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which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited. Adverse drug reactions from psychotropic medicines in the paediatric population: analysis of reports to the Danish Medicines Agency over a decade
1Department of Pharmacology and Pharmacotherapy, Section for Social Pharmacy, Faculty of
Pharmaceutical Sciences, University of Copenhagen and FKL Research Centre for Quality in Medicine Use,
Universitetsparken 2, DK- 2100 Copenhagen, Denmark
Abstract Background
The prescribing of psychotropic medicines for the paediatric population is rapidly increasing. In attempts to
curb the use of psychotropic medicine in the paediatric population, regulatory authorities have issued various
warnings about risks associated with use of these products in childhood. Little evidence has been reported
about the adverse drug reactions (ADRs) of these medicines in practice. As spontaneous reports are the main
source for information about previously unknown ADRs, we analysed data submitted to a national ADR
database. The objective was to characterise ADRs reported for psychotropic medicines in the Danish
Findings
All spontaneous ADR reports from 1998 to 2007 for children from birth to 17 years of age were included.
The unit of analysis was one ADR. We analysed the distribution of ADRs per year, seriousness, age and
gender of the child, suspected medicine and type of reported ADR. A total of 429 ADRs were reported for
psychotropic medicines and 56 % of these were classified as serious. Almost 20 % of psychotropic ADRs
were reported for children from birth up to 2 years of age and one half of ADRs were reported in
adolescents, especially for antidepressants and psychostimulants. Approximately 60 % of ADRs were
reported for boys. Forty percent of all ADRs were from the category 'nervous and psychiatric disorders'. All
but one ADR reported for children below two years were serious and two of these were fatal. A number of
serious ADRs reported in children from birth up to 2 years of age were presumably caused by mothers' use
of psychotropic medicines during pregnancy.
Conclusion
The high number of serious ADRs reported for psychotropic medicines in the paediatric population should
be a concern for health care professionals and physicians. Considering the higher number of birth defects
being reported greater care has to be given while prescribing these drugs for pregnant women.
Findings Background
The prescribing of psychotropic medicines for the paediatric population is rapidly increasing in many
countries including Denmark. In attempts to curb the use of psychotropic medicine in the paediatric
population, regulatory authorities have issued various warnings about risks associated with use of these
products in childhood [1-4]. A systematic review detected seventeen studies since 2000 that reported
information about the occurrence of ADRs in paediatric populations [5]. Nearly one third of all ADRs
reported in children were due to psychotropic medicines, especially CNS stimulants and antidepressants.
However, more detailed information about the characteristics of ADRs from psychotropic medicines in the
general paediatric population is lacking and little evidence has been reported about safety and long-term
effects of these medicines in practice [6-8]. Lack of knowledge of adverse drug reactions (ADRs) at the point
of licensing of new medicines renders spontaneous ADR reporting an important contributor to knowledge
about safety of medicines [9]. As spontaneous reports are the main source for information about new and
previous unknown ADRs we conducted an analysis of all spontaneous ADR reports for psychotropic
We used data from the national Danish ADR database, which contains information about all spontaneous
reports submitted to the Danish Medicines Agency (DKMA) [10]. ADRs reported for children from 0 to 17
years of age were included. We analysed the distribution of ADRs per year, seriousness, age and gender of
the child, suspected medicine and type of reported ADR (system organ class [SOC]). ADRs were classified
as serious on the following criteria: death, life-threatening, requiring hospitalisation or prolongation of
existing hospitalisation, resulting in persistent or significant disability/incapacity, a congenital anomaly/birth
defect and other medically important conditions.
From 1998 to 2007 a total of 2437 individual ADR reports containing information about 4500 ADRs were
reported for children. Of these, 210 reports corresponding to 429 ADRs were submitted for psychotropic
medicines. Figure 1 shows the annual distribution of the reported ADRs. There were wide fluctuations in the
number of ADRs reported annually, with an increase in number from 2003 to 2005 followed by a decrease in
Table 1 shows the distribution of reported ADRs by therapeutic group and medicine, age of patient and
seriousness. Almost one fifth of ADRs were reported for children below 2 years and one half of all ADRs
were reported for adolescents (from 11 to 17 years of age), and 45% of these were serious. Totally, 59% of
all ADRs were reported for boys. More than one half of all ADRs were classified as 'serious'. Table 2
displays characteristics of ADRs reported for children below two years. Two deaths were reported for
citalopram and fluoxetin due to chorioamnionitis and persistent foetal circulation, respectively. ADRs among
children up to 2 years of age encompassed a wide range of reactions, e.g. convulsion, feeding disorder,
neonatal priapism, apnoea and ventricular septal defects. Seven ADRs: drug exposure during pregnancy,
neonatal respiratory depression, apnoea and pallor were reported as "maternal drugs affecting foetus".
