressful task. The results suggest that adolescents with a history of depression and STBs experience blunted parasympathetic responses to stress along with compensatory efforts. Our findings contribute to a better understanding of STBs among youths and underscore that future studies should examine physiological risk factors for these psychopathological outcomes., (© 2019 Society for Psychophysiological Research.)

Published

2019

34. Dysregulated behavioral responses to hedonic probes among youth with depression histories and their high-risk siblings.

Author

Panaite V, Bylsma LM, Kovacs M, O'Leary K, George CJ, Baji I, Benák I, Dochnal R, Kiss E, Vetró Á, Kapornai K, and Rottenberg J

Subjects

Adolescent, Child, Female, Happiness, Humans, Male, Child Behavior psychology, Depression psychology, Sadness psychology, Siblings psychology

Abstract

Affect dysregulation in response to rewarding stimuli has been proposed as a vulnerability factor for major depressive disorder (MDD). However, it remains unclear how affective behavioral dynamics may be altered among individuals who are at high risk for depression but not currently depressed. We examined the dynamics of affective facial behavior during hedonic probes among 3 groups of adolescents: remitted probands who had histories of childhood-onset MDD (n = 187), never-depressed siblings of probands (high familial risk; n = 207), and healthy controls (n = 166). Participants' happy and sad facial expressions were coded during 3 hedonic laboratory tasks: receiving a preferred prize, describing a positive autobiographical memory, and watching a humorous film. Happy and sad behavioral dynamics were indexed by mean level- and time-dependent reactivity, variability (mean of the squared successive differences), and inertia (autocorrelation). Relative to controls, probands and siblings exhibited a more rapid decrease in happy behaviors, and probands exhibited higher inertia of sad behaviors during hedonic probes. Both probands and siblings exhibited lower inertia of sad behaviors while receiving a desired prize, which highlights the importance of context variation in testing hypotheses. Overall, our study provides new evidence that hedonic behavioral dysregulation, as reflected in dynamic facial behavior, may highlight depression vulnerability. (PsycINFO Database Record (c) 2019 APA, all rights reserved).

Published

2019

35. The Development of Mood Repair Response Repertories: I. Age-Related Changes Among 7- to 14-Year-Old Depressed and Control Children and Adolescents.

Author

Kovacs M, Lopez-Duran NL, George C, Mayer L, Baji L, Kiss E, Vetró Á, and Kapornai K

Subjects

Adolescent, Age Factors, Child, Depressive Disorder, Major diagnosis, Depressive Disorder, Major therapy, Diagnostic and Statistical Manual of Mental Disorders, Female, Humans, Male, Adaptation, Psychological physiology, Affect physiology, Depressive Disorder, Major psychology, Parents psychology, Sadness physiology, Sadness psychology

Abstract

The purpose of this study was to test developmentally informed hypotheses about regulatory responses to sadness that attenuate versus exacerbate it (adaptive versus maladaptive mood repair responses, respectively) across late childhood, early adolescence, and mid-adolescence. In a multi-site study in Hungary, clinic-based, 7- to 14-year-olds with Diagnostic and Statistical Manual of Mental Disorders' (4th ed., text rev.) depressive disorders (N = 697; 55% male) and age/sex matched (at 1:2) nondepressed, school-based controls (N = 1,394) reported on their usual responses to sadness/dysphoria; parental reports were obtained separately. Adaptive and maladaptive response repertoire scores were compared across ages within and across subject groups, and by informant, controlling for confounds. Contrary to Hypothesis 1, older (vs. younger) youths in both groups reported fewer adaptive regulatory responses. Maladaptive response repertoires were unrelated to age among controls but significantly increased with age among depressed youths, particularly the girls. Partially supporting Hypothesis 2, subject groups differed in age-related trajectories of mood repair repertories, but not as expected (e.g., younger depressed children reported larger adaptive response repertoires than did controls). Parental reports revealed no developmental changes in offspring's mood repair repertories. Parent-offspring reports were most discordant for younger (vs. older) offspring, tended to converge around age 11, and were consistently and significantly larger in the depressed sample. Self-reported adaptive mood repair repertories appear to have been laid down by late childhood and then undergo "trimming" across ages 7-14 years. The extensive maladaptive mood repair response repertoires of depressed youths, which increased with age, distinguish them primarily from controls. Therefore, reducing maladaptive regulatory responses to sadness should be a priority when treating depressed youths.

