Schizophrenia

The evidence base demonstrating the efficacy of antipsychotic medication in the treatment of early-onset schizophrenia is relatively limited, but growing. A Cochrane review (Reference Kennedy, Kumar and DattaKennedy 2007) for childhood-onset schizophrenia (age at onset <13 years) found six studies (Table 1) with a total of 256 children and adolescents. The SGAs used were clozapine, risperidone and olanzapine. Although noting improvements with antipsychotic treatment, there was little to support the use of one antipsychotic over another, with the exception of clozapine over haloperidol. No superiority of SGAs over FGAs was found. A further systematic review and meta-analysis of 15 studies of antipsychotics in children and adolescents (up to the year 2003) showed a 55.7% average response to SGAs compared with 72.3% for FGAs. The effect size of 0.36 in favour of the FGAs was not significant (Reference Armenteros and DaviesArmenteros 2006). The review was limited by the methodological quality of the studies which included only two randomised controlled trials (RCTs) of FGAs – loxapine (Reference Pool, Bloom and MielkePool 1976) and haloperidol (Reference Spencer, Kafantaris and Padron-GayolSpencer 1992).

TABLE 1 Randomised controlled trials of antipsychotic medication for the treatment of schizophrenia

Study	Participants	Treatment	Duration	Effectiveness	Adverse effects
Reference Faretra, Dooher and DowlingFaretra 1970	n = 60, 87% childhood-onset schizophrenia Age 5–12 years	Fluphenazine: up to 1.25 mg three times a day, n = 30 Haloperidol: up to 1.25 mg three times a day, n = 30	8 weeks	CGI: no differences fluphenazine v. haloperidol	EPS, fluphenazine v. haloperidol Relative risk 0.6 (95% CI 0.21–2.13)
Reference Engelhardt, Polizos and WaizerEngelhardt 1973	n = 30 Age 6–12 years	Fluphenazine: mean 10.4 mg/ day, n = 15 Haloperidol: mean 10.4 mg/ day, n = 15	12 weeks	Clinical Global Improvement CPRS: no differences fluphenazine v. haloperidol	EPS, fluphenazine v. haloperidol Relative risk 2.0 (95% CI 0.5–2.46)
Reference Pool, Bloom and MielkePool 1976	n = 75 Mean age ∼15.5 years	Loxapine 87.5 mg/day Haloperidol 9.8 mg/day Placebo	4 weeks	Both treatments significantly reduced BPRS total ratings compared with placebo No significant differences observed between active treatment groups	EPS (e.g. muscle rigidity) noted in 19 (73%) of 26 receiving loxapine and 18 (72%) of 25 patients receiving haloperidol Sedation also problematic
Reference Realmuto, Erickson and YellinRealmuto 1984	n = 21 Mean age ∼15.5 years	Thiothixene 16.2 mg Thioridazine 178 mg	6 weeks	Both treatments significantly reduced BPRS total scores	Marked sedation
Reference Spencer, Kafantaris and Padron-GayolSpencer 1992	n = 16 Mean (s.d.) age: ∼8.9 years	Crossover design: haloperidol 1.8 mg/day v. placebo	6 weeks	CGI–I much/very much improved: 12 (75%) patients of 16; marked reduction in severity of persecutory ideation and hallucinations	Sedation
Reference Kumra, Frazier and JacobsenKumra 1996	n = 21 Mean (s.d.) age: 14.0 (2.3) years	Clozapine 176 (149) mg/day Haloperidol 16 (8) mg/day	6 weeks	Clozapine > haloperidol in terms of positive (SAPS total) and negative symptoms (SANS total)	Clozapine: high rates of neutropenia and seizures
Reference Sikich, Hamer and BashfordSikich 2004	n = 50, broad psychotic disorders Mean (s.d.) age: 14.7 (2.7) years	Risperidone 4 (1.2) mg/day Olanzapine 12.3 (3.5) mg/day Haloperidol 5.0 (2.0) mg/day	8 weeks	BPRS–C reduction >20%: risperidone 74%, olanzapine 88%, haloperidol 54% All CGI–I much/very much improved	EPS and weight gain more than reported in adult studies
