Author |
Topic: Fresh Research - G Protein-Coupled Receptors (Read 681 times) |
|
floridian
Guest
|
 |
Fresh Research - G Protein-Coupled Receptors
« on: Nov 25th, 2003, 2:28pm » |
 Quote  Modify
 Remove
|
This article discusses posibility that "G protein-coupled receptors" interact with trace amines ("minor" neurotransmitters) to contribute to clusters and migraines. The abstract is fairly vague, the connection is not 100%, but this line of research could yield valuable information over time.
Quote:Headache. 2003 Nov;43(10):1125-1126.
D'Andrea G, Terrazzino S, Fortin D, Coc P, Balbi T, Leon A. Elusive amines and primary headaches: historical background and prospectives. Neurol Sci. 2003;24(suppl 2):S65-S67.
Although the role of trace amines such as tyramine, octopamine and synephrine in the pathogenesis of migraine has been debated for decades, this issue remains still unresolved. In spite of a relevant body of work, the inability to demonstrate specific receptors for these compounds and the lack of sensitive non-radioactive methods for the detection of trace amines in biological samples have limited their investigation in humans. However the recent identification of a new, large family of G protein-coupled receptors, some of which bind and are activated by trace amines, has focused renewed attention on these compounds. This discovery, together with the possibility of providing novel insights for evaluation of the pathophysiological role of trace amines in primary headaches, may offer new opportunities for pharmacololgical [sic] strategies acting on these receptors. In light of the new scientific background, this review outlines a historical perspective and summarizes evidence supporting a role of trace amines in the pathogenesis of migraine and cluster headache. Comment: This article reminds me of the early articles on migraine which suggested that 5-HT was taken up by platelets, transported, and then taken up by sympathetic nerves before being released as a false transmitter. Might these trace amines act similarly as surrogate transmitters? DSM |
|
|
|
 IP Logged |
|
|
|
CJohnson
New Board Old Timer
Cannot kill the family, Battery is found in me
Gender: 
Posts: 442
|
|
Re: Fresh Research - G Protein-Coupled Receptors
« Reply #1 on: Dec 16th, 2003, 12:06pm » |
Quote Modify
|
on May 30th, 2003, 8:26am, dougW wrote:another article in Cephalalgia, Volume 23 Issue 5 Page 354 - June 2003. Studies before have shown messed up 5HT processes, now another.
I can't get the full article (yet).
Doug Wright
Abnormal 5-HT1D receptor function in cluster headache: a neuroendocrine study with sumatriptan
L Pinessi, I Rainero, W Valfrč, R Lo Giudice, M Ferrero, C Rivoiro, E Arvat1, L Gianotti1, P Del Rizzo2 & P Limone2
The purpose of this study was to assess the sensitivity of 5-HT1D receptors in patients with episodic cluster headache using sumatriptan as a pharmacological probe. The drug, a selective 5-HT1B/1D agonist, stimulates the secretion of growth hormone and inhibits the release of prolactin, adrenocorticotropic hormone (ACTH) and cortisol. These effects may be used to explore the function of serotonergic systems in vivo. We administered subcutaneous sumatriptan and placebo to 20 patients with cluster headache (10 in the active phase and 10 in the remission period) and to 12 controls. The sumatriptan-induced increase of growth hormone concentrations was significantly (P < 0.05) blunted in patients with active cluster headache. Prolactin and ACTH responses to the drug were significantly (P < 0.05) reduced in patients with cluster headache, both in the active and in the remission period. Our results suggest that cerebral serotonergic functions mediated by 5-HT1D receptors are altered in patients with episodic cluster headache.
|
|
on May 30th, 2003, 12:04pm, CJohnson wrote: This post and the previous one (twin study) suggest the possibilty of an anomoly in the gene (or genes) which encode for the 5HT1D receptor, or even an anomoly in the gene which encodes serotonin transporter proteins.
In fact, in 1996, NIH researchers reported finding a repeated stretch of DNA in the gene that encodes for the serotonin transporter protein. These researchers postulate that persons with shorter repeats in this gene may produce substandard quantities of the serotonin transport protein.
If that is the case, then longer repeats might produce too many of these proteins. If too many of these transporter proteins are present and active in the synapse, then serotonin could be swept from the synapse by these proteins at too rapid a rate. This action could prevent an adequate amount of serotonin from settling into the serotonin receptors.
More wild speculation. If the production of these proteins is regulated according to circadean rhythm (which the hypothalamus influences) maybe these proteins are being produced and released too often, in direct relation with the anomoly in the circadean rhythm.
PFDANs
-Curtis |
|
|
|
IP Logged |
Through water and fire. From the lowest dungeon to the highest peak, I fought the Beast. Until at last, I threw down my enemy and smote his ruin upon the mountainside.
|
|
|
|
|
|
Home
Help
Search
Members
Member Map
Login
Register
Reply
Notify of replies
Send Topic
Print
test rss