Serotonin in Fear and Anxiety
Abstract
That the neurotransmitter serotonin (5-HT) has a central role in fear and anxiety is
supported by numerous experimental and clinical studies. Arguably the most illustrative
example is the effect of serotonergic-acting drugs, and in particular the selective
serotonin reuptake inhibitors (SSRIs), in the treatment of anxiety disorders. Interestingly,
long-term administration is required to induce a dampening effect on anxiety, while on
the contrary acute administration can aggravate the symptoms in susceptible individuals.
Freezing behaviour is a well-established measure of fear and anxiety, foremost assessed
in studies performed on rodents. The bulk of the experiments presented in this thesis
investigate the effect of pharmacological manipulations of the serotonin system on
conditioned and unconditioned freezing behaviour.
In paper I, the importance of an intact serotonergic neurotransmission in fear
conditioning was explored. The serotonin system was compromised by administration of
the serotonin-depleting agent para-chlorophenylalanine (PCPA). PCPA impaired both acquisition and expression of conditioned fear without imposing an effect on memory
consolidation, supporting the notion that fear-induced release of serotonin primarily
promotes rather than dampens fear conditioning.
In paper II, the effects of 5-HT2A receptor agonism and antagonism alone and in
combination with administration of an SSRI were investigated. The first main finding was
that while administration of neither the 5-HT2A receptor antagonist MDL 100907 nor the
5-HT2A receptor inverse agonist pimavanserin consistently reduced expression of
conditioned freezing, a marked reduction of fear was observed after administration of
either drug combined with an SSRI. The second main finding was that administration of
both a selective agonist for the 5-HT2A receptor and the psychedelic drug psilocybin
reduced expression of conditioned freezing, an effect that was totally abolished by coadministration
with MDL 100907. The experiments demonstrated that the 5-HT2A
receptors have the ability to modulate fear expression in both directions, putatively
involving 5-HT2A receptor populations in different areas of the brain.
In paper III, the effects of chronic and acute administration of an SSRI were compared.
Chronic administration but not acute administration induced a dampening effect on
anxiety. Since these findings mirror the clinical situation, context-conditioned freezing
could supposedly be applied in animal studies on the mechanism of action for the sluggish
effects of SSRIs in anxiety disorders.In paper IV, the effect of acute administration of an SSRI was evaluated in a model of
unconditioned fear. Acoustic noise bursts constituted the unconditioned stimulus. The
SSRI increased the expression of unconditioned fear. Unconditioned models are
tentatively related to panic disorder, the condition in which aggravation of anxiety after
acute administration of an SSRI is most pronounced, suggesting that noise burst induced
freezing presumably could be a useful tool in preclinical studies on the anxiety-provoking
effects of SSRIs.
In paper V, the effect of 5-HT6 receptor manipulations on gut motility was explored. It was
found that 5-HT6 receptor antagonists reduced defecation in both stressed (fear
conditioned) and non-stressed animals while an agonist for the same receptor was void
of effect. This mechanism could putatively be utilized in the treatment of irritable bowel
syndrome with diarrhea (IBS-D).
In summary, the studies on rats presented in this thesis suggest that i) intact serotonergic
transmission is required for both acquisition and expression of conditioned fear, ii) that
the 5-HT2A receptor has an important role in modulating conditioned fear, iii) that chronic
administration of an SSRI, in contrast to acute administration, reduces conditioned fear,
iv) that acute administration of an SSRI increases unconditioned fear and v) that 5-HT6
receptor antagonism impairs gut motility.
Parts of work
I. Hagsäter SM, Pettersson R, Holmäng A and Eriksson E, “Serotonin depletion reduces both acquisition and expression of context-conditioned fear”, Submitted II. Hagsäter SM, Pettersson R, Pettersson C, Atanasovski D, Näslund J and Eriksson E, “A complex impact of the 5-HT2A receptor on conditioned fear revealed by systemic administration of different 5-HT2A ligands including pimavanserin and psilocybin”, Submitted III. Pettersson R, Hagsäter SM, Carlsson B, Karlsson L and Eriksson E, “Chronic but not acute administration of escitalopram reduces context-conditioned fear”, Submitted IV. Hagsäter SM, Thorén J, Pettersson R and Eriksson E, “Selective serotonin reuptake inhibition increases noise burst-induced unconditioned and context conditioned freezing”, Acta Neuropsychiatrica, 2019, 31, 46-51, ::doi::10.1017/neu.2018.26 V. Hagsäter SM, Lisinski A and Eriksson E, “5-HT6 receptor antagonism reduces defecation in rat: A potential treatment strategy for irritable bowel syndrome with diarrhea”, European Journal of Pharmacology, 2019, 864, 172718, ::doi::10.1016/j.ejphar.2019.172718
Degree
Doctor of Philosophy (Medicine)
University
University of Gothenburg. Sahlgrenska Academy
Institution
Institute of Neuroscience and Physiology. Department of Pharmacology
Disputation
Fredagen den 6 november 2020, kl. 13.00, Hörsal Carl Kylberg, Medicinaregatan 7B, Göteborg https://gu-se.zoom.us/j/66927706333?pwd=bkl0ZzFDK3Q2MVZrVGpuMEtqV3pOQT09
Date of defence
2020-11-06
melker.hagsater@neuro.gu.se
Date
2020-10-16Author
Hagsäter, Melker
Keywords
serotonin
anxiety
fear
SSRI
IBS
Publication type
Doctoral thesis
ISBN
978-91-8009-001-8 (PDF)
978-91-8009-000-1 (PRINT)
Language
eng