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18652-93-2

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18652-93-2 Usage

Description

METHOHEXITAL, also known as Brevital Sodium, is a short-acting barbiturate that belongs to the class of sedative-hypnotic drugs. It is used primarily as an anesthetic agent and possesses sedative, hypnotic, and anticonvulsant properties. METHOHEXITAL acts on the central nervous system, depressing its activity and inducing a state of unconsciousness, making it suitable for various medical procedures.

Uses

Used in Anesthesia:
METHOHEXITAL is used as an intravenous anesthetic agent for inducing and maintaining general anesthesia during surgical procedures. Its rapid onset and short duration of action make it an ideal choice for short surgeries and diagnostic procedures.
Used in Electroconvulsive Therapy:
METHOHEXITAL is used as a general anesthetic in electroconvulsive therapy (ECT) to induce a seizure while minimizing the patient's awareness and discomfort. It is often combined with a muscle relaxant to reduce the risk of injury during the procedure.
Brand Name:
Brevital Sodium (King) is the brand name under which METHOHEXITAL is marketed, providing healthcare professionals with a reliable and effective anesthetic option for various medical applications.

Check Digit Verification of cas no

The CAS Registry Mumber 18652-93-2 includes 8 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 5 digits, 1,8,6,5 and 2 respectively; the second part has 2 digits, 9 and 3 respectively.
Calculate Digit Verification of CAS Registry Number 18652-93:
(7*1)+(6*8)+(5*6)+(4*5)+(3*2)+(2*9)+(1*3)=132
132 % 10 = 2
So 18652-93-2 is a valid CAS Registry Number.
InChI:InChI=1/C14H18N2O3/c1-5-7-8-10(3)14(9-6-2)11(17)15-13(19)16(4)12(14)18/h6,10H,2,5,9H2,1,3-4H3,(H,15,17,19)

18652-93-2SDS

SAFETY DATA SHEETS

According to Globally Harmonized System of Classification and Labelling of Chemicals (GHS) - Sixth revised edition

Version: 1.0

Creation Date: Aug 18, 2017

Revision Date: Aug 18, 2017

1.Identification

1.1 GHS Product identifier

Product name METHOHEXITAL

1.2 Other means of identification

Product number -
Other names -

1.3 Recommended use of the chemical and restrictions on use

Identified uses For industry use only.
Uses advised against no data available

1.4 Supplier's details

1.5 Emergency phone number

Emergency phone number -
Service hours Monday to Friday, 9am-5pm (Standard time zone: UTC/GMT +8 hours).

More Details:18652-93-2 SDS

18652-93-2Downstream Products

18652-93-2Related news

Seizures during intracarotid METHOHEXITAL (cas 18652-93-2) and amobarbital testing10/01/2019

BackgroundMethohexital and amobarbital have been used as agents for Wada testing in the presurgical evaluation of patients with epilepsy. Previous experience with methohexital as an anesthetic indicates that methohexital may decrease seizure threshold and may trigger seizures.detailed

Short communicationLanguage assessment in Wada test: Comparison of METHOHEXITAL (cas 18652-93-2) and amobarbital09/27/2019

IntroductionMethohexital has replaced amobarbital during Wada testing at many centers. The objective of our study was to compare the use of methohexital and amobarbital during Wada testing regarding language and memory lateralization quotients as well as speech arrest times.detailed

Comparison of METHOHEXITAL (cas 18652-93-2) and etomidate as anesthetic agents for electroconvulsive therapy in affective and psychotic disorders09/26/2019

BackgroundECT is a well-established treatment for severe depression. The available data on psychosis are limited, but reliable. Its therapeutic potential relies on the induction of a generalized seizure. Besides other narcotics, methohexital and etomidate are used for general anesthesia in ECT. ...detailed

Original ContributionEvaluation of METHOHEXITAL (cas 18652-93-2) as an alternative to propofol in a high volume outpatient pediatric sedation service09/25/2019

