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抗凝血药物-Lovenox(R) 获FDA批准上市

2010-02-26 11:41:16  作者:新特药房  来源:互联网  浏览次数:1306  文字大小:【】【】【
简介: Lovenox(R) 是低分子肝素,在美国获批用于最广泛的适应症 赛诺菲-安万特 (Sanofi-aventis) 今天宣布,美国食品与药物管理局 (FDA) 已经批准了抗凝血的 Lovenox(R)(依诺肝素钠注射液)的补充新药申请 ...
关键字:Lovenox(R)

 Lovenox(R) 是低分子肝素,在美国获批用于最广泛的适应症

    赛诺菲-安万特 (Sanofi-aventis) 今天宣布,美国食品与药物管理局 (FDA) 已经批准了抗凝血的 Lovenox(R)(依诺肝素钠注射液)的补充新药申请 (sNDA)。Lovenox(R) 用于治疗急性 ST 段抬高心肌梗死 (STEMI) 患者。Lovenox(R) 已经显示出可以减少周期性心肌梗塞综合终点的发生率,并可降低接受溶栓治疗、药物治疗或经皮冠状动脉介入治疗 (PCI) 的急性 STEMI 患者的死亡率。

    STEMI 是一种严重的心脏病,这种疾病表现为动脉通常完全被血栓所堵塞,累积足够长时间可导致心脏肌肉损坏。

    美国食品与药物管理局批准该补充新药申请书的依据是里程碑式的 ExTRACT-TIMI 25 试验(依诺肝素和溶栓灌注法用于治疗急性心肌梗塞,溶栓法治疗心肌梗塞-25研究)成果。参与 ExTRACT-TIMI 25 试验的有20,000多名急性 STEMI 患者。ExTRACT-TIMI 25 试验的结果已经公布在2006年4月6日刊发的《New England Journal of Medicine》(新英格兰医学杂志)上。

    ExTRACT-TIMI 25 研究表明,在接受了纤维蛋白溶解治疗的 STEMI 患者中,在三十天的时间里,依诺肝素较普通肝素 (UFH) 可极大地降低这些患者的死亡率和心肌梗塞的复发率,降幅为17%(9.9% 对 12.0%,p 值小于0.001)。与普通肝素相比较的时候依诺肝素显示出来的优点,均可在30内使用经皮冠状动脉介入治疗的随机选择的患者以及采用药物治疗的患者身上看到。采用依诺肝素进行治疗的组别里,30天的重大出血率(包括颅内出血率)为2.1%,而采用普通肝素的组别的重大出血率则为1.4% (p值小于0.001)。采用依诺肝素进行治疗的组别的死亡、非致命性心肌梗塞复发以及非致命性颅内出血(净临床优点的衡量尺度)的30天综合终点率明显低于采用普通肝素的组别(10.1% 对 12.2%,p值小于0.001)。

    ExTRACT-TIMI 25 研究的首席研究员、哈佛大学医学院 (Harvard Medical School) 医学教授、布莱根妇女医院 (Brigham and Women's Hospital) Samuel A. Levine 心脏科主管、TIMI Study Groups 高级研究员 Elliott Antman 医学博士表示:“在评估可治疗 STEMI 患者的治疗选择上,此次美国食品与药物管理局对该申请的批准是一个重要的里程碑。有了这一新指示,依诺肝素现在就可以应用到各种急性冠脉综合征的治疗当中。这些病症包括不稳定性心绞痛或非 ST 段抬高心肌梗死 (UA/NSTEMI) 以及 STEMI。”

    赛诺菲-安万特还在欧洲国家(包括法国、德国、英国、意大利和西班牙)已经提交了关于 STEMI 适应症的档案。

    冠状动脉疾病和急性冠脉综合征简介

    冠状动脉疾病 (CAD) 是全球最常见的一种心脏病,同时也是全世界最严重的健康问题。每年冠状动脉疾病夺去了大约1700万人的性命,也就是说全球每三个死亡的人当中就有一个死于冠状动脉疾病。美国心脏协会表示,超过1300万美国人都有过冠状动脉疾病病史,有750万人患有急性心脏病。

