Living with Epilepsy in Adolescence in Italy: Psychological and Behavioral Impact
by
,
Katherine Turner
1,*, 
Francesca La Briola
1,
Aglaia Vignoli
1,2,
Elena Zambrelli
1,
Valentina Chiesa
1,
Laura Fongoni
1,
Olivia Baldi
1 and
Maria Paola Canevini
1,2 1
Epilepsy Center, Childhood and Adolescence Neuropsychiatry Unit, ASST Santi Paolo e Carlo, San Paolo Hospital, 20142 Milan, Italy
2
Department of Health Sciences, University of Milan, 20142 Milan, Italy
*
Author to whom correspondence should be addressed.
Healthcare 2023, 11(5), 687; https://doi.org/10.3390/healthcare11050687
Submission received: 12 December 2022
/
Revised: 10 February 2023
/
Accepted: 22 February 2023
/
Published: 25 February 2023
(This article belongs to the Special Issue Clinical and Dynamic Psychology in Medical Settings: The Patient-Centered Care)
Abstract
:Background: People with epilepsy have a higher prevalence of behavioral and neuropsychiatric comorbidities compared to the general population and those with other chronic medical conditions, although the underlying clinical features remain unclear. The goal of the current study was to characterize behavioral profiles of adolescents with epilepsy, assess the presence of psychopathological disorders, and investigate the reciprocal interactions among epilepsy, psychological functioning, and their main clinical variables. Methods: Sixty-three adolescents with epilepsy were consecutively recruited at the Epilepsy Center, Childhood and Adolescence Neuropsychiatry Unit of Santi Paolo e Carlo hospital in Milan (five of them were excluded) and assessed with a specific questionnaire for psychopathology in adolescence, such as the Questionnaire for the Assessment of Psychopathology in Adolescence (Q-PAD). Q-PAD results were then correlated with the main clinical data. Results: 55.2% (32/58) of patients presented at least one emotional disturbance. Body dissatisfaction, anxiety, interpersonal conflicts, family problems, uncertainty about the future, and self-esteem/well-being disorders were frequently reported. Gender and poor control of seizures are associated with specific emotional features (p < 0.05). Conclusions: These findings highlight the importance of screening for emotional distress, recognition of the impairments, and provision of adequate treatment and follow-up. A pathological score on the Q-PAD should always require the clinician to investigate the presence of behavioral disorders and comorbidities in adolescents with epilepsy.
1. Introduction
Adolescents with epilepsy are at increased risk of developing psychological and behavioral disorders compared to the general population and those with other chronic medical conditions [1,2].
The International League Against Epilepsy (ILAE) has identified that the prevalence of neuropsychiatric disorders in children with epilepsy is around 35–50%, and over 50% presented an intellectual disability (ID) [3].
Several investigations have reported that up to 50% of subjects go undetected and untreated. Mood, anxiety, and attention-deficit hyperactivity disorder (ADHD) occur most frequently in adolescents with epilepsy [4,5].
Neuropsychiatric symptomatology in pediatric epilepsy has been associated with different hypotheses. Firstly, the unpredictable nature of seizures could influence psychological development, thereby fostering psychiatric disorders. Moreover, coexisting neurological comorbidities may contribute to the development of psychological distress.
Several authors have found that ID is the most common neuropsychiatric manifestation in children with epilepsy (30–40%) [6,7].
Of note, anti-seizure medications may cause cognitive and behavioral side effects. Furthermore, epileptogenic circuits could be linked with modifications in brain structure and function, possibly resulting, through many different mechanisms, in neuropsychiatric manifestations [8].
Behavioral disturbances can precede epilepsy onset or may be present in the early phase; indeed, the association between epilepsy and behavioral difficulties can be bidirectional [9]. Some authors have suggested that depressed mood and anxiety may precede the onset of epilepsy and act as independent risk factors for the development of unprovoked seizures [10,11].
The worldwide pandemic caused by the SARS-CoV-2 virus was associated with an increased risk of psychiatric sequelae in the general population [12]. Furthermore, during the pandemic, a significant number of patients with epilepsy experienced worsening psychological symptoms and an increase in seizure frequency [13,14].
Within this perspective, in the present study, we investigated the psychological and behavioral sequelae experienced by a group of adolescents with epilepsy using a specific questionnaire for psychopathology in adolescence, the Assessment of Psychopathology in Adolescence (Q-PAD). We also investigated whether the clinical characteristics of epilepsy, such as epilepsy type, epilepsy onset, seizure frequency, anti-seizure medications, age, intelligence quotient (IQ), and gender interfere with emotional well-being.