Published

2019

36. Childhood adversity predicts reduced physiological flexibility during the processing of negative affect among adolescents with major depression histories.

Author

Daches S, Kovacs M, George CJ, Yaroslavsky I, Kiss E, Vetró Á, Dochnal R, Benák I, Baji I, Halas K, Makai A, Kapornai K, and Rottenberg J

Subjects

Adolescent, Child, Female, Follow-Up Studies, Humans, Male, Affect physiology, Depressive Disorder, Major physiopathology, Parasympathetic Nervous System physiopathology, Respiratory Sinus Arrhythmia physiology, Stress, Psychological physiopathology

Abstract

Background: Adversity during early development has been shown to have enduring negative physiological consequences. In turn, atypical physiological functioning has been associated with maladaptive processing of negative affect, including its regulation. The present study therefore explored whether exposure to adverse life events in childhood predicted maladaptive (less flexible) parasympathetic nervous system functioning during the processing of negative affect among adolescents with depression histories., Methods: An initially clinic-referred, pediatric sample (N=189) was assessed at two time points. At Time 1, when subjects were 10.17years old (SD=1.42), on average, and were depressed, parents reported on adverse life events the offspring experienced up to that point. At Time 2, when subjects were 17.18years old (SD=1.28), and were remitted from depression, parents again reported on adverse life events in their offspring's lives for the interim period. At time 2, subjects' parasympathetic nervous system functioning (quantified as respiratory sinus arrhythmia) also was assessed at rest, during sad mood induction, and during instructed mood repair., Results: Extent of adverse life events experienced by T1 (but not events occurring between T1 and T2) predicted less flexible RSA functioning 7years later during the processing of negative affect. Adolescents with more extensive early life adversities exhibited less vagal withdrawal following negative mood induction and tended to show less physiological recovery following mood repair., Conclusions: Early adversities appear to be associated with less flexible physiological regulatory control during negative affect experience, when measured later in development. Stress-related autonomic dysfunction in vulnerable youths may contribute to the unfavorable clinical prognosis associated with juvenile-onset depression., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

37. Positive autobiographical memory deficits in youth with depression histories and their never-depressed siblings.

Author

Begovic E, Panaite V, Bylsma LM, George C, Kovacs M, Yaroslavsky I, Baji I, Benák I, Dochnal R, Kiss E, Vetró Á, Kapornai K, and Rottenberg J

Subjects

Adolescent, Child, Female, Humans, Male, Siblings, Depression psychology, Memory, Episodic, Mental Recall physiology

Abstract

Objectives: Impaired positive autobiographical memory (AM) is closely linked to emotional disorders. AM impairments are often found in depressed adults and may be related to the difficulties such persons have in regulating their dysphoric mood. By contrast, less is known about AM disturbances among adolescents, or about the functional relationship of AM disturbances to early-onset depression., Design: A high-risk family design served to compare four groups of youth who differed in depression histories and familial depression risk., Methods: Thirty-one currently depressed probands, 185 remitted probands, 204 never-depressed siblings of probands, and 180 healthy control youth were induced into a negative mood prior to recalling positive AMs via a novel memory elicitation procedure. Several positive AM characteristics were assessed., Results: Relative to control youth, unaffected siblings and probands exhibited consistently impaired positive AMs. Moreover, we also found some evidence that probands were more impaired than siblings, who were in turn more impaired than controls, consistent with a gradient effect., Conclusions: Positive AM disturbances may not only precede the onset of depression in vulnerable youth, but also continue to persist after remission of a depressive episode. Clinical and basic research implications of the findings are discussed., Practitioner Points: Positive AM impairments may be trait-like, persist in the euthymic phase of depression, and may serve as a risk marker for early-onset depression among vulnerable adolescents. Disturbances in positive AM may negatively impact the mood-regulatory functions of positive memory recall and contribute to persistent sadness and anhedonia, which are core features of depression. Our sample of currently depressed youth was relatively small, tempering our conclusions. Although we collected data on some important covariates (e.g., socioeconomic status), we lacked information on other relevant variables such as youths' executive functioning or IQ., (© 2017 The British Psychological Society.)

Published

2017

38. Positive Affectivity is Dampened in Youths with Histories of Major Depression and Their Never-Depressed Adolescent Siblings.

