4 Consideration of the evidence
The Appraisal Committee reviewed the data available on the clinical and cost effectiveness of aripiprazole, having considered evidence on the nature of acute manic episodes in bipolar I disorder in adolescents and the value placed on the benefits of aripiprazole by people with the condition, and clinical specialists. It also took into account the effective use of NHS resources.
4.1 The Committee discussed the nature of acute manic episodes in bipolar I disorder. The clinical specialists explained that acute manic episodes can have a large impact on adolescents and their families. Symptoms of mania may include poor concentration, little need for sleep, poor temper control, irritability, reckless behaviour and lack of self-control. For adolescents, the symptoms may impact on schooling, work and social life. The impact on families may include sleep deprivation, financial pressures and family wellbeing. The Committee heard that there is often a need to resolve the manic episode quickly so that adolescents can return to normal functioning in terms of schooling, work and family life.
4.2 The Committee discussed current standard clinical management of manic episodes in bipolar I disorder in adolescents. The clinical specialists highlighted that the main aim of treatment is to maximise control of the mania and minimise the adverse reactions to treatment that are most troublesome for each individual. The Committee heard from the clinical specialists that drug treatment options for adolescents who develop acute mania include antipsychotic drugs such as aripiprazole, risperidone, olanzapine or quetiapine. The clinical specialists explained that lithium is associated with a range of practical limitations, including the need for pre- and post-treatment blood tests, a narrow therapeutic range, and significant adverse effects. The clinical specialists further explained that although lithium can be prescribed as a monotherapy, it is usually prescribed in combination with antipsychotics. They also highlighted that valproate is rarely used as a monotherapy and is usually not given to women of childbearing age because of fetal malformation risks during pregnancy and risk of polycystic ovary syndrome.
4.3 The clinical specialists confirmed that in UK clinical practice, the routinely prescribed antipsychotics for this indication are olanzapine, aripiprazole, risperidone and quetiapine, and they acknowledged that all are prescribed off-label for the adolescent population (except aripiprazole, which received its marketing authorisation for this indication in January 2013). The Committee was aware that NICE clinical guideline 38 on bipolar disorder recommends following the recommendations for adults with bipolar disorder when prescribing medication for adolescents with acute manic episodes, except that drugs should be started at lower doses. The Committee understood from the clinical specialists that no single antipsychotic drug is considered to be more clinically effective than the others, but that tolerability and adverse reactions vary between the treatments. The Committee heard from the clinical specialists that there is substantial variation between the antipsychotics in the adverse reactions associated with each treatment including weight gain, hyperprolactinaemia and sexual dysfunction, aggression, and akathisia or extrapyramidal symptoms. The clinical specialists explained that it is important for adolescents with moderate to severe manic episodes to have a range of treatment options available. This is in order to individualise treatment and to minimise adverse treatment effects, as adolescents are often less tolerant of adverse reactions than adults, leading to problems with adherence to medication.
4.4 The Committee discussed the manufacturer's decision problem, noting that the manufacturer had excluded lithium and valproate as comparators even though they were specified in the final scope issued by NICE. The Committee noted the comments from the manufacturer, ERG and the clinical specialists highlighting that lithium and valproate monotherapy are rarely used in UK clinical practice. The Committee accepted that these 2 treatments are rarely used as monotherapy and agreed that it was appropriate to consider only risperidone, olanzapine and quetiapine as the comparators, as listed in the manufacturer's decision problem.
Clinical effectiveness
4.5 The Committee considered the relevance of the USA-based NCT00110461 trial to UK clinical practice. It discussed whether the population in the trial reflected that seen in UK clinical practice. The Committee noted that the trial recruited people who were aged between 10 and 17 years and that approximately 63% of the trial participants were aged 13 or older, and so were within the UK marketing authorisation. The Committee heard from the clinical specialists that the diagnosis criteria for bipolar I disorder in children and adolescents in the UK differed from those used in the USA and it is likely that some of the participants with bipolar I disorder comorbid with ADHD in the trial would not have been diagnosed with bipolar I disorder in the UK. The clinical specialists also confirmed that it was usual in clinical trials involving children and adolescents with bipolar I disorder to exclude people with learning disabilities and those at risk of suicide. The Committee discussed the concerns raised by the ERG that most of the participants recruited to the trial were treated as outpatients, whereas in UK clinical practice, they would be usually treated as inpatients. The Committee heard from the clinical specialists that a significant proportion of people in the NHS are managed as outpatients, especially outside the major cities where there is often limited availability of inpatient facilities for this age group. The Committee concluded that the results from the NCT00110461 trial were generalisable to UK clinical practice.
