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Script éducatif : IndusClean Multi-cleaner – Le nettoyant industriel polyvalent – Acheter IndusClean

Introduction

Dans les environnements industriels, commerciaux et même résidentiels, le nettoyage efficace des surfaces, des équipements et des installations est essentiel pour garantir la sécurité, la performance et la durabilité. C’est dans ce contexte que IndusClean Multi-cleaner s’impose comme une solution de nettoyage hautement concentrée, polyvalente et respectueuse de l’environnement. Acheter IndusClean

Ce script vous propose une exploration complète de ce produit : sa composition, ses applications, ses avantages, ses précautions d’usage et ses impacts dans le monde professionnel.

Qu’est-ce que IndusClean Multi-cleaner ?

IndusClean Multi-cleaner est un solvant industriel hautement concentré, fabriqué selon des normes de qualité allemandes. Il est conçu pour éliminer efficacement les saletés tenaces telles que la graisse, l’huile, la peinture, la rouille, les résines et les encres. Ce nettoyant est utilisé dans divers secteurs : automobile, électronique, imprimerie, construction, textile, et bien plus encore. Ketamine for sale

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Principales caractéristiques :

  • Formule concentrée : à diluer avec de l’eau selon les besoins
  • Sans fumées nocives : ne dégage pas de vapeurs toxiques
  • Non inflammable : sécurité renforcée lors de l’utilisation
  • Polyvalent : adapté à une large gamme de surfaces et de matériaux

Applications industrielles

IndusClean Multi-cleaner est reconnu pour sa capacité à traiter des tâches complexes dans des environnements exigeants. Voici quelques exemples d’applications :

Secteur automobile

  • Nettoyage des jantes en alliage
  • Dégraissage des freins et des moteurs
  • Élimination des résidus de goudron et de bitume

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Industrie de l’impression

  • Nettoyage des têtes d’impression
  • Élimination des encres et des résines
  • Entretien des circuits imprimés

 Travaux de rénovation

  • Décapage de peinture sur bois
  • Nettoyage des sols industriels
  • Préparation des surfaces avant traitement
Laboratoires et ateliers
  • Nettoyage des équipements électrolytiques
  • Dégraissage des instruments de précision
  • Élimination des colles et vernis

Respect de l’environnement

Contrairement à de nombreux solvants industriels, IndusClean est formulé pour minimiser son impact écologique :

  • Biodegradable : se décompose naturellement sans polluer
  • Sans produits chimiques agressifs : ne contient pas de substances corrosives
  • Faible odeur : idéal pour les environnements fermés ou sensibles

Cette approche éco-responsable permet aux entreprises de respecter les normes environnementales tout en maintenant une efficacité optimale.

Mode d’emploi

L’utilisation correcte d’IndusClean Multi-cleaner garantit des résultats professionnels tout en assurant la sécurité de l’utilisateur.

Étapes recommandées :

  1. Dilution : selon le niveau de saleté, diluer le produit avec de l’eau (rapport recommandé : 1:5 à 1:10)
  2. Application : utiliser un chiffon, une éponge ou un pulvérisateur pour appliquer le produit sur la surface à nettoyer
  3. Temps de pose : laisser agir quelques minutes pour permettre au solvant de dissoudre les impuretés
  4. Rinçage : essuyer ou rincer à l’eau claire pour révéler une surface propre et brillante

Avantages clés

IndusClean Multi-cleaner offre une série d’avantages qui en font un choix privilégié pour les professionnels :

Avantage Description
Efficacité Élimine rapidement les taches les plus tenaces
Économie Une petite quantité suffit pour de grandes surfaces
Sécurité Non inflammable, sans vapeurs toxiques
Polyvalence Convient à de nombreux matériaux et secteurs
Durabilité Formule concentrée qui dure longtemps

Précautions d’usage

Bien que le produit soit conçu pour être sûr, certaines précautions doivent être respectées :

  • Port de gants recommandé : pour éviter tout contact prolongé avec la peau
  • Utilisation dans un espace ventilé : même si l’odeur est faible
  • Ne pas ingérer : le produit est strictement réservé à un usage externe
  • Tenir hors de portée des enfants : stockage sécurisé obligatoire

En cas de contact avec les yeux ou d’ingestion accidentelle, il est impératif de consulter un médecin immédiatement.

Conditionnement et livraison

IndusClean Multi-cleaner est généralement disponible en bouteilles de 1000 ml, conditionnées dans des emballages scellés pour garantir leur intégrité. La livraison est rapide et sécurisée, avec des options disponibles pour les clients professionnels à l’international.

Témoignages et avis

De nombreux utilisateurs professionnels ont partagé leur satisfaction :

“La qualité est toujours au rendez-vous. Livraison en un jour, efficacité impressionnante.” – Pal F., Cologne

“Un produit qui a sauvé notre atelier à plusieurs reprises. Indispensable pour le nettoyage des machines.” – Atelier mécanique, Lyon

Ces témoignages confirment la fiabilité et la performance du produit dans des contextes variés.

Conclusion

IndusClean Multi-cleaner est bien plus qu’un simple nettoyant : c’est un outil professionnel conçu pour répondre aux défis du nettoyage industriel moderne. Sa formule concentrée, sa polyvalence et son respect de l’environnement en font une solution incontournable pour les entreprises soucieuses de la qualité et de la durabilité.

Que vous soyez dans l’automobile, l’électronique, l’imprimerie ou la maintenance industrielle, IndusClean vous offre la puissance et la sécurité dont vous avez besoin pour un nettoyage impeccable.

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5CLADBA: Forensic and Research Applications

5CLADBA, also known as 5CL-ADB-A, is a synthetic cannabinoid belonging to the indazole-3-carboxamide family. It has emerged as a compound of interest in forensic toxicology and chemical research due to its potent activity at cannabinoid receptors and its structural similarity to other designer drugs. While not approved for human or veterinary use, 5CLADBA plays a critical role in laboratory investigations, analytical method development, and receptor mapping studies.

