No problem, keep us updated, i allways look further then the issues of differened substances and look for ways around it.
Baclofen: alternative for Phenibut ????
#31
Posted 27 February 2016 - 01:46 PM
#32
Posted 04 March 2016 - 11:20 AM
oh man...USPS misplaced my package!!! Now the only option for me is to get phenibut from a Chinese supplier via http://alibaba.com.
In hope of finding a good supplier, I created another post http://www.longecity...ibabacomanyone/. Will keep you updated.
#33
Posted 04 March 2016 - 05:10 PM
oh man...USPS misplaced my package!!! Now the only option for me is to get phenibut from a Chinese supplier via http://alibaba.com.
In hope of finding a good supplier, I created another post http://www.longecity...ibabacomanyone/. Will keep you updated.
Sarif,
Liftmode is generally very good about sending free replacement products if there is some kind of loss in transit; I would contact them. USPS has lost so many of my packages that now I spring for the three-day UPS shipping in the US for just about everything. Contact USPS and see if the box was insured at all, or not. Their flat-rate boxes are insured in the US for $50, although several of the overseas packages that I have shipped have been at least partially insured by the USPS for delivery to foreign customs.
#34
Posted 04 March 2016 - 05:12 PM
What do you mean misplaced your package? does it have tracking? demand it to be send to the correct adress, phone them up saying it are important items from your grandma, with a extremely eig emotional value, keep on going on how upset she will be if its lost etc, this shit got me stuff send to my closed po box for example, the post office crew was looking out for it, or got me backpay in nhs money, basicly keep going on about something exhaust the other person.
also it should have tracking how else they know its misplaced?
#35
Posted 04 March 2016 - 06:06 PM
medievil,
Since the GABAB agonism should be comparable, why is phenibut addictive and baclofen anti addictive? baclofen supresses da, so the drug is not associated with increased dopamine which makes a drug addictive, yet it looks like phenibut does increase da, is it possible the
#36
Posted 04 March 2016 - 09:22 PM
I think that you are a bit blurred regarding the difference in the psychopharmacological definitions of "dependence" versus "addiction". Addiction of course being the psychological craving for the effects of a substance over one's "normal" waking consciousness; and dependence being a physical need for a exogenous substance in order for that biological mechanism to function in the same way that it did before the initial introduction of the exogenous substance.
I said baclofen is not addictive, which it isnt, im aware i can cause dependency, theres noone that craves baclofen, but im aware it causes withdrawals
#37
Posted 04 March 2016 - 09:27 PM
I disagree that baclofen is abused, it may have relaxing have effects but its pretty much enheared off, that said benzos do increase dopamine in reward related pathways and is abused, the same is true for alcohol.
]
As I stated, I have never heard of a group of high school kids rounding up all of their buddies to gather around and "get high" on Phenibut.
That is because its a very weak drug, it does cause a high tough but kids going to school look for more potent stuff
#38
Posted 04 March 2016 - 09:30 PM
I disagree that baclofen is abused, it may have relaxing have effects but its pretty much enheared off, that said benzos do increase dopamine in reward related pathways and is abused, the same is true for alcohol.
]
As I stated, I have never heard of a group of high school kids rounding up all of their buddies to gather around and "get high" on Phenibut.
That is because its a very weak drug, it does cause a high tough but kids going to school look for more potent stuff
While on the contrary, both addiction and dependency to benzodiazepines is based almost entirely on the direct agonism of the GABA -A Receptors themselves.
I disagree entirely, addiction and abuse is entirely caused by their dopaminergic effects
#39
Posted 04 March 2016 - 09:37 PM
The NMDA Receptors also play a very important role in the case of true, psychological “addiction” as well, by blocking the association of those “reward center” memories from the hypothalumus and nucleus accumbens, with our sensory input. (ie, Things like “needle fixation”, in which cases some ex IV drug users will inject water when they get a craving, simply because the brain still associates the “ritual” act of injecting with a pleasurable reward sensation). Because NMDA Receptor antagonism blocks the formation of chloride channel-mediated substance/receptor associations, as well as increases activity in the locus coeruleus (the group of neuronal cells associated with our sense of “novelty”), NMDA Receptor modulator drugs are proving to even more and more viable and refined in developing treatments for tolerance associated with receptor down-regulation, as well as addiction by inhibiting the formation of pleasure/reward associations with habitual drug use.