2. Materials and Methods
2.1. Participants
Patients with a diagnosis of epilepsy were consecutively recruited and prospectively evaluated within this study.
The inclusion criteria included: (1) diagnosis of epilepsy; (2) aged between 14 and 19 years old; and (3) fluency in the Italian language. The exclusion criteria were: (1) intellectual disability; (2) major progressive neurological pathologies; (3) history of psychiatric disorders (diagnosis according to DSM-5); and (4) receiving medications other than antiepileptic drugs. We included patients with a total IQ under the normal range but with a normal General Ability Index (GAI). It is well known that patients with epilepsy have more difficulty in working memory and processing speed, so the GAI could be considered a more accurate representation of their intelligence.
The diagnosis of epilepsy was based on the ILAE classification [15]. Seizure types were classified according to clinical semiology provided by description from a witness or, when possible, by electroencephalogram (EEG) or video–EEG recording of the episode [16]. Patients were considered seizure-free if they were without clinical seizures for at least 1 year, using the last clinical visit documenting seizure status as the end point of follow-up. Refractory epilepsy was defined as uncontrolled seizures after at least two first-line anticonvulsant medication trials [17]. Intelligence assessments were performed according to best practice standards using the Wechsler Intelligence Scale for Children (WISC-III or WISC-IV) or Wechsler Adult Intelligence Scale (WAIS-R or WAIS-IV). For all patients, intelligence assessments were selected according to best practice standards. We classified patient IQ (intelligence quotient) as follows: normal IQ; borderline intellectual functioning (BIF); and mild, moderate, severe or profound ID according to Diagnostic and Statistical Manual of Mental Disorders, Fifth Edition (DSM-5) criteria [18].
The sample included 63 adolescents attending the Epilepsy Center, Childhood and Adolescence Neuropsychiatry Unit of Santi Paolo e Carlo Hospital, University of Milan, Milan. Two adolescents refused to participate in the study.
We enrolled our patients over a span of two years (2019–2020).
All procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and/or national research committee and with the 1964 Helsinki declaration and its later amendments or comparable ethical standards. The Ethics Committee of San Paolo Hospital reviewed and approved the study protocol.
All patients and their caregivers provided their informed written consent before being enrolled in the study.
2.2. Questionnaire
The Questionnaire for the Assessment of Psychopathology in Adolescence (Q-PAD) is a self-administered instrument to assess psychopathological domains described in the scientific literature regarding adolescents aged from 14 to 19 years. The questionnaire contains 81 items in a Likert-type scale with values from 1 to 4, formulated in a language that is familiar according to the linguistic uses of adolescents. The scores of each item are added up for each scale and then converted to percentile values. Therefore, the output of the Q-PAD consists of eight scores referring to the following main psychological areas: body dissatisfaction, anxiety, depression, substance abuse, interpersonal conflicts, family problems, uncertainty about the future, and psychosocial risks. A further ninth domain, called self-esteem and well-being, concerns well-being and adjustment and is assessed in positive terms. The questionnaire has been validated on a sample of 1454 Italian adolescents (Internal Consistency: 0.83, Test-Retest Reliability: 0.84) [19].
2.3. Data Analysis
All statistical analyses were performed using the Statistical Package for Social Sciences (SPSS) version 27.0 for Windows. Qualitative data were reported as absolute frequencies and percentages. Quantitative data were expressed as means and standard deviations (SDs).
Demographics and clinical variables of adolescents were compared with the Mann–Whitney U test or Student’s t-Test for independent samples, depending on the distribution. The normality of the data and homogeneity of variances were tested by the Shapiro–Wilk test and Levene’s test, respectively.
Significance was set at a p-value of 0.05.
We compared the questionnaires by dividing the participants according to the type of epilepsy, epilepsy onset, frequency of seizures, controlled seizures vs. uncontrolled, anti-seizure medications, age (age 14–15 years vs. 16–19 years), IQ, and gender.
3. Results
3.1. Patient Characteristics and Clinical Variables
Sixty-three patients (mean age of 17.24 ± 2.05 years, range: 14–19 years; 19 [32.8%] males, 39 [67.2%] females) were consecutively enrolled in the study; five of them had to be excluded for the following reasons: two showed moderate–severe ID, and three patients were not Italian native speakers (two Hispanic and one Arabic).
