beta-Artemether | 71963-77-4

• 物质功能分类: 原料药 - 抗寄生虫病药 - 抗疟药
• 分子结构分类: 有机化合物 - 脂质和类脂质分子 - 异戊烯醇脂质
• 英文名称: beta-Artemether
• 英文别名: (4S,5R,8S,9R,10S,12R,13R)-10-methoxy-1,5,9-trimethyl-11,14,15,16-tetraoxatetracyclo[10.3.1.04,13.08,13]hexadecane
• CAS: 71963-77-4
• 化学式: C₁₆H₂₆O₅
• 分子量: 298.37
• InChiKey: SXYIRMFQILZOAM-GXTLMGRASA-N

物化性质

• 熔点：
  86-88°C
• 比旋光度：
  D19.5 +171° (c = 2.59 in CHCl3)
• 沸点：
  359.79°C (rough estimate)
• 密度：
  1.0733 (rough estimate)
• 溶解度：
  二甲基亚砜：≥20mg/mL
• 颜色/状态：
  Crystals
• 蒸汽压力：
  4X10-5 mm Hg at 25 °C (est)
• 旋光度：
  Specific optical rotation = 177 deg at 19.5 °C

计算性质

• 辛醇/水分配系数(LogP)：
  3.1
• 重原子数：
  21
• 可旋转键数：
  1
• 环数：
  5.0
• sp3杂化的碳原子比例：
  1.0
• 拓扑面积：
  46.2
• 氢给体数：
  0
• 氢受体数：
  5

ADMET

代谢

Artemether ... 被转化为二氢青蒿素 ... 青蒿素类药物的抗疟疾效果主要来自二氢青蒿素 ...

Artemether ... /is/ converted to dihydroartemisinin ... The antimalarial effect of artemisinin compounds results primarily from dihydroartemisinin ...

来源:Hazardous Substances Data Bank (HSDB)

代谢

青蒿素在大鼠口服给药后可以完全且迅速地被吸收。然而，即使在300毫克/千克的剂量下，也获得了非常低的血浆水平。肝脏被发现是失活的主要场所。当青蒿素通过肌肉注射给药时，可以检测到显著且更持久的血浆水平。青蒿素在静脉注射后能够通过血脑屏障和血胎盘屏障。无论给药途径如何，在48小时内尿液或粪便中几乎未发现未改变青蒿素。在人给药后确定的代谢物包括去氧青蒿素、去氧二氢青蒿素和9,10-二羟基去氧青蒿素。/青蒿素/

Artemisinin is completely and rapidly absorbed after oral administration in rats. However, a very low plasma level was obtained even after a dose of 300 mg/kg. Liver was found to be the chief site of inactivation. When artemisinin was given i.m., significant and more persistent plasma levels were detected. Artemisinin was shown to pass the blood-brain and blood-placenta barriers after i.v. injection. Very little unchanged artemisinin was found in the urine or feces in 48 hours regardless of the route of administration. Metabolites identified after administration to humans include deoxyartemisinin, deoxydihydroartemisinin, and 9,10-dihydroxydeoxyartemisinin. /Artemisinin/

来源:Hazardous Substances Data Bank (HSDB)

毒理性

• 相互作用

这项研究旨在评估葡萄柚汁对阿莫地喹随时间降低生物利用度的影响。在一项随机、两阶段交叉研究中，八名健康男性受试者每天一次服用100毫克口服阿莫地喹，并随同350毫升水或350毫升双倍浓度的新鲜冷冻葡萄柚汁连续服用5天。在第1天和第5天，收集了17个血液样本，持续8小时。与第1天相比，第5天最后一次给药后的阿莫地喹平均血药峰浓度（Cmax）和平均药时曲线下面积（AUC）约为三分之一，用水（Cmax的P值为.006；AUC的P值为.005）和葡萄柚汁（Cmax和AUC的P值<.001）服用后消除半衰期没有变化。葡萄柚汁使第1天（P值为.021）和第5天（Cmax的P值为.05；AUC的P值为.004）的Cmax和AUC增加了两倍。活性代谢物双氢青蒿素在葡萄柚汁作用下Cmax（P值为.006）和AUC（P值为.001）也增加了两倍，且药代动力学参数没有时间依赖性变化。葡萄柚汁显著增加了阿莫地喹的口服生物利用度，但并未阻止随时间降低的生物利用度。这表明肠道壁中的CYP3A4是阿莫地喹的代谢酶之一，但似乎不参与自诱导过程。