Evidence for this? NMDA antagonists work for tolerance and addiction because the nmda pathway (following nitric oxide) causes changes in the receptors certain drugs act on, addiction occurs because drugs program themselves in the brain trough the nmda pathway, first sensitisation occurs making the brain sensitised to particular drugs, as most ppl notice the first time someone uses a drug they wont notice anything while the next times the effects become apparent, after that receptor downregulation occurs, addiction occuring because of association with the rewarding effects only plays a minimal role
#40
Posted 04 March 2016 - 09:39 PM
jaiho,Unfortunately, anhedonia is a very broadly-encompassing disorder in terms of pre-synaptic neurotransmitter systems, and is also highly variable among individuals. So, there isn’t really a good catch-all class of drugs that can be recommended for everyone. Early trials with mixed monoamine/catecholamine reuptake inhibitors (particularly the “Triple Reuptake Inhibitors”). That inhibit Serotonin, Dopamine, and Norepinephrine reuptake work for a large majority, but the effective dosages often have to be continually increased due to the development of tolerance to the main monoamine neurotransmitter receptor sites. Other patients respond to some acetylcholine receptor agonists, glutamate modulators, and even cannabinoids. Unfortunately, it really comes down to working with the patient in question, one-on-one to find something that works, long-term. If you’d like to send me a private message, I can advise you on some easy-to-acquire options to test out, based on your personal responses to treatment.
Exactly, im highly educated on anhedonia and as said here the treatment is highly individual, i can also provide information on effective treatments if you contact me
#41
Posted 04 March 2016 - 09:51 PM
Sarif,Having a benzodiazepine drug with a long halflife around (such as as diazepam or clonazepam suggested) could’nt hurt, but I certainly would not advise using ANY GABA -A Receptor agonist to discontinue Phenibut use unless you absolutely had to (which you really never should, if you wean down your dose gradually enough), or in very small doses. Since you already stated that you have bad impulse control in your original post, quitting Phenibut by using a benzodiazepine could potentially be substituting a mild “addiction” for a potentially much more dangerous one. I certainly would not use a week’s supply of a long-acting benzodiazepine like the suggested diazepam to discontinue Phenibut use. If you wean your dose down gradually enough for your receptors to up-regulate sufficiently (even weaning over the course of a month or two, in the most extreme cases) then you shouldn’t notice anything like the horrendous Phenibut withdrawal stories that pollute the internet. If you were to stop using Phenibut with a benzodiazepine drug, and then decided that you liked the effects of the benzodiazepine, you could be substituting dependency to a GABA -B agonist (Phenibut) to a much more severe GABA -A Receptor agonist. While Phenibut withdrawal can be very unpleasant if done abruptly, Benzodiazepine Withdrawal Syndrome can be a medical emergency, inducing Tonic Clonic, Opclonic, and Grand Mal seizures, dangerous abrupt shifts in blood-pressure, and cardiac arrhythmia. You mentioned having a difficult time with impulse control, so this is just something to keep in mind.
Stopping phenibut adddiction by gradually reducing the dose is hard, while you can easily do it the easy way,getting addicted to benzos by using them for withdrawal extremely unlikely, benzos are weak crap and deciding youd like them and getting addicted to them instead is laughable imo, like benzo withdrawal so is phenibut withdrawal a medical emergency, it can such as benzos cause life treatening seizures. I am very impulsive and have a extremely addictive personality and short term use of benzos is absolutely no issue, its highly unlikely that someone addicted to phenibut would get addicted to benzos as those are pretty much useless reward free drugs.
Saying that phenibut addiction is benign compared to benzos is extremely ignorant, withdrawal from phenibut is dangerous and life treatening simular to GHB addiction.
I would say that withdrawing of phenibut by dose reduction is too hard to be practical
I would second the suggestion of clonazepam, like diazepam its a extremely good benzo for withdrawals
#42
Posted 14 March 2016 - 07:00 PM
medievil,
" I disagree entirely, addiction and abuse is entirely caused by their dopaminergic effects "
That’s ridiculous. The Dopamine/Norepinephrine Reuptake Inhibitor antidepressants Bupropion and some tricyclics like Amineptine produce much greater synaptic dopamine influx than benzodiazepines or Phenibut, yet I have never heard any confirmed or sustained cases of anyone abusing or reporting a “high” from these compounds. Additionally, the indirect dopamine influx that is caused by indirect a2Ca-subunit Sodium Channel Activity as a consequence of Benzodiazepine Binding Site agonism occurs almost entirely in the prefrontal cortex, in the frontal and parietal lobes, while the dopamine reuptake inhibition that occurs due to the action of drugs like Amineptine is more widespread - even reaching some regions of the nucleus accumbens, yet no “high” or reward pathway association is associated with these drugs.