Demographic and clinical data were collected from the patients’ medical charts.
Forty (69.0%) patients had focal epilepsy (23 [39.7%] focal epilepsy of unknown etiology, 17 [29.3%] structural focal epilepsy); 18 patients (31.0%) had generalized genetic epilepsy (GGE).
The mean age of epilepsy onset was 10.05 years (±5.1), and the mean duration since diagnosis was 8.07 years (±5.82).
Characteristics of patients are presented in Table 1.
3.2. Psychological Variables
The Q-PAD findings suggest the presence of at least one neuropsychiatric disturbance in 55.2% (32/58) of the adolescents with epilepsy. Our sample had a clinical range of body dissatisfaction (19.0%), anxiety (19.0%), depression (6.9%), substance abuse (1.7%), interpersonal conflicts (22.4%), family problems (25.9%), and uncertainly about the future (22.4%). Moreover, concerning self-esteem/well-being, 31.0% had a normal range, 20.7% borderline values and 48.3% showed a clinical range (Figure 1, Table 2).
Statistically significant differences were found considering age as a covariate: older adolescents (age 16–19 years) showed more interpersonal conflicts (mean = 63.5 ± 26.86 vs. mean = 42.89 ± 30.0) and uncertainty about the future (mean = 55.77 ± 29.27 vs. mean = 37.39 ± 27.16) than younger patients (age 13–15 years; p = 0.016, p = 0.022 respectively).
3.3. Clinical Variables x Psychological Variables
We evaluated the association between some of the clinical variables and the psychological constructs. The type and the onset of epilepsy had no impact on Q-PAD measures. However, we found a statistically significant difference between adolescents with controlled seizures vs. uncontrolled seizures on anxiety, depression, interpersonal conflicts, family problems, and psychosocial risks (p < 0.05, Figure 2).
In relation to treatment (monotherapy vs. polytherapy) and IQ (Normal IQ vs. Borderline Intellectual Functioning), we found no differences in the psychological dimensions investigated (p > 0.05). Finally, with respect to gender, we found no differences in the psychological dimensions investigated apart from depression; girls tended to be more depressed (mean = 54.74 ± 27.77) than boys (mean = 37.89 ± 24.39, p = 0. 027).
4. Discussion
Although most studies on epilepsy and psychological variables have gathered information from parents and teachers, an interesting aspect of our work was to focus on the patient’s point of view. As a general result, our data showed that adolescents with epilepsy have a high rate of neuropsychiatric disturbances (55.2%, 32/58), in accordance with the literature [20,21]. We found a clinical range of body dissatisfaction (19.0%), anxiety (19.0%), depression (6.9%), substance abuse (1.7%), interpersonal conflicts (22.4%), family problems (25.9%), uncertainly about the future (22.4%), and low self-esteem/well-being (48.3%). These findings are thus in accordance with a previous meta-analysis by Lin and colleagues, showing that subjects with epilepsy are at increased risk for neuropsychiatric disorders, such as internalizing behaviors (anxiety, mood and social disorders) prevailing over externalizing functioning (aggressive outbursts or conduct disorders) [20]. While these manifestations may be considered consequences of epilepsy, increasing evidence suggests that these disturbances might precede the onset of epilepsy and seizures. Therefore, epilepsy and neuropsychiatric issues may have a bidirectional correlation, sharing a common underlying pathogenesis [10,11].
Psychiatric disorders, in particular mood and anxiety disorders, may be a reaction to psychosocial obstacles, lower quality of life, and perceived stigmatization by parents [11]. Providing patients, especially those with drug-resistant seizures, with psychological support to orientate their psychological patterns to efficacious ones, improve the overall quality of life and emotional well-being, and reduce fatigue, should be seriously considered. Such cognitive–behavioral programs could help adolescents to adopt more effective ways of coping with their clinical conditions and experience easier psychosocial adjustment [22,23]. Moreover, we found that older adolescents (aged from 16 to 19 years) have more interpersonal conflicts and uncertainty about the future compared to younger adolescents (aged from 14 to 15 years); this result is consistent with previous studies [24].
Considering the clinical variables, our results showed that the type of epilepsy, anti-seizure medication, epilepsy onset, epilepsy duration, and IQ do not influence the answers to the questionnaire.
The scores on the Q-PAD were markedly higher in people with refractory epilepsy, which represents, therefore, one of the major risk factors for poor mental health in childhood.
