110429-35-1

中文名稱鹽酸帕羅西汀

英文名稱 PAROXETINE-D4 HCL

CAS 110429-35-1

分子式 C19H23ClFNO4

分子量 383.84

MOL 文件 110429-35-1.mol

更新日期 2026/04/08 11:03:30

110429-35-1 結構式

基本信息物理化學性質安全數(shù)據(jù) 上下游產(chǎn)品信息圖譜信息鹽酸帕羅西汀價格(試劑級) 常見問題列表

基本信息

中文別名

半水帕羅西汀
D4-鹽酸帕羅西汀
鹽酸帕羅西汀半水合物
鹽酸帕羅西汀半水合物, 選擇性5-羥色胺重吸收抑制劑 (SSRI)
(辦證)鹽酸帕羅西汀PAROXETINE HYDROCHLORIDE HEMIHYDRAT
(-)-(3S,4R)-PAROXETINE HYDROCHLORIDE HEMIHYDRATE
(-)-反式-4R-(4-氟苯基)-3S-{[3',4'-(亞甲二氧基)苯氧基]甲基}-哌啶鹽酸鹽半水合物

英文別名

PAROXETINE-D4 HCL
BRL29060A hemihydrate
PAROXETINE HCL HEMIHYDRATE
Paroxetine-D4 hydrochloride
PAROXETINE-D4 HCL USP/EP/BP
PAROXETINE HYDROCHLORIDE 1/2H2O
paroxetine hydrochloride hydrate
Paroxetine Hydrochloride (350 mg)
PAROXETINE HEMIHYDRATE, EP/BP/USP
BRL29060 hydrochloride hemihydrate

所屬類別

原料藥：抗抑郁、躁狂藥

物理化學性質

熔點121-131 C

儲存條件Inert atmosphere,2-8°C

溶解度Slightly soluble in water, freely soluble in methanol, sparingly soluble in ethanol (96 per cent) and in methylene chloride.

形態(tài)粉末

顏色白色

最大波長(λmax)292nm(H2O)(lit.)

Merck14,7043

InChIInChI=1/C19H20FNO3.ClH.H2O/c20-15-3-1-13(2-4-15)17-7-8-21-10-14(17)11-22-16-5-6-18-19(9-16)24-12-23-18;;/h1-6,9,14,17,21H,7-8,10-12H2;1H;1H2/t14-,17-;;/s3

InChIKeyQRQSGFFISBKLMZ-BGBHMREKNA-N

SMILESC([C@@H]1CNCC[C@H]1C1C=CC(F)=CC=1)OC1C=CC2OCOC=2C=1.Cl.O |&1:1,6,r|

CAS 數(shù)據(jù)庫110429-35-1

安全數(shù)據(jù)

危險性符號(GHS) 有害 (GHS07)

GHS07,GHS09

警示詞警告

危險性描述H302-H317-H319-H411

防范說明P261-P273-P280-P301+P312-P302+P352-P305+P351+P338

危險品標志F,C,Xn

危險類別碼11-34-36/37/38-22

安全說明16-26-36/37/39-45-36

危險品運輸編號UN 3077 9 / PGIII

WGK Germany3

RTECS號TM4569320

危險等級IRRITANT

海關編碼29349990

上下游產(chǎn)品信息

上游原料

下游產(chǎn)品

帕羅西汀

圖譜信息

鹽酸帕羅西汀(110429-35-1)核磁圖(¹HNMR)

鹽酸帕羅西汀價格(試劑級)

報價日期	產(chǎn)品編號	產(chǎn)品名稱	CAS號	包裝	價格
2026/03/03	46263	鹽酸帕羅西汀半水合物 Paroxetine hydrochloride hemihydrate, 98%	110429-35-1	1g	434元
2025/12/22	HY-B0492A	鹽酸帕羅西汀 Paroxetine hydrochloride hemihydrate	110429-35-1	100 mg	600元
2025/12/22	HY-B0492A	鹽酸帕羅西汀 Paroxetine hydrochloride hemihydrate	110429-35-1	10 mM * 1 mLin DMSO	660元

常見問題列表

生物活性

Paroxetine hydrochloride hemihydrate 是一種抗抑郁藥，為高效的五羥色胺再攝取抑制劑，能抑制 GRK2 活性，IC50 值為 14?μM。

靶點

IC50: 14?μM (GRK2)

體外研究

Paroxetine (1?μM and 10?μM) distinctly restrains T cell migration induced by CX3CL1 through inhibiting GRK2. Paroxetine inhibits GRK2 induced activation of ERK. Paroxetine (10 μM) reduces pro-inflammatory cytokines in LPS-stimulated BV2 cells. Paroxetine (0-5 μM) leads to a dose-dependent inhibition on LPS-induced production of TNF-α and IL-1β in BV2 cells. Paroxetine also inhibits lipopolysaccharide (LPS)-induced nitric oxide (NO) production and inducible nitric oxide synthase (iNOS) expression in BV2 cells. Paroxetine (5 μM) blocks LPS-induced JNK activation and attenuates baseline ERK1/2 activity in BV2 cells. Paroxetine relieves microglia-mediated neurotoxicity, and suppresses LPS-stimulated pro-inflammatory cytokines and NO in primary microglial cells.

體內(nèi)研究

Paroxetine treatment obviously attenuates the symptoms of CIA rats. Paroxetine treatment clearly prevents the histological damage of joints and alleviates T cells infiltration into synovial tissue. Paroxetine reveals a strong effect on inhibiting CX3CL1 production in synovial tissues. Paroxetine (20 mg/kg/day) reduces the myocyte cross-sectional area in rat and ROS formation in the remote myocardium. Paroxetine reduces the susceptibility to ventricular tachycardia. Paroxetine treatment following MI decreases LV remodeling and susceptibility to arrhythmias, probably by reducing ROS formation. In CCI paroxetine-treated group, paroxetine (10 mg/kg, i.p.) produces hyperalgesia at days 7 and 10 (P<0.01), but a decrease in pain behavior is seen at day 14. Moreover, paroxetine (10 mg/kg) significantly attenuates tactile hypersensitivity when compared to CCI vehicle-treated group.

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