    急性冠脉综合征 (ACS) 是一个总称,用于形容因冠状动脉狭窄而导致的一组临床症状以及伴随有急性心肌局部缺血的任何类型的临床症状。急性心肌局部缺血是由冠状动脉疾病导致的心肌对氧的供求失衡所造成的。

    所有急性冠脉综合征都需要进行立即治疗。其治疗方法是多层面的,旨在尝试保护受损心肌免受进一步的损害、恢复动脉中的血液流动以及减轻心脏对氧的需求。在急诊室,首要目标是迅速鉴别 MI (STEMI) 患者,排除胸痛的其他原因,并把患者按照风险高低划分组别,提供适宜的治疗,以便把对心肌的损伤和心肌局部缺血降低到最小程度。

    血液回流到心脏(灌注法)可以通过使用某些药物(纤维蛋白溶解药)、摧毁血栓或通过手术(经皮冠状动脉介入治疗)进行治疗来实现。治疗急性冠脉综合征的药物选择包括:使用抗血小板药物来防止血小板粘合在一起从而形成血栓,使用抗凝血剂来阻止血栓。抗凝血剂可防止血栓进一步恶化以及新血栓的形成,但是抗凝血剂却不能够溶解血栓。

    Lovenox(R) 简介

    Lovenox(R) 是一种抗血栓形成药剂中的独特化学实体,是一种低分子肝素 (LMWH)。作为全球最畅销的低分子肝素,Lovenox(R) 可通过肝磷脂苄基酯的碱降解而得到,大约是普通肝素分子大小的三分之一。Lovenox(R) 是被人们研究最为广泛的低分子肝素,15年来治疗了96个国家的1.3亿名患者。

    Lovenox(R) 在美国获批用于与阿斯匹林一起预防不稳定心绞痛和非 Q 段(非 ST 抬高心肌梗死)的局部缺血并发症,用于治疗深静脉血栓 (DVT)。深静脉血栓可能导致肺动脉栓塞 (PE),与苄丙酮香豆素钠 (warfarin sodium) 一起治疗急性深静脉血栓住院患者(无论有无肺动脉栓塞),以及与苄丙酮香豆素钠一起治疗无肺动脉栓塞的急性深静脉血栓门诊病人。其中的预防适用于可能会患得血栓并发症的作过腹部手术的患者、做过髋关节置换术的患者(正在住院治疗或住院治疗之后)以及患得急性病期间移动严重受限导致可能会患得血栓并发症的医疗患者。

    深静脉血栓和肺动脉栓塞简介

    深静脉血栓引起了身体深静脉内的血栓的形成,常常发生在较低的末端。每年,美国有多达两百万人患得深静脉血栓。肺动脉栓塞是深静脉血栓的一种严重并发症,有时可导致人丧命,每年美国有约300,000人死于这种并发症,多于乳腺癌和艾滋病致死人数的总和。

    深静脉血栓潜在的主要问题是阻碍了涉及到的深静脉内的血液流动,这是由于在深静脉内形成了血栓。血液流动不畅可导致急性的腿疼和肿胀等症状。血栓的部分从深静脉的形成位置被驱逐出来,随着血液流动而在血管中行走,最后抵达肺部并留在那里的时候便形成了肺动脉栓塞。有很多与肺动脉栓塞有关的症状,但是最常见的包括呼吸急促以及在深呼吸时侧胸疼痛加剧。有很多可导致深静脉血栓的常见的风险因素,其中包括长期不能移动、大型手术、慢性病、癌症、年龄大于40岁、外伤、口服避孕药、怀孕以及产后。

