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Misc Selegeline and PEA

D

DTREE

Greenlighter
Joined
Jul 15, 2012
Messages
8
Hi guys,

Today I tested a combo of selegeline and PEA, I know this can be a dangerous combination and its highly addictive for sure!
But that's no problem for me ;) I can handle that.
Are there any meds or supps I could take to minimize side effects like high bloodpressure?



A short "report".
T: 00:00 2mg selegeline sublingual and a cup of green tea.
T: 00:15 1gr of PEA
T: 00:30 start running
T: 00:40 noticing a small buzz and feeling of euphoria
T: 00:50 I completed 5km's of running at a speed of 11,5km/h this is the moment where I usually stop and get pain everywhere :p
T: 00:55 OH MY GOD, the combo kicks in, I feel like I can run forever... i'm running on the beat of a hardcore track, I'm one with the music and I kan keep going.
T: 00:60: 500mg PEA
T: 00:90: completed a 10,5km run with an average speed of 11,5km/h! a personal record, if you know a month ago I couldnt even run1km :)
T: 0100: 250mg PEA, feeling great
T:120 the effect starts wearing off, take another 250mg of PEA
T: 160 slow come down
T: 200 still feeling quiet good, but be aware that this stuff is highly addictive!

I know it was probably extremely stupid to complete a run on this stuff, but this was just a test..
 
Btw this stuff suppresses hunger like a mad man

Does anyone know if you will test positive on amphetamines with this combination?


A study:

J Neuropsychiatry Clin Neurosci. 1996 Spring;2):168-71.
Sustained antidepressant effect of PEA replacement.Sabelli H, Fink P, Fawcett J, Tom C.
Rush University and the Center for Creative Development, Chicago, Illinois, USA.

Phenylethylamine (PEA), an endogenous neuroamine, increases attention and activity in animals and has been shown to relieve depression in 60% of depressed patients. It has been proposed that PEA deficit may be the cause of a common form of depressive illness. Fourteen patients with major depressive episodes that responded to PEA treatment (10-60 mg orally per day, with 10 mg/day selegiline to prevent rapid PEA destruction) were reexamined 20 to 50 weeks later. The antidepressant response had been maintained in 12 patients. Effective dosage did not change with time. There were no apparent side effects. PEA produces sustained relief of depression in a significant number of patients, including some unresponsive to the standard treatments. PEA improves mood as rapidly as amphetamine but does not produce tolerance.
 
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