Adolescents with active epilepsy are at higher risk for anxiety, mood disorders, interpersonal conflicts, and family problems and have higher psychosocial risk. All these outcomes should be closely followed up to identify a possible pathway away from stigma and loneliness as early as possible [25].
Some authors have suggested that higher rates of anxiety and mood disorders are associated with the occurrence of seizures in public places [26].
Davies et al. reported that both uncomplicated and complicated epilepsy groups showed a substantial increase in emotional and behavioral disorders. However, only the complicated epilepsy group (identified as having additional neurological problems or severe learning difficulties) was associated with a markedly increased rate of hyperactive and pervasive developmental disorders [27].
Adolescence is characterized by physical, psychological, and emotional changes. Young people may feel intense emotions, fear for the future, low self-esteem, and difficulties with peers. Epilepsy has an important psychological and social impact on adolescents at this critical time of life [28]. The fact that mental health disturbances are much more commonly associated with epilepsy than with other chronic pathologies, such as diabetes or asthma, indicates that the psychological consequences of epilepsy are not an inevitable result of a chronic and potentially life-threatening disease that requires daily therapy; neurological pathology and social stigma are likely to be key risk factors [27,29].
It is well known that female patients may suffer from mood disorders 2–3 times more often than males; our data are in accordance with the findings that the female gender had an increased incidence of depressive disorders compared to males [30,31].
The early identification and appropriate management of these disturbances should translate into better seizure control, fewer anti-seizure medications and side effects, improved quality of life, reduced costs of healthcare delivery, and better outcomes for society as a whole [3,27,32].
The COVID-19 epidemic increased the prevalence of mental health problems such as depression, anxiety, and sleep disorders in people with epilepsy [33]. During the unprecedented lockdown in Italy, many patients with chronic conditions lost their regular follow-up programs; for this reason, it is crucial to monitor the impact of COVID-19 on this vulnerable cohort [34].
This research has an important strength: to our knowledge, this is the first work to investigate the influence of behavioral disorders in adolescents with epilepsy by focusing on the patient’s point of view and perspective.
Our work has some limitations to disclose. Firstly, the study was conducted in a single center, reflecting the practice style of our tertiary Epilepsy Center, and the subjects were referred to our epilepsy center for pharmacoresistant epilepsy. Secondly, we did not have any controls with another chronic pathology to verify whether they demonstrated similar psychiatric profiles. Thirdly, the study was questionnaire-based, and an in-depth clinical psychiatric interview with a specific focus on psychological/psychiatric problems was missing, in particular concerning the assessment of disease severity.
5. Conclusions
Adolescents with epilepsy exhibit specific psychobiological profiles. Future research is warranted to evaluate the implications from both a research perspective (the genes and circuits implicated) and from a clinical perspective. Our results encourage physicians to always explore psychological issues in adolescents with epilepsy and suggest potential areas of intervention. In conclusion, the psychological assessment of adolescents affected by epilepsy should be integrated with clinical practice to promote early diagnosis and management, considering the higher prevalence of behavioral disturbances in this population.
Author Contributions
K.T. formulated the idea of the study; F.L.B., A.V., E.Z., V.C. and M.P.C. recruited patients for the study; K.T. analyzed data; K.T., F.L.B., L.F., O.B. and M.P.C. interpreted data; K.T. drafted the paper. All authors revised the draft versions, read, and approved the final manuscript. All authors have read and agreed to the published version of the manuscript.
Funding
This research received no external funding.
Institutional Review Board Statement
The study was conducted in accordance with the Declaration of Helsinki and approved by the Ethics Committee of San Paolo Hospital of Milano (ADO-EPI--13).
Informed Consent Statement
Informed consent was obtained from all subjects and caregivers involved in the study.
Data Availability Statement
The data presented in this study are available upon request from the corresponding author.
Acknowledgments
We are grateful to all patients and families who participated in the study.
Conflicts of Interest
The authors declare no conflict of interest.