    深静脉血栓的治疗办法包括在某些危险疾病情况下进行预防以及对确诊的深静脉血栓患者进行急性治疗。对深静脉血栓的治疗有几种治疗办法,其中包括提早活动、抗血栓压力带或器械、腿部压力设备以加强血液流动,还有抗凝血剂和/或血液稀释药物。就与深静脉血栓有关的迹象和症状向您的医疗保健专业人士进行咨询是非常重要的。

 New Data Reveals That Enoxaparin Results in Significant Cost Savings Compared to Unfractionated Heparin (UFH) in Treatment of in-Hospital Patients at Risk for Venous Thromboembolism (VTE); - Thrombosis Management Clinical Effectiveness Initiative(R) (CEI) Study Demonstrates Cost Savings of More Than $1,000 Per Discharge With Enoxaparin

BRIDGEWATER, NJ - June 20 - A large scale study providing the first actuarial-based analysis of prophylaxis with enoxaparin compared to unfractionated heparin (UFH) in patients at risk for venous thromboembolism (VTE) was published today in Pharmacy & Therapeutics (P&T). The study, "Cost Implications of Using Unfractionated Heparin or Enoxaparin in Medical Patients At-Risk for Venous Thromboembolic Events," reveals that patients treated with enoxaparin (a low-molecular weight heparin [LMWH]) had an average savings in cost per discharge of $1,002 compared to patients treated with UFH, despite higher drug acquisition costs for enoxaparin. This four-year retrospective study (1999-2003) of more than 17,000 medical patients at risk of VTE in 15 hospitals nationwide including Brigham & Women's Hospital, Banner Good Samaritan Medical Center and Thomas Jefferson University Hospital, were part of the Thrombosis Management Clinical Effectiveness Initiative (CEI) conducted by Aon Corporation's Life Sciences Practice.

"The data support that, because of its cost-effectiveness, enoxaparin may be the preferred treatment strategy for prophylaxis in those at risk for deep-vein thrombosis and pulmonary embolism," said lead author Richard M. Weinberg, M.D. (Chief Quality Officer, Stamford Hospital, CT). "While UFH is inexpensive to purchase, the use of enoxaparin is associated with savings in several areas, including ICU charges, laboratory tests and medical-surgical supplies. This more than compensates for enoxaparin's higher acquisition cost."

In addition, data from the CEI study found that the lower total in-patient costs were not attributable to a shorter length of hospital stay, but resulted from savings achieved in several hospital cost centers including the ICU, laboratory and medical-surgical supplies. The most significant cost savings achieved by substituting enoxaparin for UFH occurred among patients with respiratory disease with a major complication or co-morbidity and unstable angina.

Research Design and Method

The CEI study included an analysis of administrative data from 89,584 medical patients at risk for VTE, hospitalized in 15 mid-to-large (< 300 beds and > 600 beds) hospitals nationwide. Based on principal diagnosis, secondary diagnosis, significant procedures, age, sex and discharge status, all discharges were categorized into severity adjusted "diagnosis related groups" (DRGs). Included in the analysis were DRGs in which at least 50% of patients had a length of hospital stay of five or more days. As a result, 10,953 patients receiving UFH and 6,246 receiving enoxaparin were compared based on the total cost of care associated with each therapy choice.

Key Findings

  • The severity-adjusted total savings, summed across all 47 included diagnoses, showed that thromboprophylaxis with enoxaparin was less costly by $1,002 per discharge compared with UFH.
  • In 74% of the included DRGs (n=35), lower costs were observed with enoxaparin compared with UFH.
  • In 36.2% of the included DRGs (n=17), differences were statistically significant, 32% (n=15) showing lower costs with enoxaparin.
  • The largest cost-savings with the enoxaparin treatment were achieved in the diagnostic category of respiratory disease with a major complication or co-morbidity and unstable angina.
  • A breakdown of costs per cost center revealed that the savings for ICU, laboratory and medical-surgery supplies comprised a large part of total savings.
  • Those treated with enoxaparin had a 0.6-day longer mean length of hospital stay compared with patients taking UFH.

