Despite some advances, the pharmacological treatment of schizophrenia continues to be a challenge (Kane & Correll, Reference Kane and Correll2010), especially in poor treatment responders, who represent a difficult to treat population with low rates of recovery that have not increased over time (Jaaskelainen et al. Reference Jaaskelainen, Juola, Hirvonen, McGrath, Saha, Isohanni, Veijola and Miettunen2013).
In patients with poor response to antipsychotics (AP), current evidence-based guidelines recommend a range of different strategies, such as waiting for a delayed response, checking adherence, dose adjustment, switching to another AP. If these strategies are ineffective and at least two trials of different APs, prescribed at adequate dose and length of treatment, have failed to provide substantial benefit, patients are considered treatment-resistant (Suzuki et al. Reference Suzuki, Remington, Mulsant, Rajji, Uchida, Graff-Guerrero and Mamo2011, Reference Suzuki, Remington, Mulsant, Uchida, Rajji, Graff-Guerrero, Mimura and Mamo2012). In treatment-resistant cases, guidelines recommend clozapine and, only if this attempt has failed, the combination of clozapine with a second AP (Lehman et al. Reference Lehman, Lieberman, Dixon, McGlashan, Miller, Perkins and Kreyenbuhl2004; NICE, 2009). Although guidelines suggest this combination strategy in selected circumstances only, in clinical practice combining two APs is quite common (Gallego et al. Reference Gallego, Bonetti, Zhang, Kane and Correll2012), ranging between 10 and 30% of those receiving AP treatment (Correll & Gallego, Reference Correll and Gallego2012).
The evidence in support of AP combination has been summarised by a number of systematic reviews that attempted to quantify the beneficial and harmful effects of this strategy, but so far results have been rather contradictory, with low confidence in overall treatment estimates. Probably, the inclusion of studies with small sample sizes, heterogeneity in study quality and the inclusion of studies where a second AP is added to a first one together with studies where two AP drugs are simultaneously prescribed from the beginning of treatment, are possible explanations for such heterogeneity and uncertainty (Barbui et al. Reference Barbui, Signoretti, Mule`, Boso and Cipriani2009; Correll et al. Reference Correll, Rummel-Kluge, Corves, Kane and Leucht2009; Sommer et al. Reference Sommer, Begemann, Temmerman and Leucht2012; Taylor e t al. Reference Taylor, Smith, Gee and Nielsen2012).
In order to overcome these limitations, Galling et al recently conducted a systematic review and meta-analysis focused on the efficacy and tolerability of AP combination strategies v. monotherapy in schizophrenia (Galling et al. Reference Galling, Roldán, Hagi, Rietschel, Walyzada, Zheng, Cao, Xiang, Zink, Kane, Nielsen, Leucht and Correll2017). A total of 31 randomised controlled trials (RCTs) with 2073 participants were included, and studies were grouped and analysed according to quality. RCTs that employed an open-label design and an ‘observed-case’ analysis were defined as low-quality, while RCTs that employed a double-blind approach and carried out an ‘intention-to-treat’ analysis were defined as high-quality. In double-blind studies, the addition of a second AP to current AP treatment was compared with the addition of placebo, whereas in open-label studies, the addition of a second AP was compared with AP continuation in monotherapy. Pragmatically, therefore, the review included only trials in which monotherapy was compared with the addition of a second AP, excluding trials in which patients started treatment with two APs from the beginning. This choice was made to resemble ordinary practice as much as possible.
Efficacy analyses included only RCTs that used efficacy as the primary outcome (22 studies; N = 1342; 13 high-quality and 9 low-quality studies). A number of efficacy measures were analysed, including symptoms reduction; response; reduction of positive, negative and depressive symptoms; reduction in the Clinical Global Impression Scale-Improvement (CGI-I) and functioning. AP combination was superior to monotherapy in terms of total symptoms reduction (16 studies, N = 694, standardised mean difference (SMD) = −0.53, 95% confidence interval (CI) −0.87 to −0.19) and response rate. However, subgroup analysis showed that this finding was confirmed in low-quality studies (seven studies, N = 316, SMD = −0.83, 95% CI −1.16 to −0.50), but not in high-quality studies (nine studies, N = 378, SMD = −0.30, 95% CI −0.78 to 0.19). Overall, clozapine in combination with other APs was superior to clozapine alone (SMD = −0.52, 95% CI −0.90 to −0.14), but again this was confirmed only in the subgroup of low-quality studies and not in high-quality studies. No advantage of any specific AP combination was shown, and this also applied to clozapine, in line with findings from previous reviews (Barbui et al. Reference Barbui, Signoretti, Mule`, Boso and Cipriani2009).
Meta-regression analysis found that when converting AP doses into chlorpromazine equivalents, in comparison with standard AP dose, high AP dose was associated with less symptom improvement. Also, higher baseline symptom severity was associated with less symptom improvement, and this result was confirmed in the subgroup of high-quality studies.
Interestingly, negative symptoms, which are clinically perceived as particularly resistant to treatment, significantly improved when combining a D2 antagonist with a D2 partial agonist (eight studies, N = 532, SMD = −0.41, 95% CI −0.79 to −0.03), even though there were only four high-quality trials confirming this result in subgroup analysis (SMD = −0.28, 95% CI −0.55 to −0.009).
