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59729-37-2
  • names:

    Fexinidazole

  • CAS號(hào):

    59729-37-2

    MDL Number:
  • MF(分子式): C12H13N3O3S MW(分子量): 279.31
  • EINECS: Reaxys Number:
  • Pubchem ID: Brand:BIOFOUNT
非昔硝唑
非昔硝唑(Fexinidazole,59729-37-2)用于研究用于治療疾病,南美錐蟲病和南美錐蟲病。
貨品編碼 規(guī)格 純度 價(jià)格 (¥) 現(xiàn)價(jià)(¥) 特價(jià)(¥) 庫存描述 數(shù)量 總計(jì) (¥)
YZM000772-10mg 10mg 99.92% ¥ 1518.00 ¥ 1518.00 2-3天
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YZM000772-5mg 5mg 99.92% ¥ 926.25 ¥ 926.25 2-3天
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中文別名 非昔硝唑(Fexinidazole,59729-37-2),非辛達(dá)唑
英文別名 Fexinidazole(非昔硝,59729-37-2)
CAS號(hào) 59729-37-2
Inchi InChI=1S/C12H13N3O3S/c1-14-11(13-7-12(14)15(16)17)8-18-9-3-5-10(19-2)6-4-9/h3-7H,8H2,1-2H3
InchiKey MIWWSGDADVMLTG-UHFFFAOYSA-N
分子式 Formula C12H13N3O3S
分子量 Molecular Weight 279.31
溶解度Solubility 生物體外In Vitro:DMSO溶解度50 mg/mL(179.01 mM;Need ultrasonic)H2O< 0.1 mg/mL(insoluble)
性狀 固體粉末,Power
儲(chǔ)藏條件 Storage conditions -20°C 3 years年 4°C 2 years年 / In solvent溶液中:-80°C 6 months月 -20°C 1 month月
非昔硝唑(Fexinidazole,59729-37-2)實(shí)驗(yàn)注意事項(xiàng):
1.實(shí)驗(yàn)前需戴好防護(hù)眼鏡,穿戴防護(hù)服和口罩,佩戴手套,避免與皮膚接觸。
2.實(shí)驗(yàn)過程中如遇到有毒或者刺激性物質(zhì)及有害物質(zhì)產(chǎn)生,必要時(shí)實(shí)驗(yàn)操作需要手套箱內(nèi)完成以免對(duì)實(shí)驗(yàn)人員造成傷害
3.實(shí)驗(yàn)后產(chǎn)生的廢棄物需分類存儲(chǔ),并交于專業(yè)生物廢氣物處理公司處理,以免造成環(huán)境污染Experimental considerations:
1. Wear protective glasses, protective clothing and masks, gloves, and avoid contact with the skin during the experiment.
2. The waste generated after the experiment needs to be stored separately, and handed over to a professional biological waste gas treatment company to avoid environmental pollution.
Tag:非昔硝唑MSDS,非昔硝唑蒸汽壓,非昔硝唑合成,非昔硝唑標(biāo)準(zhǔn),非昔硝唑應(yīng)用,非昔硝唑合成,非昔硝唑沸點(diǎn),非昔硝唑閃點(diǎn),非昔硝唑用途,非昔硝唑溶解度,非昔硝唑價(jià)格,非昔硝唑作用,非昔硝唑結(jié)構(gòu)式,非昔硝唑用處,非昔硝唑毒理性質(zhì),非昔硝唑物理性質(zhì)
產(chǎn)品說明 非昔硝唑(Fexinidazole,59729-37-2) 一種5-硝基咪唑藥物
IntroductionFexinidazole(非昔硝,59729-37-2)Fexinidazole is a 5-nitroimidazole drug currently in clinical
Application1Fexinidazole is a 5-nitroimidazole drug currently in clinical development for the treatment of human sleeping sickness (human African trypanosomiasis [HAT]), caused by infection with species of the pr
Application2Fexidazole can produce active amines with indirect toxicity and mutagenic effects on trypanosomes. It is active in vitro against Trypanosoma gambiae and many other trypanosoma subspecies (including Tr
Application3
Fexinidazole: First Global Approval Drugs 2019/PMID: 30635838
Determination of an Optimal Dosing Regimen for Fexinidazole, a Novel Oral Drug for the Treatment of Human African Trypanosomiasis: First-in-Human Studies Clinical Pharmacokinetics 2014/PMID: 24535888
Heterogeneity in the in vitro susceptibility of Loa loa microfilariae to drugs commonly used in parasitological infections Parasites & Vectors 2018/PMID: 29615094
Systemic and Target-Site Pharmacokinetics of Antiparasitic Agents Clinical Pharmacokinetics 2020/PMID: 32100246
Evaluation of the in vitro trypanocidal activity of methylated flavonoid constituents of Vitex simplicifolia leaves BMC Complementary and Alternative Medicine 2015/PMID: 25886869

Toosendanin relatives, trypanocidal principles from Meliae Cortex

Abstract

Africa Trypanosomiasis remains a serious health problem, but the approved drugs for this disease are so few that novel trypanocidal compounds are demanded. In search for trypanocidal principles from medicinal plants, we found MeOH extracts of Meliae Cortex with potent activity through the screening from about 300 kinds of methanolic extract. By bioassay-guided fractionation from this extract through the liquid-liquid partition and subsequent chromatographic technique using silica gel and ODS, finally we disclosed toosendanin (1) and its relatives as active principles. These active congeners showed not only potent trypanocidal activity but also little cytotoxicity to display the excellent selective index. Taking the isolated amount as well as trypanocidal activity into consideration, 1 was disclosed to be the responsible active principle in Meliae Cortex. Additionally, the derivatives of 1 were chemically prepared from 1 and bioactivity of them were also evaluated. Through the comparison with their trypanocidal activity among the isolated relatives and the synthesized derivatives of 1, the epoxide moiety was revealed to be essential for their potent trypanocidal activity. Furthermore, 3-O-acetyl group and 7-hydroxyl group were presumed to be important functional groups and introduction of methylpropionyl group into hemiacetal hydroxy moiety was clarified to enhance their typanocidal activity.


Fexinidazole: First Global Approval

Abstract

Fexinidazole Winthrop (hereafter referred to as fexinidazole) is a DNA synthesis inhibitor developed by the Drugs for Neglected Diseases initiative (DNDi), in collaboration with Sanofi, for the oral treatment of human African trypanosomiasis (HAT) [commonly known as 'sleeping sickness'] and Chagas' disease. The drug is a 5-nitroimidazole derivative first discovered by Hoechst AG (now part of Sanofi) and was identified by the DNDi in 2005 as having activity against Trypanosoma brucei gambiense and T. b. rhodesiense. Under Article 58 of Regulation (EC) no. 726/2004 (a regulatory mechanism for reviewing new medicines destined for use outside of the EU), fexinidazole has been granted a positive opinion by the EMA for the treatment of both the first-stage (haemo-lymphatic) and second-stage (meningo-encephalitic) of HAT due to T. b. gambiense (g-HAT) in adults and children aged ≥ 6 years and weighing ≥ 20 kg. This approval will facilitate and support marketing authorization application in endemic countries in 2019; following registration, fexinidazole will be distributed via the WHO to endemic countries for g-HAT. Phase 3 evaluation of fexinidazole for g-HAT is ongoing in the Democratic Republic of the Congo and Guinea and the drug is also in development for Chagas' disease, with a study currently ongoing in Spain. Clinical development for visceral leishmaniasis is discontinued. This article summarizes the milestones in the development of fexinidazole leading to this first approval for g-HAT.

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