Randomized controlled clinical trial comparing the efficacy and tolerability of aripiprazole and sodium valproate in the treatment of Tourette syndrome

Tourette syndrome (TS), also known as Gilles de la Tourette syndrome, is a childhood-onset condition characterized by chronic motor and vocal tics. It has been estimated that about 1% of school-age children have TS [1]. But unfortunately the exact mechanisms have not been elucidated. Family studies [2] show that the incidence of TS in first-degree relatives of TS patients is 10–100 times higher than that of the general population. Probably the most accepted current hypothesis regarding the underlying pathophysiology and pathological anatomy of TS is that there is an impairment of cortical inhibition of motor programs that are spontaneously generated in the basal ganglia and expressed. Available evidence also supports involvement of cortico–striatal–thalamo–cortical (CSTC) circuits and their interconnecting brain regions in the pathophysiology of tics [3]. Several neurotransmitters, including dopamine, GABA and glutamate, play an important role within CSTC circuitry and have been proposed to have roles in both habitual behavior formation and in the pathophysiology of tics [4‐8]. Multiple neurotransmitter abnormalities and their signaling may also lead to dysfunction of the CSTC neural network and subsequent clinical manifestations of TS. The pathogenesis of TS is also associated with excessive neurotrophic effects and pro-toxic effects of excitatory amino acids (EAA) in the brain [9]. Astrocyte-specific induction of knockout of EAAT2 in mice has been shown to result in pathological repetitive self-modification and twitch-like head shaking associated with glutamate hyperexcitability [10]. Short-term sodium valproate treatment augmented EAAT1 translocation to the cell membrane, whereas prolonged or chronic sodium valproate treatment resulted in an upregulation of EAAT1 mRNA and protein levels, as well as glutamate transport and production of glutamine. The treatment of TS involves appropriate education and support. Tics can be treated with habit reversal cognitive behavioral therapy [11], pharmacotherapy [12], local intramuscular injections of botulinum toxin [13] and some severe, refractory cases have responded to deep brain stimulation surgery (DBS) [14]. However, the cost of treatment and the risk of surgery still restrict its widespread development. How to control tics quickly for people whose condition seriously affects the daily life is very important.

The atypical antipsychotic aripiprazole is a dopamine D2- and serotonin 5-hydroxytryptamine (5-HT)1A receptor partial agonist and 5-HT2A receptor antagonist [15] that is approved by the United States and South Korea for the treatment of tic disorder. Generally, pediatric patients whose oral aripiprazole at doses of 5-, 10-, 15-, or 30 mg/day and adjusted according to the efficacy and side effects. Sodium valproate controls tics by regulating central GABA system function including enhancing gamma-aminobutyric acid (GABA) synthesis and inhibiting GABA degradation and directly stimulating GABA-A receptors to increase GABA levels and up-regulate excitatory amino acid transporter (EAAT)1 mRNA and protein levels and sodium valproate injection is the first line of medication to control the status of epilepsy. In order to understand the efficacy of sodium valproate injection in controlling the patients with a diagnosis of TS, our department selected 24 patients with acute severe tic and compared with oral aripiprazole.