Reference YaoYao 2003	n = 42 childhood- onset schizophrenia Mean age ∼11 years	Risperidone 0.25–3 mg/day, n = 21 Haloperidol 0.5–12 mg/day, n = 21	6 weeks	BPRS	Risperidone fewer EPS than haloperidol Relative risk 0.10 (95% CI 0.03–0.36, NNT = 2 (95% CI 2–3)
Reference XiongXiong 2004	n = 60 Age 7–16 years Mean age ∼13 years Length of illness 9–9.5 years	Risperidone 0.5–5 mg/day, n = 30 Chlorpromazine 50–400 mg/ day, n = 30	8 weeks	BPRS: no improvement No difference between risperidone and chlorpromazine	Restless Relative risk 1.5 (95% CI 0.27–8.34)
Reference Shaw, Sporn and GogtayShaw 2006	n = 25 Mean age ∼12 years	Clozapine 327 (113) mg/day Olanzapine 18.1 (4.3) mg/day	8 weeks	Clozapine > olanzapine improvement in negative symptoms (SANS)	Marked weight gain at 4 kg during the 8-week trial noted in both groups. At 2-year follow-up, 6 (40%) of 15 patients were observed to have dyslipidaemia
Reference Kumra, Kranzler and Gerbino-RosenKumra 2008	n = 39 Mean (s.d.) age: 15.6 (2.1) years	Clozapine 403.1 (201.8) mg/day Olanzapine 26.2 (6.5) mg/day	12 weeks	> 30% BPRS reduction: 66% clozapine, 33% olanzapine Clozapine > ‘high-dose’ olanzapine negative symptoms (SANS) CGI much/very much improved	Weight gain High incidence of dyslipidaemia
Reference Kryzhanovskaya, Schulz and McDougleKryzhanovskaya 2009	n = 107 Mean (s.d.) age: 16.2 (1.3) years	Olanzapine 11.1 (4.0) mg/day v. placebo	6 weeks	Olanzapine > placebo in terms of improvement from baseline to end-point on the BPRS–C (P = 0.003) and CGI–S (P = 0004) respectively Treatment response rate was not significantly different between olanzapine (37.5%) and placebo (25.7%)	Mean weight gain 4.3 (3.3) kg with olanzapine
Reference Sanford and KeatingSanford 2007	n = 302 Mean age 15.5 years (range 13–17)	Aripiprazole 10 mg/day, aripiprazole 30 mg/day v. placebo	6 weeks	Aripiprazole (10 mg and 30 mg doses) > placebo improvement from baseline to end-point on the PANSS	Mild to moderate severity Extrapyramidal disorder, somnolence, akathisia
Reference Haas, Eerdekens and KushnerHaas 2009b	n = 257 Age 13–17 years	Risperidone low dose 0.15–1.6 mg/day (n = 132) v. high dose 1.5–6.0 mg/day (n = 125) risperidone	8 weeks	PANSS total score improvement (mean (s.d.)) was significantly (P < 0.001) greater with high- (−23.6 (22.8)) v. low- dose (−12.5 (20.3)) risperidone	All adverse events > with high dose, e.g. hypertonia 4.5% low dose v. 14.4% high dose
Reference Sikich, Frazier and McClellanSikich 2008	n = 119: schizophrenia 66%, schizoaffective 34%	Olanzapine 2.5–20 mg/day, risperidone 0.5–6.0 mg/day or molindone 10–140 mg/day + benztropine 1 mg/day	8 weeks	No significant differences in response rates: molindone 50%, olanzapine 34%, risperidone 46%	Olanzapine significant weight gain and lipid changes

The recent US multicentre RCT, Treatment of Early-Onset Schizophrenia Spectrum Disorders (TEOSS; Reference Sikich, Frazier and McClellanSikich 2008), was designed to test whether SGAs are superior to FGAs in treating schizophrenia and schizoaffective disorder (Table 1). It was one of the largest studies involving 119 young people (aged 8–19 years). Results showed that risperidone and olanzapine (SGAs) were not superior to the FGA molindone. Given the side-effect profile of SGAs, particularly weight gain and metabolic problems, the authors questioned the current, almost exclusive, use of SGAs to treat early-onset schizophrenia and schizoaffective disorder. Indeed, given the similar findings of a lack of superiority of SGAs over FGAs in two large pragmatic trials for adults with schizophrenia (CATIE and CUtLAS; Reference Lewis and LiebermanLewis 2008), there are questions about the National Institute for Health and Clinical Excellence (NICE) guidelines (National Collaborating Centre for Mental Health 2002) recommending SGAs as first-line treatment.