Analytical Chemistry and Detection

In forensic laboratories, 5CLADBA is used as a reference standard for developing and validating detection methods. Its presence in seized materials and biological samples has prompted the need for accurate identification using advanced techniques such as:

  • Gas Chromatography–Mass Spectrometry (GC–MS)
  • Liquid Chromatography–Tandem Mass Spectrometry (LC–MS/MS)
  • Fourier Transform Infrared Spectroscopy (FTIR)

These methods allow forensic scientists to differentiate 5CLADBA from other synthetic cannabinoids and quantify its concentration in complex matrices such as blood, urine, or plant material.

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Receptor Binding and Pharmacological Research

5CLADBA exhibits high affinity for CB1 and CB2 receptors, making it a valuable tool for studying the endocannabinoid system. Researchers use it to explore:

  • Cannabinoid receptor activation pathways
  • Dose-response relationships
  • Structure-activity correlations
  • Potential toxicological effects of synthetic cannabinoids

Its potency and receptor selectivity provide insights into how synthetic cannabinoids interact with neural and immune systems, contributing to broader pharmacological understanding.

Forensic Toxicology and Casework

In forensic casework, 5CLADBA is often detected in:

  • Drug seizures involving herbal mixtures or powders
  • Postmortem toxicology screens
  • Impaired driving investigations
  • Drug-facilitated crime analyses

Its detection helps forensic professionals determine the presence of synthetic cannabinoids in criminal or accidental contexts. Because 5CLADBA is not always scheduled under national drug laws, its identification may support legal arguments under analog acts or contribute to public health surveillance.

Chemical Synthesis and Auxiliary Use

Beyond toxicology, 5CLADBA is used as a raw material and auxiliary reagent in chemical synthesis. Its functional groups allow it to participate in:

  • Halogenation
  • Condensation reactions
  • Polymerization studies
  • Catalytic processes

These properties make it useful in developing specialty chemicals, dyes, and performance materials, particularly in controlled research environments.

Safety and Compliance

Due to its potency and potential toxicity, 5CLADBA must be handled with strict safety protocols:

  • Use of gloves, goggles, and protective clothing
  • Storage in cool, dry, secure conditions
  • Disposal through licensed chemical waste services

It is sold only to licensed laboratories and verified researchers, with clear disclaimers that it is not for human consumption and not for use in food, drugs, or cosmetics.

Conclusion

5CLADBA is a versatile and scientifically valuable compound that supports forensic investigations, toxicological research, and chemical development. Its role in understanding synthetic cannabinoids and enhancing analytical capabilities makes it a key asset in modern laboratory science. Continued research and regulatory awareness are essential to ensure its safe and effective use in professional settings.

 

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Introduction to 4-HO-MET

 4-HO-MET (4-hydroxy-N-methyl-N-ethyltryptamine), also known as metocin, is a synthetic psychedelic compound belonging to the tryptamine class. It’s structurally similar to psilocin, the active compound in psilocybin mushrooms, and was first synthesized by chemist Alexander Shulgin

 Chemical Profile of 4-HO-MET

  • Class: Psychedelic tryptamine
  • Structure: Analog of psilocin
  • Mechanism: Likely acts as a partial agonist at serotonin receptors, especially 5-HT2A, which is associated with psychedelic effects

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 Origin of 4-HO-MET

 The Man and His Rediscovery

Alexander “Sasha” Shulgin (1925–2014) was a pioneering American chemist and pharmacologist best known for his synthesis and personal exploration of hundreds of psychoactive compounds, particularly in the phenethylamine and tryptamine families leading to the discovery of 4-HO-MET amongst many others.

Key Contributions: Rediscovery of MDMA
  • Shulgin is credited with reintroducing MDMA (Ecstasy) to the scientific and therapeutic community in the late 1970s.
  • He advocated for its use in psychotherapy, especially for enhancing emotional communication.

 Alexander Shulgin’s influence on psychedelic therapy is profound and enduring. Here’s how his work shaped the field:

Compounds He Created or Popularized

Shulgin synthesized and explored over 230 psychoactive compounds, many of which are still studied today. Some of the most notable include:

Compound Class Known Effects
MDMA Empathogen Emotional openness, reduced fear, enhanced communication
2C-B Phenethylamine Visuals, euphoria, mild stimulation
DOM DOx family Long-lasting visuals, altered time perception
4-HO-MET Tryptamine Psilocin-like visuals, shorter duration
5-MeO-DiPT Tryptamine Auditory distortions, body sensations
2C-T-7 Phenethylamine Introspection, visuals, potential toxicity at high doses

 

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Each compound was meticulously documented in his books PiHKAL and TiHKAL, which include synthesis instructions, dosage guidelines, and subjective trip reports

Influence on Psychedelic Therapy: Scientific Legacy

  • Shulgin’s self-experimentation and detailed documentation laid the groundwork for modern psychedelic pharmacology.
  • His work inspired researchers to explore psychedelics as therapeutic tools for depression, PTSD, anxiety, and addiction.

Therapeutic Philosophy

  • He believed psychedelics could unlock deep emotional and spiritual insights, especially when used in safe, intentional settings.
  • His wife, Ann Shulgin, was a Jungian lay therapist who used MDMA and 2C-B in therapeutic sessions, helping clients explore their unconscious and shadow selves

Cultural Impact

  • Shulgin’s home lab, known as “The Farm,” became a hub for scientists, therapists, and psychonauts.
  • His open sharing of chemical knowledge fostered a community of responsible exploration, influencing groups like MAPS (Multidisciplinary Association for Psychedelic Studies)
 Enduring Legacy
  • Shulgin is often called the “Godfather of Ecstasy” for his role in bringing MDMA to therapeutic use.
  • His work continues to inspire the psychedelic renaissance, with clinical trials now exploring compounds he first synthesized.
  • His books remain seminal texts for chemists, therapists, and psychonauts alike.