However, the remaining ADRs were probably also caused by mothers' use of psychotropic medicines during
pregnancy, as the indications for use were reported as depression, anxiety, panic disorder and schizophrenia.
The share of serious psychotropic ADRs was higher than the share of serious ADRs in Danish children in
general (40%) [11]. In the general Danish paediatric population, half of all ADRs were reported in children
from birth up to 2 years of age, but for psychotropic medicines more than half of all ADRs were reported for
adolescents which reflect a more extensive use of psychotropic medicine in 11 to 17- year-olds [9]. The
majority of serious ADRs were reported in infants in contrast to reports submitted to Health Canada where
60% of all ADRs for psychotropic medicines were reported in 13 to 19-year-olds, and only 12% in infants
[12]. A number of ADRs were reported for Danish children below 2 years, probably due to the mother's
intake of psychotropic medicine, primarily antidepressants and antipsychotics, during pregnancy. Serious
ADRs such as 'neonatal withdrawal syndrome', 'ventricular septal defects' and 'premature labour' were
reported. The risks of malformations as well as preterm delivery of babies due to use of antidepressants
during pregnancy have been reported previously in the literature and is supported by our results [13-16].
The largest share of ADRs (42%) was reported for psychostimulants (ATC group N06B), followed by 31%
for antidepressants (ATC group N06A) and 24% for antipsychotics (ATC group N05A). More than one half
of the ADRs reported for antipsychotics were caused by the drugs ziprasidone, olanzapine and risperidone.
Although only 2.5% of ADRs were reported for anxiolytics and sedatives (ATC group N05B and N05C),
predominantly in infants, all these ADRs were serious. Two-thirds of the ADRs reported for antidepressants
(ATC group N06A) were reported for infants and adolescents and exclusively for the medicines sertraline,
citalopram and fluoxetine and seventy-five percent of these were serious. For psychostimulants (ATC group
N06B) 50% of ADRs were serious and reported for children from six to nine years of age, and 40% of the
reports were associated with methylphenidate and atomoxetine. With one exception, all 70 ADRs reported
for children less than one year of age were serious.
Table 3 shows the distribution of reported ADRs by system organ class (SOC). The largest shares of ADRs
were reported for the SOCs 'psychiatric disorders' (20% of total), 'nervous system disorders' (20% of total)
and 'general disorders and administration site conditions' (12% of total). Less than 1% of the total number of
reports concerned the following SOCs: 'ear and labyrinth disorders', 'endocrine disorders', 'hepatobiliary
disorders', 'immune system disorders', 'pregnancy, puerperium and perinatal conditions' and 'surgical and
medical procedures'. The largest shares of serious ADRs, about 25% of all were reported for the SOCs:
'psychiatric disorders' and 'nervous system disorders'. The distribution between serious and non-serious
ADRs within SOCs varied. More than seventy-five percent of ADRs reported from the SOCs: 'nervous
system disorders', 'musculoskeletal and connective tissue disorders' and 'congenital, familial and genetic
There are huge gaps in the evidence on the safety of medicines in children as only few medicines prescribed
for children are tested in clinical trials and licensed for use in this population. In addition, information about
serious and long-term ADRs is sparse due to the limitations embedded in the design of randomised,
controlled clinical trials which are used primarily to test hypotheses about efficacy rather than safety and
children are usually excluded from clinical trials of medicines for ethical reasons [17]. Therefore, it is very
important to systematically analyse and evaluate data reported to the spontaneous reporting programmes as
these reports are the major source for new information about possibly serious and previously unknown
ADRs [18]. Several of the reported ADRs were birth defects, an area where we have very limited knowledge.
Conclusions
The high number of serious ADRs reported for psychotropic medicines in the paediatric population should
be a concern for health care professionals and physicians. Considering the higher number of birth defects
being reported greater care has to be given while prescribing these drugs for pregnant women.
Competing interests
The authors declare that they have no competing interests.
Authors' contributions
LA and EHH designed the study, analysed data and wrote the first version of the manuscript. LA did the
sampling. Both authors read and approved the final version of the manuscript.
Acknowledgements
We would like to thank the Danish Medicines Agency for placing data at our disposal.
References
1. European Medicines Agency/CHMP/128918/2005. Press Release: European Medicines Agency finalises review of
antidepressants in children and adolescents. Available at:
http://www.ema.europa.eu/pdfs/human/press/pr/12891805en.pdf [Accessed 18 February 2010].
