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ChemicalBook >> CAS DataBase List >>Ripasudil hydrochloride dihydrate

Ripasudil hydrochloride dihydrate

CAS No.
887375-67-9
Chemical Name:
Ripasudil hydrochloride dihydrate
Synonyms
RIPASUDIL HYDROCHLORIDE HYDRATE;K-115 HCL;K 115; K115;K115 HCL 2H2O;K-115 (HCl H2O);Ripasudil (K-115);K115 HCl Dihydrate;Ripasudil free base;K 155 HCl dihydrate;RipasudilHCl Hydrate
CBNumber:
CB52667596
Molecular Formula:
C15H21ClFN3O3S
Molecular Weight:
377.86
MDL Number:
MFCD26960897
MOL File:
887375-67-9.mol
MSDS File:
SDS
TDS File:
TDS
Last updated:2026-04-24 14:58:19
Product description Number Pack Size Price
Ripasudil (hydrochloride hydrate) ≥98% 19920 1mg $44
Ripasudil (hydrochloride hydrate) ≥98% 19920 5mg $164
Ripasudil (hydrochloride hydrate) ≥98% 19920 10mg $263
Ripasudil (hydrochloride hydrate) ≥98% 19920 25mg $493
Ripasudil HCl hydrate FR162274 25mg $220
More product size

Ripasudil hydrochloride dihydrate Properties

storage temp. Store at -20°C
solubility insoluble in EtOH; ≥123.2 mg/mL in DMSO; ≥41.7 mg/mL in H2O
form solid
color White to off-white
Stability Hygroscopic
FDA UNII 016TTR32QF

SAFETY

Risk and Safety Statements

Risk Statements  24/25-26-28
Safety Statements  28-38-41-48
HS Code  29339900

Ripasudil hydrochloride dihydrate price More Price(85)

Manufacturer Product number Product description CAS number Packaging Price Updated Buy
Cayman Chemical 19920 Ripasudil (hydrochloride hydrate) ≥98% 887375-67-9 1mg $44 2026-04-30 Buy
Cayman Chemical 19920 Ripasudil (hydrochloride hydrate) ≥98% 887375-67-9 5mg $164 2026-04-30 Buy
Cayman Chemical 19920 Ripasudil (hydrochloride hydrate) ≥98% 887375-67-9 10mg $263 2026-04-30 Buy
Cayman Chemical 19920 Ripasudil (hydrochloride hydrate) ≥98% 887375-67-9 25mg $493 2026-04-30 Buy
Biosynth FR162274 Ripasudil HCl hydrate 887375-67-9 25mg $220 2026-06-04 Buy
Product number Packaging Price Buy
19920 1mg $44 Buy
19920 5mg $164 Buy
19920 10mg $263 Buy
19920 25mg $493 Buy
FR162274 25mg $220 Buy

Ripasudil hydrochloride dihydrate Chemical Properties,Uses,Production

Description

Ripasudil hydrochloride hydrate (Glanatec®) was approved in Japan in 2014 for the treatment of glaucoma and ocular hypertension. Originally discovered by D. Western Therapeutics Institute, Inc. and licensed by the Kowa Company, Ltd, ripasudil functions as a selective Rho-kinase inhibitor and reduces intraocular pressure by stimulation of aqueous humour drainage of the trabecular meshwork. While this recent approval allows for use of ripasudil as a twice-daily monotherapy treatment when other drugs cannot be used or are not effective, clinical trials using ripasudil as a combination therapy with other glaucoma drugs have shown promising results in the treatment of primary open-angle glaucoma or ocular hypertension. Currently, the Kowa Company is also pursuing trials focused on the use of ripasudil for the treatment of diabetic retinopathy and diabetic macular edema.

Uses

Ripasudil (Glanatec TM, Kowa Pharmaceutical), a close derivative of fasudil, is another Rho kinase inhibitor approved in Japan at the end of 2014 for the treatment of glaucoma and ocular hypertensionwhen other therapeutic agents are not effective or cannot be administered. Additionally, ripasudil has been tested in diabetic retinopathy clinical trials and shown to promote corneal endothelial cell proliferation, endothelium regeneration, and wound healing.

Uses

Ripasudil Hydrochloride Dihydrate is a derivative of fasudil and a rho kinase inhibitor (1,2). It is used for the treatment of glaucoma and ocular hypertension.