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 Effects
Positive Effects Negative Effects
Visual hallucinations Nausea
Enhanced creativity Muscle tension
Euphoria Paranoia
Ego dissolution Temperature dysregulation
Connection with nature Delusions (at high doses)

Users often describe the experience as visually intense but less psychologically heavy than psilocybin mushrooms

Duration & Dosage

  • Onset: 15–40 minutes
  • Peak: 2–3 hours
  • Total duration: 4–6 hours
  • After-effects: May linger for 2–12 hours
  • Common dosage: 10–20 mg orally; higher doses (20–30 mg) yield stronger effects
Safety & Legality
  • Legality: Varies by country; legal in some regions as a research chemical
  • Toxicity: No known lethal dose; generally considered non-toxic at standard doses
  • Risks: As with all psychedelics, psychological vulnerability and set/setting play a major role in the experience.

Author of PiHKAL & TiHKAL :Together with his wife Ann Shulgin, he wrote:

  • PiHKAL: Phenethylamines I Have Known and Loved
  • TiHKAL: Tryptamines I Have Known and Loved

These books are part autobiography, part chemistry manual, documenting the synthesis and subjective effects of numerous compounds.

Shulgin Rating Scale

He developed a scale to quantify the intensity and nature of psychedelic experiences, which became widely used in psychopharmacology.

Shulgin Philosophy & Legacy

  • Shulgin believed in cognitive liberty—the right to explore one’s own consciousness.
  • He tested most of his creations on himself, starting with microdoses and meticulously recording effects.
  • His work laid the foundation for modern psychedelic research and inspired generations of scientists, therapists, and psychonauts.
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What Are Cannabinoids?

Cannabinoids are naturally occurring compounds found in the cannabis plant. They interact with the body’s endocannabinoid system, influencing mood, pain, appetite, and more. The most well-known cannabinoids include:

  • THC (Tetrahydrocannabinol): Responsible for the psychoactive “high”
  • CBD (Cannabidiol): Non-intoxicating, known for calming and therapeutic effects
  • THCA (Tetrahydrocannabinolic Acid): Precursor to THC, found in raw cannabis
  • CBG, CBN, CBC: Lesser-known cannabinoids with unique benefits

Each cannabinoid has distinct effects, and their combinations can produce the entourage effect, enhancing therapeutic outcomes.

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Key Differences

Feature Persy Diamond Vapes Cannabinoids
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Cannabinoids are the foundation of all cannabis products. Whether in flower, edibles, tinctures, or vapes, they determine the effect profile. For example:

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Use Cases

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Research chemicals are substances that are often used in scientific and medical studies but may not be approved for human consumption or general use. Discussing their use requires extreme caution, and promoting or encouraging misuse can be harmful or illegal. The following content is intended for educational and informational purposes only, focusing on safe, ethical, and legal practices in research environments.

Understanding the Correct Use of Research Chemicals: A Guide for Safe and Ethical Practice

Research chemicals play a vital role in advancing science, medicine, and technology. From studying neurological pathways to testing new therapeutic compounds, these substances help researchers explore the unknown. However, their correct use requires strict adherence to safety protocols, legal guidelines, and ethical standards.

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Whether you’re a lab technician, academic researcher, or student in the field, understanding how to handle research chemicals responsibly is essential.

What Are Research Chemicals?

Research chemicals are compounds used primarily for laboratory and scientific research. They may include:

  • Novel psychoactive substances (NPS) for neurological studies
  • Synthetic cannabinoids or stimulants for pharmacological testing
  • Unapproved analogs of known drugs for structural analysis
  • Experimental compounds in toxicology or biochemistry

These chemicals are often not approved by regulatory bodies like the FDA or EMA for human or veterinary use. Their safety profiles, long-term effects, and interactions may be unknown — which is why they’re strictly for controlled research.

Correct Use: Best Practices in a Research Setting

To ensure safety and integrity, researchers must follow these key guidelines:

1. Source from Reputable Suppliers

Only purchase research chemicals from certified, transparent vendors who provide:

  • Certificates of analysis (COA)
  • Purity reports
  • Batch tracking
  • Compliance with local regulations

Avoid anonymous or unverified sources, especially online marketplaces that lack accountability.

2. Understand the Chemical Profile

Before handling any substance:

  • Review its molecular structure, known effects, and toxicity data
  • Study relevant literature and peer-reviewed research
  • Consult safety data sheets (SDS) for handling instructions

Knowledge is your first line of defense.

3. Use Proper Lab Equipment

Always work in a controlled environment with:

  • Fume hoods or ventilated enclosures
  • Gloves, goggles, and lab coats
  • Spill kits and emergency wash stations

Never handle volatile or unknown compounds without full protective gear.

4. Label and Store Correctly

Research chemicals should be:

  • Clearly labeled with name, concentration, and hazard warnings
  • Stored in temperature-controlled, secure cabinets
  • Separated from incompatible substances

Proper labeling prevents accidents and ensures traceability.

5. Document Everything

Maintain detailed records of:

  • Dosages and concentrations used
  • Experimental conditions
  • Observations and outcomes
  • Disposal methods

Documentation supports reproducibility and protects against liability.

Legal and Ethical Considerations

Using research chemicals outside of approved settings can be illegal and dangerous. Researchers must:

  • Comply with local, national, and international laws
  • Avoid any human or animal testing unless approved by ethics boards
  • Never distribute or promote chemicals for recreational use
  • Report adverse findings or safety concerns transparently

Ethical research protects both the public and the integrity of science.