" Evidence for this? NMDA antagonists work for tolerance and addiction because the nmda pathway (following nitric oxide) causes changes in the receptors certain drugs act on, addiction occurs because drugs program themselves in the brain trough the nmda pathway, first sensitisation occurs making the brain sensitised to particular drugs, as most ppl notice the first time someone uses a drug they wont notice anything while the next times the effects become apparent, after that receptor downregulation occurs, addiction occuring because of association with the rewarding effects only plays a minimal role "
Sure, (Baird & Crousse 1997; Eckhert et al 2001, etc). I also point to several of the publications of Alan Reirdon and David Nichols. This is well established. For an example that I happen to have handy, look at Methadone and the cited references from the Wikipedia page:
Levomethadone is a full µ-opioid agonist Dextromethadone does not affect opioid receptors but binds to the glutamatergic NMDA (N-methyl-D-aspartate) receptor, and thus acts as a receptor antagonist against glutamate. Methadone has been shown to reduce neuropathic pain in rat models, primarily through NMDA antagonism. Glutamate is the primary excitatory neurotransmitter in the CNS. NMDA receptors have a very important role in modulating long term excitation and memory formation. NMDA antagonists such as dextromethorphan (DXM), ketamine (a dissociative anaesthetic, also M.O.A+.), tiletamine (a veterinary anaesthetic) and ibogaine (from the African tree Tabernanthe iboga, also M.O.A+.) are being studied for their role in decreasing the development of tolerance to opioids and as possible for eliminating addiction/tolerance/withdrawal, possibly by disrupting memory circuitry. Acting as an NMDA antagonist may be one mechanism by which methadone decreases craving for opioids and tolerance, and has been proposed as a possible mechanism for its distinguished efficacy regarding the treatment of neuropathic pain. The dextrorotary form (d-methadone) acts as an NMDA antagonist and is devoid of opioid activity: it has been shown to produce analgesia in experimental models of chronic pain. Methadone also acted as a potent, noncompetitive α3β4 neuronal nicotinic acetylcholine receptor antagonist in rat receptors, expressed in human embryonic kidney cell lines.[47]
^ From the Methadone Wikipedia page, under the pharmacology section.
The above statements are very vague and unclear. In all honesty, I don't even know which specific mechanism you are referencing. (Perhaps if you elaborated a bit more). It sounds to me like you are stating that all psychoactive drugs have some binding affinity for, and action at, NMDA Receptors, before binding to their target receptors. ?.. This is not true at all, and in fact, most psychoactive drugs have no affinity for, or action at the NMDA Receptors at all, yet many of those same drugs' development of tolerance and addiction can be slowed and deterred by the use of an NMDA Receptor antagonist.
" Stopping phenibut adddiction by gradually reducing the dose is hard, while you can easily do it the easy way,getting addicted to benzos by using them for withdrawal extremely unlikely, benzos are weak crap and deciding youd like them and getting addicted to them instead is laughable imo, like benzo withdrawal so is phenibut withdrawal a medical emergency, it can such as benzos cause life treatening seizures. I am very impulsive and have a extremely addictive personality and short term use of benzos is absolutely no issue, its highly unlikely that someone addicted to phenibut would get addicted to benzos as those are pretty much useless reward free drugs.
Saying that phenibut addiction is benign compared to benzos is extremely ignorant, withdrawal from phenibut is dangerous and life treatening simular to GHB addiction.
