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Methoxisopropamine or MXiPr( also known as 3- MeO- 2 ′- Oxo- PCiPr, Isopropyloxetamine, Isopropyxetamine) is a new dissociative substance of the arylcycloheximine class. It’s the structural analogue of MXE. The medium of action is unknown, but it’s presumably an NMDA receptor antagonist producing dissociative and euphoric goods.

You can buy MXiPr online at a price:

QUANTITY Disc (%) Price per gram
1 g
2 g 28 % 25
5 g 40 % 21
10 g 54 % 16
25 g 72 % 9.50
50 g 80 % 7
100 g 82 % 6.20
250 g 86 % 4.90
500 g 88 % 4.20
1000 g 89 % 3.80


Methoxisopropamine or MXiPr( also known as 3- MeO- 2 ′- Oxo- PCiPr, Isopropyloxetamine, Isopropyxetamine) is a new dissociative substance of the arylcycloheximine class. It’s the structural analogue of MXE. The medium of action is unknown, but it’s presumably an NMDA receptor antagonist producing dissociative and euphoric goods.
The circumstances girding the origin of MXiPr are unknown. It first appeared on the online business for exploration chemicals in late 2020 and was specifically retailed as a legal relief for MXE or ketamine. The first batch allegedly smelled like plastic and was suspected of containing contaminations. The alternate batch had a fully different” pokemon card” smell.
Its private goods are similar to ketamine and MXE and include sedation, loss of movement control, pain relief, internal visions, abstract thinking, swoon and dissociation. Its private goods are described as substantially analogous to O- PCE or MXE, but more changeable and ecstatic, making it indeed more distant from the ketamine goods. It’s supposed to be a strong serotonin reuptake asset like MXE.
veritably little data exists on the pharmacological parcels, metabolism and toxin of MXiPr.
It’s recommended that detriment reduction practices be rigorously stuck to when using this substance.
History and Culture
MXiPr first appeared for trade on the online business for exploration chemicals in late 2020.
MXiPr, or( IUPAC) 2-( 3- methoxyphenyl)- 2-(( propane-2-yl) amino) cyclohexane-1-one, is classified as an arylcyclohexylamine( 3) medicine. It has an isopropyl group in the nitrogen bonding fragment, as well as a double oxygen bond at the 2′ of the cyclohexyl ring and a methoxy group at position 3 of the phenyl ring, which it shares with MXE.
This section of pharmacology is deficient.
veritably little is known about the pharmacology of this substance, but as an arylcyclohexamine we can assume that it’s an NMDA receptor antagonist. NMDA receptors allow electrical signals to pass between neurons in the brain and spinal cord; the receptor must be open for the signal to pass through. Dissociative medicines close NMDA receptors by blocking them. This disabling of neurons results in a loss of perceptivity, bloodied movement, and eventually an nearly identical to the well- known” k- hole.”
Given the structural similarity with MXE and according to user reviews, this substance can be a strong means for re-uptake of serotonin (SRI). The combination of MXiPr with other drugs acting on serotonin should be avoided.
Early user reviews suggest that MXiPr demonstrates two states, the first occurs at a dosage of about 5-20 mg and produces a two-hour nitrous oxide-like experience, the alternative mesa occurs at 20-40 mg and produces a failure-like experience, but is usually considered chaotic, with noticeably warmer or “comforting”, which can also reach to the real ecstasy. Some experimenters advise caution when experimenting with an increased dose. There are reports of body tension for 2 days after taking a low dose and seizures at very high.
MXiPr has similar premises to MXE and O-PCE, but there are some viewer justifications that suggest it may have a potentially increased threat of causing seizures and amnesia. perhaps these side effects can be avoided by reducing the harm, keeping the pills low, using rarely and avoiding combinations.
The products listed below cite the Private Goods Index (SEI), an open literature study based on user reports.
Physical effects
– Stimulation and dissociative action
– At low and moderate doses, MXiPr significantly stimulates, and at higher levels, sensations become dissociative.
– the sensations of the “high body” MXiPr robotic body can be described as a sharp, pleasant tinkling sensation localized in the arms, legs and head.
– The perception of the lightness of the body creates the feeling that the body is floating and has become completely light. This effect is really characteristic of MXiPr and strangely stimulating. It encourages physical exercise in small or moderate doses, making the body light and relaxed in movements.
– Loss of movement control – Loss of control over large and small movements, as well as balance, is common when taking MXiPr and becomes especially serious at high dosages. This means that before starting (if you have no experience), you need to sit down so as not to fall and hurt yourself.
– Spatial disorientation
