Background
Although early-onset schizophrenia has similar schizophrenic symptoms as adult-onset schizophrenia in terms of cognition, emotion, and perception, it also has own characteristics. Although the incidence of early-onset schizophrenia is low [
1], hundreds of thousands of patients with early-onset schizophrenia can be found in China. Furthermore, the prognosis of children and adolescents is not as good as that of adult patients, with a lower response rate to treatment, a higher occurrence rate of mental disabilities and poor outcomes [
2,
3]. Accordingly, the early detection and timely and effective treatment for patients with early-onset schizophrenia are particularly critical.
Antipsychotic medication remains the first-line treatment for schizophrenia. However, children and adolescents are in a special stage of growth and development, and many factors, such as efficacy, safety and acceptability, need to be considered during drug treatment. Atypical antipsychotics have proven to be safer and more effective, so they gradually have become the first-line drugs in the treatment of schizophrenia in children and adolescents [
4,
5]. For example, a meta-analysis [
6] that included randomized controlled studies between 1967 and 2017 showed that aripiprazole, olanzapine, risperidone, paliperidone and quetiapine have a significantly better therapeutic effect on patients with early-onset schizophrenia than placebo and that paliperidone, risperidone, olanzapine and quetiapine are somewhat better accepted than placebo. However, an increased risk of metabolic syndrome still exists in patients who are using atypical antipsychotics [
7]. Ray, et al. [
8] found that high-dose antipsychotics were associated with increased accidental mortality in children and adolescents. More importantly, few antipsychotics at present have been approved to be used in children and adolescents, which has led to off-label use in treatment [
9].
At present, little solid evidence exists regarding the use of antipsychotics in patients with early-onset schizophrenia, which lags significantly behind studies on adult patients’ medication and reflects a large disparity from actual clinical needs. Thus, exploring the current status of drug treatment for early-onset schizophrenia may be helpful in choosing reasonable medications in clinical practice. Hence, this study aims to provide references on clinical medication for children and adolescents by conducting a retrospective analysis of the drug regimens of 746 inpatients with early-onset schizophrenia to analyse the status of drug use and its changes.
Discussion
In this study, almost all inpatients were prescribed atypical antipsychotics, and the top five most commonly used antipsychotics were aripiprazole, olanzapine, risperidone, paliperidone and clozapine. A combination of antipsychotics was prescribed in 23.1% of patients. The combination of aripiprazole and olanzapine was that most commonly seen in the AOS group, and the combination of risperidone and clozapine was that most commonly used in the COS group. Olanzapine and risperidone were used more frequently in men, whereas aripiprazole was used less frequently. Olanzapine and paliperidone were used more frequently in AOS patients, and risperidone was used more frequently in COS patients.
In this study, female patients accounted for 59.9% of patients, which seems to be unusual. The reason may be that the older male patients with obvious impulsive and aggressive behaviours may have been admitted to the adult ward in our hospital. The mean age of onset was 12.94 ± 2.28 years, and patients with COS accounted for 33.9% of the sample. The younger the age of onset is, the more difficult the treatment is [
11]. Children and adolescents are different from adults in terms of physiology, anatomy, developmental maturity, and response and tolerance to drugs. The same patient has non-linear differences in drug clearance and metabolic capacity at different growth stages. Dosage, frequency, etc. will have be significantly impacted. Children have strong metabolisms and are more sensitive to drugs than adults, and they may be more susceptible to the side effects of drugs than adults [
12]. Therefore, the choice of drugs is critical, and the adjustment of medication needs to be timely and accurate [
13].