I would say that withdrawing of phenibut by dose reduction is too hard to be practical
I would second the suggestion of clonazepam, like diazepam its a extremely good benzo for withdrawals "
A little over a year ago, we analyzed a meta-analysis of 180 subjects all using standard therapeutic doses (500mg up to 2000mg daily) of Phenibut, specifically for Situational Anxiety and/or Panic Attack Disorder. All of these participants were under the supervision of qualified psychiatrists or pharmacologists that are highly trained to spot potential problems during treatment. Out of all participants, not one experienced any significant difficultly in gradually weaning down their dose after the duration of the study. Now, I am absolutely aware that some people (particularly those who order large supplies from the internet) have a difficult time stopping Phenibut, particularly when they use much more than is required to chase that tiny dopamine influx. However, if not one of our study participants experienced any significant withdrawal syndrome upon gradually discontinuing Phenibut in doses from 500mg - 2000mg, than I am certain that many of the people who post in these forums with the crazy Phenibut withdrawal horror stories could do the same, as long as they exercised good self-control, and stick to a logical dose-reduction regimen. Now, I agree; some people are simply too impulsive to do this, and have addictive personalities through no fault of their own. However, although Phenibut’s GABA -B Receptor agonism, and it’s action as a gabapentinoid blocker at a2o-subunit containing Voltage-Gated Ca+ Channels do produce mild physical dependence, I still can’t justify calling Phenibut a serious drug of addiction. Not all that long ago, Phenibut was a well-kept secret, that many had to either synthesize it themselves, or contact a foreign lab to produce it. It may be that because it has become cheaper and more widely available that many internet order users are reporting having just a hard time “kicking it”, and although it may produce a mild mood boost, I can’t see many people actually “craving a hit of Phenibut”, just like you stating that nobody “craves” Baclofen. I have been doing this for years, and although I agree with you that 98% of the population that is exposed to Baclofen will not crave it’s effects, there are those few out there that do. (Just like the very small minority that abuse dopamine and serotonin antagonists like Chlorpromazine or Tramadol, which make the majority of people feel like shit).
" Stopping phenibut adddiction by gradually reducing the dose is hard, while you can easily do it the easy way,getting addicted to benzos by using them for withdrawal extremely unlikely, benzos are weak crap and deciding youd like them and getting addicted to them instead is laughable imo, like benzo withdrawal so is phenibut withdrawal a medical emergency, it can such as benzos cause life treatening seizures. I am very impulsive and have a extremely addictive personality and short term use of benzos is absolutely no issue, its highly unlikely that someone addicted to phenibut would get addicted to benzos as those are pretty much useless reward free drugs.
Saying that phenibut addiction is benign compared to benzos is extremely ignorant, withdrawal from phenibut is dangerous and life treatening simular to GHB addiction.
I would say that withdrawing of phenibut by dose reduction is too hard to be practical
I would second the suggestion of clonazepam, like diazepam its a extremely good benzo for withdrawals "
-J. Gona
Oracle Laboratories
NeuroPsych Institute
Edited by Oracle Laboratories, 14 March 2016 - 07:04 PM.
#43
Posted 15 March 2016 - 01:01 PM
J. Gona,
Thank you for taking the time to provide such a well written and informative response. I've often considered trying low doses of phenibut (<600 mg/day) to help with pretty severe social anxiety and mild depression but haven't yet due to all the horror stories I've read online about tolerance and addiction to the substance. Based on the information you've provided, it would appear low daily doses (<2g/day) shouldn't be a problem as long as a person slowly tapers down their dosage if/when deciding to discontinue use. While I may not understand everything you wrote, I look forward to reading (and learning from) your future contributions to this site.
#44
Posted 15 March 2016 - 06:04 PM
Hi there,
I always refused to test phenibut because its deregulation of GABA-B receptors, and all the horrors stories heard on the internet, and the fast tolerance.
I have strong social anxiety, and successfully tried Kava in the past. Only problem with Kava: the taste is strong, and it takes some time to prepare.
Also Kava cost more per dose than phenibut.
The advantage of Kava: no tolerance, a reverse tolerance instead where you become more sensitive to the kavalactones the more often you consume.
However Phenibut is still in my watch list, and recently I noticed this thread on reddit: https://www.reddit.c...essions_report/
So it seems that F-Phenibut is somewhere in between Baclofen and Phenibut in regards of effects and tolerance/potency.
If this compound is as effective as Phenibut as making you a social butterfly, and has low tolerance and low addiction potential, this could become the silver bullet in term of anxiety control.
But for the moment it's still a research chemical, so who knows the safety and side effects?
#45
Posted 15 March 2016 - 08:59 PM
....
If you’re interested, I can put you in touch with Roger Hutton (a colleague of mine from The Indiana Neural Research Center)
......
-J. GonaPsychopharmacologist,Psychotropic Treatment Specialist
Oracle Laboratories
NeuroPsych Institute
Odd...
For such a prominent biochemist and drug developer , I cannot find a SINGLE trace on the net of a John Gona ( except for a programmer in Indiana), of an Oracle Laboratories ( except for the health department affairs of the well known Oracle database corporation, wich seems totally unrelated to this ) , absolutely no trace of "Oracle Laboratories Journal of Applied and Investigative Pharmacology, and The NeuroPsych Journal of Psychopharmacology" or "NeuroPsych Laboratory Press"
Zero references on the net of the "Indiana Neural Research Center" or Roger Hutton...