Bipolar disorder

There is an increasing trend to use antipsychotics in children and adolescents with bipolar disorder, both in the acute manic phase and as mood stabilisers (Reference Olfson, Blanco and LiuOlfson 2006), although the evidence base for this age group relies largely upon open trials and case reports. A small, double-blind, placebo-controlled study found that quetiapine in combination with divalproex was more effective for the treatment of adolescent bipolar mania than divalproex alone (Reference DelBello, Schwiers and RosenbergDelBello 2002), while separately, quetiapine appears to act faster than divalproex (Reference DelBello, Kowatch and AdlerDelBello 2006) (Table 2). A short-term (3 weeks) multicentre double-blind RCT involving out-patient and in-patient adolescents aged 13–17 years with an acute manic or mixed episode (Reference Tohen, Kryzhanovskaya and CarlsonTohen 2007) showed a significant benefit of olanzapine over placebo in reducing Young Mania Rating Scale scores (effect size 0.84). Risperidone also appears effective in the manic stage of the illness (Reference Haas, DelBello and PandinaHaas 2009a) (Table 2).

TABLE 2 Randomised controlled trials of antipsychotic medication for the treatment of bipolar disorder

Study	Participants	Treatment	Duration	Effectiveness	Adverse effects
Reference DelBello, Schwiers and RosenbergDelBello 2002	n = 30, bipolar I disorder, mixed or manic YMRS score >20 Mean age 14.3 years	Divalproex 20 mg/kg + quetiapine 450 mg/day or placebo	6 weeks	More patients showed greater YMRS improvements with addition of quetiapine (87%) than placebo (53%) (P < 0.05)	No EPS Sedation: quetiapine 80% v. placebo 33%
Reference DelBello, Kowatch and AdlerDelBello 2006	n = 50, bipolar I disorder, manic, mixed	Quetiapine 400–600 mg/ day v. divalproex	4 weeks	No differences in YMRS improvement Quetiapine faster onset of action	Sedation, dizziness and gastrointestinal upset 30–60%
Reference Tohen, Kryzhanovskaya and CarlsonTohen 2007	n = 160, 107 placebo Mean age 15.1 years (s.d. = 1.3)	Olanzapine 2.5–20 mg/ day v. placebo	3 weeks	The mean baseline to LOCF end-point change in the YMRS total olanzapine > placebo −7.65 v. −9.99, P < 0.001; effect size 0.84	Weight gain; rise in hepatic enzymes and prolactin in olanzapine group
Reference Haas, DelBello and PandinaHaas 2009a	n = 169 Age 10–17 years	Risperidone low dose 0.5–2.5 mg/day (n = 50) v. high dose 3–6 mg/day (n = 61) v. placebo (n= 58)	3 weeks	Mean (s.d.) improvement in YMRS total score was greater in both risperidone groups (0.5–2.5 mg: −18.5 (9.7); 3−6 mg: −16.5 (10.3)) v. placebo (−9.1 (11.0)) (P < 0.001)	Somnolence: 19% placebo v. 42% low dose and 52% high dose

Expert guidelines on the treatment of paediatric bipolar disorder (Reference Kowatch, Fristad and BirmaherKowatch 2005) recommend the use of mood stabilisers or SGAs. A combination of mood stabilisers and SGAs is advocated in some cases. Indeed, polypharmacy has become more common. The choice of medication depends on the phase of the illness, presence of psychosis, presence of rapid cycling, risk of side-effects and, crucially, patient and family acceptance. Second-generation antipsychotics are recommended for treating psychotic symptoms but they also act as mood stabilisers. It is important to note that premature discontinuation of antipsychotic medication leads to a recurrence of psychotic symptoms in a large percentage of cases (Reference Kafantaris, Coletti and DickerKafantaris 2001).

According to expert consensus guidelines (Reference Kowatch, Fristad and BirmaherKowatch 2005), both clozapine and electro-convulsive therapy are considered treatments of last resort. It is suggested that clozapine be reserved for patients with bipolar disorder who have failed to respond adequately to at least two trials of a combination treatment regimen that includes at least two of the following: lithium, an anticonvulsant, and an antipsychotic.

