The Big & Dandy 3-MeO-PCP Thread (Part 1)

[THCified]

^ Interesting! Could you pls elaborate on your experience? How were 30mgs? What happened?

I've had my very first 10mgs (oral) at once dose this week, and i didn't like it. I think it's better to start as low as possible and add more if needed.

After taking 10mgs i seriously thought that i enjoy the afterglow even more than the actual high

 

[dextroflicks]

this stuff is like the viagra of dissociatives, well worth its price imo, lasts long is spectacularly clean and has one of the best dissociative euphoric rushes of dissociatives ingeneral. But it's ability to make sex better still amazes me, 500 mg 3-meo-pcp for me and gf was a fucking amazing week, All of it was administered IM
ps: dont smoke weed with dosages of 15mg & up, anxiety, paranoia, muscle spasms (but only if mixed with weed)

 

[amanitadine]

For such a ki value at the NMDAR 3-MeO PCP remains amazingly lucid. 45 mg IM of the HBr (it is quality, ive compared to the earliest high quality HCl and 84% of the "strength" seems proper. I can "feel" 6 mg ) recently and i was no where near a "hole" state, but a wonderful transcedence when eyes closed and headphones on, with emotional insight. Eyes open, could speak coherently, with a bit of effort, (searching for the words, etc) and move around ok. Strange one it is. I also have a huge permanent tolerance with arylcyclohexylamines, although ive abstained for a long time until recently. It's a weird one. Much less "druggy" than MXE or 3-MeO PCE. It does have a compulsion to it though, and used consecutive days a "dark side" can emerge.

 

[foolsgold]

is the ban on these same day as noids been told so tuesday no more legal pcp/ket ones in the uk

 

[Transform]

That's correct foolsgold. 3-MeO-PCP and all other arylcyclohexamines (dissociatives) except DXM become class B on Tuesday in the UK.

Cannabinoids and O-desmethyltramadol are also included in the ban.

 

[dextroflicks]

they always schedule the good ones

 

[amanitadine]

Hmmm i wonder why that could possibly be

 

[dextroflicks]

its history in the making, most drugs were once RC's

 

[pharmakos]

its history in the making, most drugs were once RC's

i'm pretty sure at one point in time if you wanted to buy some LSD-25 you just filled out a mail order form and mailed it to Sandoz or some other company, lol

 

[dextroflicks]

i'm pretty sure at one point in time if you wanted to buy some LSD-25 you just filled out a mail order form and mailed it to Sandoz or some other company, lol

4 years ago i was buying ketamine in the veterinary pharmacy with no script back at home in eastern europe

 

[foolsgold]

That's correct foolsgold. 3-MeO-PCP and all other arylcyclohexamines (dissociatives) except DXM become class B on Tuesday in the UK.

Cannabinoids and O-desmethyltramadol are also included in the ban.

damn it man thats gutting pay debts or stock up grrrrr

 

[DroneLore]

What's the deal with IMing this? Is it as common an ROA as with ketamine and mxe? If I am used to IMing 30 - 50 mg of MXE, and barely get threshold effects from sniffing 50 mg of MXE, what's a good ball park to begin researching 3meopcp?

 

[knock]

IMing is popular. I think I did it once. It was so effective, I can't remember much of it, except for coming to in a daze! I normally just snort it, but it makes me sneeze after a few snorts, which is a waste. Best to snort your whole dose in one go. Plugging I find less effective, I plugged 40mg last night and I felt it but if I'd snorted it, it would have been much better.

 

[Halif]

wow, knock! Isn't 40mg plugged a rather large dose for 3-MeO-PCP?!

I haven't used this one for about a year or so now, but if I recall correctly I was weighing out doses under 20mg and getting quite strong effects from it. Perhaps it was so strong because I also had MXE in my system....

 

[Transform]

10mg was plenty for me, and that was sublingual!

 

[Solipsis]

I understand from my housemate's experiences that snorting may change the effects and increase chances of mania or similar side-effects, at least it seems that way. He takes it subglingually now and is very happy with that. According to him, IM would not be so interesting, because it is already excellent sublingually. I'd like to hear from others what benefits there are except for effectivity / economic reasons.

Actually tomorrow I am trying 3-MeO-PCP and I am very curious and excited.

Not sure yet what dose I will try, I'll let my housemate give me some advice. He will be joining me.

 

[Confield]

I'm also settled with sublingual ROA for now, it seems quite effective and it's easy. Only downside for me is that swallowing chemicals or traces of them frequently causes acid reflux type of symptoms, heartburn and so on. For that reason I tried IM couple of times. It was very pleasant too, but I was sort of disappointed that ~15 mg IM seemed only as effective as 15 mg sublingual would have. Maybe a bit stronger? If I had proper filters and sterile equipment I would still switch to IM to prevent gastrointestinal problems or damage to mucous membranes and teeth. I only had a cotton ball filter to work with, and I had to heat up the dose in a spoon for the powder to dissolve, so that was kind of dirty. I guess I got away with that, no signs of infection or other nasty stuff.

I've sometimes done it nasally too but I wouldn't personally recommend it. It does the job but it's a bit painful and there will be lingering discomfort in the nasal cavity and throat, at least for me.

I've been thinking about the "anti-depressant afterglow" which I get from 3-MeO-PCP and other dissociatives and what's the deal with this phenomenon. Is it actually a (hypo)manic episode of some sort which is triggered by the drug? I'm thoroughly enjoying it though, I'm productive and life feels good. If I keep taking the drug, overdoing it, shit gets too manic/delusional and eventually the drug loses it's positive effects and there will be a phase of rebound depression.

Is this effect related to the NMDA antagonism or what? I don't really understand much about neurochemistry and stuff like that, so feel free to enlighten me about this subject because this is very interesting to me.

 

[DroneLore]

I recently tried 3-MeO-PCP for the first time. It was after a bit of an MXE bender. I gave a friend the MXE to hold on to, so I could not do it for 24 hours. The following day, we finished off the MXE together. I got really, really messed up on MXE, in a way it's never affected me before. Sorry, I guess that's a story for another time...

Anyway, I just wanted to give some background. I started off IMing the 3meo at very low doses, like 2 mg. The largest shot was probably 4 or 5 mg, and I think I consumed between 10 and 20 over the course of a few hours. I definitely have some tolerance as I had been consistently IMing MXE at doses between 20 and 50 mg for several days.

I think tomorrow I am going to try a single 10 mg IM shot of 3-MeO-PCP. I hope to achieve something similar to the effects I got earlier tonight: feeling kind of sober but definitely knowing I'm not sober, still being able to talk, not feeling stupid (MXE does those two to me, hard). It was very recreational, and subtle but in the best way. I would rather not get all monged out--are chances good that, given my tolerance, a 10 mg IM shot will give me what I am looking for?

 

[Sun Drugs]

What kind of stuff do you all like to do on this? I know that on MXE I like to lie back, listen to ambient music, and watch nature documentaries. Based on reading this thread though, it seems like 3-MeO-PCP won't nearly "couchlock" you as much as other dissociatives though...and that there is not nearly as much confusion and difficulty with moving your body. Would it be possible for someone to do something like play musical instruments on a 10mg for someone with moderate dissociative tolerance? I know that the dosages vary greatly, but I'd like to know other people's experiences on this.

 

[wayab]

^it's very good for that