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<p data-start="347" data-end="592">2-Fluoro-Deschloroketamine (commonly abbreviated <a href="https://en.wikipedia.org/wiki/2-Fluorodeschloroketamine"><strong data-start="396" data-end="406">2F-DCK</strong></a>) is a dissociative anesthetic belonging to the <em data-start="454" data-end="475">arylcyclohexylamine</em> class — a chemical family that includes ketamine, PCP (phencyclidine), MXE (methoxetamine), and related analogues.</p>
<p data-start="594" data-end="897">Its molecular formula is <strong data-start="619" data-end="632">C13H16FNO</strong>, and it is structurally similar to <em data-start="668" data-end="693">deschloroketamine (DCK)</em>, differing by the substitution of a fluorine atom at the 2-position on the aromatic ring. This minor change significantly alters receptor affinity and potency, making 2F-DCK pharmacologically distinct.</p>
<p data-start="899" data-end="1149">In its pure form, 2F-DCK typically appears as <strong data-start="945" data-end="1003">white crystalline powder or small translucent crystals</strong>. It is also found in solution or pressed tablet form in unregulated online markets. It is <em data-start="1094" data-end="1099">not</em> approved as a medication anywhere in the world.</p>
<hr data-start="1151" data-end="1154" />
<h3 data-start="1156" data-end="1203"><strong data-start="1160" data-end="1203">Pharmacology and Mechanism of Action</strong></h3>
<p data-start="1205" data-end="1524">Like other arylcyclohexylamines, 2F-DCK acts primarily as a <strong data-start="1265" data-end="1339">non-competitive antagonist of the NMDA (N-methyl-D-aspartate) receptor</strong>, a subtype of glutamate receptor. NMDA antagonism interferes with excitatory neurotransmission, producing dissociation — a feeling of detachment from body, perception, and environment.</p>
<p data-start="1526" data-end="1569">Additional pharmacological effects include:</p>
<ul data-start="1570" data-end="1817">
<li data-start="1570" data-end="1654">
<p data-start="1572" data-end="1654"><strong data-start="1572" data-end="1621">Dopamine and serotonin transporter inhibition</strong> (mild, compared with stimulants)</p>
</li>
<li data-start="1655" data-end="1727">
<p data-start="1657" data-end="1727"><strong data-start="1657" data-end="1686">Sigma-1 receptor activity</strong>, possibly influencing mood and cognition</p>
</li>
<li data-start="1728" data-end="1817">
<p data-start="1730" data-end="1817"><strong data-start="1730" data-end="1770">Voltage-gated ion channel modulation</strong>, which can affect muscle tone and coordination</p>
</li>
</ul>
<p data-start="1819" data-end="1989">These interactions produce the characteristic <em data-start="1865" data-end="1911">dissociative, anesthetic, and hallucinogenic</em> profile similar to that of ketamine but with distinct kinetics and potency.</p>
<hr data-start="1991" data-end="1994" />
<h4 data-start="1996" data-end="2041"><strong data-start="2000" data-end="2041">Onset and Duration (Reported Data)</strong></h4>
<p data-start="2043" data-end="2167">While no clinical pharmacokinetic studies exist, user and toxicology reports describe the following approximate durations:</p>
<div class="_tableContainer_1rjym_1">
<div class="group _tableWrapper_1rjym_13 flex w-fit flex-col-reverse" tabindex="-1">
<table class="w-fit min-w-(--thread-content-width)" data-start="2169" data-end="2407">
<thead data-start="2169" data-end="2210">
<tr data-start="2169" data-end="2210">
<th data-start="2169" data-end="2177" data-col-size="sm">Route</th>
<th data-start="2177" data-end="2185" data-col-size="sm">Onset</th>
<th data-start="2185" data-end="2192" data-col-size="sm">Peak</th>
<th data-start="2192" data-end="2210" data-col-size="sm">Total Duration</th>
</tr>
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<tbody data-start="2253" data-end="2407">
<tr data-start="2253" data-end="2302">
<td data-start="2253" data-end="2266" data-col-size="sm">Intranasal</td>
<td data-start="2266" data-end="2277" data-col-size="sm">5–15 min</td>
<td data-start="2277" data-end="2289" data-col-size="sm">30–90 min</td>
<td data-start="2289" data-end="2302" data-col-size="sm">2–3 hours</td>
</tr>
<tr data-start="2303" data-end="2348">
<td data-start="2303" data-end="2310" data-col-size="sm">Oral</td>
