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Chemical Identity & Background
Pyrazolam is a pyrazolo-benzodiazepine, a synthetic psychoactive compound structurally related to traditional benzodiazepines but containing a pyrazolo ring fused to the core benzodiazepine scaffold.
Its full chemical name is 8-bromo-1-methyl-6-(2-chlorophenyl)-4H-[1,2,4]-triazolo[4,3-a][1,4]-benzodiazepine.
This structure makes it closely related to alprazolam and triazolam, but it was developed primarily for research purposes and was never licensed for medical use in any country.
In its raw form, Pyrazolam typically appears as a white to off-white crystalline powder. It has been distributed in “research chemical” markets, sometimes pressed into tablets or dissolved in liquid for measurement purposes.
Pharmacology and Mechanism of Action
Pyrazolam acts as a positive allosteric modulator of GABA_A receptors, enhancing the action of the inhibitory neurotransmitter GABA. This produces the classic benzodiazepine-type effects:
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Anxiolytic (anti-anxiety)
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Sedative/hypnotic
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Anticonvulsant
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Muscle relaxant
However, pharmacological studies and anecdotal toxicology data show that Pyrazolam is distinct in that it lacks significant hypnotic or muscle-relaxant action at typical active doses. Instead, it produces primarily anxiolytic and calming effects without strong sedation.
This difference has made it a subject of pharmacological interest, since it may interact with certain GABA_A receptor subtypes differently than other benzodiazepines.
Potency and Pharmacokinetics
Pyrazolam is considered a moderate-potency benzodiazepine analogue, with activity comparable to or slightly higher than alprazolam on a milligram-to-milligram basis.
Pharmacokinetic data indicate:
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Rapid onset: within 30–60 minutes of exposure.
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Elimination half-life: roughly 17–22 hours, allowing for once-daily pharmacological activity.
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No active metabolites, meaning the compound itself is responsible for its duration of effect, unlike diazepam or diclazepam, which have long-lasting breakdown products.
Because of the absence of active metabolites, pyrazolam’s sedative effects tend to be shorter-lived and more predictable, though this also increases withdrawal potential with frequent exposure.



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