Synthesis

While initial synthetic routes to ripasudil were carried out via a stepwise functionalization of 4-fluoroisoquinoline-5-sulfonyl chloride (238), more recent reports describe an efficient route to ripasudil employing a late stage-coupling of Boc-diazepane (237) with 4-fluoroisoquinoline-5-sulfonyl chloride (238), enabling synthesis on multi-kilogram scale and isolation of the drug in high purity. This optimized route to ripasudil begins with 2-nitrobenzene sulfonyl chloride (NsCl)- mediated protection of (S)-2-amino-1-propanol (234) in 82% yield. In this case, use of the NaHCO3/THF/H2O conditions were essential for preventing bis-nosylation.228 Alcohol activation with methanesulfonyl chloride (MsCl) in N-methyl morpholine (NMM) took place smoothly to give the corresponding mesylate 235 in 91% yield. Direct mesylate displacement with 3-aminopropanol and subsequent amine protection as the carbamate ((Boc)2O) in a one-pot fashion provided the corresponding Boc-amino propanol product 236 in 95% yield over 2 steps. With the acyclic diazepane precursor 236 in hand, employment of the intramolecular Fukuyama-Mitsunobu N-alkyl cyclization conditions (diisopropyl azodicarboxylate (DIAD)/PPh3) allowed generation of the diazepane in 75% yield. Nosyl group cleavage with thiophenol/K2CO3 provided the Boc-diazepane 237 in 65% overall yield and 98% purity following a pH-controlled aqueous workup. Finally, 4-fluoroisoquinoline- 5-sulfonyl chloride (238)aprepared via subjection of 4- fluoroisoquinoline (239) to sulfur trioxide and sulfuric acid followed by treatment with thionyl chloride and finally 4 N HCl in ethyl acetateawas involved in a 1-pot, two-step procedure in which this sulfonyl chloride was coupled with diazepane 237 (TEA/MeCN) to access the ripasudil framework in quantitative yield. Synthesis of the final drug target by deprotection with 4 M HCl in ethyl acetate followed by neutralization with aqueous sodium hydroxide provided the free base of ripasudil in 93% yield and 99.8% purity. Conversion to the more stable hydrochloride dihydrate form could be performed by treatment of the free base with 1 M HCl/EtOH and subsequent heating of the hydrochloride in H2O/acetone to provide ripasudil hydrochloride dihydrate XXIX in 83% yield.

Synthesis_887375-67-9

in vivo

in optic nerve crush (nc) c57bl/6 mice model, oral administration of k-115 (1 mg/kg/d) increased 34 ± 3% survival of rgcs after nc [2].

IC 50

ROCK2: 19 nM (IC50); ROCK1: 51 nM (IC50); CaMKIIa: 370 nM (IC50); PKACa: 2.1 μM (IC50); PKC: 27 μM (IC50)

References

shimokawa h, takeshita a. rho-kinase is an important therapeutic target in cardiovascular medicine[j]. arteriosclerosis, thrombosis, and vascular biology, 2005, 25(9): 1767-1775.yamamoto k, maruyama k, himori n, et al. the novel rho kinase (rock) inhibitor k-115: a new candidate drug for neuroprotective treatment in glaucomanovel rho kinase inhibitor[j]. investigative ophthalmology & visual science, 2014, 55(11): 7126-7136.tanihara h, inoue t, yamamoto t, et al. phase 1

Ripasudil hydrochloride dihydrate Preparation Products And Raw materials

Raw materials

Preparation Products

Global( 111)Suppliers
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Henan Tianfu Chemical Co.,Ltd.
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InvivoChem
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HANGZHOU LEAP CHEM CO., LTD.
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Ripasudil hydrochloride dihydrate Spectrum

K-115 HCL Ripasudil free base RipasudilHCl Hydrate K115 HCl Dihydrate (2S)-1-[(4-Fluoro-5-isoquinolinyl)sulfonyl]hexahydro-2-methyl-1H-1,4-diazepine monohydrochloride dihydrate K-115 (HCl H2O) Ripasudil HCl Dihydrate K115 HCL 2H2O Ripasudil Hydrochloride Dihydrate Ripasudil (K-115) K-115 Hydrochloride Dihydrate Ripasudil (K-115), 98%, a highly selective and potent Rho-kinase inhibitor Ripasudil(K-115)hydrochloridedihydrate Ripasudil (K115) dihydrate K 115; K115 Ripasudil dihydrate (K15) Ripasudil Monohydrochloride Dihydrate Ripasudil hydrochloride dihydrate( K115 ) 4-Fluoro-5-[(2S)-2-methyl-1,4-diazepane-1-sulfonyl]isoquinoline dihydrate hydrochloride Ripasudil (K-115) HCl dihydrate K 155 HCl dihydrate K-115|||Ripasudil hydrochloride dihydrate Ripasudil, 10 mM in DMSO RIPASUDIL HYDROCHLORIDE HYDRATE 887375-67-9 C15H23ClFN3O4S C15H18FN3O2SHCl2H2O C15H18FN3O2SClH2H2O
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