desomorphine has been researched along with Necrosis* in 6 studies
1 review(s) available for desomorphine and Necrosis
Article | Year |
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The harmful chemistry behind krokodil (desomorphine) synthesis and mechanisms of toxicity.
"Krokodil" is the street name for the homemade injectable mixture that has been used as a cheap substitute for heroin. Its use begun in Russia and Ukraine and nowadays is being spread over several other countries. Desomorphine is the semi-synthetic opioid claimed to be the main component of krokodil and considered to be responsible for its psychoactive characteristics. The starting materials for desomorphine synthesis are codeine tablets, alkali solutions, organic solvent, acidified water, iodine and red phosphorus, all of which are easily available in retail outlets, such as supermarkets, drugstores, etc. The resulting product is a light brown liquid that is called krokodil. People who inject krokodil present a great variety of serious signs and symptoms, including thrombophlebitis, ulcerations, gangrene, and necrosis, quickly evolving to limb amputation and death. These effects are thought to result from the toxic components produced as byproducts during the homemade drug synthesis. In this work, we reviewed several aspects of krokodil use, including its epidemiology, pharmacology and the chemical properties of the main active ingredient (desomorphine). To enhance our understanding of the clinical and toxic effects and to support the implementation of harm reduction measures, we also describe the "bathtub chemistry" of krokodil and the content of the final solution. Topics: Amputation, Traumatic; Codeine; Gangrene; Humans; Illicit Drugs; Molecular Structure; Necrosis; Neurotoxicity Syndromes; Osteonecrosis; Skin; Substance Abuse, Intravenous | 2015 |
5 other study(ies) available for desomorphine and Necrosis
Article | Year |
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The authors reply to: "Doubts about first report of krokodil use in Canada".
Topics: Adult; Canada; Codeine; Humans; Leg Ulcer; Male; Necrosis | 2020 |
Doubts about first report of krokodil use in Canada.
Topics: Adult; Canada; Codeine; Humans; Leg Ulcer; Male; Necrosis | 2019 |
"Krokodil" drug - Related osteonecrosis of midface: A case series.
Krokodil is a cheap and effective home-made substitute for heroin. It is widely used over the territory of the former USSR (Russia, Ukraine, Armenia and others). Krokodil drug-related midface ON often occurs as a complication of maxillary ON. Treatment of Krokodil drug-related ON of the midface is challenging. It is difficult to determine the ON zone preoperatively and intraoperatively, due to the complex anatomy of the midface and the different periods of the disease onset in different areas. The aim of this study is to show variations of the clinical course and treatment options of Krokodil drug-related ON of the midface. In this study, 3 cases of Krokodil drug-related midface ON are reported. The main clinical feature of midface ON is extraoral fistula in the midfacial zone with purulent discharge or extraoral exposure of zygomatic bone. Surgery is the main treatment method for Krokodil drug-related midface osteonecrosis. Surgery includes necrotic bone removal and defect closure. Usually an extraoral approach is used to expose necrotic bone. Intraoral maxillary sinus floor defect is closed with the use of a buccal fat pad to prevent formation of oroantral communication. Drug withdrawal, radical necrectomy, and proper closure of formed defects are the main factors that lead to successful treatment of Krokodil drug-related midface ON patients. Topics: Adult; Codeine; Humans; Illicit Drugs; Male; Maxilla; Middle Aged; Necrosis; Osteonecrosis; Sinus Floor Augmentation; Substance Abuse, Intravenous; Treatment Outcome | 2019 |
Necrotic leg ulcers associated with krokodil injection in a 41-year-old man.
Topics: Adult; Analgesics, Opioid; Codeine; Humans; Injections, Subcutaneous; Leg Ulcer; Male; Necrosis | 2019 |
Repeated subcutaneous administrations of krokodil causes skin necrosis and internal organs toxicity in Wistar rats: putative human implications.
"Krokodil" is the street name for an impure homemade drug mixture used as a cheap substitute for heroin, containing desomorphine as the main opioid. Abscesses, gangrene, thrombophlebitis, limb ulceration and amputations, jaw osteonecrosis, skin discoloration, ulcers, skin infections, and bleeding are some of the typical reported signs in humans. This study aimed to understand the toxicity of krokodil using Wistar male rats as experimental model.. Animals were divided into seven groups and exposed subcutaneously to NaCl 0.9% (control), krokodil mixture free of psychotropic substances (blank krokodil), pharmaceutical grade desomorphine 1 mg/kg, and four different concentrations of krokodil (containing 0.125, 0.25, 0.5, and 1 mg/kg of desomorphine) synthesized accordingly to a "domestic" protocol followed by people who inject krokodil (PWIK). Daily injections for five consecutive days were performed, and animals were sacrificed 24 hr after the last administration. Biochemical and histological analysis were carried out.. It was shown that the continuous use of krokodil may cause injury at the injection area, with formation of necrotic zones. The biochemical results evidenced alterations on cardiac and renal biomarkers of toxicity, namely, creatine kinase, creatine kinase-MB, and uric acid. Significant alteration in levels of reduced and oxidized glutathione on kidney and heart suggested that oxidative stress may be involved in krokodil-mediated toxicity. Cardiac congestion was the most relevant finding of continuous krokodil administration.. These findings contribute notably to comprehension of the local and systemic toxicological impact of this complex drug mixture on major organs and will hopefully be useful for the development of appropriate treatment strategies towards the human toxicological effects of krokodil. Topics: Analgesics, Opioid; Animals; Codeine; Heart; Humans; Illicit Drugs; Injections, Subcutaneous; Kidney; Liver; Lung; Male; Necrosis; Organ Size; Oxidative Stress; Rats; Rats, Wistar; Skin Diseases; Tissue Distribution | 2017 |