4.6 The Committee then considered the clinical-effectiveness results of the NCT00110461 trial, which showed that aripiprazole was associated with a statistically significant reduction in total YMRS score when compared with placebo throughout the 30-week study duration based on the last observation carried forward dataset. The Committee understood that the marketing authorisation is restricted to 12 weeks' treatment because of high discontinuation rates and the lack of a statistically significant difference in efficacy outcomes beyond 12 weeks when the analysis was based on the observed case dataset. The Committee discussed the usefulness of the YMRS score as the primary outcome and heard from the clinical specialists that this score is a well-recognised tool used in clinical trials for assessing symptoms of mania but that the tool is not routinely used by all clinicians in the UK. The clinical specialists explained that any changes in the YMRS are clearly evident in the change in severity of the symptoms of the individual. The Committee accepted that the YMRS is a valid tool for measuring the severity of symptoms of mania. It concluded that evidence from the trial demonstrated a reduction in manic symptoms in those receiving aripiprazole for 12 weeks compared with those receiving placebo.
4.7 The Committee considered the adverse event data from the NCT00110461 trial. Extrapyramidal disorder and somnolence were statistically significantly more common in those receiving either 10 mg or 30 mg aripiprazole compared with those receiving placebo. Akathisia was statistically significantly more common, but only in those receiving the 30 mg dose of aripiprazole compared with those receiving placebo. It noted there were no statistically significant increases in weight gain or BMI in those receiving aripiprazole compared with those receiving placebo at 4 weeks. The Committee heard from the clinical specialists that the patterns of adverse events seen in the trial were consistent with the use of aripiprazole in other indications. The clinical specialists also stated that for this group, in the short term, somnolence may help in the management of acute mania. The Committee noted the lack of long-term safety data for aripiprazole, but was aware that the risk management plan agreed with the EMA included a long-term (up to 2 years) study to evaluate the safety and tolerability of aripiprazole as maintenance treatment in adolescents with schizophrenia, and children and adolescents with bipolar disorder. The Committee concluded that current evidence suggests that the tolerability and range of adverse reactions associated with aripiprazole are acceptable. The Committee was aware that the population in the NCT00110461 trial was broader than that in the UK marketing authorisation, because the trial included children aged younger than 13 years and those with mixed episodes. The Committee understood that the EMA had restricted the licence for aripiprazole to adolescents aged 13 or older because of safety concerns in younger people. The Committee noted that the manufacturer had presented clinical efficacy and safety results in its submission by age group, that is, for ages 10–12 years and 13–17 years. The Committee noted that the subgroup analysis by age group suggested that there was no change in treatment effect between the age subgroups, but that the younger age group experienced a greater increase in mean weight and BMI changes from baseline at week 12. The Committee noted that the manufacturer provided baseline data on the current episode type (manic or mixed) but a subgroup analysis by age group and episode type was not presented. The Committee understood that these subgroups were post hoc subgroups. It was also aware that the subgroup analyses were based on small numbers of people in the groups, which increased the uncertainty in the results. The Committee therefore concluded that evidence of treatment effect should be based on the whole trial population of NCT00110461.
4.8 The Committee noted that there were no head-to-head comparisons of aripiprazole with the other comparator antipsychotics. The Committee considered the manufacturer's approach to conducting a network meta-analysis to determine the relative efficacy and tolerability of aripiprazole, risperidone, olanzapine and quetiapine. The Committee noted and accepted the ERG's concerns about the network meta-analysis (see sections 3.37–3.39). The Committee was aware that using a random-effects model in the network meta-analysis as suggested by the ERG produced results similar to those obtained by the manufacturer. The Committee therefore accepted the results of the network meta-analysis as a reasonable basis for the economic model given the evidence available.
4.9 The Committee considered the clinical effectiveness evidence of aripiprazole compared with risperidone, olanzapine and quetiapine obtained from the network meta-analysis. It noted that the results suggested that aripiprazole and the other antipsychotics showed greater efficacy than placebo but that no statistically significant differences in efficacy were found between aripiprazole and the other antipsychotics. It then considered the adverse-event profile of aripiprazole compared with risperidone, olanzapine and quetiapine. It was aware that the results suggested that the extrapyramidal symptoms and somnolence occurred more frequently with aripiprazole than with risperidone or quetiapine but that these results were not statistically significant. The Committee also noted that the results suggested that clinically significant weight gain was statistically significantly less likely with aripiprazole than with olanzapine or quetiapine. The Committee was aware of the testimony from the clinical specialists about the importance of having a range of treatments available in order to individualise treatment, minimise adverse treatment effects and therefore increase adherence to medication. The Committee heard from the clinical specialists that avoiding weight gain may be of considerable importance to adolescents. The Committee concluded that based on the evidence available, aripiprazole was as effective as other antipsychotics for treating acute mania and had a comparable and acceptable adverse reaction profile.
