In a primary care cohort of over 200,000 people we observed a DM incidence in patients with AP which was higher than that observed in the general population (OR 1.45; 1.22–1.73). Schizophrenia did not prove to be a separate risk factor from DM.2

Evidence suggests that the association is higher with “second generation” AP (and, among them, with olanzapine and clozapine). The measurements which compare incidence (RR) or their analogues (OR) showed a mean increase in risk of 2–3 times when comparing treated patients with non treated patients or patients treated with an AP of poorer profile with one of lower hyperglycaemic capacity. When the difference of means was used it was observed that values were between 4 and 10mg/dl of blood sugar.

Putting the Bradford Hill criteria into practice has shown that this criterion should not be reduced to the measure of association magnitude, but should include aspects such as the statistical significance or internal validity of the study. In the literature there is great disparity in presentation of the resulting event, and a lack of control on potentially important factors of confusion, such as level of psychiatric symptomatology.

Adults with schizophrenia are the most common study group, but the development of DM from AP in adults with bipolar disorder and in children (with diverse disorders) has been observed.3

The growing interest in studying this issue in the child and teenage population is notable, particularly because there may be a certain lack of vigilance in this age group of this and other adverse AP effects.4

In the elderly, the repercussions of AP on blood sugar may be lower.5 In diabetic patients it has been observed that taking these drugs worsens metabolic control.6 The association between the use of AP and the development of DM has been studied using different types of designs, both observational and experimental.

A large part of the available evidence is based on cross-sectional studies, but meta-analyses and systematic reviews with longitudinal studies exist which confirm the effect of the AP.

Correlation between plasmatic concentration of the drug (not dose administered) and the appearance of metabolic type adverse effects7 have been described for olanzapine and clozapine.

Different biological hypotheses exist which could explain the relationship between the consumption of AP and the appearance of DM, such as the antigenic effect of serotonergic receptors, weighted increase or resistance to leptin.8

Changing AP for others of a more favourable metabolite profile leads to a significant reduction in blood sugar levels, according to a recent systematic review.9 However, in this review only 2 clinical trials were used for analysis.

AP have been linked to the appearance of metabolic adverse effects other than DM. Also, the induction of DM has been described as an adverse event from other pharmacological groups.

This approximation reflects how with the Bradford Hill criteria different types of evidence may be included in one setting. The effect of AP on blood sugar is, in our opinion, a fact. The medical implication of these data arises from the need to monitor this effect in all patients prescribed with AP, which today is a group represented by subjects with different sociodemographic indications and characteristics. Although the metabolic repercussion of AP could be stabilized over time,10 long-term control is required. Given their particular vulnerability, greater efforts should be made for further control in children and teenagers.