The aim of this study was to evaluate the effect of grapefruit juice on the decreasing bioavailability over time of artemether. In a randomized, two-phase crossover study, eight healthy male subjects took 100 mg oral artemether with 350 mL water or with 350 mL double-strength fresh frozen grapefruit juice once daily for 5 days. On day 1 and day 5, 17 blood samples were collected over a period of 8 hours. The mean peak artemether plasma concentration (Cmax) and the mean area under the concentration-time curve (AUC) after the last dose at day 5 were about one third compared with day 1, without a change in the elimination half-life after intake with water (P = .006 for Cmax; P = .005 for AUC) and with grapefruit juice (P < .001 for Cmax and AUC). Grapefruit juice increased Cmax (P = .021) and AUC (P < .001) twofold on day 1 (P = .021) and day 5 (P = .05 for Cmax; P = .004 for AUC). Dihydroartemisinin, the active metabolite, showed a twofold increase in Cmax (P = .006) and AUC (P = .001) with grapefruit juice, without time-dependent changes of pharmacokinetic parameters. Grapefruit juice significantly increased the oral bioavailability of artemether but did not prevent the time-dependent reduction in bioavailability. It suggests that CYP3A4 in the gut wall is one of the metabolizing enzymes of artemether but seems to not be involved in the autoinduction process.

来源:Hazardous Substances Data Bank (HSDB)

毒理性

• 相互作用

关于退热药可能削弱宿主对疟疾防御能力的担忧，因为使用退热药与寄生虫清除延迟有关。然而，这似乎是由于延迟了细胞粘附，这很可能是有益的。在疟疾治疗中没有理由不使用退热药。对乙酰氨基酚（扑热息痛）和布洛芬是降低发热的首选药物。

There has been some concern that antipyretics might attenuate the host defense against malaria, as their use is associated with delayed parasite clearance. However, this appears to result from delaying cytoadherence, which is likely to be beneficial. There is no reason to withhold antipyretics in malaria. ...Paracetamol (acetaminophen) and ibuprofen are the preferred options for reducing fever.

来源:Hazardous Substances Data Bank (HSDB)

毒理性

• 解毒与急救

基本治疗：建立专利气道（如需要，使用口咽或鼻咽气道）。如有必要，进行吸痰。密切观察呼吸不足的迹象，并在需要时辅助通气。通过非循环呼吸面罩以10至15升/分钟的速度给予氧气。监测肺水肿，并在必要时进行治疗……。监测休克，并在必要时进行治疗……。预防癫痫发作，并在必要时进行治疗……。对于眼睛污染，立即用水冲洗眼睛。在转运过程中，用0.9%的生理盐水（NS）连续冲洗每只眼睛……。不要使用催吐剂。对于摄入，如果患者能吞咽、有强烈的干呕反射且不流口水，则用温水冲洗口腔，并给予5毫升/千克，最多200毫升的水进行稀释……。在去污后，用干燥的无菌敷料覆盖皮肤烧伤……。/毒物A和B/

Basic treatment: Establish a patent airway (oropharyngeal or nasopharyngeal airway, if needed). Suction if necessary. Watch for signs of respiratory insufficiency and assist ventilations if needed. Administer oxygen by nonrebreather mask at 10 to 15 L/min. Monitor for pulmonary edema and treat if necessary ... . Monitor for shock and treat if necessary ... . Anticipate seizures and treat if necessary ... . For eye contamination, flush eyes immediately with water. Irrigate each eye continuously with 0.9% saline (NS) during transport ... . Do not use emetics. For ingestion, rinse mouth and administer 5 ml/kg up to 200 ml of water for dilution if the patient can swallow, has a strong gag reflex, and does not drool ... . Cover skin burns with dry sterile dressings after decontamination ... . /Poisons A and B/

来源:Hazardous Substances Data Bank (HSDB)

毒理性

• 解毒与急救

高级治疗：对于昏迷的患者、严重肺水肿的患者或严重呼吸窘迫的患者，考虑进行口咽或鼻咽气管插管以控制气道。使用带气囊的面罩进行正压通气技术可能有益。考虑对肺水肿进行药物治疗...。对于严重的支气管痉挛，考虑给予β激动剂，如沙丁胺醇...。监测心率和必要时治疗心律失常...。开始静脉输注D5W/SRP：“保持开放”，最小流量/。如果出现低血容量的迹象，使用0.9%生理盐水（NS）或乳酸钠林格氏液。对于伴有低血容量迹象的低血压，谨慎给予液体。注意液体过载的迹象...。使用地西泮或劳拉西泮治疗癫痫...。使用丙美卡因氢氯化物协助眼部冲洗...。/毒物A和B/