References
- Russ, S.A.; Larson, K.; Halfon, N. A National Profile of Childhood Epilepsy and Seizure Disorder. Pediatrics 2012, 129, 256–264. [Google Scholar] [CrossRef]
- Batchelor, R.; Taylor, M.D. Young adults with epilepsy: Relationships between psychosocial variables and anxiety, depression, and suicidality. Epilepsy Behav. 2021, 118, 107911. [Google Scholar] [CrossRef] [PubMed]
- Kerr, M.P.; Mensah, S.; Besag, F.; de Toffol, B.; Ettinger, A.; Kanemoto, K.; Kanner, A.; Kemp, S.; Krishnamoorthy, E.; Jr, W.C.L.; et al. International consensus clinical practice statements for the treatment of neuropsychiatric conditions associated with epilepsy. Epilepsia 2011, 52, 2133–2138. [Google Scholar] [CrossRef] [PubMed]
- Reilly, C.; Agnew, R.; Neville, B.G. Depression and anxiety in childhood epilepsy: A review. Seizure 2011, 20, 589–597. [Google Scholar] [CrossRef] [PubMed] [Green Version]
- Chong, L.; Jamieson, N.J.; Gill, D.; Singh-Grewal, D.; Craig, J.C.; Ju, A.; Hanson, C.S.; Tong, A. Children’s Experiences of Epilepsy: A Systematic Review of Qualitative Studies. Pediatrics 2016, 138, e20160658. [Google Scholar] [CrossRef] [PubMed] [Green Version]
- Huemer, J.; Plattner, B.; Planer, N.; Steiner, H.; Feucht, M. Psychopathology in adolescents with TLE and FLE. Eur. J. Paediatr. Neurol. 2016, 20, 880–887. [Google Scholar] [CrossRef]
- Kanner, A.M. Is depression associated with an increased risk of treatment-resistant epilepsy? Research strategies to investigate this question. Epilepsy Behav. 2014, 38, 3–7. [Google Scholar] [CrossRef]
- LaFrance, W.C., Jr.; Kanner, A.M.; Hermann, B. Chapter 20 Psychiatric Comorbidities in Epilepsy. In International Review of Neurobiology; Academic Press: Cambridge, MA, USA, 2008; Volume 83, pp. 347–383. [Google Scholar] [CrossRef]
- Mula, M. Bidirectional link between epilepsy and psychiatric disorders. Nat. Rev. Neurol. 2012, 8, 252–253. [Google Scholar] [CrossRef]
- Kanner, A.M. Psychiatric comorbidities and epilepsy: Is it the old story of the chicken and the egg? Ann. Neurol. 2012, 72, 153–155. [Google Scholar] [CrossRef]
- Kanner, A.M. Can neurobiological pathogenic mechanisms of depression facilitate the development of seizure disorders? Lancet Neurol. 2012, 11, 1093–1102. [Google Scholar] [CrossRef]
- Racine, N.; McArthur, B.A.; Cooke, J.E.; Eirich, R.; Zhu, J.; Madigan, S. Global Prevalence of Depressive and Anxiety Symptoms in Children and Adolescents During COVID-19. JAMA Pediatr. 2021, 175, 1142. [Google Scholar] [CrossRef] [PubMed]
- Tashakori-Miyanroudi, M.; Souresrafil, A.; Hashemi, P.; Ehsanzadeh, S.J.; Farrahizadeh, M.; Behroozi, Z. Prevalence of depression, anxiety, and psychological distress in patients with epilepsy during COVID-19: A systematic review. Epilepsy Behav. 2021, 125, 108410. [Google Scholar] [CrossRef]
- Abokalawa, F.; Ahmad, S.F.; Al-Hashel, J.; Hassan, A.M.; Arabi, M. The effects of coronavirus disease 2019 (COVID-19) pandemic on people with epilepsy (PwE): An online survey-based study. Acta Neurol. Belg. 2021, 122, 59–66. [Google Scholar] [CrossRef] [PubMed]
- Scheffer, I.E.; Berkovic, S.; Capovilla, G.; Connolly, M.B.; French, J.; Guilhoto, L.; Hirsch, E.; Jain, S.; Mathern, G.W.; Moshé, S.L.; et al. ILAE classification of the epilepsies: Position paper of the ILAE Commission for Classification and Terminology. Epilepsia 2017, 58, 512–521. [Google Scholar] [CrossRef] [Green Version]
- Fisher, R.S.; Cross, J.H.; French, J.A.; Higurashi, N.; Hirsch, E.; Jansen, F.E.; Lagae, L.; Moshé, S.L.; Peltola, J.; Perez, E.R.; et al. Operational classification of seizure types by the International League Against Epilepsy: Position Paper of the ILAE Commission for Classification and Terminology. Epilepsia 2017, 58, 522–530. [Google Scholar] [CrossRef] [Green Version]