– Suppression of tactile sensations this is incomplete or completely suppresses the sense of touch, creating a feeling of dispassion in the extremities. It is responsible for the anesthetic properties of this substance.
– Pain relief
– Dizziness – Although this is unusual, some people report dizziness under the influence of MXiPr, especially when it is used in combination with other substances.
– Nausea
– A high dose of MXiPr can sometimes lead to nausea and vomiting. For most people, this unexpectedly turns out not to be as undesirable as they initially expected, due to the concomitant lack of physical sensations.
-Visual distortion
– Abnormal flickering
– High blood pressure (link required) this effect is usually observed with regular dosages.
Other effects:
Improved music perception
Temporary disorientation
Increased libido – it is reported that this is observed when taking lower doses.
Visual effects
Increase visual susceptibility or suppress visual susceptibility – While smaller doses of this substance usually cause a moderate increase in visual susceptibility, this effect quickly disappears because a person’s general visual abilities are suppressed with an increase in the dose of the drug. Frame rate suppression, double vision, image recognition suppression, waking dream (setting, decor and geography, perspective visions, scenarios and plots) Machine geography Inner waking dream (independent objects; setting, geography and geographical references; promising visions, scenarios and plots), cognitive effect, anxiety suppression, disinhibition, cognitive fainting. It is reported that fainting from this substance is stronger than from other dissociatives like O-PCE, but weaker than from MXE. Increased creativity of abstract thinking, mania of deja vu – some addicts reported mania associated with this substance. The frequency of which is not defined. It is strongly recommended to use harm reduction methods and not to consume this substance in large quantities or constantly. Most likely, it is more common than other arylcyclohexylamines, but less common compared to PCP and 3-MeO-PCP. Delusional effect-most likely, this effect is more common in MXiPr than in most other arylcyclohexylamines, but is less common compared to substances like 3-MeO-PCP, with dream reinforcement and memory suppression
MXiPr is a hallucinogen that causes the following side effects
– sound deformations, such noises, high tones and notes, tone changes, echoes.
– the sound suppression effect becomes less distinguishable and more distant.
MXiPr also results in the following effects
– Disabling tactile sensations
– Disabling visual sensations leads to the appearance of a “k-shaped hole”.
– Disabling memory
Oddly enough, MXiPr has been reported to cause seizures when taking really high doses.
It is strongly recommended to use harm reduction methods when using this substance.
MXiPr can never be taken with other NMDA receptor antagonists, the usual use of MXiPr can be considered relatively addictive with a high probability of abuse and can cause poisoning in certain consumers.
Tolerance to MXiPr develops with prolonged and repeated use. This leads to the fact that drugs have to be administered more and more new doses to achieve the same effect.
After that, it takes about 3-7 days for the exposure to halve, and 1-2 weeks to return to the starting position (in the absence of further use).
Toxicological and pharmacological substances are not yet fully known.
With regard to its long-term health effects with repeated use and over an excessively long period of time, it is assumed that MXiPr causes problems with the bladder and urinary tract, similar to those observed with ketamine, but to a lesser extent. This is due to the fact that MXiPr is much more effective than ketamine, so it is necessary to consume significantly less of this substance. Symptoms of ketamine-induced cystitis can be severe and can be described as
the frequency of urination is the need to clean the bladder every few moments.
The desire to urinate can be described as an unforeseen, alluring need to urinate.
Legal status
Germany MXiPr is controlled in accordance with the NpSG (New Psychoactive Substances Act).
Hungary and trade were banned in April 2021.
Technical Information:

Product Name: Methoxisopropamine, MXiPr, 3- MeO- 2 ′- Oxo- PCiPr

Other Name(s):  Isopropyloxetamine, Isopropyxetamine

IUPAC Name: 2-(3-methoxyphenyl)-2-(propan-2-ylamino)cyclohexan-1-one


Molar Mass: 261.36 g/mol

Molecular Formula: C16H23NO2

InChi Code: InChI=1S/C16H23NO2/c1-12(2)17-16(10-5-4-9-15(16)18)13-7-6-8-14(11-13)19-3/h6-8,11-12,17H,4-5,9-10H2,1-3H3



Formulation: A crystalline solid



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1 review for MXiPr

  1. Rated 4 out of 5

    Renard Erker

    Is there an mxipr in stock? I ordered 2 grams from you an hour ago, but I have not received a response. How to pay and receive the package? What is the problem?

    • admin

      Available in stock. We have sent you all the necessary information again to your e-mail specified in the order. Please check again.

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