Author

Kovacs M, Bylsma LM, Yaroslavsky I, Rottenberg J, George CJ, Kiss E, Halas K, Benák I, Baji I, Vetro Á, and Kapornai K

Abstract

While hedonic capacity is diminished during clinical depression, it is unclear whether that deficit constitutes a risk factor and/or persists after depression episodes remit. To examine these issues, adolescents with current/past major depression (probands; n=218), never depressed biological siblings of probands (n=207), and emotionally-well controls (n=183) were exposed to several positively valenced probes. Across baseline and hedonic probe conditions, controls consistently reported higher levels of positive affect than high-risk siblings, and siblings reported higher levels of positive affect than probands (remitted and depressed probands' reports were similar). Extent of positive affect across the protocol predicted adolescents' self-reports of social support network and parental reports of offspring's use of various adaptive mood repair responses in daily life. Attenuated hedonic responding among youths remitted from depression offers partial support for anhedonia as a trait, while its presence among never depressed high-risk siblings argues for anhedonia as a potential diathesis for clinical depression.

Published

2016

39. Parasympathetic nervous system activity predicts mood repair use and its effectiveness among adolescents with and without histories of major depression.

Author

Yaroslavsky I, Rottenberg J, Bylsma LM, Jennings JR, George C, Baji I, Benák I, Dochnal R, Halas K, Kapornai K, Kiss E, Makai A, Varga H, Vetró Á, and Kovacs M

Subjects

Adolescent, Depressive Disorder, Major psychology, Electrocardiography, Female, Heart Rate physiology, Humans, Male, Respiratory Sinus Arrhythmia physiology, Affect physiology, Depressive Disorder, Major physiopathology, Emotions physiology, Parasympathetic Nervous System physiopathology

Abstract

Depressive disorders that onset in the juvenile years have been linked to far-reaching adverse consequences, making it imperative to elucidate key mechanisms and contributory factors. Excessive use of regulatory responses that exacerbate sadness (maladaptive mood repair) or insufficient use of regulatory responses that reduce it (adaptive mood repair) may reflect behavioral mechanisms of depression risk. Cardiac vagal control, indexed by patterns of respiratory sinus arrhythmia (RSA), has received attention as a putative physiological risk factor for depression. Although mood repair and RSA are related, the nature of this relationship is not well characterized in the context of depression risk. Therefore, we tested alternative models of the relationships between RSA patterns (at rest and in response to a sad film), trait mood repair, and the effectiveness of a mood repair response in the laboratory (state mood repair) among adolescents with depression histories (n = 210) and emotionally healthy peers (n = 161). In our data, a mediation model best explained the association between the key constructs: Adolescents with normative RSA patterns exhibited lower levels of depression and trait maladaptive mood repair, and benefited more from instructed (state) mood repair in the laboratory. By contrast, adolescents with atypical RSA patterns exhibited higher levels of depression and dispositional maladaptive mood repair, which, in turn, mediated the relations of RSA patterns and depression symptoms. Atypical RSA patterns also predicted reduced benefits from laboratory mood repair., ((c) 2016 APA, all rights reserved).)

Published

2016

40. Familiality of mood repair responses among youth with and without histories of depression.

Author

Bylsma LM, Yaroslavsky I, Rottenberg J, Kiss E, Kapornai K, Halas K, Dochnal R, Lefkovics E, Baji I, Vetrό Á, and Kovacs M

Subjects

Adolescent, Case-Control Studies, Child, Female, Humans, Male, Parents psychology, Siblings psychology, Young Adult, Adaptation, Psychological, Affect, Depressive Disorder, Major psychology

Abstract

Affect regulation skills develop in the context of the family environment, wherein youths are influenced by their parents', and possibly their siblings', regulatory responses and styles. Regulatory responses to sadness (mood repair) that exacerbate or prolong dysphoria (maladaptive mood repair) may represent one way in which depression is transmitted within families. We examined self-reported adaptive and maladaptive mood repair responses across cognitive, social and behavioural domains in Hungarian 11- to 19-year-old youth and their parents. Offspring included 214 probands with a history of childhood-onset depressive disorder, 200 never depressed siblings and 161 control peers. Probands reported the most problematic mood repair responses, with siblings reporting more modest differences from controls. Mood repair responses of parents and their offspring, as well as within sib-pairs, were related, although results differed as a function of the regulatory response domain. Results demonstrate familiality of maladaptive and adaptive mood repair responses in multiple samples. These familial associations suggest that relationships with parents and siblings within families may impact the development of affect regulation in youth.