Care to enlighten us, "John " ?
Edited by BlueCloud, 15 March 2016 - 09:21 PM.
#46
Posted 16 March 2016 - 01:57 AM
I'd quite like to try the pure 'R' isomer of Phenibut someday.
R-phenibut binds to the α2–δ subunit of voltage-dependent calcium channels and exerts gabapentin-like anti-nociceptive effects
Highlights
- R-phenibut binds to the α2–δ subunit of the voltage-dependent calcium channel (VDCC).
- The binding affinity of R-phenibut for the α2–δ subunit of the VDCC is 5 times higher than that for GABAB receptor.
- R-phenibut exerts gabapentin-like anti-nociceptive effects in the formalin-induced paw-licking and CCI tests.
- The anti-nociceptive effects of R-phenibut are not mediated through GABABreceptor
Also quite noteworthy:
R-phenibut is responsible for the pharmacological activity of racemic phenibut, and this activity correlates with its binding affinity for GABAB receptors. In contrast, S-phenibut does not bind to GABAB receptors.
http://www.sciencedi...09130571530037X
#47
Posted 16 March 2016 - 12:18 PM
....
If you’re interested, I can put you in touch with Roger Hutton (a colleague of mine from The Indiana Neural Research Center)
......
-J. GonaPsychopharmacologist,Psychotropic Treatment Specialist
Oracle Laboratories
NeuroPsych Institute
Odd...
For such a prominent biochemist and drug developer , I cannot find a SINGLE trace on the net of a John Gona ( except for a programmer in Indiana), of an Oracle Laboratories ( except for the health department affairs of the well known Oracle database corporation, wich seems totally unrelated to this ) , absolutely no trace of "Oracle Laboratories Journal of Applied and Investigative Pharmacology, and The NeuroPsych Journal of Psychopharmacology" or "NeuroPsych Laboratory Press"
Zero references on the net of the "Indiana Neural Research Center" or Roger Hutton...
Care to enlighten us, "John " ?
Well, I certainly do not claim to be a "prominent biochemist and drug developer" compared to many university academic or government institution researchers. I am simply one of many independent pharmacologists operating biochemical and/or analytical laboratories, not affiliated with a government institution or a state university, like almost all researchers and facilities associated with Oracle Laboratory Institute (under the umbrella of Orial NeuroPsych Institute) - a network of independent facilities and researchers. No, Oracle Database Corporation is completely unrelated. Our Journal of Applied and Investigative Pharmacology (a publication of NeuroPsych Laboratory Press) covers findings related to the research undertaken by the researchers and facilities affiliated with Oracle Laboratory Institute. Unfortunately our main website is down for renovation, and the stored back-up version is incomplete (and was long ago abandoned to complete our main site). Once everything is back online, I had already intended to share pertinent publications with the membership here. (Although I was advised by the moderation team that in order to share our website links here, I would need to contact the site to setup banner ads).
Indiana Neural Research Center, as far as I know is a post-graduate organization of Indiana University / Purdue University of Indianapolis. I am not entirely sure what Roger's official affiliation is as far as Purdue anymore, but I will attempt to dig up his NMDA Receptor Modeling work and post a link here, so long as is does not violate the pay-gate agreement with the publisher.
Unfortunately, as a new member, I can only make a limited number of posts, so I cannot possibly to respond to everything that I would like to. In good time.
-J. Gona
#48
Posted 16 March 2016 - 12:26 PM
(Accidental post, cannot delete)..
Edited by Oracle Laboratories, 16 March 2016 - 12:28 PM.
#49
Posted 16 March 2016 - 12:30 PM
Oracle Laboratory Institute (under the umbrella of Orial NeuroPsych Institute) - a network of independent facilities and researchers.
I just find it very odd that no search engine ( I tried Google and Bing ) is able to come up with even a SINGLE direct or indirect link or reference to any of these characters ( John Gona, Robert Hutton) or institutes or laboratories ( except for Indiana university, on wich a search on their own website doesn't show any Neural research Center or Robert Hutton )....
But perhaps your work, as well as your laboratories and institutes, are super-secret and confidential, to the point of becoming invisible and leaving no trace whatsoever on the World Wide Web...Very hard in this day and age. I'm quite...uuh... impressed.
Edited by BlueCloud, 16 March 2016 - 12:43 PM.