<td data-start="2310" data-end="2322" data-col-size="sm">20–40 min</td>
<td data-start="2322" data-end="2335" data-col-size="sm">60–120 min</td>
<td data-start="2335" data-end="2348" data-col-size="sm">3–5 hours</td>
</tr>
<tr data-start="2349" data-end="2407">
<td data-start="2349" data-end="2370" data-col-size="sm">Intramuscular (IM)</td>
<td data-start="2370" data-end="2380" data-col-size="sm">2–5 min</td>
<td data-start="2380" data-end="2392" data-col-size="sm">30–60 min</td>
<td data-start="2392" data-end="2407" data-col-size="sm">1.5–3 hours</td>
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<p data-start="2409" data-end="2653">The duration tends to be <strong data-start="2434" data-end="2457">shorter and cleaner</strong> than that of MXE or PCP analogues, but longer than that of ketamine. Reports indicate that 2F-DCK may feel more <em data-start="2570" data-end="2609">clear-headed yet emotionally detached</em> compared to ketamine’s dreamlike effects.</p>
<hr data-start="2655" data-end="2658" />
<h5 data-start="2660" data-end="2718"><strong data-start="2664" data-end="2718">Subjective and Physiological Effects </strong></h5>
<p data-start="2720" data-end="2773"><strong data-start="2720" data-end="2755">Subjective dissociative effects</strong> (dose-dependent):</p>
<ul data-start="2774" data-end="3004">
<li data-start="2774" data-end="2835">
<p data-start="2776" data-end="2835">Depersonalization and derealization (“out-of-body” feeling)</p>
</li>
<li data-start="2836" data-end="2869">
<p data-start="2838" data-end="2869">Visual and auditory distortions</p>
</li>
<li data-start="2870" data-end="2898">
<p data-start="2872" data-end="2898">Analgesia and body numbing</p>
</li>
<li data-start="2899" data-end="2931">
<p data-start="2901" data-end="2931">Euphoria or emotional blunting</p>
</li>
<li data-start="2932" data-end="2960">
<p data-start="2934" data-end="2960">Time perception distortion</p>
</li>
<li data-start="2961" data-end="3004">
<p data-start="2963" data-end="3004">Cognitive disorganization and memory gaps</p>
</li>
</ul>
<p data-start="3006" data-end="3027"><strong data-start="3006" data-end="3026">Physical effects</strong>:</p>
<ul data-start="3028" data-end="3272">
<li data-start="3028" data-end="3064">
<p data-start="3030" data-end="3064">Slowed movement and slurred speech</p>
</li>
<li data-start="3065" data-end="3087">
<p data-start="3067" data-end="3087">Loss of coordination</p>
</li>
<li data-start="3088" data-end="3120">
<p data-start="3090" data-end="3120">Nystagmus (rapid eye movement)</p>
</li>
<li data-start="3121" data-end="3153">
<p data-start="3123" data-end="3153">Nausea, dizziness, or vomiting</p>
</li>
<li data-start="3154" data-end="3213">
<p data-start="3156" data-end="3213">Increased heart rate and blood pressure (sympathomimetic)</p>
</li>
<li data-start="3214" data-end="3272">
<p data-start="3216" data-end="3272">At higher doses: catalepsy or temporary unresponsiveness</p>
</li>
</ul>
<p data-start="3274" data-end="3384"><strong data-start="3274" data-end="3291">After-effects</strong> can include fatigue, confusion, anxiety, or depressive symptoms as NMDA activity rebounds.</p>
<p data-start="3386" data-end="3540">These effects make 2F-DCK pharmacologically interesting but medically concerning due to unpredictable potency and the absence of standardized dosage data.</p>
<p data-start="4332" data-end="4421">
<hr data-start="4423" data-end="4426" />
<h5 data-start="4428" data-end="4472"><strong data-start="4432" data-end="4472">Forensic and Analytical Detection</strong></h5>
<p data-start="4474" data-end="4502">2F-DCK has been detected in:</p>
<ul data-start="4503" data-end="4610">
<li data-start="4503" data-end="4534">
<p data-start="4505" data-end="4534">Seized powders and crystals</p>
</li>
<li data-start="4535" data-end="4568">
<p data-start="4537" data-end="4568">Postmortem toxicology samples</p>
</li>
<li data-start="4569" data-end="4610">
<p data-start="4571" data-end="4610">Biological fluids of impaired drivers</p>
</li>
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<p data-start="4612" data-end="4916">Detection typically requires <strong data-start="4641" data-end="4662">LC-MS/MS or GC-MS</strong> with reference standards. Immunoassays for ketamine or PCP often fail to identify 2F-DCK due to its structural uniqueness. Analytical laboratories rely on <strong data-start="4818" data-end="4840">spectral libraries</strong> and retention-time databases (e.g., SWGDRUG, Cayman Chem reference data).</p>