Published

2016

41. BDNF Val66Met polymorphism and stressful life events in melancholic childhood-onset depression.

Author

Rimay T, Benak I, Kiss E, Baji I, Feher A, Juhasz A, Strauss J, Kennedy J, Barr C, Kovacs M, Vetro A, and Kapornai K

Subjects

Adolescent, Age of Onset, Child, Depressive Disorder, Major epidemiology, Female, Humans, Hungary epidemiology, Male, Methionine genetics, Polymorphism, Single Nucleotide, Valine genetics, Brain-Derived Neurotrophic Factor genetics, Depressive Disorder, Major genetics, Depressive Disorder, Major psychology, Life Change Events

Abstract

Introduction: Brain-derived neurotrophic factor (BDNF) polymorphisms have been examined for their contribution toward depression with equivocal results. More homogeneous phenotypes might be used to improve our understanding of genetic liability to depression. The aim of our study was to (a) test for an association between the BDNF Val66Met polymorphism and childhood-onset melancholic depression and (b) to examine the interactive effects of stressful life events (SLE) and the Val66Met polymorphism on the risk of childhood-onset melancholic depression., Materials and Methods: A total of 583 depressed probands were involved in this study (162 of the melancholic subtype). Diagnoses were derived through the Interview Schedule for Children and Adolescents - Diagnostic Version and life event data were collected using an Intake General Information Sheet., Results: Overall, 27.8% of the participants fulfilled the criteria for melancholy. In the melancholic group, the proportion of females was higher (53.1%), although there were more males in the overall depressed sample. We detected no significant differences in genotype or allele frequency between the melancholic and the nonmelancholic depressed group. The BDNF Val66Met polymorphism and SLE interaction was not significantly associated with the melancholy outcome., Conclusion: In our study, females were more prone to developing the early-onset melancholic phenotype. To our knowledge, this is the first study to investigate the differentiating effect of the genotype and the G×E interaction on the melancholic phenotype in a large sample of depressed young patients. We did not find an association between the melancholic subtype of major depression and the BDNF genotype and SLE interaction in this sample, which is representative of the Hungarian clinic-referred population of depressed youths.

Published

2015

42. Mood repair via attention refocusing or recall of positive autobiographical memories by adolescents with pediatric-onset major depression.

Author

Kovacs M, Yaroslavsky I, Rottenberg J, George CJ, Baji I, Benák I, Dochnal R, Halas K, Kiss E, Vetró Á, and Kapornai K

Subjects

Adolescent, Adult, Age of Onset, Child, Female, Humans, Male, Young Adult, Attention physiology, Depressive Disorder, Major physiopathology, Memory, Episodic, Mental Recall physiology

Abstract

Background: Impaired emotion regulation is increasingly recognized as a core feature of depressive disorders. Indeed, currently and previously depressed adults both report greater problems in attenuating sadness (mood repair) in daily life than healthy controls. In contrast, studies of various strategies to attenuate sad affect have mostly found that currently or previously depressed adults and controls were similarly successful at mood repair in the laboratory. But few studies have examined mood repair among depression-prone youths or the effects of trait characteristics on mood repair outcomes in the laboratory., Methods: Adolescents, whose first episode of major depressive disorder (MDD) had onset at age 9, on average (probands), and were either in remission or depressed, and control peers, watched a sad film clip. Then, they were instructed to engage in refocusing attention (distraction) or recalling happy memories. Using affect ratings provided by the youths, we tested two developmentally informed hypotheses about whether the subject groups would be similarly able to attenuate sadness via the two mood repair strategies. We also explored if self-reported habitual (trait) mood repair influenced laboratory performance., Results: Contrary to expectations, attention refocusing and recall of happy memories led to comparable mood benefits across subjects. Control adolescents reported significantly greater reductions in sadness than did depressed (Cohen's d = .48) or remitted (Cohen's d = .32) probands, regardless of mood repair strategy, while currently depressed probands remained the saddest after mood repair. Habitual mood repair styles moderated the effects of instructed (state) mood repair in the laboratory., Conclusions: Whether depressed or in remission, adolescents with MDD histories are not as efficient at mood repair in the laboratory as controls. But proband-control group differences in mood repair outcomes were modest in scope, suggesting that the abilities that subserve affect regulation have been preserved in probands to some degree. Further information about the nature of mood repair problems among youths with depression histories would help to better understand the clinical course of MDD and to design personalized interventions for depression., (© 2015 Association for Child and Adolescent Mental Health.)

