诺华抗癌药Jakavi达真性红细胞增多症III期临床主要终点

2016-06-20 medsci MedSci原创

近日,诺华公布了抗癌药物Jakavi在真性红细胞增多症中的关键III期临床试验数据,显示该药物的疗效优于最佳疗法。 这项名为RESPONSE-2的III期临床试验数据显示,治疗28周时,最佳疗法实现红细胞比容(红细胞体积占血细胞总体积的百分比)控制的百分比为18.7,而Jakavi (ruxolitinib)为62.2%,Jakavi显著优于当前的最佳疗法(BAT)。 真性红细胞增多症(pol

近日,诺华公布了抗癌药物Jakavi在真性红细胞增多症中的关键III期临床试验数据,显示该药物的疗效优于最佳疗法。

这项名为RESPONSE-2的III期临床试验数据显示,治疗28周时,最佳疗法实现红细胞比容(红细胞体积占血细胞总体积的百分比)控制的百分比为18.7,而Jakavi (ruxolitinib)为62.2%,Jakavi显著优于当前的最佳疗法(BAT)。

真性红细胞增多症(polycythemia vera,PV)是一种慢性、无法治愈的血液癌症,该病与血细胞生产过剩相关,导致血液增稠,血液凝块风险增加。这些血凝块可导致严重心血管并发症,如中风和心脏病发作,从而增加病发率和死亡率。目前全球每年约有10万名患者。临床治疗中,大约有25%的PV患者对羟基脲(hydroxyurea)治疗产生抵抗(反应不足)或不耐受(不可接受的副作用),被认为病情控制不佳,通常定义为红细胞压积>45%,白细胞和/或血小板计数升高,可能伴有衰弱症状和/或脾脏肿大,这类患者病情恶化的风险升高。因此在PV临床治疗中,是否需要放血治疗以及脾脏体积是否缩小是衡量患者病情是否得到控制的2个关键性指标。

参与这项临床试验的患者脾脏未发生肿大,也并未对羟基脲(hydroxyurea)治疗产生抵抗或不耐受,因此不属于晚期的真性红细胞增多症患者。这项临床试验的负责人、意大利英苏布里亚大学Francesco Passamonti表示,Jakavi 能够有效控制PV患者的病情,是治疗PV非常有效的二线药物。除了达到临床试验的主要终点之外,Jakavi治疗后实现血液学完全缓解的患者是最佳疗法(BAT)的五倍以上(Jakavi:23%;BAT:5.3%),症状完全缓解的患者比例更多(Jakavi:50%;BAT:7.7%)。

同时,一项名为COMFORT-I的III期临床试验数据表明,与安慰剂相比,Jakavi能够显著延长中至重度骨髓纤维化患者的总体生存期。前者的死亡风险超过70%。而Jakavi能将患者的死亡风险降低31%。

Jakavi(ruxolitinib)是一种口服JAK1和JAK2酪氨酸激酶抑制剂,于2011年和2014年获FDA批准用于骨纤维化和真性红细胞增多症(PV)的治疗,该药也是FDA批准的首个骨纤维化和“真红”治疗药物。在欧洲,Jakavi于2012年和2015年分别获批骨纤维化和PV适应症。

原始出处:

Novartis’ Jakavi comes out on top in rare blood cancer trial

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time=2016-06-22, status=1, ipAttribution=), GetPortalCommentsPageByObjectIdResponse(id=1594444, encodeId=3407159444458, content=<a href='/topic/show?id=b317956200' target=_blank style='color:#2F92EE;'>#III期#</a>, beContent=null, objectType=article, channel=null, level=null, likeNumber=0, replyNumber=0, topicName=null, topicId=null, topicList=[TopicDto(id=9562, encryptionId=b317956200, topicName=III期)], attachment=null, authenticateStatus=null, createdAvatar=, createdBy=a12645, createdName=智智灵药, createdTime=Wed Jun 22 02:25:00 CST 2016, time=2016-06-22, status=1, ipAttribution=)]
    2016-12-22 juliusluan78
  5. 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  6. 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  7. 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time=2016-06-22, status=1, ipAttribution=), GetPortalCommentsPageByObjectIdResponse(id=1594444, encodeId=3407159444458, content=<a href='/topic/show?id=b317956200' target=_blank style='color:#2F92EE;'>#III期#</a>, beContent=null, objectType=article, channel=null, level=null, likeNumber=0, replyNumber=0, topicName=null, topicId=null, topicList=[TopicDto(id=9562, encryptionId=b317956200, topicName=III期)], attachment=null, authenticateStatus=null, createdAvatar=, createdBy=a12645, createdName=智智灵药, createdTime=Wed Jun 22 02:25:00 CST 2016, time=2016-06-22, status=1, ipAttribution=)]
    2016-06-22 sunylz
  8. 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  9. 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日本制药巨头卫材的抗癌药Lenvima上个月拿下FDA肾细胞癌批文,目前已经在美国、日本、欧洲共获得分化型甲状腺癌和肾细胞癌两个适应症。近日,卫材和瑞士制药巨头诺华展开合作,将在美国推出Lenvima+Afinitor (everolimus)组合疗法。诺华的Afinitor本月初获得欧盟委员会批准新适应症,用于起源于胃肠道(gastrointestinal,GI)或肺部(lung)的不可切除性、

诺华Afinitor获欧盟批准治疗非功能性胃肠道和肺部神经内分泌肿瘤(NET)

瑞士制药巨头诺华(Novartis)抗癌药Afinitor(everolimus,依维莫司,片剂)近日在欧盟监管方面传来喜讯。欧盟委员会批准Afinitor的新适应症,用于起源于胃肠道(gastrointestinal,GI)或肺部(lung)的不可切除性、局部晚期或转移性、进展性、分化良好型(1级或2级)非功能性神经内分泌肿瘤(neuroendocrine tumor,NET)成人患者的治疗

诺华突破性药物bimagrumab临床后期研究遭遇滑铁卢

诺华公司最近表示,公司开发的用于治疗散发性包涵体肌炎新药bimagrumab(BYM338)在一项最新的临床IIb/III期研究中未能达到首要终点而宣告失败。这一结果对公司研发部门造成重创,甚至有人认为这是诺华公司研发部门近年来遭遇的最大失败。 对于BYM338,诺华公司一直寄予厚望。此前公司已经获得了美国FDA授予的突破性药物认证。公司还希望将这种药物拓展到包括COPD在内的多种疾病治疗中去。

药不提当年勇:诺华心衰药物Entresto拟按真实世界有效性收费

近日诺华宣布和两个主要健康保险公司Cigna和Aetna签署其心衰药物Entresto的支付协议。诺华将提供一个基线折扣,然后根据Entresto在真实世界的表现增加(如果未达到预期疗效)或降低(超过预期疗效)这个折扣。但是双方并未公布具体内容,比如预期疗效、折扣具体数目等。在政府控制药价比较严的欧洲,如英国的NICE,经常和药厂达成这类协议。但这将是美国市场第一个主动按质论价的新药。在此之前