<p data-start="4918" data-end="5111">Recent analytical studies by European and Asian forensic institutes have documented 2F-DCK’s mass fragmentation pattern and stability profile, supporting its identification in seized materials.</p>
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<h3 data-start="950" data-end="1001">Pharmacology &amp; subjective effects (high level)</h3>
<p data-start="1002" data-end="1890"><a href="https://en.wikipedia.org/wiki/4-MeO-PCP?utm_source=chatgpt.com">4-MeO-PCP</a> is a <strong data-start="1017" data-end="1044">dissociative anesthetic</strong> whose primary pharmacology is antagonism at the <strong data-start="1093" data-end="1110">NMDA receptor</strong> — the same receptor family targeted by PCP and ketamine — but affinity and activity differ by analogue. Compared with PCP, available binding data and pharmacological summaries indicate 4-MeO-PCP generally has <strong data-start="1320" data-end="1377">lower NMDA affinity than PCP but higher than ketamine</strong> in some assays; it also shows measurable affinity for σ (sigma) receptors and monoamine transporters, which may shape its subjective profile. In humans it produces <strong data-start="1542" data-end="1674">dissociation, derealization, perceptual distortion, analgesia, and at higher doses agitation, delirium, or psychosis-like states</strong>. Reported active doses span a wide range, reflecting variability in samples and tolerance; some reports indicate oral doses in the tens of milligrams range for moderate effects.</p>
<p>Technical Information<br />
Formal Name: 1-[1-(4-methoxyphenyl)cyclohexyl]-piperidine, monohydrochloride<br />
CAS Number: 2185-93-5<br />
Purity: ?98%<br />
Formulation: A crystalline solid<br />
?max: 231, 272 nm<br />
SMILES: COC(C=C1)=CC=C1C2(N3CCCCC3)CCCCC2.Cl<br />
InChi CodeInChI=1S/C18H27NO.ClH/c1-20-17-10-8-16(9-11-17)18(12-4-2-5-13-18)19-14-6-3-7-15-19;/h8-11H,2-7,12-15H2,1H3;1H<br />
InChi Key: FYAFJNVLHWQLHK-UHFFFAOYSA-N<br />
Side effects<br />
4-MeO-PCP has caused a fatality in combination with 4-HO-MET, venlafaxine, olanzapine, lorazepam and hydroxyzine.</p>
<p>Chemical and physical<br />
Formula: C18H27NO</p>
<h4 data-start="1892" data-end="1929">Why the <strong data-start="1903" data-end="1914">crystal</strong> form matters</h4>
<p data-start="1930" data-end="2645">Crystal form (solid hydrochloride salt vs. freebase or solution) affects <em data-start="2003" data-end="2069">handling, purity assessment, dosing, and route of administration</em>. The crystalline hydrochloride is often the form submitted to forensic labs and sold by chemical suppliers because it is more stable and easier to characterize analytically. Crystals may be visually indistinguishable from other white powders/crystals, so <strong data-start="2325" data-end="2364">visual identification is unreliable</strong> and laboratory testing is required. Crystalline material also enables accurate weighing in controlled settings — but in illicit contexts, purity and cutting with other substances are common, which makes powdered/crystalline samples hazardous.</p>
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		<pubDate>Wed, 15 Mar 2023 10:57:35 +0000</pubDate>
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<p>Buy 5F-PCN Powder (also known as 5F-MN-21) is an azaindole-based synthetic cannabinoid that is presumed to be a potent agonist of the CB1 receptor and has been sold online as a designer drug. It is closely related to NNE1. Given the known metabolic liberation (and presence as an impurity) of amantadine in the related compound APINACA, it is suspected that metabolic hydrolysis of the amide group of 5F-PCN may release 1-naphthylamine, a known carcinogen.</p>
<p>5F-MN-21 is also a designer drug with pronounced physiological and psychoactive effects.D The toxicological and physiological properties of 5F-PCN are not known. Synthetic cannabinoids like 5F-PCN might display high affinity for peripheral CB1 and CB2 cannabinoid receptors.</p>
<p>The toxicological and physiological properties of 5F-PCN are not known. Synthetic cannabinoids like 5F-PCN might display high affinity for peripheral CB1 and CB2 cannabinoid receptors.</p>