Discontinuation due to any cause and due to tolerability issues did not differ between AP combination and monotherapy. However, AP combination was associated with less insomnia and higher prolactin levels, while AP combination with aripiprazole was associated with reduced prolactin plasma levels and weight, confirming previous findings (Li et al. Reference Li, Tang and Wang2013). As a general limitation, few studies reported data about side effects (9 of 31).
The authors suggested that the gap between the results of double-blind and open-label studies might be explained by the so-called salience bias (Galling et al. Reference Galling, Roldán, Hagi, Rietschel, Walyzada, Zheng, Cao, Xiang, Zink, Kane, Nielsen, Leucht and Correll2017), which means that, when the allocation is known, effectiveness may be strongly influenced by clinicians’ and patients’ expectations. In particular, there is evidence that lack of double blindness is associated with inflated estimates of treatment effect, and this is particularly important when response criteria are subjective, as it happens with rating scale scores (Schulz et al. Reference Schulz, Chalmers, Hayes and Altman1995). If investigators are not blinded, their attitudes for or against an intervention may be directly transferred to participants (Wolf, Reference Wolf1950), may enhance or reduce the overall intensity of their support/assistance to patients (performance bias) and may lead to differential assessment of outcomes (information or ascertainment bias) (Schulz & Grimes, Reference Schulz and Grimes2002). Moreover, if participants are not blinded, knowledge of group assignment can affect responses to the intervention received (Schulz et al. Reference Schulz, Chalmers and Altman2002). This is particularly relevant in this case, as combining two medications is generally perceived as more effective than monotherapy both by clinicians and patients.
Overall, the interpretation of this review is limited by the heterogeneity of trials, which inevitably included populations of patients with different characteristics. For example, the choice of including both clozapine and non-clozapine combination trials might have led to the inclusion of two different types of population, as in clinical practice prescription of clozapine is limited to treatment-resistant patients (Gillespie et al. Reference Gillespie, Samanaite, Mill, Egerton and MacCabe2017). Although translating evidence into recommendations is a sophisticated process that involves different stages, the results of this review, in the context of previous evidence summaries, suggest that clinicians should:
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– Avoid starting polypharmacy as a first step, since increased effectiveness is uncertain, while poor adherence, difficulties in the overall treatment management (Kane et al. Reference Kane, Kishimoto and Correll2013), interactions with other drugs and increased risk of medical unwanted events (Oderda et al. Reference Oderda, Young, Asche and Pepper2012; Barbui et al. Reference Barbui, Conti and Cipriani2014; Hsu et al. Reference Hsu, Esmaily-Fard and Lee2015; Nosè et al. Reference Nosè, Recla, Trifiro and Barbui2015; Yu et al. Reference Yu, Jiang, Shao, Zhou, Shi and Ruan2016) are all expected negative consequences of polypharmacy;
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– Use combination of two APs only after trials with at least two APs in monotherapy have been adequately conducted (in terms of dose and length of treatment) (Suzuki et al. Reference Suzuki, Remington, Mulsant, Uchida, Rajji, Graff-Guerrero, Mimura and Mamo2012) and after an adequate trial with clozapine in monotherapy (Lehman et al. Reference Lehman, Lieberman, Dixon, McGlashan, Miller, Perkins and Kreyenbuhl2004; Barbui et al. Reference Barbui, Signoretti, Mule`, Boso and Cipriani2009; NICE, 2009);
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– The choice of an AP combination strategy should be made taking into consideration the characteristics of individual patients, carefully assessing comorbidities (e.g. heart disease, metabolic syndrome) and concurrent medical treatments, aiming to prescribe the less harmful AP (Leucht et al. Reference Leucht, Cipriani, Spineli, Mavridis, Orey, Richter, Samara, Barbui, Engel, Geddes, Kissling, Stapf, Lässig, Salanti and Davis2013). If weight gain or increased prolactin is expected to be a challenging issue, or if negative symptoms are a clinical problem, then aripiprazole may be added (Arango et al. Reference Arango, Buchanan, Kirkpatrick and Carpenter2004);
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– When prescribing two AP concurrently, the overall AP dose should be carefully considered, as most AP adverse effects are dose-dependent (Ray et al. Reference Ray, Chung, Murray, Hall and Stein2009; Barbui et al. Reference Barbui, Bighelli, Carrà, Castellazzi, Lucii, Martinotti, Nosè and Ostuzzi2016);
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– All choices should be made as part of a shared decision-making process that involves patients, family members, carers and other persons that may have a formal or informal role in the treatment programme.
This meta-analysis has important implications for research, as it pointed out that further studies with a focus on side effects and tolerability are needed. The relationship between combination of APs with D2 partial agonists and negative symptoms also should be investigated by means of trials comparing combination to switching strategies, helping better understand whether the effect is due to a specific effect of D2 partial agonists (Galling et al. Reference Galling, Roldán, Hagi, Rietschel, Walyzada, Zheng, Cao, Xiang, Zink, Kane, Nielsen, Leucht and Correll2017).
In conclusion, current evidence on patients with poor response to AP monotherapy is still weak, and large, pragmatic, high-quality trials are needed to better support clinicians and patients in making clinical decisions on this compelling issue.
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Conflict of interest
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