"The significant cost savings demonstrated by the data, combined with the overall beneficial safety and efficacy profile of enoxaparin, have important implications for hospital administrators," said Dr. Geno J. Merli, Ludwig Kind Professor of Medicine and Director Jefferson Center for Vascular Diseases, Jefferson Medical College and Thomas Jefferson University Hospital. "Hospital decision-makers should look to these results when considering cost-effective VTE prevention protocols."

The Thrombosis Management CEI was supported through a grant by sanofi-aventis U.S., the makers of LOVENOX(R) (enoxaparin sodium injection).

About Venous Thromboembolism (VTE)

Venous thromboembolism refers to two serious conditions: Deep-Vein Thrombosis (DVT) and pulmonary embolism. According to the American Heart Association, DVT blood clots affect up to 2 million Americans each year, and complications kill up to 200,000 people in the U.S. annually - more than breast cancer and AIDS combined.

Treatments for DVT include early mobilization, sequential compression devices to prevent blood clotting, and anticoagulants and/or blood-thinning drugs.

About Lovenox(R)

Lovenox(R) (enoxaparin sodium injection) is a unique chemical entity in a class of antithrombotic agents known as low-molecular-weight heparins (LMWH). The No. 1 selling low-molecular-weight heparin in the world, Lovenox(R) is obtained by alkaline degradation of heparin benzyl ester and is about one-third the molecular size of unfractionated heparin. Numerous clinical studies have demonstrated that Lovenox(R) is a safe and effective way to significantly reduce the incidence of DVT in a wide range of patient populations, and is the only LMWH that is more effective than unfractionated heparin in the prophylaxis of ischemic complications of UA and NSTEMI when administered concomitantly with aspirin. This has been demonstrated by more than 15 years of use in the treatment of 130 million patients in 96 countries. With numerous national and international clinical studies demonstrating its safety and efficacy, Lovenox(R) is the most widely studied LMWH.

Important Safety Information

LOVENOX(R) (enoxaparin sodium injection) cannot be used interchangeably with other low-molecular-weight heparins or unfractionated heparin, as they differ in their manufacturing process, molecular weight distribution, anti-Xa and anti-IIa activities, units, and dosage.

When epidural/spinal anesthesia or spinal puncture is employed, patients anticoagulated or scheduled to be anticoagulated with low-molecular-weight heparins or heparinoids are at risk of developing an epidural or spinal hematoma, which can result in long-term or permanent paralysis.

The risk of these events is increased by the use of postoperative indwelling epidural catheters or by the concomitant use of drugs affecting hemostasis. Patients should be frequently monitored for signs and symptoms of neurological impairment.

(See boxed WARNING- http://products.sanofi-aventis.us/lovenox/Boxed%20Warning ).

As with other anticoagulants, use with extreme caution in patients with conditions that increase the risk of hemorrhage. Dosage adjustment is recommended in patients with severe renal impairment. Unless otherwise indicated, agents that may affect hemostasis should be discontinued prior to LOVENOX(R) therapy. Bleeding can occur at any site during LOVENOX(R) therapy. An unexplained fall in hematocrit or blood pressure should lead to a search for a bleeding site.

(See WARNINGS- http://products.sanofi-aventis.us/lovenox/Warnings and PRECAUTIONS- http://products.sanofi-aventis.us/lovenox/Precautions ).

Thrombocytopenia can occur with LOVENOX(R). In patients with a history of heparin-induced thrombocytopenia, LOVENOX(R) should be used with extreme caution. Thrombocytopenia of any degree should be monitored closely. If the platelet count falls below 100,000/mm(3), LOVENOX(R) should be discontinued. Cases of heparin-induced thrombocytopenia have been observed in clinical practice.

(See WARNINGS- http://products.sanofi-aventis.us/lovenox/Warnings ).

The use of LOVENOX(R) has not been adequately studied for thromboprophylaxis in pregnant women with mechanical prosthetic heart values.