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<h3 data-start="809" data-end="857">What does “powder” form mean &amp; why it matters | Order Research chemical Canada</h3>
<ul data-start="859" data-end="1405">
<li data-start="859" data-end="993">
<p data-start="861" data-end="993">The “powder” or crystalline form refers to the unformulated active compound in solid form (often as a crystalline or fine powder).</p>
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<p data-start="996" data-end="1108">In research or analytical laboratories, this form allows measurement, purity checks, structural analysis, etc.</p>
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<p data-start="1111" data-end="1178">In illicit or unregulated contexts, powder form is risky because:</p>
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<p data-start="1184" data-end="1276">Dosage is difficult to control. Even small errors can lead to unexpectedly strong effects.</p>
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<p data-start="1282" data-end="1325">Impurities or adulterants may be present.</p>
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<p data-start="1331" data-end="1405">There may be mislabeling or confusion with other synthetic cannabinoids.</p>
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<p>Please store this synthetic cannabinoid in a cool and dry place. Stability of the cannabinoid compound 5F-PCN up to 2 years under correct storage conditions.</p>
<p>Legal status<br />
Swedens public health agency suggested to classify 5F-PCN as hazardous substance on November 10, 2014.</p>
<p>Chemical and physical data<br />
Formula: C23H22FN3O</p>
<p>Molar mass: 375.4 g/mol g·mol?1</p>
<h4 data-start="1412" data-end="1464">Pharmacology &amp; Effects (what is known / expected)</h4>
<ul data-start="1466" data-end="2016">
<li data-start="1466" data-end="1807">
<p data-start="1468" data-end="1807">As a synthetic cannabinoid agonist at <strong data-start="1506" data-end="1513">CB₁</strong>, 5F-PCN is presumed to produce <strong data-start="1545" data-end="1573">cannabinoid-like effects</strong>: altered perception, psychoactive “high,” possible relaxation or euphoria. Because it’s “full agonist” (or presumed potent), the effects may be stronger and more unpredictable than natural THC. <span class="" data-state="closed"><span class="ms-1 inline-flex max-w-full items-center relative top-[-0.094rem] animate-[show_150ms_ease-in]" data-testid="webpage-citation-pill"><a class="flex h-4.5 overflow-hidden rounded-xl px-2 text-[9px] font-medium transition-colors duration-150 ease-in-out text-token-text-secondary! bg-[#F4F4F4]! dark:bg-[#303030]!" href="https://www.unodc.org/LSS/Substance/Details/247a999d-694b-4597-92c8-6aef8f27954d?utm_source=chatgpt.com" target="_blank" rel="noopener"><span class="relative start-0 bottom-0 flex h-full w-full items-center"><span class="flex h-4 w-full items-center justify-between"><span class="max-w-[15ch] grow truncate overflow-hidden text-center">UNODC</span><span class="-me-1 flex h-full items-center rounded-full px-1 text-[#8F8F8F]">+1</span></span></span></a></span></span></p>
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<p data-start="1810" data-end="2016">There is very limited data on <em data-start="1840" data-end="1847">human</em> pharmacokinetics (onset, duration, metabolism), side effect profile, or dose ranges. Most knowledge is from structural analogues and early-warning / forensic reports.</p>
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<p data-start="508" data-end="870"><a href="https://en.wikipedia.org/wiki/Ketamine">Ketamine</a> is a <strong data-start="522" data-end="549">dissociative anesthetic</strong> belonging to the <strong data-start="567" data-end="596">arylcyclohexylamine class</strong>, developed in the 1960s by Parke-Davis as a safer alternative to PCP (phencyclidine). It functions primarily as a <strong data-start="711" data-end="755">non-competitive NMDA receptor antagonist</strong>, meaning it blocks the action of glutamate — a neurotransmitter responsible for excitatory signals in the brain.</p>