This study found that almost all patients were prescribed second-generation antipsychotics (SGAs), with only 5.5% of patients prescribed with first-generation antipsychotics (FGAs). The use of antipsychotics (APs), especially SGAs, is on the rise in the paediatric population worldwide [
14,
15]. This may relate to the fact that most SGAs have slightly adverse effects on children and adolescents in terms of safety and pharmacokinetics [
13,
16]. For instance, a meta-analysis [
6] showed that aripiprazole, olanzapine, risperidone, and paliperidone and quetiapine had significantly better efficacy than the placebo for EOS patients. Clozapine (only for refractory patients) was the most effective. In addition, the acceptability of paliperidone, risperidone, olanzapine and quetiapine was higher than that of the placebo. Considering the efficacy and safety of aripiprazole, olanzapine, risperidone and paliperidone, the Food and Drug Administration (FDA) has approved these four drugs in the treatment of mental illness in children and adolescents, among which paliperidone and aripiprazole were also approved by the CFDA for the treatment for mental disorders in children and adolescents in September 2017 and January 2018, respectively. Despite the efficacy of APs having been proven, its use in children and adolescents still faces compounding challenges. An unmet challenge is the side effects caused by atypical antipsychotics, especially metabolic syndrome [
17,
18]. Rates of metabolic problems are higher in young first-episode patients [
19], and children and adolescents appear to be at greater risk of weight gain from antipsychotics than adults [
20]. The effects of induced weight gain for atypical antipsychotic drugs vary, with olanzapine having the strongest effect; moreover, typical antipsychotic drugs may also cause significant weight gain, among which chlorpromazine has the strongest effect [
21]. In conclusion, children and adolescents are at a developmentally sensitive stage of life; thus, the balance between the need for symptom improvement and drug-induced adverse reactions should be considered when prescribing antipsychotics.
The second challenge is a lack of evidence that antipsychotics improve cognitive function. Cognitive dysfunction is the core symptom of schizophrenia [
22]. Studies have shown that schizophrenia patients suffer from impairments in processing speed, working memory, social cognition and other areas [
23]. Recent longitudinal studies have also shown that poor cognitive ability seems to be associated with consistently poor functional outcomes [
24]. Cognitive function is of great concern to children and adolescents. However, the effects of antipsychotics on cognitive function are not yet fully understood. This lack of clarity exists despite research showing that SGAs can improve cognitive performance [
25,
26]. However, the effect size is small [
27]. Some studies have found that the cognitive improvement observed in first-episode schizophrenia may be due to exercise effects (e.g., exposure, familiarity, and/or programmed learning) [
28]. Furthermore, metabolic problems secondary to atypical antipsychotics are common, which are associated with cognitive impairment [
29]. That is, the metabolic side effects of antipsychotics may exacerbate cognitive impairment [
30]. Excessive dopamine blockade has been linked to cognitive impairment [
31]. Recent studies have shown that cognitive function can be improved by reducing the dose of risperidone and olanzapine, and mechanistically, the cognitive improvement that occurs after dose reduction of an antipsychotic may be the result of decreased dopamine D2 receptor blockade [
32].
The third challenge is that most available antipsychotics have limited effects on negative symptoms and are studied almost exclusively in adults. Negative symptoms are associated with long-term poor prognosis [
33]. Some studies have shown that certain antipsychotics can relieve negative symptoms. For example, a meta-analysis [
34] showed that 18 antipsychotics significantly reduced negative symptoms compared to placebo, with clozapine, amisubril, olanzapine, levotipine and risperidone (to a lesser extent) significantly reducing negative symptoms more than others. A prospective, large-scale, randomized trial [
35] compared the efficacy of fixed doses of cariprazine and risperidone in the treatment of negative symptoms. In this 26-week study, cariprazine was superior to risperidone in terms of negative symptoms and function improvement. However, the effect of cariprazine on negative symptoms in children and adolescents has not been studied. A combination of antipsychotics and antidepressants may also improve negative symptoms while addressing some mood disorders associated with schizophrenia [
36]. However, there is no clear information on the effect of this combination on the negative symptoms or on the mechanism of action. Patients, especially children and adolescents, rarely complain of negative symptoms, and more pressing positive symptoms may distract the clinician [
37]. Clinicians should carefully monitor and actively manage all clinically relevant negative symptoms. Drug development targeting negative symptoms has yielded positive results for selected monotherapies in a handful of recent well-designed clinical trials, but effective treatment of negative symptoms remains an unmet medical need for schizophrenia to date.