Cost effectiveness
4.10 The Committee considered the manufacturer's economic model and the ERG's critique and exploratory analysis. It noted that the ERG considered the manufacturer's model to be transparent, robust, and well structured. The Committee agreed that the model structure was appropriate.
4.11 The Committee considered the manufacturer's base case in which strategies with aripiprazole used at any stage of the treatment pathway (that is, strategies 2 to 4) were compared with a treatment strategy without aripiprazole (strategy 1). The Committee noted that the manufacturer had undertaken a number of deterministic sensitivity analyses (see section 3.32). The Committee was aware that the main parameters that could make the strategies including aripiprazole become less cost effective were the rates of response applied during the treatment phase. The Committee noted that a higher response rate during the treatment phase resulted in people leaving hospital earlier, which had both cost and health-related quality-of-life benefits. The Committee was also aware that the manufacturer's probabilistic sensitivity analyses suggested that there was uncertainty surrounding the ICERs and it understood that this may be a result of the lack of statistically significant differences in response rates obtained from the network meta-analysis for the 4 antipsychotics. The Committee noted that the results from the manufacturer's probabilistic sensitivity analyses indicated that for the 3 strategies that include aripiprazole, the majority of the probabilistic sensitivity iterations indicated cost effectiveness or dominance. The Committee therefore agreed that the base-case results suggested that a treatment strategy that includes aripiprazole is a cost-effective option when compared with a treatment strategy without it.
4.12 The Committee then considered the impact of the position of aripiprazole within the treatment pathway on the cost effectiveness results. The Committee discussed the results of the manufacturer's base case as presented in the incremental analysis. The Committee noted that the pathway in which aripiprazole was positioned second, that is strategy 2, dominated all of the other strategies. The Committee also noted that a comparison of the ranges of costs and QALYs (in the base case, costs ranged from £74,133 to £75,066, and QALYs ranged from 2.516 to 2.525) across the strategies showed that they were similar. The Committee noted that the treatment pathway without aripiprazole (strategy 1) was dominated by each of the other treatment pathways including aripiprazole in over half of the probabilistic sensitivity analysis iterations, and that the probability of strategy 1 being the most cost-effective strategy was half the probabilities for strategy 2 and strategy 3 for all of the thresholds explored by the ERG (see section 3.41). Given that each of the strategies was dominated by every other strategy in at least some of the probabilistic iterations, the Committee agreed that the results were not sufficiently robust to make a recommendation on the position of aripiprazole in the treatment pathway. The Committee concluded that aripiprazole should be recommended as an option for the treatment of moderate to severe manic episodes in bipolar I disorder in adolescents.
Summary of Appraisal Committee's key conclusions
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TA292 |
Appraisal title: Aripiprazole for treating moderate to severe manic episodes in adolescents with bipolar I disorder |
Section |
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Key conclusion |
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Aripiprazole is recommended as an option for treating moderate to severe manic episodes in adolescents with bipolar I disorder, within its marketing authorisation (that is, up to 12 weeks of treatment for moderate to severe manic episodes in bipolar I disorder in adolescents aged 13 and older). |
1.1 |
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The Committee concluded that based on the evidence available, aripiprazole was as effective as other antipsychotics for treating acute mania and had a comparable and acceptable adverse reaction profile. |
4.9 |
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The Committee agreed that the base-case results suggested that a treatment strategy that includes aripiprazole is a cost-effective option when compared with a treatment strategy without aripiprazole. Given that each of the strategies was dominated by every other strategy in at least some of the probabilistic iterations, the Committee agreed that the results were not sufficiently robust to make a recommendation on the position of aripiprazole in the treatment pathway. The Committee concluded that aripiprazole should be recommended as an option for the treatment of moderate to severe manic episodes in bipolar I disorder in adolescents. |
4.11 4.12 |
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Current practice |
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Clinical need of participants, including the availability of alternative treatments |
The Committee heard that the symptoms of mania in adolescents may impact on their schooling, work and family life and there is often a need to resolve the manic episode quickly. The Committee discussed the drug treatments available for adolescents and understood antipsychotics such as olanzapine, risperidone and quetiapine are routinely used off-label. Clinical specialists explained that it is important for adolescents with acute manic episodes to have a range of treatment options available. This is in order to individualise treatment and to minimise adverse treatment effects, as adolescents are often less tolerant of adverse reactions than adults, leading to problems with adherence to medication. |
4.1–4.3 |
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The technology |
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Proposed benefits of the technology How innovative is the technology in its potential to make a significant and substantial impact on health-related benefits? |
The Committee understood from the clinical specialists that no single antipsychotic drug is considered to be more clinically effective than the others, but that tolerability and adverse reactions vary between the treatments. |
4.3 |
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What is the position of the treatment in the pathway of care for the condition? |
The Committee heard from the clinical specialists that the treatment options for adolescents who develop acute mania include an antipsychotic drugs (such as aripiprazole, risperidone, olanzapine or quetiapine), lithium or valproate. The clinical specialists explained that lithium and valproate are not routinely used as monotherapy for this patient population. |