<p data-start="872" data-end="1112">In medicine, it’s sold as <strong data-start="898" data-end="909">Ketalar</strong> and related formulations. It exists as a <strong data-start="951" data-end="988">racemic mixture (R/S enantiomers)</strong> or, in some countries, as <strong data-start="1015" data-end="1029">esketamine</strong> (the S-enantiomer) — which has higher potency and is used in depression therapy.</p>
<h3 data-start="1119" data-end="1156"><strong data-start="1125" data-end="1156">Forms: Powder and Liquid</strong></h3>
<ul data-start="1158" data-end="1652">
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<p data-start="1160" data-end="1262"><strong data-start="1160" data-end="1176">Liquid form:</strong> The injectable medical version (clear solution), used for anesthesia and analgesia.</p>
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<p data-start="1265" data-end="1431"><strong data-start="1265" data-end="1281">Powder form:</strong> Typically results from the evaporation of the liquid formulation or direct synthesis. The powder is crystalline and ranges from white to off-white.</p>
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<p data-start="1434" data-end="1652">In clinical labs, powdered Ketamine can be reconstituted for injection or used in analytical testing. In unregulated environments, powder form introduces risks of <strong data-start="1597" data-end="1651">dosage inaccuracy, adulteration, and contamination</strong>.</p>
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<li>Ketamine is a medication mainly used for starting and maintaining anesthesia. It induces a trance-like state while providing pain relief, sedation, and memory loss. Other uses include for chronic pain, sedation in intensive care, and depression.</li>
<li>Ketamine is frequently used in severely injured people and appears to be safe.</li>
<li>A clinical practice guideline supports the use of ketamine as a dissociative sedative in emergency medicine.</li>
<li>It is the drug of choice for people in traumatic shock who are at risk of hypotension.</li>
<li>Low blood pressure is harmful to people with severe head injury and ketamine is least likely to cause low blood pressure, often even able to prevent it.</li>
<li>Ketamine is also used for pain management.</li>
<li>Low doses of ketamine may reduce morphine use, nausea, and vomiting after surgery. Ketamine is used for pain relief. Buy Ketamine HCL Crystal Powder Online Without Prescription.</li>
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<h4 style="text-align: left;" data-start="1659" data-end="1691"><strong data-start="1665" data-end="1691">Mechanism of Action</strong></h4>
<p style="text-align: left;" data-start="1693" data-end="1766">Ketamine’s main mechanism is <strong data-start="1722" data-end="1750">NMDA receptor antagonism</strong>. This produces:</p>
<ul style="text-align: left;" data-start="1767" data-end="1965">
<li data-start="1767" data-end="1837">
<p data-start="1769" data-end="1837"><strong data-start="1769" data-end="1786">Dissociation:</strong> Detachment from body and environment perception.</p>
</li>
<li data-start="1838" data-end="1905">
<p data-start="1840" data-end="1905"><strong data-start="1840" data-end="1854">Analgesia:</strong> Pain relief without total loss of consciousness.</p>
</li>
<li data-start="1906" data-end="1965">
<p data-start="1908" data-end="1965"><strong data-start="1908" data-end="1935">Amnesia and anesthesia:</strong> Especially at higher doses.</p>
</li>
</ul>
<p style="text-align: left;" data-start="1967" data-end="1996">Additional receptor activity:</p>
<ul style="text-align: left;" data-start="1997" data-end="2252">
<li data-start="1997" data-end="2086">
<p data-start="1999" data-end="2086"><strong data-start="1999" data-end="2031">Opioid receptor interaction:</strong> Partial μ-opioid agonism, contributing to analgesia.</p>
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<p data-start="2089" data-end="2164"><strong data-start="2089" data-end="2115">Monoaminergic effects:</strong> Increases dopamine and serotonin transmission.</p>
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<p data-start="2167" data-end="2252"><strong data-start="2167" data-end="2196">AMPA receptor modulation:</strong> Believed to underlie its rapid antidepressant effect.</p>
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<h6><strong>Short Term Effects Of Ketamine</strong></h6>