Advanced treatment: Consider orotracheal or nasotracheal intubation for airway control in the patient who is unconscious, has severe pulmonary edema, or is in severe respiratory distress. Positive-pressure ventilation techniques with a bag valve mask device may be beneficial. Consider drug therapy for pulmonary edema ... . Consider administering a beta agonist such as albuterol for severe bronchospasm ... . Monitor cardiac rhythm and treat arrhythmias as necessary ... . Start IV administration of D5W /SRP: "To keep open", minimal flow rate/. Use 0.9% saline (NS) or lactated Ringer's if signs of hypovolemia are present. For hypotension with signs of hypovolemia, administer fluid cautiously. Watch for signs of fluid overload ... . Treat seizures with diazepam or lorazepam ... . Use proparacaine hydrochloride to assist eye irrigation ... . /Poisons A and B/

来源:Hazardous Substances Data Bank (HSDB)

毒理性

• 人类毒性摘录

/病例报告/ 总共有83名患有恶性疟疾的孕妇接受了青蒿琥酯或青蒿素的给药，通常随后再使用奎宁或氯喹，直到分娩每周进行随访。总体而言，73例妊娠（88%）产下活婴，3例（4%）流产，2例（3%）死产。没有发现先天性异常，46名随访超过一年的儿童都正常发育。

/CASE REPORTS/ A total of 83 pregnant women with Plasmodium falciparum malaria, administered artesunate or artemether, often followed by quinine or mefloquine, were followed weekly until delivery. Overall 73 pregnancies (88%) resulted in live births, 3 (4%) in abortions, and 2 (3%) in still births. There were no congenital abnormalities and the 46 children followed for more than a year all developed normally

来源:Hazardous Substances Data Bank (HSDB)

吸收、分配和排泄

少量或没有给予的药物或二氢青蒿素可以在尿液中回收。/二氢青蒿素/

Little or none of the administered drugs or dihydroartemisinin is recovered in urine. /Dihydroartemisinin/

来源:Hazardous Substances Data Bank (HSDB)

吸收、分配和排泄

肌肉给药后，药代动力学表明阿莫地喹（AM）在给药后2到4小时达到血浆峰值水平，消除缓慢，并且随着重复给药有累积的趋势。主要代谢物二氢青蒿素（DHA）的水平较低。脑脊液（CSF）中的AM水平低于血浆水平的10%。口服给药后，AM的浓度远低于肌肉给药。DHA在第1天的浓度较高，但在第7天几乎为零，这表明在狗体内DHA迅速失活。第8次口服给药后2小时，CSF中未检测到AM或DHA，这可能是狗口服AM后未出现神经毒性的原因。

After intramuscular administration pharmacokinetics indicated peak plasma levels of artemether (AM) at 2 to 4 hours post-dose, slow elimination and a tendency to accumulate after repeated administration. Only low levels of the major metabolite, dihydroartemisinin (DHA), were found. AM levels in the cerebrospinal fluid (CSF) were < 10% of plasma levels. After oral administration AM concentrations were considerably lower than after i.m. administration. The concentration of DHA was high on day 1 but almost nil on day 7 indicating its fast inactivation in dogs. Two hours after the 8th oral administration neither AM nor DHA was detected in CSF which may explain the absence of neurotoxicity in dogs after oral administration of AM.

来源:Hazardous Substances Data Bank (HSDB)

