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Drug information update: agomelatine

Published online by Cambridge University Press:  02 January 2018

Daniel Whiting
Affiliation:
University Department of Psychiatry, Warneford Hospital, Oxford
Philip J. Cowen*
Affiliation:
University Department of Psychiatry, Warneford Hospital, Oxford
*
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Summary

Agomelatine is a new antidepressant, licensed for the treatment of unipolar major depression, with a mode of action that combines activation of melatonin receptors with blockade of 5-HT2C receptors. Agomelatine is notable for its short duration of action in the body and modest side-effect burden; however, a number of theoretical and practical challenges have limited its adoption into mainstream treatment in the UK. Current meta-analyses show marginal clinical benefits of agomelatine relative to placebo and an association with occasional increases in liver transaminases. Theoretically it is not clear whether agomelatine does block brain 5-HT2C receptors in humans at therapeutic doses and the optimum daily timing of administration in depression has not been clearly established. However, agomelatine's novel mode of action justifies further study, perhaps with the eventual aim of matching its use in depression to patients with specific disturbances in circadian rhythm.

Type
Special Articles
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution (CC-BY) license (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution, and reproduction in any medium, provided the original work is properly cited.
Copyright
Copyright © Royal College of Psychiatrists, 2013

The melatonin analogue, agomelatine, is the first antidepressant approved by the European Medicines Agency which is not monoaminergic. Agomelatine is proposed to act as an agonist at melatonin (MT1 and MT2) receptors, and an antagonist at 5-HT2C receptors. Controlled studies have suggested favourable efficacy and tolerability profiles; however, agomelatine is not without its controversies, with recent meta-analyses showing only marginal advantages over placebo. It is nevertheless an intriguing agent pharmacologically and here we provide a synopsis of its proposed mechanisms of action, indications and side-effects in the treatment of unipolar major depression.

Mechanism of action

Disturbances of the sleep-wake cycle and diurnal variation in mood are common symptoms of depression. A role for abnormalities in circadian rhythm in the pathophysiology of depression therefore makes intuitive sense, and has long been explored in treatments such as sleep deprivation and light therapy. Reference Boivin1 However, it is not yet clearly established whether there is a consistent circadian ‘phase-shift’ in patients with major depression or (as seems more likely in this heterogeneous disorder) that some, but not all, patients have variable kinds of circadian disturbances. For example, the pineal hormone melatonin is a reliable marker of circadian rhythm and the activity of the circadian ‘oscillator’ in the suprachiasmatic nucleus (SCN). However, despite many studies it is still not clear whether there are abnormalities in the amplitude and timing of melatonin secretion in patients with depression. Reference Germain and Kupfer2 Nevertheless, it is known that in both animals and humans appropriately timed administration of melatonin has the capacity to shift circadian rhythms, and melatonin is used for this purpose, for example, in delayed sleep-phase syndrome. Reference Pandi-Perumal, Trakht, Spence, Srinivasan, Dagan and Cardinali3

Agomelatine (N-[2-(7-methoxy-1-napthyl)ethyl]acetamide) is a melatonin analogue, binding with high affinity to MT1 and MT2 G-protein coupled receptors. Reference Millan, Gobert, Lejeune, Dekeyne, Newman-Tancredi and Pasteau4 Melatonin receptors are expressed in numerous regulatory areas of the brain, including the SCN. Reference Pandi-Perumal, Trakht, Srinivasan, Spence, Masetroni and Zisapel5 MT1 activation regulates amplitude of circadian rhythmicity via inhibition of SCN neurons, and MT2 activation is involved in phase-shifts and entrainment of the rhythm. Reference San and Arranz6 Additionally, and distinctly from melatonin, agomelatine is a competitive antagonist at 5-HT2C and 5-HT2B receptors, and in animal studies, 5-HT2C antagonism has the ability to increase noradrenaline and dopamine release in the prefrontal cortex. Reference Millan, Gobert, Lejeune, Dekeyne, Newman-Tancredi and Pasteau4

