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ChemicalBook--->CAS DataBase List--->12244-57-4

12244-57-4

12244-57-4 Structure

12244-57-4 Structure
IdentificationBack Directory
[Name]

Sodium aurothiomalate
[CAS]

12244-57-4
[Synonyms]

autm
kidon
D00992
tauredon
myocrisin
miochrysin
Miocrisina
Myocrisine
myochrysine
chrysothios
taure(o)don
GOLDTHIOMALATE
Myochrysine (tn)
sodiumaurithiomalate
SODIUM AUROTHIOMALATE
aurothiomaleatesodium
disodiumaurothiomalate
Gold sodium thiomaleate
SODIUM AUROTHIOMALATE(I)
Gold sodium thiomalate (usp)
Sodium aurothiomalate (jp15)
disodium 2-(auriothio)succinate
mercapto-succinicacigoldsodiumsalt
(mercaptobutanedioato(1-))golddisodiumsalt
((1,2-dicarboxyethyl)thio)-goldisodiumsalt
Sodiumaurothiomalate(I),99.9%(metalsbasis)
((1,2-dicarboxyethyl)thio)golddisodiumsalt
(dihydrogenmercaptosuccinato)golddisodiumsalt
mercapto-butanedioicacimonogold(1+)sodiumsalt
(1,2-dicarboxyethylthio)gold disodium salt hydrate
Butanedioic acid, mercapto-, monogold(1+) sodium salt
(1,2-Dicarboxyethylthio)gold hydrate disodium salt, Gold sodium thiomalate hydrate
NSCLC,inhibit,NF-kB,PKC,A427,Aurothiomalate,Erk,SCLC,Inhibitor,H460,H1703,Aurothiomalate sodium,thioredoxin,Mek,A549,H1437,reductase,anti-rheumatoid,H510,LAC,H187,TrxR,Protein kinase C,LACs,H2170,TNFa
[EINECS(EC#)]

235-479-7
[Molecular Formula]

C4H3AuNa2O4S
[MDL Number]

MFCD00064304
[MOL File]

12244-57-4.mol
[Molecular Weight]

390.08
Chemical PropertiesBack Directory
[Definition]

White to yellowish-white powder; odorless; metallic taste. Affected by light. Very soluble in water; practically insoluble in alcohol and ether; aqueous solutions are colorless to pale yellow; pH (5% solution) 5.8–6.5.
[storage temp. ]

4°C, away from moisture
[form ]

Solid
[color ]

Off-white to light yellow
[Water Solubility ]

Very soluble in water. Practically insoluble in alcohol, ether
[Merck ]

14,4518
Hazard InformationBack Directory
[Uses]

Medicine (antirheumatic).
[Brand name]

Myochrysine (Merck).
[Physical properties]

White to yellowish white powder; odorless; metallic taste; highly soluble in water; practically insoluble in ethanol and ether.
[Production Methods]

Gold(I) thiomalate is prepared by reacting sodium thiomalate with gold(I) halide. It is stored in the dark and otherwise protected from light.
[Pharmaceutical Applications]

Sodium aurothiomalate is a commonly used gold-based DMARD and is indicated for active progressive RA. It is administered by deep intramuscular injection. Administration is started with a test dose of 10mg followed by weekly intervals of 50 mg doses. An improvement is expected to be seen once 300–500 mg is administered. Treatment should be discontinued if there is no improvement after administering 1 g or 2months. Intervals of administration should be gradually increased to 4weeks in patients in whom an effect can be seen. If any blood disorders or other side effects such as GI bleedings or proteinuria are observed, sodium aurothiomalate should be discontinued.
[Clinical Use]

Active progressive rheumatoid arthritis in adults
[Synthesis]

Synthesis: a solution of thiomalic acid and 3 equivalents of sodium hydroxide are mixed with an aqueous suspension of gold(I) iodide. The product, a mixture of the mono- and disodium salts, is precipitated by the addition of ethanol.
Sodium aurothiomalate synthesis
[Drug interactions]

Potentially hazardous interactions with other drugs
ACE-inhibitors: flushing and hypotension reported in combination.
Penicillamine: increased risk of toxicity - avoid.
[Metabolism]

Mainly excreted in the urine with smaller amounts in the faeces.
Safety DataBack Directory
[Hazard Codes ]

Xn
[Risk Statements ]

20/21/22-43
[Safety Statements ]

36
[WGK Germany ]

3
[RTECS ]

MD5435000
[Safety Profile]

Poison by subcutaneous and intramuscular routes. Moderately toxic bj intravenous ' route. Human systemic effects: aggression, agranulocytosis, aplastic anemia, cell count changes, changes in circulation, cholestatic jaunhce, dermatitis, encephalitis, fasciculations, flaccid paralysis without anesthesia, hemorrhage, hepatitis (hepatocellular necrosis), increased body temperature, interstitial fibrosis, muscle weakness, proteinuria, recording from peripheral motor nerve, depressed renal function tests, somnolence, structural changes in nerve sheath, thrombocytopenia, uncharacterized allergc reaction, changes in blood, teeth, and supporting structures. Experimental teratogenic and reproductive effects. When heated to decomposition it emits very toxic Na2O and SOx.
[Hazardous Substances Data]

12244-57-4(Hazardous Substances Data)
Spectrum DetailBack Directory
[Spectrum Detail]

Sodium aurothiomalate(12244-57-4)1HNMR
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