吸收、分配和排泄

这项研究调查了肌肉注射蒿甲醚及其主要血浆代谢物双氢青蒿素的药代动力学，研究对象是恶性疟疾严重发作的患者。研究纳入了6名急性肾衰竭（ARF）的重症恶性疟疾患者和11名没有ARF的患者。他们接受了肌肉注射蒿甲醚的负荷剂量160毫克，随后连续6天每天80毫克（总剂量640毫克）。有无ARF的患者对治疗的初始反应良好；寄生虫和发热清除时间分别为66（30至164）和76（36至140）小时（中位数（范围））。在治疗开始后的7天内，没有患者在周围血液涂片中再次出现寄生虫血症。昏迷患者的意识恢复时间为51.6（22至144）小时。蒿甲醚在注射160毫克剂量后1小时就可以在血浆中检测到，在大多数情况下，24小时内降至检测不到的水平。与没有ARF的患者相比，ARF患者的Cmax显著较高（2.38（1.89至3.95）vs 1.56（1.05至3.38）ng/mL/mg剂量），Vz/F（5.45（3.2至6.9）vs 8.6（4.2至12.3）L/kg）和CL/F（7.4（5.4至13.8）vs 19.1（8.5至25.1）mL/min/kg）显著较低。此外，ARF患者的t1/2z显著更长（7.0（5.5至10.0）vs 5.7（4.2至6.6）小时）。两组之间双氢青蒿素的药代动力学相似。ARF显著改变了肌肉注射蒿甲醚的药代动力学。这些变化可能是由于吸收/生物利用度提高、系统性清除减少或药物血浆蛋白结合改变所导致的。

The pharmacokinetics of intramuscular artemether and its major plasma metabolite-dihydroartemisinin, were investigated in patients with severe manifestations of falciparum malaria. Six severe falciparum malaria patients with acute renal failure (ARF) and 11 without ARF were recruited into the study. They were treated with intramuscular artemether at a loading dose of 160 mg, followed by daily doses of 80 mg for another 6 days (total dose 640 mg). Patients with and without ARF showed a good initial response to treatment; the parasite and fever clearance times were 66 (30 to 164) and 76 (36 to 140) hr (median (range)), respectively. None had reappearance of parasitaemia in their peripheral blood smear within 7 days of initiation of treatment. In comatose patients, the time to recovery of consciousness was 51.6 (22 to 144) hr. Artemether was detected in plasma as early as 1hr after a 160 mg dose, and declined to undetectable levels within 24 hr in most cases. Patients with ARF had significantly higher Cmax (2.38 (1.89 to 3.95) vs 1.56 (1.05 to 3.38) ng/mL/mg dose), and lower Vz/F (5.45 (3.2 to 6.9) vs 8.6 (4.2 to 12.3) L/kg) and CL/F (7.4 (5.4 to 13.8) vs 19.1 (8.5 to 25.1) mL/min/kg) when compared to those without ARF. In addition, t1/2z, was significantly longer in ARF patients (7.0 (5.5 to 10.0) vs 5.7 (4.2 to 6.6) hr). The parmacokinetics of dihydroartemisinin in the two groups were comparable. ARF significantly modified the pharmacokinetics of intramuscular artemether. The changes could be contributed to either improved absorption/bioavailability, a reduction of systemic clearance, or a change in plasma protein binding of the drug.

来源:Hazardous Substances Data Bank (HSDB)

吸收、分配和排泄

Dihydroartemisinin口服给药后迅速吸收，大约2.5小时后达到峰值水平。通过直肠给药的吸收速度较慢，峰值水平在大约给药后4小时出现。血浆蛋白结合率约为55%。通过肠道和肝脏葡萄糖醛酸化的消除半衰期大约为45分钟。

Dihydroartemisinin is rapidly absorbed following oral administration, reaching peak levels after around 2.5 hr. Absorption via the rectal route is somewhat slower, with peak levels occurring around 4 hr after administration. Plasma protein binding is around 55%. Elimination half-life is approximately 45 min via intestinal and hepatic glucuronidation. /Dihydroartemisinin/

来源:Hazardous Substances Data Bank (HSDB)

安全信息

• 危险品标志：
  Xn
• 安全说明：
  S24/25
• 危险类别码：
  R22
• WGK Germany：
  3
• 海关编码：
  2932999099
• 危险品运输编号：
  OTH
• 危险标志：
  GHS07
• 危险性描述：
  H302

制备方法与用途

简介

蒿甲醚和本芴醇是近年来研制成功的两种结构和作用不同的新型抗疟药。这两种药物通常单独使用。

蒿甲醚的特点在于快速杀灭疟原虫，但治疗后患者血中残留的原虫复燃率较高。

性状

蒿甲醚为白色结晶或结晶性粉末，味苦且无臭。

性质

本品在丙酮和三氯甲烷中极易溶解，在乙醇或乙酸乙酯中易溶，在水中几乎不溶。它对疟原虫红内期有直接杀灭作用，但对组织期无效；在实验动物中的毒性较低。蒿甲醚在体内吸收快、分布广、排泄迅速。电镜观察显示其主要影响鼠疟原虫的膜系结构，并推测其抗疟机制是干扰了疟原虫表膜与线粒体的功能。