Common Misuses to Avoid

Unfortunately, some individuals misuse research chemicals for recreational or unregulated purposes. This can lead to:

  • Severe health risks
  • Legal consequences
  • Contamination of scientific data
  • Damage to professional reputation

If you’re not conducting formal research, do not handle or consume research chemicals. They are not designed for casual use and can be unpredictable or harmful.

The Role of Education and Awareness

Institutions and researchers should promote:

  • Training programs on chemical safety
  • Public awareness campaigns about misuse
  • Collaboration with regulatory bodies

The goal is to foster a culture of responsibility, where innovation thrives without compromising safety.

Final Thoughts

Research chemicals are powerful tools — but only when used correctly. At their best, they unlock new discoveries and deepen our understanding of biology, chemistry, and medicine. At their worst, they pose serious risks when mishandled or misused.

If you’re working with these substances, treat them with the respect they demand. Follow protocols. Stay informed. And always prioritize safety over shortcuts.

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Tetrodotoxin

Tetrodotoxin Pufferfish Extract, a neurotoxin C11H17N3O8 that is found especially in pufferfishes and that blocks nerve conduction by suppressing permeability of the nerve fiber to sodium ions Tetrodotoxin Pufferfish Extract. Tetrodotoxin (TTX) is a potent neurotoxin. Its name derives from Tetraodontiformes, an order that includes pufferfish, porcupinefish, ocean sunfish, and triggerfish; several of these species carry the toxin. Although tetrodotoxin was discovered in these fish and found in several other animals (e.g., in blue-ringed octopuses, rough-skinned newts, and moon snails), it is actually produced by certain infecting or symbiotic bacteria like Pseudoalteromonas, Pseudomonas, and Vibrio as well as other species found in Tetrodotoxin (TTX) is a selective sodium channel blocker nonprotein toxin. The consumption of an organism containing TTX can cause neurological and gastrointestinal symptoms. TTX, widely distributed among marine as well as terrestrial animals, induces dangerous intoxication. This toxin is mainly isolated from the skin, viscera, ovaries, and liver of the pufferfish. The toxin is produced by various species of bacteria, and TTX-bearing animals absorb and accumulate it through the food chain. TTX is commonly used in many laboratories as a pharmacological tool because of its ability to selectively block the sodium channels on the nerve membrane. No antidote is available for clinical use. animals.

Tetrodotoxin Pufferfish Extract (TTX) is a potent neurotoxin responsible for many human intoxications and fatalities each year. The origin of TTX is unknown, but in the pufferfish, it seems to be produced by endosymbiotic bacteria that often seem to be passed down the food chain.

The ingestion of contaminated pufferfish, considered the most delicious fish in Japan, is the usual route of toxicity. This neurotoxin, reported as a threat to human health in Asian countries, has spread to the Pacific and Mediterranean, due to the increase of temperature waters worldwide. Tetrodotoxin Pufferfish Extract

Detection of body fluids

Tetrodotoxin may be quantified in serum, whole blood or urine to confirm a diagnosis of poisoning in hospitalized patients or to assist in the forensic investigation of a case of fatal overdosage. Most analytical techniques involve mass spectrometric detection following gas or liquid chromatographic separation

Tetrodotoxin. The pufferfish has an endosymbiotic (a form of symbiosis in which one organism lives inside the other) bacterium in its body that produces tetrodotoxin, a toxin that is selective for voltage-gated sodium channels. In fact, this bacterium can be found in a variety of marine and terrestrial species in which tetrodotoxin is also found, including the blue-ringed octopus (Bane et al., 2014; Magarlamov et al., 2017). Despite the presence of this dangerous toxin, pufferfish (“fugu”) is a delicacy in Japan. Specially trained chefs purposely leave some tetrodotoxin in the fish they prepare so the consumer can experience the desired side effects of the meal: a tingling sensation in their mouth and a sense of euphoria.

Tetrodotoxin Pufferfish Extract. TTX, for which there is no known antidote, inhibits sodium channel producing heart failure in many cases and consequently death. In Japan, a regulatory limit of 2 mg eq TTX/kg was established, although the restaurant preparation of “fugu” is strictly controlled by law and only chefs qualified are allowed to prepare the fish. Due to its paralysis effect, this neurotoxin could be used in the medical field as an analgesic to treat some cancer pains.Bromazolam for sale USA

Toxicity

TTX is extremely toxic. The Material Safety Data Sheet for TTX lists the oral median lethal dose (LD50) for mice as 334 μg per kg. For comparison, the oral LD50 of potassium cyanide for mice is 8.5 mg per kg,[40] demonstrating that even orally, TTX is more poisonous than cyanide. TTX is even more dangerous if administered intravenously; the amount needed to reach a lethal dose by injection is 8 μg per kg in mice. Tetrodotoxin Pufferfish Extract

The toxin can enter the body of a victim by ingestion, injection, inhalation, or through abraded skin.

Poisoning occurring as a consequence of the consumption of fish from the order Tetraodontiformes is extremely serious. The organs (e.g. liver) of the pufferfish can contain levels of tetrodotoxin sufficient to produce the described paralysis of the diaphragm and corresponding death due to respiratory failure. Toxicity varies between species and at different seasons and geographic localities, and the flesh of many pufferfish may not be dangerously toxic.

The mechanism of toxicity is through the blockage of fast voltage-gated sodium channels, which are required for the normal transmission of signals between the body and the brain. As a result, TTX causes loss of sensation, and paralysis of voluntary muscles including the diaphragm and intercostal muscles, stopping breathing.

Tetrodotoxin Pufferfish Extract

Tetrodotoxin is a sodium channel blocker. It inhibits the firing of action potentials in neurons by binding to the voltage-gated sodium channels in nerve cell membranes and blocking the passage of sodium ions (responsible for the rising phase of an action potential) into the neuron. This prevents the nervous system from carrying messages and thus muscles from contracting in response to nervous stimulation.