BackgroundPropofol is a preferred agent for many pediatric sedation providers because of its rapid onset and short duration of action. It allows for quick turn around times and enhanced throughput. Occasionally, intravenous (IV) methohexital (MHX), an ultra-short acting barbiturate is utilized i...detailed

Case ReportPositive pharmacologic provocative testing with METHOHEXITAL (cas 18652-93-2) during cerebral arteriovenous malformation embolization09/24/2019

A middle-aged patient underwent staged endovascular embolization of a Spetzler-Martin grade V right parietal arteriovenous malformation(AVM).In the fifth endovascular embolization, after methohexital 10 mg injection into a right posterior choroidal artery feeding the AVM nidus, there was an imme...detailed

Clinical studySuperselective METHOHEXITAL (cas 18652-93-2) challenge prior to intracranial endovascular embolization☆09/09/2019

Pharmacologic provocative testing (PT) and intraoperative neurophysiologic monitoring (IONM) both mitigate and predict risks associated with endovascular embolization procedures. We present a series of patients undergoing endovascular intracranial embolization predominantly for AVMs both under g...detailed

18652-93-2Relevant articles and documents

Asymmetric catalysis, 125: Synthesis of the stereoisomers of methohexital by palladium-catalyzed allylation

Brunner, Henri,Deml, Irmgard,Dirnberger, Wolfgang,Ittner, Karl-Peter,Rei?er, Walter,Zimmermann, Markus

, p. 51 - 59 (1999)

Allylation of 1-methyl-5-(1'-methylpent-2'-ynyl)barbituric acid (MBS) with allyl acetate using in situ catalysts of palladium(II) acetylacetonate and chiral phosphane imine ligands resulted in the enantioselective formation of 5-allyl-1-methyl-5-(1'-methylpent-2'-ynyl)barbituric acid (Methohexital), an important anesthetic drug. Both, MBS and Methohexital contain two stereogenic carbon atoms. In MBS, the asymmetric centre in the barbiturate system is labile due to enolization. The asymmetric centre in the hexyne side chain is stable and racemic. The two asymmetric centres of Methohexital are stable and give rise to four stereoisomers, two diastereomeric racemates. An analysis of the isomers of MBS and Methohexital was established on the basis of 1H NMR and, in particular, GC including a base-line separation of the four stereoisomers of Methohexital. The stereoselectivity of the allylation is difficult to control, because the new quaternary asymmetric centre in the barbiturate ring of Methohexital is formed within the nucleophile, attacking the η3-allyl ligand of the catalyst from the side opposite to the palladium atom. Classical optically active ligands, such as diop or norphos, give only 2-6 % ee. Chiral phosphane imine ligands are a successful class of compounds, synthesized by Schiff base condensation of (2-formylphenyl)diphenylphosphane with optically active primary amines. The most efficient ligands have a hydroxymethyl and a bulky alkyl substituent at the asymmetric centre in the imine part, e.g. the L-iso-leucinol and the L-tert-leucinol derivatives 5 and 7. In the Pd-catalyzed allylation of MBS a kinetic resolution and the effect of the enantioselective catalyst interplay, the contributions of which are separated. For MBS the best stereoselectivity factor of the kinetic resolution s = k(R)/k(S) was 2.6 and 83 % 'ee' were achieved. The corresponding values for Methohexital were s = 3.5 and 80 % ee in the α-dl pair. For 10 mixtures of Methohexital stereoisomers the anesthetic doses for rats were determined. With 9.1 mg/kg body weight of the animal the sample obtained from the catalysis with the D-α-phenylglycinol derivative 8 gave a much lower anesthetic dose than the widely used narcotic BrevimytalNatrium, the sodium salt of the α-dl racemate of Methohexital, with 13.0 mg/kg body weight.

Chiral separation of heterocyclic drugs by HPLC: Solute-stationary phase base-pair interactions

Feibush,Figueroa,Charles,et al.

, p. 3310 - 3318 (2007/10/02)

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