Depression

According to the NICE guidelines (National Institute for Health and Clinical Excellence 2005), the treatment for mild cases of juvenile depression consists of brief psychosocial interventions followed by a trial of CBT and then antidepressant medication, if required. The ADAPT study (Reference Goodyer, Dubicka and WilkinsonGoodyer 2007), however, points to the earlier use of selective serotonin reuptake inhibitors (SSRIs) for moderate to severe depression, with little benefit seemingly conferred by the addition of CBT.

The effects of SGAs on serotonin (5-HT) receptors – as 5-HT_2A and 5-HT_2C antagonists, and as a partial 5-HT_1A agonist in the case of aripiprazole – suggest that this class of drugs may be useful in treating depression. Available evidence from randomised placebo-controlled trials involving adults supports the partial effectiveness of olanzapine and quetiapine as augmenters of SSRIs in treatment-resistant depression (defined as a failure to respond to at least one adequate trial of an antidepressant) (Reference Shelton and PapakostasShelton 2008). For children and adolescents, however, such evidence is at present lacking.

Pervasive developmental disorder

It is generally held that there are no indications for the use of antipsychotics in treating the core symptoms of autism or pervasive developmental disorder. However, the Research on Pediatric Psychopharmacology Autism Network (Reference McDougle, Scahill and AmanMcDougle 2005) showed improvements in the areas of sensory motor behaviours, affectual reactions and sensory responses in children with autism given risperidone (Table 3). Small-scale RCTs point to a significantly greater reduction in sensory motor and language subscale scores on the Ritvo–Freeman Real Life Rating Scale with risperidone v. haloperidol (Reference Miral, Gencer and Inal-EmirogluMiral 2008), and an improvement in divided attention in young children with autism prescribed risperidone (Reference Troost, Lahuis and SteenhuisTroost 2005) (Table 3). However, the main indication for the use of antipsychotics appears to be to control temper tantrums, irritability, aggression and rapid mood changes. Six RCTs support the use of risperidone in reducing these behaviours (Reference Chavez, Chavez-Brown and SopkoChavez 2007). An RCT of olanzapine (Reference Hollander, Wasserman and SwansonHollander 2006) found an overall improvement on the Clinicians Global Impressions–Improvement (CGI–I) scale, but no changes in aggression or irritability. There is less evidence supporting the use of other SGAs such as ziprasidone and aripiprazole (Reference Chavez, Chavez-Brown and SopkoChavez 2007). A small RCT by Reference Luby, Mrakotsky and StaletsLuby et al (2006) pointed to the relative safety of risperidone in the pre-school population (children under 5 years old), which is important as this is an age group likely to be targeted for this developmental disorder.

TABLE 3 Randomised controlled trials of antipsychotic medication for the treatment of pervasive developmental disorder and Tourette syndrome/tics