- Kwan, P.; Arzimanoglou, A.; Berg, A.T.; Brodie, M.J.; Allen Hauser, W.; Mathern, G.; Moshé, S.L.; Perucca, E.; Wiebe, S.; French, J. Definition of drug resistant epilepsy: Consensus proposal by the ad hoc Task Force of the ILAE Commission on Therapeutic Strategies. Epilepsia 2010, 51, 1069–1077. [Google Scholar] [CrossRef] [PubMed]
- American Psychiatric Association. Diagnostic and Statistical Manual for Mental Disorders—Fifth Edition (DSM 5); American Psychiatric Association: Washington, DC, USA, 2013. [Google Scholar]
- Sica, C.; Chiri, L.R.; Favilli, R.; Marchetti, I. Questionario per la Valutazione Della Psicopatologia in Adolescenza; Erickson: Trento, Italy, 2011. [Google Scholar]
- Lin, J.J.; Mula, M.; Hermann, B.P. Uncovering the neurobehavioural comorbidities of epilepsy over the lifespan. Lancet 2012, 380, 1180–1192. [Google Scholar] [CrossRef] [PubMed] [Green Version]
- Verrotti, A.; Carrozzino, D.; Milioni, M.; Minna, M.; Fulcheri, M. Epilepsy and its main psychiatric comorbidities in adults and children. J. Neurol. Sci. 2014, 343, 23–29. [Google Scholar] [CrossRef] [PubMed]
- Michaelis, R.; Tang, V.; Goldstein, L.H.; Reuber, M.; LaFrance, W.C., Jr.; Lundgren, T.; Modi, A.C.; Wagner, J.L. Psychological treatments for adults and children with epilepsy: Evidence-based recommendations by the International League Against Epilepsy Psychology Task Force. Epilepsia 2018, 59, 1282–1302. [Google Scholar] [CrossRef] [PubMed]
- Michaelis, R.; Tang, V.; Wagner, J.L.; Modi, A.C.; Jr, W.C.L.; Goldstein, L.H.; Lundgren, T.; Reuber, M. Psychological treatments for people with epilepsy. Cochrane Database Syst. Rev. 2017, 10, CD012081. [Google Scholar] [CrossRef]
- Puka, K.; Widjaja, E.; Smith, M.L. The influence of patient, caregiver, and family factors on symptoms of anxiety and depression in children and adolescents with intractable epilepsy. Epilepsy Behav. 2017, 67, 45–50. [Google Scholar] [CrossRef]
- Baker, G.A.; Spector, S.; McGrath, Y.; Soteriou, H. Impact of epilepsy in adolescence: A UK controlled study. Epilepsy Behav. 2005, 6, 556–562. [Google Scholar] [CrossRef] [PubMed]
- Siqueira, N.F.; Oliveira, F.L.B.B.; Siqueira, J.A.; De Souza, E.A.P. In adolescents with epilepsy, high scores of anxiety and depression are associated with occurrence of seizures in public places. Arq. de Neuro-Psiquiatria 2015, 73, 205–211. [Google Scholar] [CrossRef] [PubMed] [Green Version]
- Davies, S.; Heyman, I.; Goodman, R. A population survey of mental health problems in children with epilepsy. Dev. Med. Child Neurol. 2007, 45, 292–295. [Google Scholar] [CrossRef]
- Ragni, B.; Cappelletti, S.; De Stasio, S.; Tondo, I.; Specchio, N.; Vigevano, F.; Gentile, S. The impact of epilepsy on adolescence: A quali-quantitative investigation using focus group. Mediterr. J. Clin. Psychol. 2020, 8, 2. [Google Scholar]
- Caplan, R.; Siddarth, P.; Stahl, L.; Lanphier, E.; Vona, P.; Gurbani, S.; Koh, S.; Sankar, R.; Shields, W.D. Childhood absence epilepsy: Behavioral, cognitive, and linguistic comorbidities. Epilepsia 2008, 49, 1838–1846. [Google Scholar] [CrossRef] [PubMed]
- Alfstad, K.; Torgersen, H.; Van Roy, B.; Hessen, E.; Hansen, B.H.; Henning, O.; Clench-Aas, J.; Mowinckel, P.; Gjerstad, L.; Lossius, M.I. Psychiatric comorbidity in children and youth with epilepsy: An association with executive dysfunction? Epilepsy Behav. 2016, 56, 88–94. [Google Scholar] [CrossRef]
- Alfstad, K.; Clench-Aas, J.; Van Roy, B.; Mowinckel, P.; Gjerstad, L.; Lossius, M.I. Psychiatric symptoms in Norwegian children with epilepsy aged 8-13 years: Effects of age and gender? Epilepsia 2011, 52, 1231–1238. [Google Scholar] [CrossRef]