Published

2015

43. Juvenile onset depression alters cardiac autonomic balance in response to psychological and physical challenges.

Author

Bylsma LM, Yaroslavsky I, Rottenberg J, Jennings JR, George CJ, Kiss E, Kapornai K, Halas K, Dochnal R, Lefkovics E, Benák I, Baji I, Vetró Á, and Kovacs M

Subjects

Adolescent, Age of Onset, Case-Control Studies, Female, Hand Strength, Heart Rate physiology, Humans, Male, Autonomic Nervous System physiopathology, Depressive Disorder physiopathology, Task Performance and Analysis

Abstract

Cardiac autonomic balance (CAB) indexes the ratio of parasympathetic to sympathetic activation (Berntson, Norman, Hawkley, & Cacioppo, 2008), and is believed to reflect overall autonomic flexibility in the face of environmental challenges. However, CAB has not been examined in depression. We examined changes in CAB and other physiological variables in 179 youth with a history of juvenile onset depression (JOD) and 161 healthy controls, in response to two psychological (unsolvable puzzle, sad film) and two physical (handgrip, and forehead cold pressor) challenges. In repeated measures analyses, controls showed expected reductions in CAB for both the handgrip and unsolvable puzzle, reflecting a shift to sympathetic relative to parasympathetic activation. By contrast, JOD youth showed increased CAB from baseline for both tasks (p's<.05). No effects were found for the forehead cold pressor or sad film tasks, suggesting that CAB differences may arise under conditions requiring greater attentional control or sustained effort., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2015

44. The association between major depressive disorder in childhood and risk factors for cardiovascular disease in adolescence.

Author

Rottenberg J, Yaroslavsky I, Carney RM, Freedland KE, George CJ, Baji I, Dochnal R, Gádoros J, Halas K, Kapornai K, Kiss E, Osváth V, Varga H, Vetró A, and Kovacs M

Subjects

Adolescent, Adult, Age of Onset, Cardiovascular Diseases genetics, Child, Epidemiologic Methods, Exercise physiology, Female, Humans, Male, Middle Aged, Obesity epidemiology, Parents, Sedentary Behavior, Siblings, Smoking epidemiology, Cardiovascular Diseases epidemiology, Depressive Disorder, Major epidemiology, Family Health statistics & numerical data, Genetic Predisposition to Disease epidemiology

Abstract

Objective: Depression in adults is associated with risk factors for cardiovascular disease (CVD). It is unclear, however, when the association between clinical depression and cardiac risk factors develops or how early in life this association can be detected., Methods: In an ongoing study of pediatric depression, we compared CVD risk factors including smoking, obesity, physical activity level, sedentary behavior, and parental history of CVD across three samples of adolescents: probands with established histories of childhood-onset major depressive disorder (n = 210), never-depressed siblings of probands (n = 195), and controls with no history of any major psychiatric disorder (n = 161)., Results: When assessed during adolescence, 85% of the probands were not in a major depressive episode. Nevertheless, at that assessment, probands had a higher prevalence of regular smoking (odds ratio [OR] = 12.54, 95% confidence interval [CI] = 4.36-36.12) and were less physically active than controls (OR = 0.59, CI = 0.43-0.81) and siblings (OR = 0.70, CI = 0.52-0.94) and had a higher rate of obesity than did controls (OR = 3.67, CI = 1.42-9.52). Parents of probands reported high rates of CVD (significantly higher than did parents of controls), including myocardial infarction and CVD-related hospitalization (ORs = 1.62-4.36, CIs = 1.03-15.40). Differences in CVD risk factors between probands and controls were independent of parental CVD., Conclusions: Major depression in childhood is associated with an unfavorable CVD risk profile in adolescence, and risks for pediatric depression and CVD may coincide in families. Effective prevention and treatment of childhood depression may be a means to reduce the incidence of adult CVD.