Study	Participants	Treatment	Duration	Effectiveness	Adverse effects
Pervasive developmental disorder
Reference McCracken, McGough and ShahMcCracken 2002	n = 101 with autism Mean age 9.2 years Age range 5–17 years	Risperidone 1.8 (0.7) mg/day (n = 49) v. placebo (n = 52)	8 weeks	Mean (s.d.) ABC–I score: 56.9% decrease with risperidone (from 26.2 (7.9) at baseline to 11.3 (7.4) at 8 weeks v. 14.1% decrease with placebo (from 25.5 (6.6) to 21.9 (9.5)) (P < 0.001) Effect size −1.2	Tiredness during the day (P < 0.0001), excessive appetite (P < 0.0001), difficulty waking (P < 0.05), excessive saliva or drooling (P = 0.04), and dizziness or loss of balance (P = 0.04), increased appetite (73%), fatigue (59%), drowsiness (49%). Weight gain 2.7 kg risperidone v. 0.8 kg placebo
Reference Shea, Turgay and CarrollShea 2004	n = 79: PDD n = 41, controls n =39 Mean age 7.5 years	Risperidone 1.17 (0.7) mg/day	8 weeks	Mean ABC–I score: with risperidone decrease from 18.9 at baseline to 6.8 at end-point; placebo 21.2 to 14.7 (P < 0.001) Effect size −0.8	Somnolence: 72.5% risperidone v. 7.7% placebo Mean weight gain 2.7 kg v. 1.0 kg EPS: tremor, hypokinesia, increased systolic blood pressure, tachycardia
Reference Nagaraj, Singhi and MalhiNagaraj 2006	n = 39 with autism Age range 2–9 years	Risperidone 0.5 mg/ day for 2 weeks then 1 mg/day	6 months	> 20% improvement on the CARS: risperidone 12/19 v. placebo 0/20, P < 0.001	Sedation
Reference Troost, Lahuis and SteenhuisTroost 2005	n = 24 with PDD Age range 5–17 years	Risperidone discontinuation	8 weeks	8/12 risperidone relapsed v. 3/12 placebo, P = 0.04	Weight gain of 5.7 kg with risperidone
Reference Hollander, Wasserman and SwansonHollander 2006	n = 11 with PPD Age 6–14 years	Olanzapine mean (s.d.) dose: 10 (2) mg/day	8 weeks	CGI–I: 50% on olanzapine v. 20% on placebo were responders	Weight gain 3.3 kg on olanzapine v. 0.9 kg placebo
Reference Luby, Mrakotsky and StaletsLuby 2006	n = 23 with ASD Age 2.5–6 years	Risperidone 0.5–1.5 mg/day (n = 11) v. placebo (n= 12)	6 months	No significant differences in autism severity scores	Weight gain and hyperprolactinaemia
Reference Miral, Gencer and Inal-EmirogluMiral 2008	n = 28 with autism Age 7–17 years	Risperidone mean (s.d.) dose: 2.6 (1.3) mg/day (n = 13) Haloperidol 2.6 (0.8) mg/day (n = 15)	10 weeks	Reduction from baseline in Ritvo–Freeman Real Life Rating Scale, sensory motor (subscale I) and language (subscale V) scores, risperidone > haloperidol (P < 0.05) ABC and Turgay DSM–IV PDD reduction in scale scores, risperidone > haloperidol (P < 0.05 and P < 0.01 respectively)	Few EPS
Tourette syndrome/tics
Reference Sallee, Nesbitt and JacksonSallee 1997	n = 22 Age 7–16 years	Pimozide 3.4 (1.6) mg/day v. haloperidol 3.5 (2.2) mg/day v. placebo	24 weeks crossover trial	Pimozide > placebo P = 0.05 Tourette syndrome/tic subscale score 26 Effect size 0.5 Haloperidol v. placebo: P not significant Effect size 0.3	41% of those on haloperidol experienced side-effects, mainly EPS
Reference Sallee, Kurlan and GoetzSallee 2000	n = 28 Mean age 11.5 years	Ziprasidone 28.2 mg/day (n = 16) v. placebo (n = 12)	8 weeks	Tic severity: −39% ziprasidone v. −16% placebo (P = 0.02) Effect size −0.8	Weight gain 0.7 kg ziprasidone v. 0.8 kg placebo
Reference Gaffney, Perry and LundGaffney 2002	n=21	Risperidone 1.5 mg/ day (n = 9) Clonidine 0.18 mg/ day (n = 12)	8 weeks	Response similar in both groups Tics reduced: 21% risperidone v. 26% clonidine	Weight gain: 2.1 kg risperidone v. 0.1 kg clonidine Sedation: clonidine > risperidone
Reference Scahill, Leckman and SchultzScahill 2003	n = 26 Mean age 11.1 years	Risperidone 2.5 mg/ day (n = 12) v. placebo (n = 14)	8 weeks	Tic severity reduced: 36% risperidone v. 9% placebo (P < 0.01); effect size 1.0	No EPS Weight gain: 2.8 kg risperidone v. 0 kg placebo
Reference Gilbert, Batterson and SethuramanGilbert 2004	n = 9 Mean age 11 years	Crossover: risperidone 2.5 mg/ day and pimozide 2.4 mg/day	4 weeks	Greater reduction in tic severity with risperidone (42%) v. pimozide (21%), P = 0.05	Weight gain: 1.9 kg risperidone v. 1.0 kg pimozide

Conduct disorder

Conduct disorder is often associated with psychosocial stressors and adversity. Environmental, social and psychological interventions are therefore the first line of treatment. Treatment of comorbid conditions such as attention-deficit hyperactivity disorder, which may require medication, is important; however, antipsychotic medication for ‘pure’ conduct disorder is not often used in routine clinical practice in the UK.

