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thiethylperazine

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thiethylperazine Basic information

Product Name:
thiethylperazine
Synonyms:
  • Tietylperazine
  • Ethylthioperazine.
  • 2-ethylsulfanyl-10-[3-(4-methylpiperazin-1-yl)propyl]phenothiazine
  • 2-ethylthio-10-(3-(4-methylpiperazin-1-yl)propyl)phenothiazine
  • thiethylperazine
  • 2-(Ethylthio)-10-[3-(4-methyl-1-piperazinyl)propyl]-10H-phenothiazine
  • Torecane
  • 10H-Phenothiazine, 2-(ethylthio)-10-[3-(4-methyl-1-piperazinyl)propyl]-
CAS:
1420-55-9
MF:
C22H29N3S2
MW:
399.62
EINECS:
215-819-0
Mol File:
1420-55-9.mol
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thiethylperazine Chemical Properties

Melting point:
62-64°
Boiling point:
bp0.01 227°
Density 
1.1684 (rough estimate)
refractive index 
1.5605 (estimate)
storage temp. 
4°C, protect from light
solubility 
DMSO : 100 mg/mL (250.24 mM; Need ultrasonic)
pka
7.66±0.10(Predicted)
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Safety Information

Hazardous Substances Data
1420-55-9(Hazardous Substances Data)
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thiethylperazine Usage And Synthesis

Originator

Torecan,Boehringer Ingelheim,US,1961

Uses

Thiethylperazine acts both as a peripheral and as a central antiemetic.

Definition

ChEBI: A member of the class of phenothiazines that is perazine substituted by a ethylsulfanyl group at position 2.

Manufacturing Process

26.1 parts of 3-ethylmercapto-phenothiazine (melting point 95°C to 97°C), 4.7 parts of finely pulverized sodium amide and 120 parts by volume of absolute xylene are heated to boiling for two hours, under reflux and while stirring the reaction mixture, at an oil-bath temperature of 180°C. Without interrupting the heating, a solution of 20.0 parts of 1-methyl-4-(3'- chloropropyl-1')-piperazine (boiling point 95°C to 97°C at a pressure of 10 mm Hg) in 20 parts by volume of xylene is added dropwise in the course of 1 1/2 hours. After heating 3 more hours, the reaction mixture is cooled and 10.0 parts of ammonium chloride added; the mixture is then shaken out three times, using 50 parts by volume of water each time. The xylene solution is extracted with 250 parts by volume of aqueous tartaric acid of 15% strength, after which the tartaric acid extract is washed with 80 parts by volume of benzene and then rendered phenolphthalein-alkaline by the addition of 60 parts by volume of concentrated aqueous caustic soda solution. The base which precipitates is taken up in a total of 150 parts by volume of benzene; the benzene layer is dried over potassium carbonate and is then evaporated under reduced pressure. The residue from the evaporation is distilled in a high vacuum. After separating a preliminary distillate which passes over up to 226°C under a pressure of 0.01 mm Hg the main fraction - 3-ethylmercapto- 10-[3'-(1''-methyl-piperazyl-4'')-propyl-1']-phenothiazine - which distills at 226°C to 228°C under the last-mentioned pressure is collected. The analytically pure base boils at 227°C under a pressure of 0.01 mm Hg and melts at 62°C to 64°C.
Upon the addition of ethanolic HCl to a solution, cooled to 0°C, of 26.38 parts of the free base in 130 parts by volume of absolute ethanol, until a Congoacid reaction is achieved, the crystalline dihydrochloride of 3-ethylmercapto- 10-[3'-(1''-methyl-piperazyl-4'')-propyl-1']phenothiazine is precipitated. The analytically pure salt has a melting point of 214°C to 216°C (bubbles); it begins to sinter at 205°C. The dimaleate melts at 188°C to 190°C after sintering from 180°C (recrystallized from methanol).

Therapeutic Function

Antiemetic

Trade name

Torecan (Boehringer Ingelheim)

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