The February edition of The Psychiatrist features a number of articles about psychotropic polypharmacy. Taylor concludes that ‘rates of antipsychotic polypharmacy seem not to have changed’ ^{Reference Taylor1} while Langan & Shajahan conclude that ‘polypharmacy is an increasingly encountered clinical scenario’ ^{Reference Langan and Shajahan2} without providing any evidence for this. Both authors assert that polypharmacy is by and large very undesirable with little evidence backing its use, with the possible exception of using aripiprazole as co-therapy with clozapine in order to reduce patients' weight. ^{Reference Fleischhacker, Heikkinen, Olie, Landsberg, Dewaele and McQuade3} We work in the Trust (now Health Board) in which Tungaraza et al did their research into polypharmacy and concluded that ‘only a third of individuals were on one psychotropic medication’. ^{Reference Tungaraza, Gupta, Jones, Poole and Slegg4} This implies poor adherence with National Institute for Health and Clinical Excellence (NICE) guidelines on schizophrenia which suggest that polypharmacy is best avoided unless there are exceptional circumstances and clozapine has been offered. We would like to explore the results of this last study as well as its underlying presumptions.

First, is it the patients? It is surprising that this is the first community study looking at polypharmacy and we obviously applaud Tungaraza et al for having conducted it. We also agree with the general sentiment that polypharmacy is by and large undesirable. However, the patient group they investigated is on the whole quite an ill cohort. The Schizophrenia Service in the old North East Wales Trust where Tungaraza et al conducted the study is moderately recovery focused. The standard of primary care is high and many people with good outcome and responsive schizophrenic illnesses are looked after in primary care, mostly on antipsychotic monotherapy. The patients in secondary care often include people who used to live in hospital settings, and have complex illnesses and problems that are often treatment resistant. They would all fall into the remit of having a severe and enduring mental illness as prescribed by the National Service Framework for Wales. In other words, these are patients with complex problems and significant comorbidity. Achim et al put the combined comorbidity of anxiety-type disorders at a staggering 50.1%. ^{Reference Achim, Maziade, Raymond, Olivier, Mérette and Roy5} Dernovsek & Sprah remind us that 40% of people with chronic psychotic disorders have clinical levels of depression and 60% have anxiety symptoms. ^{Reference Dernovsek and Sprah6} In a sample we examined, the rate of active symptoms of an anxiety disorder was 10%. ^{Reference Sharma, Lepping, Cummins, Copeland, Parhee and Mottram7} These patients need treatment for their depressive and anxiety disorders as well as for their schizophrenia, which almost always requires additional medication on top of the antipsychotic. In summary, the patients that are seen in community care today are a cohort of patients with complex and often treatment-resistant problems and with high levels of comorbidity.

Second, is it the guidelines? Guidance is only guidance, so there is an expectation that exceptions may occur. The main problem with guidance, however, is that it is only as good as the evidence that it is based on. Lack of evidence for efficacy is not the same as evidence for lack of efficacy. Because something has a poor research base does not automatically make it unreasonable or ineffective. We agree that there have not been many large-scale studies looking at polypharmacy, but there have been some studies that suggest that polypharmacy might be useful in limited situations and circumstances. Mortimer reaffirms that ‘amisulpride has the best evidence as an affective adjunct to clozapine treatment’. ^{Reference Mortimer8} The other problem with evidence-based research that primarily considers randomised controlled trials is that it always looks at an average. This does not take into account the fact that although some patients will have a good effect from an intervention, others will have no effect from a particular intervention even if the overall effect size might be average. This means that to get an average effect size we need some people who had particularly good effects and others who had no effect. Although we admit that we often do not know who is going to respond particularly well, it is clearly necessary to find inventive solutions for people whose illness will otherwise remain treatment resistant. Additionally, the recent update of the NICE guidelines for schizophrenia take into account the increasing amount of evidence that suggests that second-generation antipsychotics are not a homogeneous group and some of them are clearly more effective than others. ^{Reference Leucht, Corves, Arbter, Engel, Li and Davis9} This evidence is emerging and has been changing the way in which psychiatrists practice all around the world.

Third, is it the drugs? Karunakaran et al ^{Reference Karunakaran, Tungaraza and Harborne10} have shown that clozapine/aripiprazole combinations can be a useful regime to allow people on clozapine to reduce their clozapine dose without a loss of efficacy. Similar studies have shown such effects for amisulpride and quetiapine. The service that Tungaraza et al researched in North Wales has a specialist clozapine clinic and a high number of patients on clozapine (143 in February 2010). Many of them are enabled to reduce their clozapine dose and thus their clozapine-related side-effects by introducing a second antipsychotic. We question whether this should be seen as good practice rather than condemned as polypharmacy.

In conclusion, rather than lamenting that only a third of patients studied in North East Wales were on monotherapy, we think it would be more appropriate to applaud the fact that no patient was on more than two antipsychotics. Most of the patients on two antipsychotics would have been on clozapine and either aripiprazole or amisulpride, which is used in order to reduce side-effects caused by clozapine. Additional psychotropic medication would primarily include antidepressants used to treat depression and anxiety disorders in our patients with schizophrenia or mood stabilisers in bipolar affective disorder, both following current NICE guidelines. This means that we have followed NICE guidelines even if it means using polypharmacy. We therefore feel that in many of the cases that sound like undesirable polypharmacy there may actually be very good reasons in accordance with guidance why two or three psychotropic drugs are being used. This is in order to benefit patients whose side-effect profile can be improved and their debilitating anxiety or depressive disorders treated on top of the treatment for their schizophrenic illness. We would therefore like to see a more balanced view with regard to polypharmacy in a patient group that is often non-responsive to medication and usually has complex comorbidities.

Furthermore, we would dispute the notion that Taylor ^{Reference Taylor1} suggested: that non-medical prescribers may improve the situation. We have concerns which are rather in contrast to this. Non-medical prescribers are more likely to follow guidance but if guidance changes or is flawed, as we have seen with the NICE guidelines for schizophrenia, non-medical prescribers are more likely to lack the flexibility to respond adequately to these challenges and may therefore contribute to suboptimal treatment rather than improve it. Lastly, we wholeheartedly embrace the recommendations that Langen & Shajahan put forward, ^{Reference Langan and Shajahan2} which ask for the regular review of all instances of polypharmacy including clear documentation as to why polypharmacy is continuously used.