The antidepressant effects of agomelatine are claimed to derive from a synergism between its melatonergic and 5-HT2C actions. Thus results from animal experimental studies of behavioural models of depression show that melatonin or 5-HT2C antagonists alone are insufficient to produce the full antidepressant activity of agomelatine. Reference Tardito, Molteni, Popoli and Racagni7 Similarly, agomelatine produces an increase in gene expression of brain-derived neurotrophic factor (BDNF) in prefrontal cortex that is not reproduced with melatonin or 5-HT2C antagonism alone. Reference Molteni, Calabrese, Pisoni, Gabriel, Racagni and Riva8 Brain-derived neurotrophic factor has been implicated in depression and the response to antidepressant therapy. Reference Sen, Duman and Sanacora9

However, the affinity of agomelatine for 5-HT2C receptors is significantly lower than its ability to bind melatonin receptors. Reference Millan, Gobert, Lejeune, Dekeyne, Newman-Tancredi and Pasteau4 It is therefore worth noting that there is currently no evidence that at clinically used doses agomelatine blocks brain 5-HT2C receptors in humans and in fact some evidence to the contrary. Reference Sharpley, Rawlings, Brain, McTavish and Cowen10 In contrast, the melatonergic action of agomelatine has been supported by small healthy volunteer studies in humans which indicate that agomelatine can phase-alter the timing of circadian rhythms. For example, a double-blind placebo study of eight healthy young men showed that agomelatine given at 18.00h produced phase advancement as demonstrated by an earlier drop in core body temperature equivalent to melatonin administration. Reference Krauchi, Cajochen, Mori, Graw and Wirz-Justice11 In a group of older men, 15 days of agomelatine administered at 18.30h phase-advanced the drop in core body temperature by 1.5-2 h, but without significantly affecting any sleep parameters including rapid eye movement (REM) sleep. Reference Leproult, Van Onderbergen, L'hermite-Balériaux, Van Cauter and Copinschi12

Dose and pharmacokinetics

The starting dose of agomelatine is 25 mg taken at ‘bedtime’, increasing to 50 mg if indicated after 2 weeks. 13 Agomelatine is well absorbed after oral administration but subject to extensive first-pass metabolism, which causes significant variation in drug plasma levels between individuals. Peak plasma levels occur within 1-2 h after ingestion and the terminal half-life of the drug is also between 1 and 2 h. Therefore, accumulation of agomelatine does not occur. Agomelatine is metabolised in the liver by CYP1A2 and should therefore not be given with potent CYP1A2 inhibitors such as ciprofloxacin and fluvoxamine. Caution is recommended when using agomelatine with moderate CYP1A2 inhibitors such as propranolol and oestrogens. Conversely, smoking induces CYP1A2 activity and can lower agomelatine levels (www.medicines.org.uk/EMC/medicine/21830/SPC/Valdoxan).

Indications

Agomelatine is licensed by the European Medicines Agency for the treatment of major depressive episodes in adults. There is currently insufficient randomised trial evidence to consider agomelatine in treatment-resistant depression or in bipolar depression, although some open case series are available.

Clinical effects and efficacy

Although narrative reviews of the efficacy of agomelatine emphasise its superior efficacy relative to placebo and certain other antidepressants such as sertraline and fluoxetine, Reference Hickie and Rogers14 formal meta-analyses have found these effects to be less convincing Reference Singh, Singh and Kar15,Reference Barbui and Cipriani16 and of uncertain clinical significance. For example, Singh et al Reference Singh, Singh and Kar15 examined 9 double-blind randomised controlled trials of 3943 patients with major depression in which agomelatine was compared with either other antidepressants or placebo. In pooled analyses, agomelatine was significantly but marginally better than placebo (standardised mean difference in depression rating scales of –0.26). Data from five trials on 1698 patients showed again marginal superiority of agomelatine over the aggregated results of other antidepressants (fluoxetine, paroxetine, sertraline and venlafaxine) but not over any of the other agents examined individually. However, clear separation from placebo is not a problem unique to agomelatine among new antidepressants, perhaps partly because of the methodological difficulties involved in placebo-controlled, regulatory trials. Reference Rihmer, Dome, Baldwin and Gonda17