Its mechanism of action, selective blocking of the sodium channel, was shown definitively in 1964 by Toshio Narahashi and John W. Moore at Duke University, using the sucrose gap voltage clamp technique.

The association of bacterial species with the production of the toxin is unequivocal – Lago and coworkers state, “[e]ndocellular symbiotic bacteria have been proposed as a possible source of eukaryotic TTX by means of an exogenous pathway, and Chau and coworkers note that the “widespread occurrence of TTX in phylogenetically distinct organisms… strongly suggests that symbiotic bacteria play a role in TTX biosynthesis” – although the correlation has been extended to most but not all metazoans in which the toxin has been identified.

History

The therapeutic uses of puffer fish (tetraodon) eggs were mentioned in the first Chinese pharmacopoeia Pen-T’so Ching (The Book of Herbs, allegedly 2838–2698 BC by Shennong; but a later date is more likely), where they were classified as having “medium” toxicity, but could have a tonic effect when used at the correct dose. The principal use was “to arrest convulsive diseases”.

In the Pen-T’so Kang Mu (Index Herbacea or The Great Herbal by Li Shih-Chen, 1596) some types of the fish Ho-Tun (the current Chinese name for tetraodon) were also recognized as both toxic yet, at the right dose, use as part of a tonic. Increased toxicity in Ho-Tun was noted in fish caught at sea (rather than river) after the month of March.

It was recognized that the most poisonous parts were the liver and eggs, but that toxicity could be reduced by soaking the eggs, noting that tetrodotoxin is slightly water-soluble, and soluble at 1 mg/ml in slightly acidic solutions.

The German physician Engelbert Kaempfer, in his “A History of Japan” (translated and published in English in 1727), described how well known the toxic effects of the fish were, to the extent that it would be used for suicide and that the Emperor specifically decreed that soldiers were not permitted to eat it. There is also evidence from other sources that knowledge of such toxicity was widespread throughout Southeast Asia and India.

The first recorded cases of TTX poisoning affecting Westerners are from the logs of Captain James Cook from 7 September 1774. On that date Cook recorded his crew eating some local tropic fish (pufferfish), and then feeding the remains to the pigs kept on board.

The crew experienced numbness and shortness of breath, while the pigs were all found dead the next morning. In hindsight, it is clear that the crew survived a mild dose of tetrodotoxin, while the pigs ate the pufferfish body parts that contain most of the toxin, thus being fatally poisoned.

The toxin was first isolated and named in 1909 by Japanese scientist Dr. Yoshizumi Tahara. It was one of the agents studied by Japan’s Unit 731, which evaluated biological weapons on human subjects in the 1930s.

On the contrary, there has been a failure in a single case, that of newts (Taricha granulosa), to detect TTX-producing bacteria in the tissues with the highest toxin levels (skin, ovaries, muscle), using PCR methods, although technical concerns about the approach have been raised.

Critically for the general argument, Takifugu rubripes puffers captured and raised in a laboratory on controlled, TTX-free diets “lose toxicity over time,” while cultured, TTX-free Takifugu niphobles puffers fed on TTX-containing diets saw TTX in the livers of the fishes increase to toxic levels.

Hence, as bacterial species that produce TTX are broadly present in aquatic sediments, a strong case is made for ingestion of TTX and/or TTX-producing bacteria, with accumulation and possible subsequent colonization and production.

Nevertheless, without clear biosynthetic pathways (not yet found in metazoans, but shown for bacteria), it remains uncertain whether it is simply via bacteria that each metazoan accumulates TTX; the question remains as to whether the quantities can be sufficiently explained by ingestion, ingestion plus colonization, or some other mechanism.

Symptoms and treatment

The diagnosis of pufferfish poisoning is based on the observed symptomatology and recent dietary history. Symptoms typically develop within 30 minutes of ingestion, but may be delayed by up to four hours; however, if the dose is fatal, symptoms are usually present within 17 minutes of ingestion. Paresthesia of the lips and tongue is followed by developing paresthesia in the extremities, hypersalivation, sweating, headache, weakness, lethargy, incoordination, tremor, paralysis, cyanosis, aphonia, dysphagia, and seizures. The gastrointestinal symptoms are often severe and include nausea, vomiting, diarrhea, and abdominal pain; death is usually secondary to respiratory failure. There is increasing respiratory distress, speech is affected, and the victim usually exhibits dyspnea, mydriasis, and hypotension. Paralysis increases, and convulsions, mental impairment, and cardiac arrhythmia may occur. The victim, although completely paralyzed, may be conscious and in some cases completely lucid until shortly before death, which generally occurs within 4 to 6 hours (range ~20 minutes to ~8 hours). However, some victims enter a coma. If the patient survives 24 hours, recovery without any residual effects will usually occur over a few days. Therapy is supportive and based on symptoms, with aggressive early airway management. If ingested, treatment can consist of emptying the stomach, feeding the victim activated charcoal to bind the toxin, and taking standard life-support measures to keep the victim alive until the effect of the poison has worn off. Alpha adrenergic agonists are recommended in addition to intravenous fluids to combat hypotension; anticholinesterase agents “have been proposed as a treatment option but have not been tested adequately”. Toad vemom for sale No antidote has been developed and approved for human use, but a primary research report (preliminary result) indicates that a monoclonal antibody specific to tetrodotoxin is in development by USAMRIID that was effective, in one study, for reducing toxin lethality in tests on mice.

 

Potential medicinal use

The deathstalker’s powerful venom contains the 36-amino acid peptide chlorotoxin (ribbon diagram shown). This blocks small-conductance chloride channels, immobilizing its prey. Scorpion venom is a mixture of neurotoxins; most of these are peptides, and chains of amino acids.