#50
Posted 16 March 2016 - 01:01 PM
My name is John Gona, and I am the founder of Oracle Laboratory Institute and NeuroPsych Laboratory Press (which encompasses Oracle Laboratories Journal of Applied and Investigative Pharmacology, and The NeuroPsych Journal of Psychopharmacology. I am a biochemist and drug developer. My actual title is Phsychopharmacologist, and Psychotropic / Nootropic Treatment Specialist.
....
My research has led to the development of dozens of novel drugs, and even more derivatives and intermediate compounds.......
I have also helped to develop and improve various laboratory analytical instruments at our facilities and associate's facilities, such as Scanning Electron Microscopes; High-Performance Liquid & Gas Chromatographers; Polarimeters;.....
In addition to my laboratory research work, I also act as a pharmaceutical consultant for many pharmacological institutions, psychiatrists, neurologists, medical doctors, and work alongside these institutions, helping to develop custom-tailored treatment plans for their patients.
A more extensive background of my research experience, novel compound developments, publications, technological patent applications, and collaborative institutions can be provided upon request.
Wow... truly impressive achievements. Even more impressive to achieve all this while keeping your name, your work and your "laboratories" completely hidden from public eyes, Internet, and search engines. Probably an even greater achievement than your scientific and technological innovations. My hat is off to you sir
Now, let's be serious for a minute. You obviously possess a certain amount of serious scientific knowledge. So, why this whole masquerade and this whole fictitious persona and world you invented ? What is exactly the point ??? Perhaps an experiment in how easy it is to fool adult rational people ?
Seriously, I'm curious.
Edited by BlueCloud, 16 March 2016 - 01:52 PM.
#51
Posted 17 March 2016 - 12:46 AM
Look, I do not know you, and have had absolutely no contact with other than the numerous posts of mine that you are trolling on this website. (Certainly no intellectual communication). I came to this site at the request of several existing members, to volunteer my time and offer my expertise to the general membership here, to clear up misinformation, misconceptions, and misinterpretations of published material that seem to be oh so prevalent online in this particular field. I came to this site as a courtesy, to volunteer some of my spare time, and I have absolutely no desire to argue with any internet poster who happens to be trolling posts that I have made here.
Aside from the large pharmacological publishers, and state university and government agency researchers that have large online collections of material, there are an equal if not greater number of independent researchers in the private sector, running privately-owned biochemical and analytical laboratories. The great part about the US is that we have the right to assemble - that means that if you are so inclined, have to necessary background education, the equipment, and the organizational skills, you can form any sort of organization that you want to. And, like myself, if you are so inclined, you can even establish a non-profit pharmacological institute. - All that is required is a group of like-minded individuals with the right skill-set and resources to pull it off. I have no desire to (and in fact, I refuse to) argue with you and defend my work on thread after thread on a website such as this. You DID bring up a valid question about our journal and online presence, and I answered it. Had you searched the same keywords that you mentioned in the threads that you are currently flaming in, you would have been directed to the main Oracle Laboratory Institute and NeuroPsych Institute website through Google, before our domain and database crashed, and all of our membership accounts, forum posts, and articles were lost. We are currently in the process of rebuilding the main site, and reactivating the main domain name.
However, perhaps it is worth giving you a bit of a brief history of Oracle Laboratory Institute.. The VAST majority of pharmacological research that is conducted in the US (and most of the established world, for that matter) is done either by private pharmaceutical company labs, or by state university journals - in conjunction with pharmaceutical companies, for the development of new commercial pharmaceutical patents. Very few truly novel and noteworthy drugs get the funding for the research required to evaluate their specific pharmacology and pharmacokinetics, without some potential for a large commercial gain as a result of the development of said compound. It is just a sad fact of life that many very interesting psychopharmacological ideas never get off the ground by mainstream university or pharmaceutical company labs, due to lack of funding, unless there is some potential for a significant monetary commercial gain as a result of the work.
Many of my personal heroes are men like Dr. Alexander Shulgin, who, after being shunned by the more established pharmaceutical companies, decided to fund and explore his own avenues of research interest. I do not know if you are new to forums like this one, but if you search across all of the nootropic and psychopharmacological forums online, you will become aware of dozens and dozens of very talented biochemists and microbiologists, who without being officially affiliated with a university or government institution, have still made huge developments in many areas of biochemistry, microbiology, genetic research, etc., all independently in their home labs, and many of these people's accomplishments are now very well-referenced discoveries, even by the mainstream university, pharmaceutical developer, and government institution pharmacologists of today.