化学性质

蒿甲醚为白色粒状结晶，可溶于甲醇、乙醇和DMSO等有机溶剂。它来源于黄花蒿叶。

用途

蒿甲醚是一种青蒿素的甲醚衍生物，主要用于抗疟疾治疗。

类别与毒性分级

• 类别：有毒物品
• 毒性分级：中毒
• 急性毒性
  • 口服（小鼠）LD50：1000毫克/公斤
  • 皮下注射（小鼠）LD50：390毫克/公斤
• 可燃性危险特性：可燃，燃烧时产生刺激烟雾。
• 储运特性：需通风、低温和干燥保存。
• 灭火剂：干粉、泡沫、沙土、二氧化碳或雾状水。

文献信息

• Compositions of pharmaceutical actives containing diethylene glycol monoethyl ether or other alkyl derivatives
  申请人：THEMIS MEDICARE LIMITED

  公开号：US10940205B2

  公开（公告）日：2021-03-09

  The present invention relates to pharmaceutical compositions of various pharmaceutical actives, especially lyophilic and hydrophilic actives containing Diethylene glycol monoethyl ether or other alkyl derivatives thereof as a primary vehicle and/or to pharmaceutical compositions utilizing Diethylene glycol monoethyl ether or other alkyl derivatives thereof as a primary vehicle or as a solvent system in preparation of such pharmaceutical compositions. The pharmaceutical compositions of the present invention are safe, non-toxic, exhibits enhanced physical stability compared to conventional formulations containing such pharmaceutical actives and are suitable for use as injectables for intravenous and intramuscular administration, as well as for use as a preformed solution/liquid for filling in and preparation of capsules, tablets, nasal sprays, gargles, dermal applications, gels, topicals, liquid oral dosage forms and other dosage forms.

  本发明涉及各种药物活性物质的药物组合物，特别是含有二乙二醇单乙醚或其 他烷基衍生物作为主要载体的冻干和亲水活性物质，和/或涉及利用二乙二醇单乙醚或其 他烷基衍生物作为主要载体或作为制备此类药物组合物的溶剂系统的药物组合物。本发明的药物组合物安全、无毒，与含有此类药物活性成分的传统制剂相比，具有更强的物理稳定性，适合用作静脉注射和肌肉注射的注射剂，也适合用作预制溶液/液体，用于填充和制备胶囊、片剂、鼻腔喷雾剂、漱口水、皮肤应用、凝胶、外用药、口服液剂型和其他剂型。
• COMPOSITIONS OF PHARMACEUTICAL ACTIVES CONTAINING DIETHYLENE GLYCOL MONOETHYL ETHER OR OTHER ALKYL DERIVATIVES
  申请人：THEMIS MEDICARE LIMITED

  公开号：US20180071390A1

  公开（公告）日：2018-03-15

  The present invention relates to pharmaceutical compositions of various pharmaceutical actives, especially lyophilic and hydrophilic actives containing Diethylene glycol monoethyl ether or other alkyl derivatives thereof as a primary vehicle and/or to pharmaceutical compositions utilizing Diethylene glycol monoethyl ether or other alkyl derivatives thereof as a primary vehicle or as a solvent system in preparation of such pharmaceutical compositions. The pharmaceutical compositions of the present invention are safe, non-toxic, exhibits enhanced physical stability compared to conventional formulations containing such pharmaceutical actives and are suitable for use as injectables for intravenous and intramuscular administration, as well as for use as a preformed solution/liquid for filling in and preparation of capsules, tablets, nasal sprays, gargles, dermal applications, gels, topicals, liquid oral dosage forms and other dosage forms.
• ARTEMISININ ANALOG, AND USE, METHOD, AND COMPOSITION FOR PROMOTING LIPID CATABOLISM AND IMPROVING SUGAR METABOLISM
  申请人：FUDAN UNIVERSITY

  公开号：US20190133997A1

  公开（公告）日：2019-05-09

  An artemisinin analog as represented by formula (A) and application thereof in preparing a pharmaceutical product for promoting lipid catabolism and/or prevention or treatment of metabolism-related disease. The artemisinin analog promotes browning of white fat to achieve body weight reduction and improve metabolism, thereby providing therapeutic effects against hyperglycemia, insulin resistance, dyslipidemia, and/or fatty liver.