In one study, agomelatine appeared effective in the maintenance treatment of depression, although in two other studies a positive effect could not be demonstrated. Reference Hickie and Rogers14

Side-effects

In controlled trials, the level of side-effects of agomelatine has generally been similar to placebo, with the exception of increased rates of nausea, diarrhoea and dizziness. Reference Zajecka, Schatzberg, Stahl, Caputo and Post18 Side-effects in the British National Formulary that are reported as ‘common’ also include constipation, headache, drowsiness, insomnia, fatigue, back pain and sweating. 13 Agomelatine appears less likely to cause sexual side-effects than selective serotonin reuptake inhibitors (SSRIs) and serotonin-noradrenaline reuptake inhibitors (SNRIs), with studies suggesting that agomelatine has similar rates of emergent sexual dysfunction to placebo and significantly lower rates than drugs such as venlafaxine. Reference Montejo, Majadas, Rizvi and Kennedy19

The most problematic side-effect of agomelatine is its association with abnormal liver function tests, and jaundice and hepatitis have also been reported. Rates of elevation of liver transaminases more than three times normal are seen in about 4.5% of patients taking 50 mg daily. Reference Zajecka, Schatzberg, Stahl, Caputo and Post18 Liver function tests are therefore required prior to initiation of agomelatine treatment and then after 3, 6, 12 and 24 weeks; agomelatine is contraindicated in people with hepatic impairment.

Conclusions

Agomelatine is an interesting antidepressant with a novel mode of action. More data are needed on the clinical effectiveness of agomelatine in real-world conditions, particularly in relation to other available antidepressant drugs. It would also be useful to have more data about the utility of agomelatine in patients with treatment-resistant depression, either as a sole antidepressant or as an augmenting agent. In an open study, Sparshatt et al Reference Sparshatt, McAllister-Williams, Baldwin, Haddad, Bazire and Weston20 followed 110 patients treated in secondary care with agomelatine; the majority (75%) had failed to respond or had relapsed while taking current antidepressant treatment. In a fifth of the patients, agomelatine was added to ongoing antidepressant treatment. About 60% of the total group continued agomelatine up until 12 weeks, which was the primary outcome measure; the majority of discontinuations were for lack of efficacy. Just under half the patients showed an improvement on the Clinical Global Impression rating scale. Assessment of the effectiveness of agomelatine in this hard-to-treat patient group is difficult from these data but the authors concluded that the fact that the majority of patients continued agomelatine treatment for at least 12 weeks was encouraging.

At present, the main place for agomelatine is probably in patients with depression who are unable to tolerate conventional antidepressants, particularly if sexual dysfunction is a problem. Because of its mode of action, it is possible that agomelatine could be most effective in patients where the depressive syndrome is associated with abnormal circadian rhythm. Identifying such patients specifically would require a carefully targeted clinical assessment and probably the use of laboratory measures such as actigraphy and measurement of dim-light melatonin onset. Reference Lewy21 This is unlikely to be a practical proposition in routine clinical settings at present.

We also need more information about the mechanism of action of agomelatine in terms of its putative interaction with 5-HT2C receptors and the most appropriate timing of administration in patients with depression. If agomelatine does indeed work through chronobiotic mechanisms, the timing of its administration in relation to the circadian cycle may be important. Hence the global instruction to administer the drug at ‘bedtime’ may not maximise its efficacy.

Footnotes

Declaration of interest

P.J.C. has been a paid member of advisory boards for Eli Lilly, Lundbeck and Servier.

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