Vortioxetine is indicated for the treatment of Major Depressive Disorder Vortioxetine has several novel pharmacological properties Vortioxetine is different from SSRIs/SNRIs due to direct effects at 5-HT receptors In addition to being a SSRI, vortioxetine has modulating activity of a variety of serotonin receptors Cognitive improvement is novel in series of antidepressant drugs

1. Vortioxetine
Review of Preclinical and Clinical Data

2. Vortioxetine: Introduction
 Indicated for the treatment of major depressive disorder (MDD)
 Approved by the FDA in September 2013 and the EMA in
October 2013
 An antidepressant with a multimodal mechanism of action
 SSRI + SERT inhibition with combined 5-HT1A antagonism
increase clinical efficacy compared to SSRI alone
 Has beneficial effect on cognitive performance
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3. Receptor Profile of Different Drugs
Lensa Zeng QY. Vortioxetine (Brintellix®): A Review. PharmaNote 2014;29(6). 3
Receptor Profiles for the New Multi‐Modal Antidepressants Compared with Commonly Used SSRIs and
SNRIs
DAT: dopamine transporter; NET: norepinephrine transporter; SERT: serotonin transporter; +: weak affinity; ++ : moderate
affinity ; +++: strong affinity

4. Function of Different Receptors
Lensa Zeng QY. Vortioxetine (Brintellix®): A Review. PharmaNote 2014;29(6). 4
Location and Clinically Relevant Function
of Selected Serotonin Subtype Receptors
5‐HT: serotonin; CNS: central nervous system; GI:
Gastrointestinal

5. Preclinical Profile of Vortioxetine
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6. Preclinical Findings
 Vortioxetine is a 5-HT3, 5-HT7 and 5-HT1D receptor antagonist,
a 5-HT1B receptor partial agonist and a 5-HT1A receptor
agonist and SERT inhibitor
 Vortioxetine's metabolites has no significant pharmacological
activities
 Pharmacological activities of vortioxetine are believed to be mediated
entirely by the parent compound
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7. Neurochemistry and in-vivo
Electrophysiology
 Vortioxetine increases extracellular 5-HT levels to more than
twice those obtained with an SSRI
 By 5-HT3 receptor antagonism
 5-HT1B auto-receptors antagonism
 5-HT1D presynaptic auto-receptors antagonism
 5-HT7 receptor antagonist
 Combining a 5-HT7 receptor antagonist and an SSRI increased
extracellular 5-HT levels in terminal areas more than the SSRI
alone
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8. Neurochemistry and in-vivo
Electrophysiology
 Vortioxetine appears to increase extracellular NE levels in
forebrain areas through activity at
 5-HT1A receptor agonism
 5-HT3 receptor blockade
 Vortioxetine increases extracellular dopamine (DA) levels in the
vHIP
 Activation of post-synaptic 5-HT1A receptors
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9. Neurochemistry and in-vivo
Electrophysiology
 Vortioxetine increases extracellular acetylcholine (ACh) and
histamine (HA)
 Positive effects on cognitive function
 Mediated via 5-HT receptor modulation
 Release of ACh is Mediated by 5-HT1A, 5-HT1B, and 5-HT3 receptors
 5-HT4 receptors increases extracellular HA
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10. Multi-target Occupancies of Vortioxetine
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Multi-target occupancies of vortioxetine in the
rat brain as measured by ex vivo binding. The
occupancies (% of total binding) of
vortioxetine at different doses for multiple
targets, 5-HT3, 5-HT7, 5-HT1B, 5-HT1A
receptors and the SERT in the rat brain are
depicted (mean +/- SEM)