4.2 |
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Adverse reactions |
The Committee was aware that extrapyramidal symptoms, somnolence and akathisia were all statistically significantly more common in those receiving aripiprazole compared with those receiving placebo in NCT0010461. It noted there were no statistically significant increases in weight gain or BMI in those receiving aripiprazole compared with those receiving placebo at 4 weeks. The Committee understood that the ERG did not consider that the frequency or nature of adverse events reported in NCT0010461 raised safety concerns about aripiprazole treatment above other antipsychotics. The Committee concluded that current evidence suggests that aripiprazole has an acceptable safety profile compared with placebo for treatment in adolescents aged 13 or older. |
4.7 |
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Evidence for clinical effectiveness |
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Availability, nature and quality of evidence |
The main clinical-effectiveness evidence came from the NCT00110461 trial with supporting evidence from the NCT00116259. The manufacturer also presented a network meta-analysis based on a network containing aripiprazole, olanzapine, risperidone, quetiapine and placebo. |
3.1 |
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The Committee accepted the results of the network meta-analysis as a reasonable basis for the economic model given the evidence available. |
4.8 |
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Relevance to general clinical practice in the NHS |
The Committee considered the relevance of the USA-based NCT00110461 trial to UK clinical practice. It discussed whether the population in the trial reflected that seen in UK clinical practice. The Committee concluded that overall the results from the NCT00110461 trial were generalisable to UK clinical practice. |
4.5 |
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Uncertainties generated by the evidence |
The Committee understood that the EMA had restricted the licence for aripiprazole to adolescents aged 13 or older because of safety concerns in younger people. The Committee noted that the subgroup analysis by age group suggested that there was no change in treatment effect between the age subgroups, but that the younger age group experienced a greater increase in mean weight and BMI changes from baseline at week 12. The Committee was also aware that the subgroup analyses were based on small numbers of people in the groups, which increased the uncertainty in the results. The Committee concluded that evidence of treatment effect should be based on the whole trial population of NCT00110461. |
4.7 |
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Are there any clinically relevant subgroups for which there is evidence of differential effectiveness? |
The Committee noted that the subgroup analysis by age group suggested that there was no change in treatment effect between the age subgroups. |
4.7 |
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Estimate of the size of the clinical effectiveness including strength of supporting evidence |
The Committee concluded that evidence from the NCT00110461 trial demonstrated a reduction in manic symptoms in those receiving aripiprazole for 12 weeks compared with those receiving placebo. |
4.6 |
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Evidence for cost effectiveness |
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Availability and nature of evidence |
The Committee considered the manufacturer's economic model and the ERG's critique and exploratory analysis. It noted that the ERG considered the manufacturer's model to be transparent, robust, and well structured. The Committee agreed that the model structure was appropriate. |
4.10 |
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Uncertainties around and plausibility of assumptions and inputs in the economic model |
The Committee was aware that the manufacturer's probabilistic sensitivity analyses suggested that there was uncertainty surrounding the ICERs and it understood that this may be a result of the lack of statistically significant differences in response rates obtained from the network meta-analysis for the 4 antipsychotics. |
4.11 |
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Incorporation of health-related quality-of-life benefits and utility values Have any potential significant and substantial health-related benefits been identified that were not included in the economic model, and how have they been considered? |
Not applicable as the Committee had no concerns about the health-related quality-of-life data used in the manufacturer's economic model. |
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Are there specific groups of people for whom the technology is particularly cost effective? |
Not applicable to this appraisal. |
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What are the key drivers of cost effectiveness? |
The Committee was aware that the main parameters that influenced the results were the rates of response applied during the treatment phase. The Committee noted that a higher response rate during the treatment phase resulted in people leaving hospital earlier, which had both cost and health-related quality-of-life benefits. |
4.11 |
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Most likely cost-effectiveness estimate (given as an ICER) |
The Committee noted that the pathway in which aripiprazole was positioned second dominated all of the other strategies. The Committee also noted that the ranges of costs and QALYs (in the base case, costs ranged from £74,133 to £75,066, and QALYs ranged from 2.516 to 2.525) across the strategies were similar. Results from the sensitivity analyses demonstrated that each of the strategies was dominated by every other strategy in at least some of the probabilistic iterations. |
4.12 |
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Additional factors taken into account |
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Patient access schemes (PPRS) |
Not applicable to this appraisal. |
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End-of-life considerations |
Not applicable to this appraisal. |
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Equalities considerations and social value judgements |
No equality issues relevant to the Committee recommendation were raised. |
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