For children admitted to hospital with severe aggression and conduct disorder, both lithium and haloperidol (dose 1–6 mg/day) reduce aggression (Reference Campbell, Small and GreenCampbell 1984); however, there are notable side-effects with both drugs. Double-blind controlled studies show that risperidone is effective in reducing symptoms (Table 4), with effect sizes ranging from 0.6 (medium) to 1.5 (very large) (Reference Jensen, Buitelaar and PandinaJensen 2007). However, the RCTs share methodological problems of small trial numbers, high drop-out rates, and selection issues, with most children having low IQs. Nevertheless, when an improvement occurs, it does so in the first 2 weeks of treatment. An important question is the length of treatment, as withdrawal may lead to a recurrence of symptoms. Long-term maintenance therapy with risperidone appears effective, with few reported adverse effects (Reference Jensen, Buitelaar and PandinaJensen 2007).

TABLE 4 Randomised controlled trials of antipsychotic medication for the treatment of disruptive behaviour disorders

Study	Participants	Treatment	Duration	Effectiveness	Adverse effects
Reference Findling, McNamara and BranickyFindling 2000	n = 20: conduct disorder n = 10, controls n = 10 Mean 9.2 years	Risperidone 0.03 mg/kg	10 weeks	RAAPP score: −1.7 risperidone v. −0.2 placebo (P < 0.05) CGI: −2.6 risperidone v. −0.1 placebo (P < 0.01) Effect size −1.0	No EPS Weight gain: 4.2 kg risperidone v. 0.7 kg placebo (P < 0.01)
Reference Buitelaar and van der GaagBuitelaar 2001	n = 38: DBD/ADHD n = 19, controls n =19 Mean age 14 years IQ 60–90	Risperidone 2.9 (0.04) mg/day v. placebo	6 weeks	CGI score: −1.6 risperidone v. +0.2 placebo (P < 0.001) Effect size −1.5 ABC significantly improved with risperidone (P < 0.05)	Risperidone: no or mild EPS Weight gain: 2.3 kg risperidone v. 0.6 kg placebo (P < 0.05)
Van Bellinghen 2001	n = 14: DBD n = 7, controls n = 7 Age 6–14 years IQ 45–85	Risperidone 1.2 (0.05) mg/day v. placebo	4 weeks	ABC score improvement in 65% risperidone v. 7% placebo	EPS similar with risperidone and placebo Weight gain: 1.8 kg risperidone v. 0.6 kg placebo (P = 0.319)
Reference Snyder, Turgay and AmanSnyder 2002	n = 110: DBD n = 53, controls n= 57 Mean age 8.7 years IQ 36–84	Risperidone 0.98 (0.03) mg/day v.placebo	6 weeks	N–CBRF conduct scale score: −15.8 risperidone v. – 6.8 placebo (P < 0.001) Effect size – 0.6	Hypertonia: 8% risperidone v. 2% placebo Somnolence: 42% v. 14% Weight gain: 2.2 kg v. 0.2 kg
Reference Aman, De Smedt and DerivanAman 2002	n = 118: DBD n = 55, controls n= 63 Age 5– 2 years IQ 36–84	Risperidone 1.2 (0.04) mg/day v. placebo	6 weeks	N–CBRF conduct scale score: −15.2 risperidone v. −6.2 placebo (P < 0.01) Effect size – 0.8 BPI aggressive scale: −6.8 risperidone v. −2.4 placebo (P < 0.01)	Low EPS: risperidone = placebo Weight gain: 15% (2.2 kg) v. 2% (0.9 kg)
Reference Hollander, Wasserman and SwansonHollander 2006	n = 11 Age 6–14 years	Olanzapine mean (s.d.) dose: 10 (2) mg/day	8 weeks	CGI–I: 50% on olanzapine v. 20% on placebo were responders	Weight gain: 3.3 kg on olanzapine v. 0.9 kg placebo
Reference Reyes, Buitelaar and TorenReyes 2006	n = 335: DBD n = 172, controls n =163 Mean age 11 years IQ =55	Risperidone 0.02 mg/kg v. placebo	6 months	DBD with N–CBRF conduct scale scores Symptom recurrence rate: 42.3% placebo v. 27.3% risperidone Hazard ratio 2.24 (95% CI 1.54–3.28)	Weight gain (3.2 kg) and somnolence (11.6%) with risperidone Infrequent EPS and prolactin- related adverse events

There are no NICE guidelines for pharmacological treatments of conduct disorder; instead, parent training is advocated (National Institute for Health and Clinical Excellence 2006). Overall, with children and adolescents medication should be reserved for those whom psychosocial treatments have failed or for whom they have proved inadequate. For severe aggression, a trial of medication may then be appropriate.