<p>When ketamine is snorted, it gets into the bloodstream quickly, and intoxication effects occur soon after it’s taken. Although it’s an anesthetic, at low doses it raises heart rate. It’s also associated with cognitive impairment during intoxication, including to speech and executive function. It can also induce mild psychedelic effects such as perceptual changes and psychotic-like experiences, which are appealing to some users but can also be distressing. At slightly higher doses, users can experience a dissociative state, where their mind feels separated from their body. This can also manifest as a feeling of depersonalization.</p>
<p>At higher doses, the anesthetic quality of ketamine becomes more pronounced. People may find it difficult to move and may feel numb, and can experience more vivid hallucinations. This is sometimes called the ‘k-hole’ by users. Amnesia can occur at this level of use. This is a particular danger of using ketamine recreationally: users are vulnerable to assault from others in this state, or can put themselves in danger by not being aware of their surroundings (for example being unaware they are outside and it is cold can lead to hypothermia, or being unaware of surroundings could lead to walking in to traffic).</p>
<p>Special K can become more dangerous when mixed with other substances. Because of its anesthetic qualities, it’s dangerous to use ketamine alongside depressants such as alcohol or opiates, as a person increases their risk of passing out or stopping breathing. Conversely, taking ketamine alongside stimulants can put extra pressure on the heart, and also increase the risk of anxiety brought on by heightened arousal, and can lead to symptoms such as palpitations.</p>
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<p>As is the case for a number of illicit recreational drugs, the research into the long-term effects of using ketamine recreationally is somewhat lacking. However, anecdotal reports that heavy Vitamin K use is associated with bladder and urinary tract problems are common, and although the mechanism by which ketamine might cause these problems isn’t well known, there is some evidence from case studies of heavy ketamine users that daily use for prolonged periods of time might lead to the thickening of the bladder wall. Heavy users sometimes report cloudy or bloody urine, pain when going to the toilet, and urge incontinence. There has only been one reported case of urinary problems in a person prescribed ketamine for medical reasons.</p>
<p>There is some evidence that prolonged heavy ketamine use is associated with memory problems. As with many of these studies, it is difficult to know with certainty whether or not there were already pre-existing differences between those who use ketamine, and those who choose not to, but the use of controls who also use other substances hopefully minimizes this problem. Interestingly, a small study of 18 ketamine users and 10 polydrug using controls also found some evidence that semantic memory impairments seen in ketamine users may reverse if a person dramatically cuts down their use. However, the same study found little evidence that impairments to episodic memory and attention improve after cessation.</p>
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<p>There’s some suggestion that ketamine could be effective for treatment-resistant depression, a notoriously difficult condition to treat (hence the name). A pilot study conducted in Oxford gave 28 patients with severe treatment-resistant depression or bipolar disorder low doses of intravenous ketamine over three weeks. The results were mixed, with eight individuals responding well to the treatment for between 25 days and 24 weeks. However, eight other people in the study didn’t complete the treatment, either because they suffered adverse reactions to the infusion, or because they were not experiencing any benefit and were becoming more anxious.</p>
<p>Ketamine is also currently being investigated as a treatment for alcohol addiction. In fact, the Medical Research Council have a call-out on their website right now looking for recently alcohol abstinent volunteers with severe alcohol use disorder to take part. So watch this space for updates on this research!</p>
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<h3><strong>KETAMINE LIQUID for sale </strong></h3>
