MEActNOW🧠Brain Inflammation Colloborative:
Anti-depressants don't work for 30% of people who take them.
This study might have discovered why
The Discovery:
Scientists at the Imperial College of London and the University of South Carolina discovered that an inflammatory molecule called histamine directly inhibited the release of serotonin in the brain of mice.
Read more here:
https://www.imperial.ac.uk/news/228353/histamine-could-player-
Histamines:
Histamines are molecules produced by mast cells that cause the typical symptoms associated with allergies such as:
- watery eyes
- runny nose
- sneezing
- itching
Histamines can also be released in the brain by mast cells and some neurons.
Histamines and Treatment Resistant Depression:
If histamine can reduce the release of serotonin from neurons in the brain, SSRIs would not work.
SSRIs increase the concentration of serotonin in the synapses by preventing serotonin reuptake.
Therefore, SSRIs work AFTER the serotonin is released
from the neuron.
Could large amounts of histamine released by mast cells in the brain during neuroinflammation (1) be to blame for treatment-resistant depression in a subset of people?
Could large amounts of histamine released by mast cells in the brain during neuroinflammation (1) be to blame for treatment-resistant depression in a subset of people?
Antihistamines For Anxiety:
This finding might explain why the antihistamine Hydroxyzine effectively treats short-term anxiety in a subset of people, which is also caused by a lack of serotonin signaling.
This finding might explain why the antihistamine Hydroxyzine effectively treats short-term anxiety in a subset of people, which is also caused by a lack of serotonin signaling.
We at the Brain Inflammation Collaborative envision a world where the cause(s) of treatment-resistant depression is widely understood promptly diagnosed and treated.
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Read the manuscript here:
Inflammation-Induced Histamine Impairs the Capacity of Escitalopram to Increase Hippocampal Extracellular Serotonin
Commonly prescribed selective serotonin reuptake inhibitors (SSRIs) inhibit the serotonin transporter to correct a presumed deficit in extracellular serotonin signaling during depression. These agents bring clinical relief to many who take them; however, a significant and growing number of individuals are resistant to SSRIs. There is emerging evidence that inflammation plays a significant role in the clinical variability of SSRIs, though how SSRIs and inflammation intersect with synaptic serotonin modulation remains unknown. In this work, we use fast in vivo serotonin measurement tools to investigate the nexus between serotonin, inflammation, and SSRIs. Upon acute systemic lipopolysaccharide (LPS) administration in male and female mice, we find robust decreases in extracellular serotonin in the mouse hippocampus. We show that these decreased serotonin levels are supported by increased histamine activity (because of inflammation), acting on inhibitory histamine H3 heteroreceptors on serotonin terminals. Importantly, under LPS-induced histamine increase, the ability of escitalopram to augment extracellular serotonin is impaired because of an off-target action of escitalopram to inhibit histamine reuptake. Finally, we show that a functional decrease in histamine synthesis boosts the ability of escitalopram to increase extracellular serotonin levels following LPS. This work reveals a profound effect of inflammation on brain chemistry, specifically the rapidity of inflammation-induced decreased extracellular serotonin, and points the spotlight at a potentially critical player in the pathology of depression, histamine. The serotonin/histamine homeostasis thus, may be a crucial new avenue in improving serotonin-based treatments for depression. SIGNIFICANCE STATEMENT Acute LPS-induced inflammation (1) increases CNS histamine, (2) decreases CNS serotonin (via inhibitory histamine receptors), and (3) prevents a selective serotonin reuptake inhibitor (SSRI) from effectively increasing extracellular serotonin. A targeted depletion of histamine recovers SSRI-induced increases in extracellular hippocampal serotonin.
The FrogI self medicate with over the counter antihistamines to treat functional tick disorder, which a neurologist attributed to stress (and I don't. Not fully anyway).
I think this is onto something.
Oh, and I've been prescribed a year and a half ago ssri and got it sent me in a turmoil. It was not good.
Kim Possible 
@MEActNOW I'm so glad that they are finally looking at antihistamines for off-label use. For me, I get a lot of pain relief from them.