11. Synaptic Transmission and Neuroplasticity
 Vortioxetine potentiate theta burst-induced LTP and counteract
5-HT-induced spontaneous inhibitory post-synaptic currents
(sIPSCs)
 Enhances excitatory synaptic transmission
 Reverse the LTP reduction
 Increases neuroplasticity
 Vortioxetine produce a significant increase in cell proliferation in the
dentate gyrus after only 1 day of treatment, whereas the SSRI fluoxetine,
tested under similar conditions, required >7 days to produce a similar
effect
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12. Synaptic Transmission and Neuroplasticity
 Vortioxetine increase dendritic length and the number of
dendrite intersections compared to vehicle controls,
 Vortioxetine accelerates the maturation of immature neurons
 Fluoxetine has no effect with above set of conditions
 Vortioxetine differs from the SSRIs fluoxetine and escitalopram
in promoting several measures of synaptic transmission
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13. Clinical Profile of Vortioxetine
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14. P’kinetics
 Bioavailability of 75% in humans
 Mean Tmax of 7–8 h
 Mean elimination half-life (T1/2) of 57 h upon oral administration
 Extensively metabolized by oxidation and subsequent
glucuronic acid conjugation
 Major metabolite is 3-methyl-4-(2-piperazine-1-yl-phenylsulfanyl)-
benzoic acid (Lu AA34443)
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15. P’kinetics
 The P450 enzymes responsible for the metabolism
 CYP2D6, CYP3A4/5, CYP2C9, CYP2C19, CYP2A6, CYP2C8, and CYP2B6
 The most important of these is CYP2D6
 No significant inhibition or induction of P450 enzymes, and is
thus less prone to drug–drug interactions
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16. P’dianamics
 Vortioxetine may exert antidepressant effects at SERT
occupancies as low as 50%
 In contrast, SSRIs and SNRIs may require SERT occupancy of at least 80%
to exert their antidepressant effects
 Vortioxetine mediates its antidepressant effects through its
activity at 5-HT receptors in addition to SERT inhibition
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17. Clinical Efficacy in MDD
 Out of 12 short-term studies, 8 studies has shown convincing clinical
efficacy in patients suffering from moderate to severe MDD
 The clinically effective doses range from 5 to 20 mg/day, which spans ~50 to
>80% SERT occupancy
 Support antidepressant effects of vortioxetine from both receptor modulation
and inhibition of the SERT
 SERT occupancies as low as 40–50% significantly increased extracellular 5-HT
levels translates into clinical efficacy in patients with MDD
 Vortioxetine's antidepressant efficacy in MDD patients with inadequate
response to SSRI or SNRI treatment may potentially support a
different mechanism of action
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18. Clinical Efficacy in MDD
 The long-term study showed that time to relapse was
statistically significantly in favor of vortioxetine compared to
placebo (hazard ratio of 2.01)
 relapse rates of 13% with vortioxetine versus 26% in the placebo group
 Efficacy of vortioxetine in treating MDD and in decreasing the
risk of recurrence of depressive episodes after remission is
achieved
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19. Cognitive Dysfunction in MDD
 In elderly patients Vortioxetine was superior to placebo on the pre-
defined primary efficacy analysis of the HAM-D24
 Analyses of pre-defined secondary outcome measures showed
superior performance versus placebo in
 Cognitive neuropsychological tests of executive function
 Attention
 Speed of processing
 Verbal learning and memory
 Path and subgroup analyses indicated that the beneficial effect of
vortioxetine on cognitive performance was largely a direct treatment
effect and not solely due to improvements in depressive symptoms
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20. Tolerability and Safety
 Well tolerated
 Vortioxetine showed better driving performance, improved
cognitive and psychomotor performance
 Most treatment-emergent adverse events (TEAEs) were of mild
or moderate intensity
 Nausea was most often transient, with a median duration of 10
to16 days
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21. Sexual Dysfunction
 The incidence of treatment-
emergent sexual dysfunction
(TESD)
 decreased libido
 abnormal orgasm
 delayed ejaculation
 erectile dysfunction
 Anorgasmia
 loss of libido
 ejaculation disorder
 disturbance in sexual arousal
 orgasmic sensation decreased
 sexual dysfunction
 and ejaculation failure
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22. Sleep Disruption
 The incidence of sleep-related TEAEs was low and not dose
related
 incidence of 2.0 to 5.1% compared to 4.4% with placebo
 SSRIs and SNRIs, which have an incidence of sleep-related
TEAEs significantly higher than placebo
 Vortioxetine is active at 5-HT1A, 5-HT1B, 5-HT3 and 5-HT7
receptors, all of which are involved in sleep stage regulation
 5-HT1A receptor stimulation promotes wakefulness
 5-HT1A and 5-HT1B receptor stimulation and 5-HT7 receptor antagonism
reduce rapid eye movement (REM) sleep
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23. Discontinuation Symptoms and Long-
term Safety
 Vortioxetine's low level of discontinuation symptoms
 partly related to its relatively long elimination half-life of 57 hours
 The long-term adverse event profile was similar to that
observed during acute 8-week short-term treatment with no
new safety findings
 Sexual dysfunction associated with long-term treatment of
vortioxetine was low overall
 Withdrawal due to TEAEs (7.9%) was comparable or lower than
with escitalopram (8.8%) or duloxetine (11.9%)
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24. Conclusion
 Vortioxetine is indicated for the treatment of Major Depressive
Disorder
 Vortioxetine has several novel pharmacological properties
 Vortioxetine is different from SSRIs/SNRIs due to direct effects at
5-HT receptors
 In addition to being a SSRI, vortioxetine has modulating activity
of a variety of serotonin receptors
 Cognitive improvement is novel in series of antidepressant
drugs
24

25. Thank You
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