Why must some of you be so hasty to make assumptions??!
permastoned, do you really think there are that many undiscovered human receptors with potential to provide new aspects of euphoria or pleasure that we have yet to experience? I do not. We know the main small molecule neurotransmitters (5-HT, DA, NE) involved in pleasure/reward.
Firstly, I did not at any stage within my post state that I was interested only in the modulation of pleasure or euphoria. Once again, that was your assumption. Secondly, yes, let us assume that I was referring to the modulation of pleasure. "We know the small main molecule NTs involved in pleasure and reward... "
But wait, we are only just beginning to understand the downstream effects of activation of any of the SUBTYPES of these receptors. The variability of effects that have been noted from even subtleties such as activation of the 5ht2a causing dopamine release and the 5ht2c causing gaba release, lead to far more many new options for drugs than one may think. Supposedly antagonism of the 5ht7a is anxiolytic and antidepressive!
So you can have an agonist, antagonist, or inverse agonist of any of these receptor subtypes... and you can have a mixture of them to achieve an acquired effect.. and you think that the best drugs modulating these systems have been discovered yet? Think again, friend.
Continuing along the line of your assumption, delta opioid agonists have been shown to be potent antidepressives. H3 Antagonists have shown promise in the treatment of depression and a wide other range of diseases. And what about all the receptors that we have not yet discovered? Let alone, as Hammilton says, the alpha 2 sigma subunit of the voltage gated ca2+ channel or the GHB receptors, not even the receptor groups that we know about have been properly explored or exploited yet! And it is so arrogant for you to think that more that modulate pleasure or euphoria will not be found. And yes, a small molecule will be able to agonise/antagonise/inversely agonise this receptor. With regards to specificity, there are many specific small molecule drugs. Down to the pointt that we have drugs such as RS-102,221 "potent and selective antagonist at the serotonin 5-HT2C receptor, with around 100x selectivity over the closely related 5-HT2A and 5-HT2B receptors.'
Now combine this information with the fact that I am referring not only to the modulation of pleasure and euphoria, but to the modulation of any function of the CNS or PNS. Satiation of appetite, urinary incontinence, insomnia, etc. There are MANY.. that is right.. MANY undiscovered receptors to be exploited.. and we haven't even exploited those that we have discovered yet!!
Recently, a growing body of experimental data has showed that other classes of endogenous compounds, such as neuropeptides and amino acids, may play a significant role in the pathophysiology of affective disorders. With the development of neuroscience, neuronal networks and intracellular pathways have been identified and characterized, describing the existence of the interaction between monoamines and receptors in turn able to modulate the expression of intracellular proteins and neurotrophic factors, suggesting that depression/antidepressants may be intermingled with neurogenesis/neurodegenerative processes.
No shit that the activation of a monoamine receptor in turn causes downstream effects within the target cell such as varsious protein expression, BDNF release, neurogenesis, etc... That is generally what the idea of activation of a GPCR is.. your article does not give your cause huge support. Instead it attempts to be a rather vague review of the mechanism of the involvements of peptides following activation of receptors...
To make a good "small molecule peptidomimetic" in the first place, you have to understand how the peptide itself works at the receptor. Hence if you don't have the right grounds, you will never even have a chance.
Again, I never at any stage implied that peptide research was not necessary in order for effective small molecules to be developed. All that I originally said was that small molecules have not lost their role of being stars of the pharmaceutical industry, and neither will they for rather long time in my opinion.
Nor am I the one who dick-sizes:
Quote:
Originally Posted by permastoned View Post
Yes.. I took 150mg of d-amp and 30 seleg and nothing. Time for permastoned to take a break from the phetty phetties. And his exams aren't even over! Poor poor permy.
Sir, you are mistaken. Firstly, the quote you post is from an entirely different thread, which was completely unrelated to this one. Secondly, what you mistook for 'dick-sizing' was in fact a desperate cry for help. If I were to dick size, it would look like this:
Oh, well, what the hell. What about the oxytocin, orexin, and human growth hormone receptors? Aren't those just a bit large... er something?
Yo' mumma just a bit large... er something...
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