In this study, the antipsychotics selected for AOS and COS patients were different. For example, olanzapine and paliperidone were used more frequently in AOS patients than COS patients. The possible reasons could be the short onset time and stronger sedative effect of olanzapine, which makes it more conducive to controlling impulsive behaviours and positive symptoms of schizophrenia. In addition, olanzapine can relieve symptoms quickly in the acute phase of psychosis [
38]. Paliperidone is a new type of monoamine antagonist, whose major ingredient is 9-hydroxyrisperidone—the active metabolite of risperidone. It is made into to a sustained-release dosage form, which delays the drug-release process and ensures a stable blood-drug concentration; it also lowers the risk of liver damage mainly due to renal excretion and reduces drug interaction, which may offer important clinical advantages. For patients with early-onset schizophrenia, taking medication once a day helps maintain the patients’ compliance. Moreover, paliperidone has less of an effect on liver function, which is much more easily accepted by children and adolescents, who are more sensitive to drug side effects [
39,
40]. Risperidone was more commonly used in patients with COS. An open controlled study abroad showed that risperidone can significantly improve the positive and negative symptoms of adolescent schizophrenia patients and cause less extrapyramidal reactions than traditional antipsychotics [
41,
42]. The frequencies of use of aripiprazole and clozapine were not significantly different in the AOS and COS groups. When taking aripiprazole, extrapyramidal syndrome, hyperprolactinemia, weight gain, metabolic disorders, sedation and other side effects are rarely seen. A randomized controlled study showed that adolescents treated with aripiprazole had a significantly longer time to exacerbation or relapse than the placebo group [
43]. It can be seen that aripiprazole is safe and effective for the treatment of early-onset schizophrenia. Meanwhile, aripiprazole can also safely treat hyperprolactinemia caused by other antipsychotics [
44]. Thus, aripiprazole is more suitable for female patients, which is consistent with the results of this study. Olanzapine was used more frequently in men in this study, which may be related to the fact that men are less troubled by endocrinology.
In this study, 23.1% of patients were prescribed multiple antipsychotics during hospitalization, of which aripiprazole and olanzapine were the most commonly used combination in the AOS group and risperidone and clozapine were the most commonly used in the COS group. In clinical practice, it is common to use multiple antipsychotic drugs during the treatment of EOS, although this is not recommended by guidelines. In this study, refractory cases accounted for approximately 30%. It has been found in clinical practice that treatment for refractory schizophrenia often requires combination treatment. Clozapine is often used jointly with other drugs, in which the dose of clozapine could be appropriately lowered to reduce the rate of adverse clozapine reactions and increase the patient’s compliance with treatment [
45]. Tiihonen, et al. [
46] have studied the relationship between the drug combination therapy for psychosis and psychosis relapse; they found that, in general, any antipsychotic combined with others can reduce the risk of psychiatric readmissions by 7–13% compared with single-drug treatment, among which the combination of aripiprazole and clozapine is associated with the lowest risk of readmission. This seems to be contrary to the current treatment guidelines advocating the principle of single-drug treatment. However, the truth is that the treatment of patients with EOS is difficult, and there are many refractory cases; thus, multiple drug treatments are often required [
45,
47]. Apart from the combined use of antipsychotics, the treatment of schizophrenia often also includes the combination of antipsychotic drugs and other psychotropic drugs. In this study, 8.8, 4.6, and 2.1% of patients used antipsychotic drugs with anti-anxiety drugs, mood stabilizers, and anti-depressant drugs, respectively. Stroup, et al. [
48] found that the addition of antidepressant drugs was associated with a significant reduction in the hospitalization rate of adult schizophrenic patients compared with the addition of another antipsychotic drug. Although the addition of mood stabilizers was not significantly related to the risk of hospitalization, it did increase the risk of death. Thus, the combination of psychotropic drugs still needs to be applied cautiously.
In psychiatric prescriptions for children and adolescents, off-label use is a common and important problem due to the small variety of drugs available. Most antipsychotic drugs are developed by foreign manufacturers and have been approved by the FDA before they are marketed in China. Therefore, clinicians in China are likely to refer to foreign guidelines and medication instructions when using these drugs in clinical diagnosis and treatment before they are approved by CFDA [
49]. In this study, we can see that paliperidone and aripiprazole were stably used before and after being approved by the CFDA for clinical use, which also confirms that clinical practice often precedes the development of guidelines, and practical experience can contribute to the development of guidelines as well. The study showed that the use of olanzapine has been less than that seen in previous years, which may result from the approval of paliperidone and aripiprazole for clinical use in China, and clinicians are also increasingly considering adolescents to be at high risk for developing metabolic syndrome. Of course, it is necessary to pay attention to the right of informed consent of patients and their families in clinical work; particularly in the case of off-label use, patients and their families should be fully informed and consenting, and they should sign the informed consents for the drug’s use.
There were several limitations to this study. First, the results of the present study are limited by its retrospective design rather than longitudinal study and this may be the case in most of previous studies concerned with retrospective data. Furthermore, the results of this study may be limited in Chinese population.
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