Many of them interfere with membrane channels that transport sodium, potassium, calcium, or chloride ions. These channels are essential for nerve conduction, muscle contraction and many other biological processes. Some of these molecules may be useful in medical research and might lead to the development of new disease treatments.

Among their potential therapeutic uses are analgesic, anti-cancer, antibacterial, antifungal, antiviral, antiparasitic, bradykinin-potentiating, and immunosuppressive drugs. As of 2020, no scorpion toxin-based drug is on sale, though chlorotoxin is being trialled for use against glioma, a brain cancer. Tetrodotoxin Pufferfish Extract Tetrodotoxin Pufferfish Extract Tetrodotoxin Pufferfish Extract Tetrodotoxin Pufferfish Extract Tetrodotoxin Pufferfish Extract Tetrodotoxin Pufferfish Extract  Tetrodotoxin Pufferfish Extract Tetrodotoxin Pufferfish Extract Tetrodotoxin Pufferfish Extract Mode of action Tetrodotoxin causes paralysis by affecting the sodium ion transport in both the central and peripheral nervous systems. A low dose of tetrodotoxin produces tingling sensations and numbness around the mouth, fingers, and toes. Higher doses produce nausea, vomiting, respiratory failure, difficulty walking, extensive paralysis, and death. As little as 1–4 mg of the toxin can kill an adult. Saxitoxin has a very different chemical structure than tetrodotoxin, but it has similar effects on the transport of cellular sodium and produces similar neurological effects. Saxitoxin is less toxic than tetrodotoxin. Some people, particularly in Asia, consider puffer fish a fine delicacy if it is carefully prepared by experienced chefs. The trick is to get just a small dose to feel mild tingling effects, but not the more serious symptoms of tetrodotoxin poisoning. In the United States tetrodotoxin poisoning is rare, but a recent US report indicated several cases of people catching and consuming puffer fish containing elevated levels of these toxins and suffering the ill effects. Treatment Treatment is supportive and symptom-based. Activated charcoal may be helpful.

Synthetic Cathinones
CategoriesCathinone

Synthetic Cathinones

Synthetic Cathinones

Synthetic Cathinones. What are synthetic cathinones?

Synthetic cathinones, more commonly known as bath salts, are human-made stimulants chemically related to cathinone, a substance found in the khat plant. Khat is a shrub grown in East Africa and southern Arabia, where some people chew its leaves for their mild stimulant effects. Human-made versions of cathinone can be much stronger than the natural product and, in some cases, very dangerous.

Synthetic cathinones usually take the form of a white or brown crystal-like powder and are sold in small plastic or foil packages labelled “not for human consumption.” They can be labelled as bath salts, plant food, jewellery cleaner, or phone screen cleaner.

Synthetic cathinones are part of a group of drugs that concern public health officials called new psychoactive substances (NPS). NPS are unregulated psychoactive mind-altering substances with no legitimate medical use and are made to copy the effects of controlled substances.

They are introduced and reintroduced into the market in quick succession to dodge or hinder law enforcement efforts to address their manufacture and sale.

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Synthetic cathinones are marketed as cheap substitutes for other stimulants such as amphetamines and cocaine. Products sold as Molly often contain synthetic cathinones instead of MDMA (see Synthetic Cathinones and Molly (Ecstasy).

Synthetic cathinones (Bath salts, eutylone, Flakka M-Cat, Monkey Dust) are a large group of manufactured chemicals which mimic the effects of other substances.

They usually come as a pill, capsule, powder or crystal. They are often mis-sold as MDMA or cocaine, but they require a lower dose which greatly increases the risk of overdose.

The effects vary a lot, and while they often have similar effects to MDMA or methamphetamine, paranoia and anxiety are more common. Synthetic cathinones found in New Zealand include N-ethylpentalone, mephedrone, methylenedioxypyrovalerone (MDPV), methylone, mexedrone, and Alpha PVP.

Pharmacology

Khat leaves are removed from the plant stalk and are kept in a ball in the cheek and chewed. Chewing releases juices from the leaves, which include the alkaloid cathinone. The absorption of cathinone has two phases: one in the buccal mucosa and one in the stomach and small intestine.

The stomach and small intestine are very important in the absorption of ingested alkaloids. At approximately 2.3 hours after chewing khat leaves, the maximum concentration of cathinone in blood plasma is reached.

The mean residence time is 5.2 ± 3.4 hours.[3] The elimination half-life of cathinone is 1.5 ± 0.8 hours. A two-compartment model for the absorption and elimination best describes this data.

However, at most, only 7% of the ingested cathinone is recovered in the urine. This indicates that the cathinone is being broken down in the body. Cathinone has been shown to selectively metabolize into R,S-(-)-norephedrine and cathine.

The reduction of the ketone group in cathinone will produce cathine. This reduction is catalyzed by enzymes in the liver. The spontaneous breakdown of cathinone is the reason it must be chewed fresh after cultivation

Synthetic Cathinones.

What are synthetic cathinones?
Synthetic cathinones is the name of a category of drugs related to the naturally occurring khat plant.1 They are stimulants, meaning that they speed up the messages between the brain and the body and have similar effects to amphetamines.

Synthetic cathinones are also part of a group of drugs known as New Psychoactive Substances (NPS). NPSs are a range of drugs that first appeared on the recreational drug market in the mid-2000s, that have been designed to mimic established illicit drugs, such as cannabis, cocaine, ecstasy and LSD. Between 2005 and 2014 more than 81 synthetic cathinone derivatives were reported to the EU Early Warning System.

Synthetic cathinones are mostly white or brown powders but also exist in the form of small, chunky crystals. They are sometimes found as capsules and less commonly as tablets.3

Types of cathinones commonly used
Mephedrone (4-MMC), M-CAT)
Methylone
Methcathinone
Buphedrone
Bupropion
Pyrovalerone
Alpha-Pyrrolidinovalerophenone (alpha-PVP)
MDPV.3,4,5

Synthetic Cathinones.