<p id="section---WhatIsKetamine">What is Ketamine?</p>
<p>While liquid ketamine is an anesthetic, ketamine is actually a special kind of anesthetic known as a <b>dissociative anesthetic</b>. At least in part, dissociative anesthesia results in a person’s immobility and a feeling of detachment from oneself and one’s own environment. Dissociative anesthesia also provides pain relief and an inability to recall what occurred while under the influence of the drug (amnesia). Ketamine also distorts a person’s sensation of sight and sound.</p>
<h4>Purchase Ketamine Online</h4>
<p>Ketamine’s ability to provide this dissociation from ‘reality’, and induce hallucinogenic effects, pain relief, as well calm and relaxation, is the major reason for its use as an illegal recreational drug.</p>
<h4 id="section---SideEffects">Ketamine For Sale</h4>
<p>While ketamine has valid uses in human and veterinary medicine for surgical purposes, its more prevalent and rampant abuse by people outside the medical field has made it a tightly controlled substance in many nations. This is because ketamine can cause serious side effects even when under the careful use and watch of a physician or veterinarian, not to mention when being used and abused outside the medical sphere by individuals with no medical training</p>
<h5 id="section---SideEffects">Side Effects Of Ketamine</h5>
<ul>
<li>Hypertension, or increased blood pressure</li>
<li>Tachycardia, an increased heart rate</li>
<li>Tachypnea, an increased respiratory rate or respiratory depression</li>
<li>Nausea and vomiting</li>
<li>Anorexia</li>
<li>Stiff muscles as well as jerky muscular movements.</li>
<li>Confusion or agitation</li>
<li>Hallucinations and delirium</li>
<li>Urinary tract toxicity</li>
<li>Violent behavior</li>
<li>Seizures</li>
<li>A life-threatening allergic reaction</li>
<li>Coma</li>
<li>Death from overdose</li>
</ul>
<p>some of this effect depends on the individual, as well as the amount of the drug taken at any given time.</p>
<p>As a drug of abuse</p>
<p>Ketamine is most often used in the dance club setting as a party drug. It produces an abrupt high that lasts for about an hour. Users report euphoria, along with feelings of floating and other “out of body” sensations. Hallucinations, similar to those experienced with LSD, are common.</p>
<p>Street names include:</p>
<ul>
<li>Cat Valium</li>
<li>KitKat</li>
<li>Special K</li>
<li>Vitamin K</li>
<li>The horse tranquilizer</li>
<li>Ket</li>
<li>Purple</li>
<li>Super K</li>
<li>Jet</li>
</ul>
<p>It is taken orally as a pill, snorted, smoked with tobacco or marijuana, or mixed into drinks. Most often, it is cooked into a white powder for snorting. Taken orally, it can cause severe nausea and vomiting.</p>
<p>Regardless of how it is ingested, its effects begin within a few minutes and last for less than an hour.</p>
<p>Higher doses can produce more intense effects known as being in the “K-hole,” where users become unable to move or communicate and feel very far away from their body.</p>
<p>Some users seek out this type of transcendental experience, while others find it terrifying and consider it an adverse effect.</p>
<p>Ketamine and alcohol</p>
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<p>Ketamine toxicity alone is unlikely to lead to death, according to the WHO. However, combining it with other substances, such as alcohol, can increase the sedative effects, possibly leading to a fatal overdose.</p>
<p>In the U.S., 1,550 emergency department (ED) visits were due to illegal ketamine use, and 71.5 percent of these also involved alcohol.</p>
<h6>Overdose</h6>
<p>The risk of overdose is high, because, for a recreational user, there is only a slight difference in dosage between obtaining the drug’s desired effects and an overdose.</p>
</div>
<div class="css-0">
<div><a name="addiction"></a>Addiction</div>
<p>Ketamine is a Class III controlled substance. Prolonged use can cause dependence, tolerance, and withdrawal symptoms. Quitting can lead to depression, anxiety, insomnia, and flashbacks.</p>
<p>Chronic users have been known to “binge” their ketamine use in an attempt to experience again the dissociative, euphoric effects of their early first use.</p>
</div>
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