(See WARNINGS- http://products.sanofi-aventis.us/lovenox/Warnings ).

LOVENOX(R) is contraindicated in patients with hypersensitivity to enoxaparin sodium, heparin, or pork products, and in patients with active major bleeding.

Please see accompanying full prescribing information- http://products.sanofi-aventis.us/lovenox/lovenox.html - including boxed WARNING- http://products.sanofi-aventis.us/lovenox/Boxed%20Warning .

Please visit http://www.lovenox.com/ for complete prescribing information, including boxed WARNING, and additional important information.

About sanofi-aventis

Sanofi-aventis is the world's third largest pharmaceutical company, ranking number one in Europe. Backed by a world-class R&D organization, sanofi-aventis is developing leading positions in seven major therapeutic areas: cardiovascular, thrombosis, oncology, metabolic diseases, central nervous system, internal medicine, and vaccines. Sanofi-aventis is listed in Paris (EURONEXT: SAN) and in New York (NYSE:SNY).

(US.ENO.06.06.003)

Reference

Weinberg M, Richard et al. Cost Implications of Using Unfractionated Heparin or Enoxaparin in Medical Patients At-Risk for Venous Thromboembolic Events. Pharmacy & Therapeutics, June 2006.

CONTACT:

Amy Ba of Sanofi-aventis
908-243-4261

   

 Lovenox®与未分级肝素的安全有效性研究将在接受正规血管再通治疗的心脏病发作患者中展开
    目前,对STEMI患者的血管再通治疗往往采用溶栓剂与阿斯匹林和未分级肝素联合治疗.使用溶栓药物可以溶解导致STEMI的血管斑块.使用抗血栓药物可以血栓再次形成的危险.
 
    ExTRACT-TIMI 25 (Enoxaparin and ThrombolysisReperfusion for Acute Myocardial Infarction Treatment-Thrombolysis In Myocardial Infarction – Study 25)将比较Lovenox®与未分级肝素对接受溶栓治疗的STEMI患者的安全性和有效性.研究中将使用的溶栓剂包括链激酶, 阿太普酶,tenecteplase 或 reteplase.
  
    ExTRACT-TIMI 25是一项随机双盲研究.它将在美国及其他24各国家的1250个医学中心进行.这将是有关Lovenox®与溶栓剂联合使用效果的最大的心血管临床试验.研究的终点被设为随机分组30天后的死亡和非致死性的再次心肌梗塞的发生情况.其他的评估项目还包括与需急诊再通治疗的病例和中风相关的胸痛.  
 
    有关Lovenox®对STEMI的疗效已经在多项有关心脏病发作的患者的临床试验中证实.
  
    据ASSENT 3 (ASsessment of the Safety and Efficacy of New Thrombolytic regimens)研究报道,接受Lovenox®和全量的tenecteplase的心脏病患者,与接受未分级肝素和全量的tenecteplase的心脏病患者相比,起出现缺血性并发症的比例更少.这与在接受半量的tenecteplase与阿昔单抗和未分级肝素的患者中得到的结果相似.但是,前者比后者更有效.
  
    ENTIRE-TIMI 23研究发现,接受tenecteplase溶栓治疗的患者中, Lovenox(R)是未分级肝素的一个有效的替代品.无论是否同时使用糖蛋白IIb/IIIa受体拮抗剂.研究者进一步发现,使用Lovenox(R)的患者,其在30天时的死亡和再发病率都要更低.
 
    HART II (Heparins and Aspirin Reperfusion Therapy)研究显示,接受Lovenox®与rt-PA,或 alteplase治疗的患者,与接受未分级肝素与rt-PA的患者相比,其90分钟时动脉再通的效果是相同的.   
    AMI-SK (Acute Myocardial Infarction – StreptoKinase)研究发现, Lovenox®与链激酶合用可以改善正常冠状动脉的血流并改善急性心肌梗塞患者的预后.

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