How do synthetic cathinones affect the brain?
Much is still unknown about how synthetic cathinones affect the human brain. Researchers do know that synthetic cathinones are chemically similar to drugs like amphetamines, cocaine, and MDMA.

A study found that 3,4-methylenedioxypyrovalerone (MDPV), a common synthetic cathinone, affects the brain in a manner similar to cocaine, but is at least 10 times more powerful. MDPV is the most common synthetic cathinone found in the blood and urine of patients admitted to emergency departments after taking bath salts.2

Synthetic cathinones can produce effects that include:

paranoia—extreme and unreasonable distrust of others
hallucinations—experiencing sensations and images that seem real but are not
increased friendliness
increased sex drive
panic attacks
excited delirium—extreme agitation and violent behaviour.

Synthetic production

Cathinone can be synthetically produced from propiophenone through a Friedel-Crafts Acylation of propionic acid and benzene. The resulting propiophenone can be brominated, and the bromine can be substituted with ammonia to produce a racemic mixture of cathinone.

A different synthetic strategy must be employed to produce enantiomerically pure (S)-cathinone. This synthetic route starts out with the N-acetylation of the optically active amino acid, S-alanine.

Then, phosphorus pentachloride (PCl5) is used to chlorinate the carboxylic acid forming an acyl chloride. At the same time, a Friedel-Crafts acylation is performed on benzene with aluminum chloride catalyst. Finally, the acetyl protecting group is removed by heating with hydrochloric acid to form enantiomerically pure S-(-)-cathinone.

Using synthetic cathinones with other drugs
The effects of combining cathinones with other drugs – including over-the-counter or prescribed medications – can be unpredictable and dangerous. The following combinations could have the following effects:

Synthetic cathinones + ice, speed or ecstasy: increase the risk of cardiovascular (heart) problems and substance-induced psychosis.7
Synthetic cathinones + alcohol + cannabis: nausea and vomiting.

Health and Safety
If possible, find out the specific cathinone you are using so you know what to expect and what a common dose is. Synthetic cathinone harm reduction advice is partly based on what is known of related drugs like amphetamines and MDMA, as not enough research has been done on individual synthetic cathinones specifically.

The use of synthetic cathinone is likely to be more dangerous when

taken in combination with alcohol or other drugs, particularly stimulants such as crystal methamphetamine (‘ice’) or ecstasy
driving or operating heavy machinery
judgment or motor coordination is required
alone (in case medical assistance is required)
the person has a mental health problem
the person has an existing heart problem.

In Australia, poisons information centres and clinical toxicology units around Australia are often contacted for advice on poisonings from synthetic cathinones. Features of these poisonings include agitation, tachycardia (increased heart rate), hypertension and in severe cases delirium, aggressive behaviour, hallucinations, hyperthermia, cardiac dysrhythmia (irregular heart beat) and seizures. Deaths have occurred due to alpha-PVP toxicity.4

Injecting synthetic cathinones can cause soft tissue and vascular damage.4

Sharing needles may also transmit:

Tetanus
Hepatitis B
Hepatitis C
HIV/AIDS.
Dependence and tolerance
There is limited data regarding people seeking treatment for synthetic cathinone dependence, however, people who use synthetic cathinones have reported a strong compulsion to redose, as well dependence.

Synthetic Cathinones

Effects of synthetic cathinones
There is no safe level of drug use. The use of any drug always carries some risk. It’s important to be careful when taking any type of drug.

Synthetic cathinones affect everyone differently, based on:

the amount taken
a person’s size, weight and health
whether the person is used to taking it
whether other drugs are taken around the same time
the strength of the drug (which can vary from batch to batch).
The individual effects and toxicity of each cathinone are distinct and can vary greatly between each person using them.

Generally speaking, in small doses the following effects may be experienced and may last for approximately 2-4 hours:

the rush of intense pleasure
feeling happy, energetic and wanting to talk more
intense connection with music
restless sleep
muscle tension (face and jaw)
blurred vision
light-headedness, dizziness
distorted sense of time
enlarged (dilated) pupils, blurred vision
dry mouth, thirst
sweating
memory loss
reduced appetite.5
Higher doses may result in the following adverse effects:

anxiety
paranoia
nose bleeds from snorting the drug
stomach pains, nausea, vomiting
skin rashes
fast or irregular heartbeat
high blood pressure and hot flushes
strong urge to re-dose
chest pain
tremors, convulsions, death.

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New Cathinone
CategoriesCathinone

New Cathinone

New Cathinone

New Cathinone. Cathinone /ˈkæθɪnoʊn/ (also known as benzoylethanamine, or β-keto-amphetamine) is a monoamine alkaloid found in the shrub Catha edulis (khat) and is chemically similar to ephedrine, cathine, methcathinone and other amphetamines. It is probably the main contributor to the stimulant effect of Catha edulis, also known as khat.

Cathinone differs from many other amphetamines in that it has a ketone functional group. Other phenethylamines that share this structure include the stimulants methcathinone, MDPV, mephedrone and the antidepressant bupropion.

Khat is usually supplied as a bundle of leaves and fresh shoots wrapped in banana leaves. It is reported to have a sharp taste and an aromatic odour. Alcoholic extracts (tinctures) of khat have occasionally been reported, especially in ‘herbal high’ sales outlets and at music festivals.

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New Cathinone. Khat (also known as qat or chat) comprises the leaves and fresh shoots of Catha edulis Forsk, a flowering evergreen shrub cultivated in East Africa and the South-West Arabian Peninsula.

Khat leaves are typically wrapped as a bundle in banana leaves. The principal active components in khat are cathinone and cathine (norpseudoephedrine) (see also Drug profile on synthetic cathinones).