- Sillanpää, M.; Besag, F.; Aldenkamp, A.; Caplan, R.; Dunn, D.W.; Gobbi, G. Psychiatric and Behavioural Disorders in Children with Epilepsy (ILAE Task Force Report): Epidemiology of psychiatric/behavioural disorder in children with epilepsy. Epileptic Disord. 2016, 18, s2–s7. [Google Scholar] [PubMed]
- Kuroda, N.; Kubota, T. Psychological impact of the COVID-19 pandemic for patients with epilepsy: A syste-matic review and meta-analysis. Epilepsy Behav. 2021, 124, 108340. [Google Scholar] [CrossRef]
- Parodi, C.; Viganò, I.; Ottaviano, E.; Massa, V.; Borghi, E.; Beretta, S.; Di Francesco, J.C.; Badioni, V.; Vignoli, A. Long-term analysis of the effects of COVID-19 in people with epilepsy: Results from a multicenter on-line survey across the pandemic waves. Epilepsy Behav. 2022, 135, 108900. [Google Scholar] [CrossRef] [PubMed]
Figure 1.
Distribution of adolescents with epilepsy on the Q-PAD. Figure legend: distribution of Q-PAD scores (minimum score, first (left) quartile, median, third (right) quartile, and maximum score), ° outlier value. Abbreviations: Q-PAD: Questionnaire for the Assessment of Psychopathology in Adolescence.
Figure 1.
Distribution of adolescents with epilepsy on the Q-PAD. Figure legend: distribution of Q-PAD scores (minimum score, first (left) quartile, median, third (right) quartile, and maximum score), ° outlier value. Abbreviations: Q-PAD: Questionnaire for the Assessment of Psychopathology in Adolescence.
Figure 2.
Q-PAD scores for adolescents with uncontrolled seizures vs. controlled seizures. Figure legend: Q-PAD scores of adolescents with uncontrolled seizures compared to patients with controlled seizures (minimum score, first (lower) quartile, median, third (upper) quartile, and maximum score). * Significant scores. ° Outlier value. Abbreviations: Q-PAD: Questionnaire for the Assessment of Psychopathology in Adolescence.
Figure 2.
Q-PAD scores for adolescents with uncontrolled seizures vs. controlled seizures. Figure legend: Q-PAD scores of adolescents with uncontrolled seizures compared to patients with controlled seizures (minimum score, first (lower) quartile, median, third (upper) quartile, and maximum score). * Significant scores. ° Outlier value. Abbreviations: Q-PAD: Questionnaire for the Assessment of Psychopathology in Adolescence.
Table 1.
Demographic and clinical characteristics.
| Variable | N = 58 |
|---|---|
| Age (years) | |
| Mean | 17.24 |
| SD | 2.05 |
| Range | 14–19 |
| Younger Adolescents (14–15 years) | 18 (31.0%) |
| Older Adolescents (16–19 years) | 40 (69.0%) |
| Gender | |
| Male | 19 (32.8%) |
| Female | 39 (67.2%) |
| Education (years) | |
| Mean | 10.36 |
| SD | 2.13 |
| Range | 7–13 |
| Type of epilepsy | |
| Focal Epilepsy | |
| Unknown | 23 (39.7%) |
| Structural | 17 (29.3%) |
| Generalized Genetic Epilepsy | 18 (31.0%) |
| Epilepsy onset (years) | |
| Mean | 10.05 |
| SD | 5.1 |
| Range | 0–18 |
| Epilepsy duration (years) | |
| Mean | 8.07 |
| SD | 5.82 |
| Range | 0-28 |
| Anti-seizure Medications | |
| Monotherapy | 26 (44.8%) |
| Polytherapy | 23 (39.7%) |
| No anti-seizure Medications | 9 (15.5%) |
| Seizure frequency | |
| Daily | 3 (5.2%) |
| Weekly | 5 (8.6%) |
| Monthly | 4 (6.9%) |
| Sporadic | 15 (25.9%) |
| None | 31 (53.4%) |
| Intelligence assessment | |
| Total IQ | |
| Mean | 86.50 |
| SD | 23.69 |
| Verbal IQ | |
| Mean | 80.66 |
| SD | 25.67 |
| Performance IQ | |
| Mean | 82.90 |
| SD | 20.80 |
| Verbal Comprehension | |
| Mean | 100.33 |
| SD | 14.54 |
| Perceptual Reasoning | |
| Mean | 113.56 |
| SD | 12.32 |
| Working Memory | |
| Mean | 96.89 |
| SD | 15.10 |
| Processing Speed | |
| Mean | 87.78 |
| SD | 14.63 |
Abbreviations: SD: standard deviation; IQ: intelligence quotient.