Published

2014

45. No association between oxytocin or prolactin gene variants and childhood-onset mood disorders.

Author

Strauss JS, Freeman NL, Shaikh SA, Vetró A, Kiss E, Kapornai K, Daróczi G, Rimay T, Kothencné VO, Dombovári E, Kaczvinszk E, Tamás Z, Baji I, Besny M, Gádoros J, DeLuca V, George CJ, Dempster E, Barr CL, Kovacs M, and Kennedy JL

Subjects

Adolescent, Age of Onset, Child, Family, Female, Gene Frequency, Genetic Association Studies, Genetic Predisposition to Disease, Humans, Male, Mood Disorders epidemiology, Receptors, Oxytocin genetics, Receptors, Prolactin genetics, Mood Disorders genetics, Oxytocin genetics, Polymorphism, Single Nucleotide, Prolactin genetics

Abstract

Background: Oxytocin (OXT) and prolactin (PRL) are neuropeptide hormones that interact with the serotonin system and are involved in the stress response and social affiliation. In human studies, serum OXT and PRL levels have been associated with depression and related phenotypes. Our purpose was to determine if single nucleotide polymorphisms (SNPs) at the loci for OXT, PRL and their receptors, OXTR and PRLR, were associated with childhood-onset mood disorders (COMD)., Methods: Using 678 families in a family-based association design, we genotyped 16 SNPs at OXT, PRL, OXTR and PRLR to test for association with COMD., Results: No significant associations were found for SNPs in the OXTR, PRL, or PRLR genes. Two of three SNPs 3' of the OXT gene were associated with COMD (p≤0.02), significant after spectral decomposition, but were not significant after additionally correcting for the number of genes tested. Supplementary analyses of parent-of-origin and proband sex effects for OXT SNPs by Fisher's Exact test were not significant after Bonferroni correction., Conclusions: We have examined 16 OXT and PRL system gene variants, with no evidence of statistically significant association after correction for multiple tests., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2010

46. No evidence of an association between two genes, EDN1 and ACE, and childhood-onset mood disorders.

Author

Dempster EL, Kiss E, Kapornai K, Daróczi G, Mayer L, Baji I, Tamas Z, Gadoros J, Kennedy JL, Vetró A, Kovacs M, and Barr CL

Subjects

Age of Onset, Child, Humans, Polymorphism, Single Nucleotide, Endothelin-1 genetics, Mood Disorders genetics, Peptidyl-Dipeptidase A genetics

Abstract

Recent evidence supports a pathological link between heart disease and depressive symptoms, suggesting that depression is both etiologic and prognostic to heart disease. Thus, biological molecules which are at the interface between heart and mind are plausible candidate genes for depressive disorders. To investigate this line of enquiry we have investigated two genes, Endothelin 1 (EDN1) and Angiotensin-converting enzyme (ACE) in a family-based sample with childhood-onset mood disorders (COMDs). EDN1 is highly expressed in endothelium where it acts as a potent vasoconstrictor, and is also expressed in the brain where it exhibits neurotransmitter characteristics. ACE acts as a potent vasopressor, and interacts with the hypothalamic-pituitary-adrenocortical (HPA) system, which is often dysregulated in mood disorders. Furthermore, ACE has recently been found to be associated with major depression. Polymorphisms were selected to best capture the genetic variation at the two loci, and to replicate previous associations. The markers were genotyped across EDN1 and ACE in a sample comprised of 382 Hungarian nuclear families ascertained through affected probands diagnosed with a mood disorders before the age of 15. We found no evidence of association between either of these genes and COMD. Consequently, we were unable to support our hypothesis that these two genes, which are involved in both vascular and brain functions are contributing to the susceptibility to mood disorders of children/adolescents., ((c) 2009 Wiley-Liss, Inc.)

