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- Business type: Lab/Research institutions
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Rivaroxaban CAS NO.366789-02-8
- Min.Order Quantity:
- 0 Metric Ton
- Purity:
- 98%min
- Port:
- Qingdao,China
- Payment Terms:
- L/C,T/T,MoneyGram
Product Details
Keywords
- 366789-02-8
- Rivaroxaban seller in China
- Rivaroxaban factory in China
Quick Details
- ProName: Rivaroxaban
- CasNo: 366789-02-8
- Molecular Formula: C19H18ClN3O5S
- Appearance: white or yellowish white flaky crystal
- Application: Used for research and industrial manuf...
- DeliveryTime: Within7-10 days after receipt of your ...
- PackAge: As customer request
- Port: Qingdao,China
- ProductionCapacity: 100 Metric Ton/Day
- Purity: 98%min
- Storage: Keep the sun from direct sunlight ;pre...
- Transportation: By Sea/Air/Courier
- LimitNum: 0 Metric Ton
Superiority
Details
| rivaroxaban basic information |
| antithrombotic drugs |
| product name: | rivaroxaban |
| synonyms: | 5-chloro-n-[[(5s)-2-oxo-3-[4-(3-oxo-4-morpholinyl)phenyl]-5-oxazolidinyl]methyl]-2-thiophenecarboxamide;bay 59-7939;rivaroxaban;5-chloro-n-(((5s)-2-oxo-3-(4-(3-oxomorpholin-4-yl)phenyl)-1,3-oxazolidin-5-yl)methyl)thiophene-2-carboxamide;2-thiophenecarboxamide, 5-chloro-n-[[(5s)-2-oxo-3-[4-(3-oxo-4-morpholinyl)phenyl]-5-oxazolidinyl]methyl];xarelto;(s)-5-chloro-n-((2-oxo-3-(4-(3-oxomorpholino)phenyl)oxazolidin-5-yl)methyl)thiophene-2-carboxamide;rivaroxaban (bay59-7939) |
| cas: | 366789-02-8 |
| mf: | c19h18cln3o5s |
| mw: | 435.88 |
| einecs: | |
| product categories: | chiral reagents;heterocycles;intermediates & fine chemicals;pharmaceuticals;sulfur & selenium compounds;api;inhibitor;rivaroxaban;pharmaceutical raw materials;inhibitors |
| mol file: | 366789-02-8.mol |
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| rivaroxaban chemical properties |
| melting point | 228-229°c |
| storage temp. | refrigerator |
| safety information |
| rivaroxaban usage and synthesis |
| antithrombotic drugs |
rivaroxaban and dabigatran etexilate are currently the most promising antithrombotic drugs, and compared to traditional antithrombotic drugs heparin, essential difference is that it does not require participation of antithrombin ⅲ, directly antagonizes the free and bound xa factor. and heparin needs to have antithrombin ⅲ and can play a role, and is invalid to the prothrombin complex of xa factor. two new oral anticoagulants are praised as as a major step forward of anticoagulant therapy and potentially fatal thrombosis prevention in the medical field, will become a new milestone in the development of cardiovascular drugs. rivaroxaban was associated research and development success by the german bayer and usa johnson & johnson. in october 2008, get approved for listing in canada and the eu, trade name is xarelto. rivaroxaban is the world's first oral direct xa factor inhibitor, can be high selectively, competitively inhibit free and bound xa factor and activity of prothrombin, in a dose - dependent manner prolonged activated partial thromboplastin time board (pt) and prothrombin time (aptt), thus prolonging the clotting time, reducing thrombin formation. having characteristics of high bioavailability, a wide spectrum of disease treatment, dose effect relationship is stable, convenient oral administration, low bleeding risk. rivaroxaban also is drug for prevention and treatment of venous thrombosis. clinically for the prevention of forming patients with deep vein thrombosis (dvt) and pulmonary embolism (pe) after hip joint and knee replacement surgery. it can also be used to prevent stroke and non-cns systemic embolism in patients with non-valvular atrial fibrillation, reduce the risk of recurrent coronary syndrome, and so on. dabigatran is a new antithrombotic drugs with a variety of characteristics developed by a german company boehringer ingelheim. in april 2008, first listed in germany and the uk, trade name was pradaxa. this is listed first oral anticoagulant drug following warfarin in the past 50 years, is another milestone in the field of anticoagulant therapy and potentially fatal thrombosis prevention. dabigatran is a new synthetic direct thrombin inhibitor, is a prodrug for oral administration, belongs to the thrombin inhibitors of non-peptides. after oral gastrointestinal absorption, it is converted to have a direct anticoagulant activity of dabigatran etexilate in vivo. drug binds to the fibrin-specific binding sites of thrombin, preventing fibrinogen from cleaving into fibrin, thereby blocking the final step of the coagulation cascade network and thrombosis. the above information is edited by the chemicalbook of liu yujie. |
| uses | for elective hip joint or knee replacement surgery in adult patients to prevent venous thrombosis (vte). |
| chemical properties | white solid |
| usage | anti-coagulant, factor x inhibitor |
| usage |
a novel antithrombotic agent. a highly potent and selective, direct fxa inhibitor |
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