Table 2.
Q-PAD scores.
| Q-PAD Scores | |
|---|---|
| Variable | N = 58 |
| Body dissatisfaction | |
| Mean | 51.59 |
| SD | 28.87 |
| Range | 9–99 |
| Normal range | 47 (81.03%) |
| Clinical range | 11 (18.97%) |
| Anxiety | |
| Mean | 57.16 |
| SD | 26.84 |
| Range | 5–97 |
| Normal range | 47 (81.03%) |
| Clinical range | 11 (18.97%) |
| Depression | |
| Mean | 49.22 |
| SD | 27.67 |
| Range | 10–99 |
| Normal range | 54 (93.10%) |
| Clinical range | 4 (6.90%) |
| Substance abuse | |
| Mean | 34.47 |
| SD | 21.85 |
| Range | 10–95 |
| Normal range | 57 (98.28%) |
| Clinical range | 1 (1.72%) |
| Interpersonal conflicts | |
| Mean | 57.10 |
| SD | 29.23 |
| Range | 5–99 |
| Normal range | 45 (77.6%) |
| Clinical range | 13 (22.4%) |
| Family problems | |
| Mean | 59.71 |
| SD | 25.67 |
| Range | 2–99 |
| Normal range | 43 (74.1%) |
| Clinical range | 15 (25.9%) |
| Uncertainty about the future | |
| Mean | 50.07 |
| SD | 29.66 |
| Range | 10–99 |
| Normal range | 45 (77.6%) |
| Clinical range | 13 (22.4%) |
| Psychosocial risk | |
| Mean | 16.44 |
| SD | 19.49 |
| Min-Max | 1–80 |
| Normal range | 58 (100%) |
| Self-esteem/well-being | |
| Mean | 48.58 |
| SD | 27.88 |
| Range | 1–99 |
| Normal range | 18 (31.6%) |
| Borderline | 12 (21.0%) |
| Clinical range | 27 (47.4%) |
Abbreviations: SD: standard deviation; Q-PAD: Questionnaire for the Assessment of Psychopathology in Adolescence.
Disclaimer/Publisher’s Note: The statements, opinions and data contained in all publications are solely those of the individual author(s) and contributor(s) and not of MDPI and/or the editor(s). MDPI and/or the editor(s) disclaim responsibility for any injury to people or property resulting from any ideas, methods, instructions or products referred to in the content. |
© 2023 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
Share and Cite
MDPI and ACS Style
Turner, K.; La Briola, F.; Vignoli, A.; Zambrelli, E.; Chiesa, V.; Fongoni, L.; Baldi, O.; Canevini, M.P. Living with Epilepsy in Adolescence in Italy: Psychological and Behavioral Impact. Healthcare 2023, 11, 687. https://doi.org/10.3390/healthcare11050687
AMA Style
Turner K, La Briola F, Vignoli A, Zambrelli E, Chiesa V, Fongoni L, Baldi O, Canevini MP. Living with Epilepsy in Adolescence in Italy: Psychological and Behavioral Impact. Healthcare. 2023; 11(5):687. https://doi.org/10.3390/healthcare11050687
Chicago/Turabian StyleTurner, Katherine, Francesca La Briola, Aglaia Vignoli, Elena Zambrelli, Valentina Chiesa, Laura Fongoni, Olivia Baldi, and Maria Paola Canevini. 2023. "Living with Epilepsy in Adolescence in Italy: Psychological and Behavioral Impact" Healthcare 11, no. 5: 687. https://doi.org/10.3390/healthcare11050687
APA StyleTurner, K., La Briola, F., Vignoli, A., Zambrelli, E., Chiesa, V., Fongoni, L., Baldi, O., & Canevini, M. P. (2023). Living with Epilepsy in Adolescence in Italy: Psychological and Behavioral Impact. Healthcare, 11(5), 687. https://doi.org/10.3390/healthcare11050687
Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.