Tourette syndrome and tics

As a treatment rationale for Tourette syndrome and tics, antipsychotics are thought to act primarily by blocking dopamine receptors, thus decreasing dopaminergic input from the substantia nigra and ventral tegmentum to the basal ganglia. Pimozide and haloperidol are effective (Reference Sallee, Nesbitt and JacksonSallee 1997); however, both have serious side-effects – haloperidol producing extrapyramidal symptoms, and pimozide prolonging the QT interval with associated risk of a fatal ventricular arrhythmia. Randomised controlled trials have shown risperidone to be superior to placebo (Reference Scahill, Leckman and SchultzScahill 2003), equally effective as clonidine – an alpha adrenergic agonist (Reference Gaffney, Perry and LundGaffney 2002) – and superior to pimozide (Reference Gilbert, Batterson and SethuramanGilbert 2004). Doses ranging from 1.0 to 2.5 mg/day are effective and neurological side-effects rare. Ziprasidone is also effective (Reference Sallee, Kurlan and GoetzSallee 2000), although cardiac side-effects with QT prolongation are concerning. These trials are limited by small numbers and short duration (Table 3).

Obsessive–compulsive disorder

The Pediatric OCD Treatment Study (POTS) Team (2004) found CBT to be an important component of treatment; however, further improvement was gained with the addition of an SSRI, sertraline. A recent review and meta-analysis (Reference Watson and ReesWatson 2008) demonstrated positive effects for CBT and medication in treating obsessive–compulsive disorder (OCD); however, there are no reported RCTs of antipsychotic augmentation with SSRIs in children and adolescents. A meta-analysis of nine studies of adults with treatment-resistant OCD (Reference Bloch, Landeros-Weisenberger and KelmendiBloch 2006) showed a significant absolute risk difference (ARD) of 0.22 (95% CI 0.13–0.31) in favour of antipsychotic augmentation; those with comorbid tics had a particularly beneficial response (ARD = 0.43, 95% CI 0.19–0.68).

Anorexia nervosa

Psychological interventions are the mainstay of treatment for eating disorders, and according to the NICE guidelines (National Collaborating Centre for Mental Health 2004) medication is not advocated for anorexia in any age group. There is some evidence for the use of olanzapine in adults with anorexia nervosa, but only 16 case reports have been published on its use in children and adolescents (Reference Mehler-Wex, Romanos and KirhheimerMehler-Wex 2008). The results of an RCT in adolescent females are awaited (Reference Spettigue, Buchholz and HendersonSpettigue 2008). Case reports reveal positive psychopathological effects and good tolerability of quetiapine in children and adolescents with severe anorexia (Reference Mehler-Wex, Romanos and KirhheimerMehler-Wex 2008). In a small subset of patients with severe treatment-resistant anorexia, extreme weight phobia, delusional body image disturbances or severe hyperactivity, a trial of an SGA may be justified. Clearly, controlled studies are needed.

Antipsychotics and pre-school children

There is a growing literature, mainly from the USA, on the use of SGAs in the very young (under 5 years of age) for the treatment of bipolar disorder and aggression in autism. There is only limited evidence for such usage and the side-effect profile is even greater in this age group (Reference Gleason, Egger and EmslieGleason 2007). If a decision is made to use this medication, it should be prescribed very cautiously and with careful monitoring alongside psychosocial interventions (see guidelines, Reference Gleason, Egger and EmslieGleason 2007). Such practice is not licensed in the UK and is not recommended.

Side-effects

The side-effect profile of antipsychotics differs according to their receptor blockade potential (Reference Correll and CarlsonCorrell 2006, Reference Correll2008). There are important differences between SGAs and FGAs in terms of weight gain and metabolic syndrome, with perhaps more similarities than originally thought with respect to extrapyramidal side-effects and hyperprolactinaemia. The major side-effects (Table 5) are discussed below.