Patients having continuous phonic tics or motor tics almost all the day had severe TS, which seriously affects the daily life and mental health of patients and the impairment scale scores is extremely high. The total tic scores was above 35 and the impairment scale scores was above 30 in this experiment, indicating that the child was in a serious state of persistence at the time of treatment. The tics had a serious impact on the daily life and psychology of the children and their family members, so it is necessary to find a way to reduce the tic symptoms quickly, effectively and safely. Oral drug aripiprazole has a unique mechanism of action which needs a period for 4–8 weeks or even more longer time in controlling tics. A 10-week multicenter, double-blind, randomized, placebo-controlled trial on 61 children and adolescents with the diagnosis of Tourette’s disorder showed that aripiprazole in comparison to placebo was effective and relatively safe in the short-term treatment [23]. Another study indicates that oral aripiprazole is a safe and effective treatment for tics in children and adolescents with Tourette’s disorder in 8 weeks [15]. Not only the complexity of tic disorders, but also the effectiveness and adverse effects of the medications are major challenges for us so we chose to start at a dose of (2.5 mg/day < 50 kg, 5 mg/day ≥ 50 kg) before bedtime; patients had no bad reaction after oral administration. On the 5th day, the patient still had obvious tic symptoms, and the average dose of 2.71 mg/day was significantly lower than the average dose reported in the literature, so we adjusted to (5 mg/day < 50 kg, 7.5 mg/day ≥ 50 kg).The average dose after 5 days was 5.2 mg/day, which was lower than the average dose of previous children and adolescents, but the patients had some discomfort including lethargy (4 cases, 33.3%) and xerostomia (2 cases, 16.67%), decreased appetite (1 case, 8.3%), decreased sleep (1 case, 8.3%), and tremor (1 case, 8.3%) [Table 4]. The adverse effects mainly occurred after the addition of treatment and the incidence of adverse effects is lower than the previous literature, which does not rule out that our observation time is short or the therapeutic dose is lower than normal. Sodium valproate (VPA) controls twitching by modulating the central GABA system and upregulating EAAT1 mRNA and protein levels. Intravenous valproic acid does not require organic solvent to dissolve, can be injected at physiological pH, minimizes the risk of reaction at the injection site, the incidence of adverse events is low, and the effect is stable. In the experiment, we chose the dose 30 mg/kg/day, once every 12 h. Adverse reactions in the experiment mainly occur in the early stage of treatment and with the treatment going on, most adverse reactions disappear and does not affect normal life at all (Fig. 2).

Current results of this randomized, open-label, control clinical trial suggest that although the two groups are all effective in the reduction of tics in children and adolescents with TS, the sodium valproate group became more lower than the aripiprazole group on the day 5, and the patient's impairment scores was also significantly lower than in the aripiprazole group. Although the family were happy with the tics scores reduction, there were still concerns about whether the condition would repeat again. The average age of the patients we selected was 6–16 years, with an average of 9–10 years. Parents lead the children to visit many medical institutions in Beijing and Shanghai, and repeatedly carry out various examinations. The cost is huge. Some parents refuse to take regular treatment, choose to continue observation and cause the patient's condition to increase year by year. Parents are under tremendous economic and psychological pressure during the process. Due to the special pathogenesis of TS, the anxiety of parents may affect the treatment of children, and some even seriously affect the patient's condition. The family are very concerned about the speed of treatment and they need a quickly way to control tics. Some patients have self-injury behaviors due to exercise tics, the body and the psychology were all under great pressure who were also concerned about if there is a way in controlling tics quickly and safely in a short time (Fig. 3).

Our results showed that the CGI-I score of the sodium valproate group was significantly better than the aripiprazole group on the 5th day. The difference between the two groups was statistically significant (Z = − 2.705, p = 0.008). It showed that with the tics scores decreased, the patients improved their self-evaluation or psychological improvement. The sodium valproate group was better than the aripiprazole group. On the 10th day, the CGI-I score of the sodium valproate group was significantly better than the aripiprazole group. The difference between the two groups was statistically significant (Z = − 3.104, p = 0.004). Although aripiprazole is widely used in the treatment of tic disorder, and parents are still worried about antipsychotic drug adverse effects. There was no significant difference between the CGI scores in 5 days and 10 days (p > 0.05) in sodium valproate group which indicates that the patient's self-evaluation has not changed significantly with the progress of the treatment over time, but the TESS score between 5 days and 10 days has statistically significant difference (p < 0.05) in the sodium valproate group. The patient indicated that the symptoms are obviously improved after 5 days of treatment, but that the improvement was not as obvious as before after 10 days of treatment and the clinical improvement did not reach the expectations of the family. Increasing the days of treatment did not significantly improve the patient's impairment score while the side effects increased (Table 4), so we recommend the treatment of sodium valproate injection for 5–7 days (Fig. 4).

Because the patients selected in this study are in a relatively serious state of tic disorder, the incidence of this condition is low in the clinic. Although our department is the main medical institution for treating tic disorder in the eastern part of Heilongjiang Province, its representativeness is still limited so we hope to cooperate with more hospitals to expand the sample size in the future (Table 4).

The study indicates that the patients treated with sodium valproate injection have a faster onset time than the patients treated with oral aripiprazole in controlling tics. Because of the limited number of patients in our studies, we hope to cooperate with more hospitals in China to expand the sample size in the future.