Published

2010

47. G72/G30 (DAOA) and juvenile-onset mood disorders.

Author

Gomez L, Wigg K, Feng Y, Kiss E, Kapornai K, Tamás Z, Mayer L, Baji I, Daróczi G, Benák I, Kothencné VO, Dombovári E, Kaczvinszk E, Besnyo M, Gádoros J, King N, Székely J, Kovacs M, Vetró A, Kennedy JL, and Barr CL

Subjects

Adolescent, Age of Onset, Child, Gene Expression Regulation, Gene Frequency genetics, Genetic Predisposition to Disease, Humans, Hungary epidemiology, Linkage Disequilibrium genetics, Meta-Analysis as Topic, Mood Disorders epidemiology, Polymorphism, Single Nucleotide genetics, D-Amino-Acid Oxidase genetics, Mood Disorders enzymology, Mood Disorders genetics

Abstract

The chromosome 13q region has been linked to bipolar disorder in a number of genome scans as well as focused linkage studies. Previously we identified linkage to the 13q32 region in a genome scan of 146 affected sibling pair families from Hungary with juvenile-onset mood disorders. Within this region are the overlapping genes G72/G30, with G72 now officially named as D-amino-acid oxidase activator (DAOA). This locus has been associated with panic disorder, schizophrenia, and bipolar disorder. In this study, we tested for association to 11 markers in these genes and mood disorders in a sample of 646 nuclear families identified with a proband with onset of a mood disorder before 14.9 years of age. We identified evidence for association to three markers within the gene (rs2391191, rs3918341, rs1935062), two of which had been associated with bipolar disorder in previous studies. When corrected for the number of markers tested, the results were no longer significant, however the prior evidence for association of this gene in multiple studies points to this gene as a potential contributor to juvenile-onset mood disorders., ((c) 2008 Wiley-Liss, Inc.)

Published

2009

48. Age and sex analyses of somatic complaints and symptom presentation of childhood depression in a Hungarian clinical sample.

Author

Baji I, Lopez-Duran NL, Kovacs M, George CJ, Mayer L, Kapornai K, Kiss E, Gádoros J, and Vetró A

Subjects

Adolescent, Affective Symptoms diagnosis, Affective Symptoms psychology, Age Factors, Child, Comorbidity, Depressive Disorder, Major psychology, Diagnostic and Statistical Manual of Mental Disorders, Female, Humans, Hungary epidemiology, Male, Models, Psychological, Multivariate Analysis, Psychiatric Status Rating Scales statistics & numerical data, Psychometrics, Psychomotor Agitation diagnosis, Psychomotor Agitation psychology, Sex Factors, Sleep Initiation and Maintenance Disorders diagnosis, Sleep Initiation and Maintenance Disorders psychology, Somatoform Disorders psychology, Depressive Disorder, Major diagnosis, Depressive Disorder, Major epidemiology, Somatoform Disorders diagnosis, Somatoform Disorders epidemiology

Abstract

Objective: To determine whether the symptom presentation of major depressive disorder (MDD) in a large clinical sample of youngsters is influenced by age, sex, and the interaction of age and sex., Method: The sample included 559 children (mean age = 11.69 years; range, 7-14 years; 247 girls) with MDD recruited from 23 mental health facilities across Hungary. Psychiatric evaluations were conducted via the semistructured Interview Schedule for Children and Adolescents-Diagnostic Version (ISCA-D). Final DSM-IV diagnoses were rendered via the best-estimate diagnostic procedure. Evaluations were conducted between April 2000 and May 2005., Results: Six depression symptoms increased with age: depressed mood (odds ratio [OR] = 1.10, P < .05), hypersomnia (OR = 1.17, P < .05), psychomotor retardation (OR = 1.11 P < .05), fatigue (OR = 1.13, P < .01), thoughts of death (OR = 1.11, P < .05), and suicidal ideation (OR = 1.18, P < .01), while psychomotor agitation decreased with age (OR = 0.91, P < .05). Boys were less likely to evidence anhedonia (OR = 0.67, P < .05), insomnia (OR = 0.68, P < .05), and hypersomnia (OR = 0.56, P < .05) but more likely to have psychomotor agitation (OR = 1.59, P < .01). There were no age-by-sex interactions. Rates of somatic complaints did not decrease with age (OR = 1.01, P > .05)., Conclusions: The symptom presentation of MDD becomes somewhat more neurovegetative as children get older. However, girls display more affective and atypical symptoms across all age groups. Somatic complaints were common regardless of age and should be considered an associated feature of depression in children and adolescents., (Copyright 2009 Physicians Postgraduate Press, Inc.)

