ダリフェナシン

￥260800 - ￥579600
化学名: ダリフェナシン
英語名: Darifenacin
別名:ダリフェナシン;2-[(3S)-1-[2-(2,3-ジヒドロ-1-ベンゾフラン-5-イル)エチル]ピロリジン-3-イル]-2,2-ジフェニルアセトアミド;ジフェニル[(3S)-1-[2-(2,3-ジヒドロベンゾフラン-5-イル)エチル]ピロリジン-3-イル]アセトアミド;(3S)-1-[2-[(2,3-ジヒドロベンゾフラン)-5-イル]エチル]-α,α-ジフェニル-3-ピロリジンアセトアミド
CAS番号: 133099-04-4
分子式: C28H30N2O2
分子量: 426.55
EINECS:
MDL Number:MFCD00896313

価格2 プロパティ安全情報説明

2物価

選択条件：

ブランド

富士フイルム和光純薬株式会社(wako)

パッケージ

250mg
1g

生産者富士フイルム和光純薬株式会社(wako)
製品番号W01MAS093128
製品説明
英語製品説明2-(1-(2-(2,3-Dihydrobenzofuran-5-yl)ethyl)-pyrrolidin-3-yl)-2,2-diphenylacetamide
包装単位250mg
価格￥260800
更新しました2024-03-01
購入

生産者富士フイルム和光純薬株式会社(wako)
製品番号W01MAS093128
製品説明
英語製品説明2-(1-(2-(2,3-Dihydrobenzofuran-5-yl)ethyl)-pyrrolidin-3-yl)-2,2-diphenylacetamide
包装単位1g
価格￥579600
更新しました2024-03-01
購入

生産者	製品番号	製品説明	包装単位	価格	更新時間	購入
富士フイルム和光純薬株式会社(wako)	W01MAS093128	2-(1-(2-(2,3-Dihydrobenzofuran-5-yl)ethyl)-pyrrolidin-3-yl)-2,2-diphenylacetamide	250mg	￥260800	2024-03-01	購入
富士フイルム和光純薬株式会社(wako)	W01MAS093128	2-(1-(2-(2,3-Dihydrobenzofuran-5-yl)ethyl)-pyrrolidin-3-yl)-2,2-diphenylacetamide	1g	￥579600	2024-03-01	購入

プロパティ

比旋光度 :25D -20.6° (c = 1.0 in methylene chloride)
沸点 :614.3±55.0 °C(Predicted)
比重(密度) :1.192±0.06 g/cm3(Predicted)
貯蔵温度 :2-8°C
溶解性 :Soluble in DMSO
外見 :Powder
酸解離定数(Pka) :pKa (25°): 9.2

安全情報

絵表示(GHS):

注意喚起語:

危険有害性情報:

コード	危険有害性情報	危険有害性クラス	区分	注意喚起語	シンボル	P コード

注意書き:

説明

Darifenacin is a novel muscarinic M3 selective antagonist for the once-daily oral treatment of urinary incontinence and overactive bladder. The majority of overactive bladder symptoms are thought to result from the overactivity of the detrusor muscle, which is primarily mediated by acetylcholine-induced stimulation of muscarinic M3 receptors in the bladder. Consequently, antimuscarinic agents have become the mainstay of overactive bladder treatment. Darifenacin has a higher level of M3 selectivity than the previously marketed antimuscarinic agents. It has K_i values of 16nM for M1, 50 nM for M2, and 1.6 nM for M3 receptors. It is slightly more M3 selective than solifenacin (M1:K_i=25 nM, M2:K_i=126 nM, M3:K_i=10 nM), which was launched in 2004. Darifenacin is significantly more selective than other muscarinics such as tolterodine, oxybutynin, and trospium, which are all essentially equipotent against M1, M2, and M3 receptors. In addition,darifenacin demonstrates greater effect on tissues in which the predominant receptor type is M3 rather than M1 or M2. In vitro darifenacin inhibits carbacholinduced contractions with greater potency in isolated guinea-pig bladder (M3) than in guinea-pig atria (M2) or dog saphenous vein (M1). In animal models, it shows greater selectivity for inhibition of detrusor contraction over salivation or tachycardia.Darifenacin is supplied as a controlled release formulation, and the recommended dosage is 7.5 mg once, daily. Darifenacin is rapidly and completely absorbed from the GI tract after oral administration, with maximum plasma levels achieved after about 7 h. The elimination half-life is approximately 3 h, but because of the controlled release characteristics of the formulation, the drug is suitable for once-daily dosing. Steady-state plasma levels are achieved within 6 days of commencing treatment. Darifenacin exhibits high-protein binding (98%), a volume of distribution of 163 L, and a clearance of 40 L/h. It has low oral bioavailability (15–19%) due to extensive first-pass metabolism by CYP3A4 and CYP2D6, but this can be saturated after multiple administrations. The major circulating metabolites are produced by monohydroxylation and N-dealkylation; however, none contribute significantly to the overall clinical effect of darifenacin. Approximately 58% of the dose is excreted in urine and 44% in feces; only a small percentage (3%) of the excreted dose is unchanged darifenacin.

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