2. Meeting highlights from the Committee for Medicinal Products for Human Use (EMEA/431407/2007). Available at:
www.emea.europa.eu/pdfs/human/press/pr/43140707en.pdf. [Accessed 18 February 2010].
3. European Medicines Agency makes recommendations for safer use of Ritalin and other methylphenidate-containing
medicines in the EU (EMEA/22315/2009). Available at:
www.ema.europa.eu/pdfs/human/referral/methylphenidate/2231509en.pdf. [Accessed 18 February 2010]
4. Cheung A, Sacks D, Dewa CS, Pong J, Levitt A: Paediatric prescribing practices and the FDA Black-box warning on antidepressants. J Dev Behav Pediatr.2008;29:213-15.
5. Aagaard L, Christensen AC, Hansen EH: Information about adverse drug reactions reported in children: a qualitative review of empirical studies. Br J Clin Pharmacol 2010: In press.
6. Garland EJ: Facing the evidence: antidepressant treatment in children and adolescents.CMAJ 2004;170:489-91.
7. Riddle MA, Labellarte MJ, Walkup JT: Paediatric psychopharmacology: problems and prospects. J Child Adolesc Psychopharmacol 1998;8:87-97.
8. Neubert A, Dormann H, Weiss J, Egger T, Criegee-Rieck M, Rascher W, Brune K, Hinz B: The impact of unlicensed and off-label drug use on adverse drug reactions in paediatric patients. Drug Saf 2004;27:1059-67.
9. Aagaard L, Thirstrup S, Hansen EH: Opening the white boxes: The licensing documentation of efficacy and safety of psychotropic medicines for children.Pharmacoepidemiol Drug Saf 2009;18:401-11.
10. Aagaard L, Stenver DI, Hansen EH: Structures and processes in spontaneous reporting systems: a comparative study of Australia and Denmark.Pharm World Sci 2008;30:563-70.
11. Aagaard L, Weber CB, Hansen EH: Adverse drug reactions in the paediatric population in Denmark: a retrospective analysis of reports made to the Danish Medicines Agency from 1998 to 2007.Drug Saf 2010:33:327-
12. Carleton BC, Smith MA, Gelin MN, Heathcote SC: Paediatric adverse drug reaction reporting: understanding and future directions. Can J Clin Pharmacol 2007;14:e45-e57.
13. Dobson R: SSRI use during pregnancy is associated with fetal abnormalities. BMJ 2006;333;824.
14. Wogelius P, Nørgaard M, Gislum M, Pedersen L, Munk E, Mortensen PB, Lipworth L, Sørensen HT:
Maternal Use of Selective Serotonin Reuptake Inhibitors and Risk of Congenital Malformations. Epidemiology.
2006;17:701-4.
15. Cuevas DC, Sanz EJ: Safety of selective serotonin reuptake inhibitors in pregnancy. Curr Drug Saf 2006;1:17-
16. Lund N, Pedersen LH, Henriksen TB: Selective serotonin reuptake inhibitor exposure in utero and pregnancy outcomes.Arch Pediatr Adolesc Med 2009;163:949-54.
17. Hansen EH: Technology assessment in a user perspective- experiences with drug technology. Int J Techn Assess Health Care 1992; 8:150-65.
18. Aagaard L, Hansen EH: Information about adverse drug reactions explored by pharmacovigilance approaches: a qualitative review of studies on antibiotics, SSRIs and NSAIDs. BMC Pharmacology 2009;9:4. Figure 1: Annual number of adverse drug reactions (ADRs) for psychotropic medicines reported in the Danish paediatric population Table 1: Number of adverse drug reactions reported for psychotropic medication in the paediatric population by age and seriousness (in italic) (1998 to 2007) Age groups (years) 11<17 Antipsychotics (N05A) Hypnotics and sedatives (N05B/N05C) Antidepressants (N06A) Psychostimulants (N06B) Total N05 and N06 Table 2: Serious ADRs from psychotropic medicines reported for children below two years of age (1998 to 2007) ATC Medicines Adverse drug reaction Indication of use Age of child
Zuclopemthixol Supraventricular tachycardia
*Indication for use not listed, but recorded as "Maternal drugs affecting foetus"; NA: not available
Table 3: Adverse drug reactions from psychotropic medicines by system organ class (descending order) System Organ Class (SOC) All ADRs (%) Serious as % of all Serious as % of
General disorders and administration site conditions
Respiratory, thoracic and mediastinal breast
disorders Metabolism and nutrition disorders
Musculoskeletal and connective tissue disorders
Congenital, familial and genetic disorders
Reproductive system and breast disorders
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