Chewing khat releases these substances into the saliva; they are rapidly absorbed and eliminated. Both cathinone and cathine are closely related to amphetamine, and the pharmacological effects of cathinone are qualitatively similar to those of amphetamine, although it is less potent.

Only fresh leaves are chewed because cathinone soon degrades into old or dry plant material. The analysis relies on the characteristic appearance of khat and the presence of cathinone and/or cathine. Khat is not under International control but is scheduled by some Member States. Cathinone and cathine are listed in the 1971 United Nations Convention on Psychotropic Substances under Schedules I and III respectively.

The principal active component in khat is S-cathinone, otherwise known as (-)-2-aminopropiophenone or, more formally, S-(-)-2-amino-1-phenyl-1-propanone. Cathinone is labile and is transformed within a few days of harvesting to a dimer (3,6-dimethyl-2,5-diphenylpyrazine).

It is for this reason that khat needs to be consumed while still fresh. Cathine (1S, 2S-norpseudoephedrine), a further psychoactive substance, arises from the metabolism of cathinone in the mature plant. Apart from common plant products such as tannins, terpenes, flavonoids and sterols, a number of other substances occur in khat including smaller amounts of 1R, 2S-norephedrine and a large number of cathedulins (polyhydroxylated sesquiterpenes).

Both cathinone and cathine are close chemical relatives of the phenethylamines. Thus cathinone is the β-keto analogue of amphetamine. A large number of synthetic cathinone derivatives have been produced, some of which have found use as active pharmaceutical agents.

Structure

Cathinone can be extracted from Catha edulis, or synthesized from α-bromopropiophenone (which is easily made from propiophenone). Because cathinone is both a primary amine and a ketone, it is very likely to dimerize, especially as a free base isolated from plant matter.

New Cathinone. The structure of cathinone is very similar to that of other molecules. By reducing the ketone, it becomes cathine if it retains its stereochemistry, or norephedrine if its stereochemistry is inverted. Cathine is a less potent version of cathinone and cathinone’s spontaneous reduction is the reason that older khat plants are not as stimulating as younger ones.

Cathinone and amphetamine are closely related in that amphetamine is only lacking the ketone C=O group. Cathinone is structurally related to methcathinone, in much the same way as amphetamine is related to methamphetamine. Cathinone differs from amphetamine by possessing a ketone oxygen atom (C=O) on the β (beta) position of the side chain.

The corresponding alcohol, cathine, is a less powerful stimulant. The biophysiological conversion from cathinone to cathine is to blame for the depotentiation of khat leaves over time. Fresh leaves have a greater ratio of cathinone to cathine than dried ones, therefore having more psychoactive effects.

There are many cathinone derivatives that include the addition of an R group to the amino end of the molecule. Some of these derivatives have medical uses as well. Bupropion is one of the most commonly prescribed antidepressants and its structure is Cathinone with a tertiary butyl group attached to the nitrogen and chlorine attached to the benzene ring meta- to the main carbon chain.

Other cathinone derivatives are strong psychoactive drugs. One such drug is methylone, a drug structurally similar to MDMA.

Effects on health
The first documentation of the khat plant being used in medicine was in a book published by an Arabian physician in the 10th century. It was used as an antidepressant because it led to feelings of happiness and excitement. Chronic khat chewing can also create drug dependence, as shown by animal studies. In such studies, monkeys were trained to push a lever to receive the drug reward. As the monkeys’ dependence increased, they pressed the lever at an increasing frequency.

New Cathinone. Khat chewing and the effects of cathinone on the body differ from person to person, but there is a general pattern of behavior that emerges after ingesting fresh cathinone:

Feelings of euphoria that last for one to two hours
Discussion of serious issues and increased irritability
The chewer’s imagination is very active
Depressive stage
Irritability, loss of appetite and insomnia
There are other effects not related to the CNS. The chewer can develop constipation and heartburn after a khat session. Long-term effects of cathinone can include gum disease or oral cancer, cardiovascular disease and depression. The withdrawal symptoms of cathinone include hot flashes, lethargy and a great urge to use the drug for at least the first two days.

Biosynthesis

New Cathinone. The synthesis of cathinone in khat begins with L-phenylalanine and the first step is carried out by L-phenylalanine ammonia lyase (PAL), which cleaves off an ammonia group and creates a carbon-carbon double bond, forming cinnamic acid.[15] After this, the molecule can either go through a beta-oxidative pathway or a non-beta-oxidative pathway.

The beta-oxidative pathway produces benzoyl-CoA while the non-beta-oxidative pathway produces benzoic acid. Both of these molecules can be converted to 1-phenylpropane-1,2-dione by a condensation reaction catalyzed by a ThDP-dependent enzyme (Thiamine diphosphate-dependent enzyme) with pyruvate and producing CO2.[15] 1-phenylpropane-1,2-dione goes through a transaminase reaction to replace a ketone with an ammonia group to form (S)-cathinone. (S)-Cathinone can then undergo a reduction reaction to produce the less potent but structurally similar cathine or norephedrine, which are also found in the plant.[15]

Aside from the beta- and non-beta-oxidative pathways, the biosynthesis of cathinone can proceed through a CoA-dependent pathway. The CoA-dependent pathway is actually a mix between the two main pathways as it starts like the beta-oxidative pathway and then when it loses CoA, it finishes the synthesis in the non-beta-oxidative pathway. In this pathway, the trans-cinnamic acid produced from L-phenylalanine is ligated to Coenzyme A (CoA), just like the beginning of the beta-oxidative pathway. It then undergoes hydration at the double bond.

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This product then loses the CoA to produce benzaldehyde, an intermediate of the non-beta-oxidative pathway. Benzaldehyde is converted into benzoic acid and proceeds through the rest of the synthesis. New Cathinone

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