Several years ago, I approached many of these independent chemists and microbiologists that I have met along the way, and together we founded what has now become NeuroPsych Institute to facilitate the documentation and dissemination of psychopharmaceutical discoveries made in the private sector, and the network of researchers and private facilities that collaboratively follow our institute’s constitution and publish via our Journal of Applied and Investigational Pharmacology (via NeuroPsych Laboratory Press) is known as the Oracle Laboratory Institute network.
I in no way ever claimed to be a doctoral professor of a major US university, or the CEO of some Fortune 500 pharmaceutical company, but rather I accurately represented the nature of mine and my team’s work. And, anybody that has the proper background, who is so inclined, and has access to the necessary resources, can found their own organization, compose their own peer-review journal, and do the exact same thing that we are doing if they are so inclined and motivated enough. We are funded through the analytical work that we do on compounds and supplement quality analysis for various chemical suppliers, are privately and to some degree self-funded, and are also funded by the in-vivo and in-vitro pharmacological analyses that we do for other institutions, and the consultation work that I do for various patients on psychotropic medications, and in conjunction with several psychiatric centers and private practice psychiatrists. I do not know where you got the idea that you have to be some kind of god to do the kind of work that I do - when all that is required is the proper background knowledge, organizational skills, and access to the necessary resources. (That is not to say that I don’t have many friends who work in community college or university or medical labs, that I sometimes recruit to help us on some projects, such as in gaining access to the newer, high-resolution Nuclear-Magnetic-Resonance Imagers and Radioisotope Brain Imaging Systems on occasion, when our own equipment is not quite enough for a particular task).
I can name dozens of independent researchers from dozens of independent labs, who publish through their own local press journals, and who are not affiliated with large-scale universities, pharmaceutical companies, or government institutions, that likely do not have much of an online footprint, or publish in large-scale pharmacological journals that are associated with such universities, pharmaceutical companies, or government laboratories. Like I said, you DID bring up a valid point in looking for our work via online search engines, and I answered that question. I will NOT, however, continue to answer it over and over again. As I said, if you were to have searched Google for the same keywords three months ago, you would have been directly forwarded to the NeuroPsych Institute domain, and subsequently, the Oracle Laboratories Institute’s main website. After our domain went down, and our database was lost, the only version of our site that is still accessible is a free-hosted draft version, void of all of our membership accounts, forum posts, and our publication files, clinical surveys, and articles that were lost. Hopefully, within a month’s time, you will again be able to visit our main domain and read everything about our inception, history, and research work to your heart’s content. However, to simply claim that I am some fictional character, who just likes to post on forums an mislead people for the hell of it, is extremely ignorant, foolish, an illogical. What would I gain by doing that; really?
To make blatant, bogus claims such as that our journal does not exist is pretty damn confident in outright fabricated “facts” of which you really don’t know what you’re talking about. It is statements like that, that can end up making someone looking very foolish.
You stated “You obviously possess a certain amount of serious scientific knowledge.” - Well, I sure as hell didn’t obtain that knowledge by reading the back of a cereal box - I did so by conducting in in-vitro and in-vivo pharmacological work, first-hand, and in conjunction with my team.
As stated, our main website and publication database is a mess, but for something tangible that I happen to have handy on the hard drive of my laptop that we recently published, have at it:
http://oracle-labs.w...-submission.pdf
Phenigabine is one of the experimental cyclic phenyl ring GABA/Phenibut derivatives that I mentioned in my above post. (Note, that this is not the final publication on the pharmacological profile of Phenigabine, or it’s clinical review; it is simply a summary draft of it's general pharmacological effects that was submitted for publication via our journal).
As I said, hopefully, within a month’s time, when our main domain name is back online, and our main website’s database is restored, you can read all about our history and work, to your heart’s content. For the mean time, as I stated, I can only make a limited amount of posts per day, and I certainly am not going to keep re-posting the same statements again and again, when I decided to volunteer my time sat this site as a courtesy to some of the membership, in the first place. So, can we end the trolling now..?
#52
Posted 17 March 2016 - 03:07 AM
It would help credibility to name the members who asked you to join. You can PM if not wishing to post names publicly.
#53
Posted 17 March 2016 - 12:17 PM
It would help credibility to name the members who asked you to join. You can PM if not wishing to post names publicly.
Come on...! Now I can understand the skepticism but, for a moment just stop and read the indepth and detailed pharmacological information that Oracle Laboratories has written.
