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5189-11-7

中文名稱(chēng) 苯噻啶蘋(píng)果酸鹽
英文名稱(chēng) Pizotifen Malate
CAS 5189-11-7
分子式 C23H27NO5S
分子量 429.53
MOL 文件 5189-11-7.mol
更新日期 2025/09/08 15:22:11
5189-11-7 結(jié)構(gòu)式 5189-11-7 結(jié)構(gòu)式

基本信息

中文別名
蘋(píng)果酸苯噻
苯噻啶蘋(píng)果酸鹽
苯噻啶蘋(píng)果酸酯
雙氯芬酸蘋(píng)果酸鹽
PIZOTIFEN蘋(píng)果酸
苯噻啶蘋(píng)果酸鹽(偏頭痛)
9,10-二氫-4-(1-甲基哌啶-4-亞基)-4H-苯并[4,5]環(huán)庚烷并[1,2-b]噻吩蘋(píng)果酸鹽 (1:1)
英文別名
mosegor
sanomtgran
bc105malate
litecmalate
malate(1:1)
Pizotifen Mala
Einecs 225-970-4
PIZOTIFEN MALATE
sandomygranmalate
PIZOTYLINE MALATE
所屬類(lèi)別
生物化工:5-HT Receptor 拮抗劑

物理化學(xué)性質(zhì)

熔點(diǎn)185-186° (dec)
儲(chǔ)存條件Keep in dark place,Inert atmosphere,2-8°C
溶解度酸水溶液(微溶,加熱)、DMSO(微溶)、甲醇(微溶)
形態(tài)固體
顏色白色至灰白色
穩(wěn)定性吸濕性
主要應(yīng)用pharmaceutical
pharmaceutical small molecule
InChI1S/C19H21NS.C4H6O5/c1-20-11-8-15(9-12-20)19-16-5-3-2-4-14(16)6-7-18-17(19)10-13-21-18;5-2(4(8)9)1-3(6)7/h2-5,10,13H,6-9,11-12H2,1H3;2,5H,1H2,(H,6,7)(H,8,9)
InChIKeyIWAWCPZVTXCFKD-UHFFFAOYSA-N
SMILES[s]1c2c(cc1)C(=C4CCN(CC4)C)c3c(cccc3)CC2.OC(CC(=O)O)C(=O)O

安全數(shù)據(jù)

危險(xiǎn)性符號(hào)(GHS)有害 (GHS07)
GHS07
警示詞警告
危險(xiǎn)性描述H302-H315-H319-H335
防范說(shuō)明P261-P305+P351+P338
危險(xiǎn)品標(biāo)志Xi
危險(xiǎn)類(lèi)別碼36/37/38
安全說(shuō)明26-37/39
WGK GermanyWGK 3
存儲(chǔ)類(lèi)別11 - Combustible Solids

應(yīng)用領(lǐng)域

用途1
本品為抗組胺類(lèi)藥,用于治療偏頭痛
苯噻啶蘋(píng)果酸鹽價(jià)格(試劑級(jí))
報(bào)價(jià)日期產(chǎn)品編號(hào)產(chǎn)品名稱(chēng)CAS號(hào)包裝價(jià)格
2026/03/03S1394苯噻啶蘋(píng)果酸鹽
Pizotifen Malate
5189-11-750mg804.86元
2025/12/22HY-B0115A苯噻啶蘋(píng)果酸鹽
Pizotifen malate
5189-11-7100 mg200元

常見(jiàn)問(wèn)題列表

生物活性
Pizotifen Malate (BC-105)用于治療經(jīng)常性偏頭痛。
靶點(diǎn)

5-HT 2A Receptor

5-HT 1C Receptor

體外研究

Pizotifen malate (BC-105 malate) is a potent 5-HT 2 receptor antagonist, with a high affinity for 5-HT 1C binding site. Pizotifen is an antidepresent 5-HT 2A receptor antagonist and has the capacity to inhibit serotonin-enhanced ADP-induced platelet aggregation.

體內(nèi)研究

The weights of the fetuses are significantly reduced by all administered doses of Pipethiadene and Pizotifen malate (BC-105 malate) ; the weights of the placentas are significantly reduced after 0.6 and 1.2 mg/kg Pipethiadene and only after the middle dose of Pizotifen malate. The means of the implantations, live, dead fetuses, resorptions and the occurrence of external, skeletal and visceral anomalies do not differ from the control group. The number of chromosome aberrations in the bone marrow cells of treated mice does not differ significantly from the negative control group. The micronucleus test reveals no elevation in the frequency of micronuclei as compared to the control group. After the two higher doses of both Pipethiadene and Pizotifen maleate, the mitotic indices are lower than in the control group.

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