TABLE 5 Side-effect profile of second-generation antipsychotics and haloperidol (first-generation antipsychotic)^a

Adverse effect	Aripiprazole	Clozapine	Olanzapine	Quetiapine	Risperidone	Ziprasidone	Haloperidol
Anticholinergic	0	+++	+	0/+	0	0	+
Parkinsonian	0/+	0	+	0	++	+	+++
Akathisia	++	+	+	+	+	+	+++
Diabetes	0/+	+++	+++	++	+	0/+	0/+
Raised lipids	0/+	++	+++	+	+	0/+	0/+
Weight gain	0/+	+++	+++	++	+	+	+
Neutropenia	0/+	+++	0/+	0/+	0/+	0/+	0/+
Orthostasis	0	+++	+	++	+	0	0
Raised prolactin	0	0	0	0	+++	0/+	+++
Lowered prolactin	++	0	0	0	0	0	0
Increased QTc	0	0/+	0	+	0	++	+++
Sedation	0	+++	++	++	0/+	0/+	+
Seizure	0/+	++	0/+	0/+	0/+	0/+	0/+
Tardive dyskinesia	0	0	0/+	0/+	0/+	0/+	+
Withdrawal dyskinesia	0/+	0	0/+	0/+	+	+	+

Assessment and monitoring

The following tests and measurements are recommended at baseline and at regular 3–6 monthly follow-up intervals: weight, blood pressure, blood tests (full blood count at baseline only, except with clozapine, for which more regular monitoring is required), liver function tests, fasting lipids, cholesterol, blood sugar and prolactin (Reference CorrellCorrell 2008). Glucose, triglyceride and LDL cholesterol levels are strongly affected by eating, therefore fasting blood values should be used. Unfortunately, fasting glucose is a highly insensitive marker because the body compensates by increasing insulin levels before hyperglycaemia develops (Reference CorrellCorrell 2008). Ideally, measurement of insulin should be available. Haemoglobin A1c is an insensitive screening test, and therefore should only be used for monitoring in patients with diabetes. Prolactin levels should be measured while fasting in the morning, as prolactin levels vary during the day and can be elevated by food, exercise, stress, as well as medications (Reference CorrellCorrell 2008).

Conclusions

Fortunately, the evidence base for the use of antipsychotics in children and adolescents has increased with a number of RCTs now available. The quality of RCTs is variable, with problems of short duration, unclear allocation, selection bias and participant drop out. Many studies are funded by the pharmaceutical industry. In the majority, however, the statistical analyses with stated primary outcome measures and intention-to-treat analyses are an improvement. The evidence is reasonably strong for antipsychotics being effective in a number of disorders such as psychosis, pervasive developmental disorder, conduct disorder and bipolar disorder; however, the side-effect profile is concerning and requires continuous monitoring.

MCQs

1. 1 The prescription of antipsychotics in children and adolescents in the USA has:

   1. a remained fairly static since 1999

   2. b decreased alongside the use of psychosocial treatments

   3. c increased only marginally

   4. d increased over sixfold between 1999 and 2002

   5. e reduced dramatically following FDA warnings.

2. 2 Weight gain as a side-effect of antipsychotic medication:

   1. a is more frequent in children and adolescents

   2. b is more frequent with FGAs

   3. c is of only marginal significance

   4. d occurs equally with all SGAs

   5. e is more frequent in adults.

3. 3 Raised prolactin levels:

   1. a are seen with all SGAs

   2. b are due to a peripheral effect of antipsychotics

   3. c continue to rise with continued use of antipsychotic medication

   4. d are irreversible

   5. e can lead to sexual side-effects.

4. 4 Clozapine:

   1. a is not recommended for children and adolescents under 18 years

   2. b is more effective that other antipsychotics in children and adolescents

   3. c is not associated with serious side-effects in children and adolescents

   4. d is recommended as a first-line treatment for schizophrenia

   5. e unlike other antipsychotics is not associated with weight gain.

5. 5 For children and adolescents with autism, antipsychotic medication:

   1. a is recommended routinely to treat core deficits

   2. b is not associated with adverse side-effects

   3. c has been shown to reduce irritability

   4. d should be used without other psychosocial interventions

   5. e is not used owing to the lack of research evidence.

MCQ answers

1		2		3		4		5
a	f	a	t	a	f	a	f	a	f
b	f	b	f	b	f	b	t	b	f
c	f	c	f	c	f	c	f	c	t
d	t	d	f	d	f	d	f	d	f
e	f	e	f	e	t	e	f	e	f