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5,5-Diphenyl-N-acetylhydantoin is a chemical compound with the molecular formula C16H14N2O2. It is a derivative of hydantoin, featuring two phenyl groups attached to the 5,5-positions of the hydantoin ring and an acetyl group (-COCH3) as a substituent on the nitrogen atom. This white crystalline solid is primarily used as a synthetic intermediate in the preparation of various pharmaceuticals and agrochemicals, particularly in the synthesis of barbiturates and other sedative-hypnotic drugs. The compound is known for its stability and reactivity, which makes it a valuable building block in organic synthesis. It is typically synthesized through the reaction of 5,5-diphenylhydantoin with acetic anhydride, and its properties, such as solubility and melting point, can be influenced by the presence of substituents and the conditions under which it is prepared.

1037-93-0

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1037-93-0 Usage

Check Digit Verification of cas no

The CAS Registry Mumber 1037-93-0 includes 7 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 4 digits, 1,0,3 and 7 respectively; the second part has 2 digits, 9 and 3 respectively.
Calculate Digit Verification of CAS Registry Number 1037-93:
(6*1)+(5*0)+(4*3)+(3*7)+(2*9)+(1*3)=60
60 % 10 = 0
So 1037-93-0 is a valid CAS Registry Number.

1037-93-0Downstream Products

1037-93-0Relevant academic research and scientific papers

Enhancement of the oral bioavailability of phenytoin by N-acetylation and absorptive characteristics

Ogiso, Taro,Tanino, Tadatoshi,Kawaratani, Dai,Iwaki, Masahiro,Tanabe, Genzoh,Muraoka, Osamu

, p. 1084 - 1089 (1998)

To improve the absorbability of phenytoin (DPH), a prodrug, N-acetyl- DPH (EDPH), was synthesized, and the absorptive characteristics and pharmacokinetics of the prodrug were evaluated in rats. EDPH was rapidly hydrolyzed to DPH in the intestinal fluid and the mucosa (rate constant, 0.055 and 0.169 min-1, respectively). The plasma concentrations of DPH after intravenous dosing of EDPH declined in a biexponential manner, although two different elimination patterns were observed in these rats. When dosed orally (25 mg/kg, DPH equivalent), the plasma levels of DPH converted from the prodrug were significantly higher and more sustained than those after DPH alone, giving bioavailability 11.4 (rapid decay) and 9.1 times (slow decay) as high, respectively, as that after DPH alone. The concentrations of DPH distributed into the mucosa of the duodenum and jejunum 1 and 5 h after oral dosing of EDPH were significantly higher than those after DPH alone. The prodrug and DPH converted from the prodrug dissolved 2-4 fold more than DPH alone in bile salt solution and bile salt-oleic acid mixed micelles, indicating the increased solubility of the prodrug in the intestinal fluid. It is concluded from the data that such high solubility of EDPH enhanced the intestinal absorption of the prodrug, part of which would be absorbed in the amide form, and thus gave the high bioavailability.

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