Published

2009

49. Further genetic evidence implicates the vasopressin system in childhood-onset mood disorders.

Author

Dempster EL, Burcescu I, Wigg K, Kiss E, Baji I, Gadoros J, Tamás Z, Kapornai K, Daróczy G, Kennedy JL, Vetró A, Kovacs M, and Barr CL

Subjects

Adolescent, Age of Onset, Family Health, Female, Gene Frequency, Genotype, Humans, Male, Arginine Vasopressin genetics, Genetic Predisposition to Disease, Mood Disorders genetics, Polymorphism, Single Nucleotide genetics

Abstract

Studies in both animals and humans advocate a role for the vasopressin (AVP) system in the aetiology of depressive symptoms. Attention has particularly focused on the role of AVP in the overactivation of the hypothalamic-pituitary-adrenal (HPA)-axis in mood disorders. Elevated AVP plasma levels have been found in mood disorder patients, which are often positively correlated with the severity of symptoms. We recently reported an association between childhood-onset mood disorders (COMD) and polymorphisms in the receptor responsible for the AVP-mediated activation of the HPA-axis (AVPR1B). As genetic variation in the vasopressinergic system could provide a mechanism to explain the endocrine alterations observed in mood disorders, we investigated other genes in this system. The gene encoding AVP is the strongest candidate, particularly as genetic variation in this gene in rodents is associated with anxiety-related behaviours. Six single-nucleotide polymorphisms (SNPs) were genotyped across the AVP gene in a sample comprised of 586 Hungarian nuclear families ascertained through affected probands with a diagnosis of COMD. In addition, AVP coding and putative regulatory regions were screened for mutations using denaturing high-performance liquid chromatography. One SNP, 3' to the AVP, gene reached significance (P = 0.03), as did the overtransmission of a five-marker haplotype with a frequency of 22% (P = 0.0001). The subsequent mutation screen failed to identify any putative functional polymorphisms. The outcome of this study, combined with our previous association between COMD and AVPR1B, implicates genetic variation in vasopressinergic genes in mediating vulnerability to COMD.

Published

2009

50. Mutation screen and association analysis of the glucocorticoid receptor gene (NR3C1) in childhood-onset mood disorders (COMD).

Author

Mill J, Wigg K, Burcescu I, Vetró A, Kiss E, Kapornai K, Tamás Z, Baji I, Gádoros J, Kennedy JL, Kovacs M, and Barr CL

Subjects

Adult, Age of Onset, Child, Chromatography, High Pressure Liquid, Female, Genetic Predisposition to Disease, Genotype, Haplotypes, Humans, Hungary, Linkage Disequilibrium, Male, Nuclear Family, Polymerase Chain Reaction, Polymorphism, Genetic, Promoter Regions, Genetic, Receptors, Glucocorticoid chemistry, Sequence Analysis, DNA, DNA Mutational Analysis, Mood Disorders genetics, Receptors, Glucocorticoid genetics

Abstract

Depressive disorders are highly heterogeneous psychiatric disorders involving deficits to cognitive, psychomotor, and emotional processing. Considerable evidence links disruption to the hypothalamic-pituitary-adrenal (HPA) axis to the etiology of depression, with specific deficits reported in glucocorticoid receptor (GR)-mediated negative feedback. Given the role of GR-mediated negative feedback in mediating response to stress, and the clear link between stress and depression, it is plausible that polymorphisms in the GR gene (NR3C1) act to increase susceptibility. Maternal behavior in rats epigenetically alters a NGF1-A transcription factor binding-site in the promoter region of the GR gene, providing a mechanism by which environmental cues can regulate GR expression and thus response to stress. The analogous region of the human GR gene (NR3C1) has not been studied, but it is possible that polymorphisms in this region may alter the binding of transcription factors known to regulate GR expression. In this study, we have performed bioinformatic analyses on the promoter region of NR3C1 to identify conserved promoter sequences and predicted transcription factor binding sites. These regions were screened with denaturing high-performance liquid chromatography (DHPLC) and direct re-sequencing, and several novel polymorphic variants were identified. We genotyped nine polymorphisms across NR3C1 in a large sample of Hungarian nuclear families ascertained through affected probands with a diagnosis of childhood-onset mood disorders (COMD). Single-marker analysis provided little evidence for an association of this gene with COMD, but multi-marker analysis across a region of high linkage disequilibrium revealed modest evidence for the biased transmission of several haplotypes., ((c) 2008 Wiley-Liss, Inc.)

Published

2009