Regardless of his credentials (what would he/she benefit from lying anyway??) the neuroscience information is quite top notch and clarifies many things. (thanks Oracle Laboratories)
#54
Posted 17 March 2016 - 02:01 PM
I don’t really understand this. It’s quite rare to come across people with the vast amount of knowledge like John Gona in longecity. Instead of criticizing him we should be thankful to him for taking the time to write the detail explanations.
Trolling is one of the main reasons serious researchers stay away from public forums like this.
I don’t know about you guys, but I for one is following his advice.
#55
Posted 17 March 2016 - 02:11 PM
Regardless of his credentials (what would he/she benefit from lying anyway??)
Well, there are a few explainations, of wich I'll refrain from posting, for now ...
Let's say we're wrong : All "John Gona from Oracle Laboratories" has to do is answer to Maxwatt's request. No big deal , right ? I mean, he even offers "A more extensive background of my research experience, novel compound developments, publications, technological patent applications, and collaborative institutions can be provided upon request." This is from his bio on his profile page on the forum. All the moderator is asking for is to PM him wich "several" members of this forum have repeatedly invited him , as he said.
This will settle the matters once and for all and we'll all move on and benefit from his posts.
As far as I know, he still haven't answered to Maxwatt's request.
Edited by BlueCloud, 17 March 2016 - 02:15 PM.
#56
Posted 17 March 2016 - 02:39 PM
FWIW, my daughter is a neuroscience PhD candidate at a top tier university, already has a masters degrees in the subject and will have five more masters or equivalents in related fields when she finishes the program.. She has done extensive research with GABA receptors. If she can spare the time to look at Oracle Labs and John Gona's papers, I will post her impression and any remarks.
Another moderator, niner, is a pharmacologist. He can offer an evaluation as well.
Edited by maxwatt, 17 March 2016 - 02:49 PM.
#57
Posted 18 March 2016 - 12:22 AM
John / Oracle Laboratories, I had a look at your Phenigabine paper. Who synthesized the analogs? Did you guys also do the PK measurements, drawing blood at various timepoints and analyzing for phenigabine at different dose levels, salt forms, and fed/fasted status? That's a lot of work. If this is representative of stuff you guys can do, there are people in our community who might want to talk to you. We're particularly interested in people who have access to analytical instrumentation and know how to use it.
#58
Posted 18 March 2016 - 12:35 PM
It would help credibility to name the members who asked you to join. You can PM if not wishing to post names publicly.
Come on...! Now I can understand the skepticism but, for a moment just stop and read the indepth and detailed pharmacological information that Oracle Laboratories has written.
Regardless of his credentials (what would he/she benefit from lying anyway??) the neuroscience information is quite top notch and clarifies many things. (thanks Oracle Laboratories)
John/Oracle Labs has provided several names, he has been active elsewhere and there is some member overlap. Niner has looked at their paper and found it interesting, knowledgeable if perhaps nonconforming as to terminology in some areas. My impression, maybe the work of a brilliant autodidact? . It's certainly worth a good look.
(As it happens, GABA blockers and agonists are an interest of mine.)
#59
Posted 18 March 2016 - 01:04 PM
John/Oracle Labs has provided several names, he has been active elsewhere and there is some member overlap.
Did the longecity members confirm that they know him and invited him here ?
If he and his labs and his team and journals are all real, I'd really love to know how they managed to publish, "patent technological innovations", "collaborate with various other institutions" ( his terms) , consult for so many people and corporations, and still manage to remain completely hidden from all internet search engines, never appear on any patent database ( despite patenting so many things), never be linked to or be cited in any external website ( other than his ), no traces from the past left in the cache of any search engine, etc..
To anyone familiar with how search engines work, that is , hands down, a FAR more impressive technological achievement than any pharmaceutical compound he and his team could ever create. Only the best minds at the NSA, or some brilliant hackers, could probably achieve a similar thing.
Edited by BlueCloud, 18 March 2016 - 01:16 PM.
#60
Posted 21 March 2016 - 10:49 PM
While there is reason for concern with OL, I think we should be kinder in requesting that he validate some of his claims or admit that he's just a talented and/or opinionated self taught individual. If it's the case that you don't wish to divulge your identity for reason of the topics you're discussing we'd be happy to validate your identity and keep it private.
If you're self taught, they'll go pretty easy on you. I don't have any scientific credentials, nor am I as knowledgeable as you appear to be and while people frequently challenge me, I deal with it and have earned more positive reputation than negative and feel like I'm contributing and heard here for the most part. I'm a member of management after all...
Also tagged with one or more of these keywords: phenibut, baclofen, troll, fake character, manipulation ?
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