这不是与Cimzia(赛妥珠单抗预填充注射器)相互作用的所有药物或健康问题的列表。
告诉您的医生和药剂师您所有的药物(处方药或非处方药,天然产品,维生素)和健康问题。您必须检查以确保服用Cimzia(塞妥珠单抗预填充注射器)对您所有的药物和健康问题都是安全的。未经医生许可,请勿开始,停止或更改任何药物的剂量。
按照医生的指示使用Cimzia(塞妥珠单抗预填充注射器)。阅读提供给您的所有信息。请严格按照所有说明进行操作。
如果我错过了剂量怎么办?
警告/警告:尽管这种情况很少见,但有些人在服药时可能会有非常严重的副作用,有时甚至是致命的副作用。如果您有以下任何与严重不良副作用相关的症状或体征,请立即告诉医生或寻求医疗帮助:
所有药物都可能引起副作用。但是,许多人没有副作用,或者只有很小的副作用。如果这些副作用或任何其他副作用困扰您或不消失,请致电您的医生或获得医疗帮助:
这些并非所有可能发生的副作用。如果您对副作用有疑问,请致电您的医生。打电话给您的医生,征求有关副作用的医疗建议。
您可以致电1-800-332-1088向FDA报告副作用。您也可以在https://www.fda.gov/medwatch报告副作用。
如果您认为服药过量,请致电毒物控制中心或立即就医。准备好告诉或显示采取了什么,采取了多少,何时发生。
注意:本文档包含有关certolizumab的副作用信息。此页面上列出的某些剂型可能不适用于Cimzia品牌。
Cimzia的常见副作用包括:感染和病毒感染。其他副作用包括:皮疹。有关不良影响的完整列表,请参见下文。
适用于certolizumab:皮下注射液,皮下注射液
皮下途径(粉剂;溶液)
严重感染-用certolizumab聚乙二醇(pegol)治疗的患者发生严重感染的风险增加,可能导致住院或死亡。发生这些感染的大多数患者都在服用诸如甲氨蝶呤或皮质类固醇之类的免疫抑制剂。如果患者出现严重感染或败血症,则应停用Certolizumab聚乙二醇。结核病患者经常出现弥漫性或肺外疾病。在使用certolizumab聚乙二醇前和治疗期间,应对患者进行潜伏性结核病检测。潜在感染的治疗应在使用certolizumab聚乙二醇之前开始进行。侵入性真菌感染包括组织胞浆菌病,球孢子菌病,念珠菌病,曲霉菌病,胚芽菌病和肺囊虫病。患有组织胞浆菌病或其他侵袭性真菌感染的患者可能会出现弥漫性疾病,而不是局部疾病。在某些活动性感染患者中,用于组织胞浆菌病的抗原和抗体检测可能为阴性。对于有严重系统疾病的侵入性真菌感染风险患者,应考虑经验性抗真菌治疗;由于军团菌和李斯特菌等机会性病原体引起的细菌,病毒和其他感染;使用西妥珠单抗聚乙二醇乙二醇酯治疗的风险和益处应谨慎对待慢性或复发性感染患者在开始治疗之前应考虑的因素。应密切监测患者使用certolizumab聚乙二醇(pegol)治疗期间和之后感染的迹象和症状的发展,包括对潜伏性结核感染呈阴性的患者可能发生的结核病在接受TNF受体阻滞剂治疗的儿童和青少年患者中已报告恶性淋巴瘤和其他恶性肿瘤,其中一些是致命的,其中certolizumab聚乙二醇是其中的一员。未将塞妥珠单抗聚乙二醇用于小儿患者。
除其所需的作用外,certolizumab(Cimzia中包含的活性成分)可能会引起某些不良作用。尽管并非所有这些副作用都可能发生,但如果确实发生了,则可能需要医疗护理。
服用certolizumab时,如果有以下任何副作用,请立即与医生联系:
比较普遍;普遍上
不常见
罕见
发病率未知
certolizumab可能会发生一些通常不需要医疗的副作用。随着身体对药物的适应,这些副作用可能会在治疗期间消失。另外,您的医疗保健专业人员可能会告诉您一些预防或减少这些副作用的方法。
请咨询您的医疗保健专业人员,是否持续存在以下不良反应或令人讨厌,或者是否对这些副作用有任何疑问:
比较普遍;普遍上
不常见
适用于certolizumab:皮下试剂盒
罕见(0.1%至1%):血管炎,红斑狼疮
罕见(少于0.1%):血管神经性水肿,结节病,血清病,脂膜炎(包括结节性红斑)
罕见(少于0.1%):机会性感染,败血症,结核病和真菌感染(念珠菌病,组织胞浆菌病,肺囊虫病)
未报告频率:病毒感染(疱疹,乳头瘤病毒,流感),肺炎,结核病,蜂窝织炎,肾盂肾炎细菌和病毒感染,ANA滴度呈阳性[参考]
常见(1%至10%):高血压
罕见(0.1%至1%):心肌病(包括心力衰竭),缺血性冠状动脉疾病,心律不齐(包括房颤),心pit,高凝(包括血栓性静脉炎,肺栓塞),水肿(包括周围,面部),瘀斑(包括血肿,瘀斑)
未报告频率:心绞痛,心肌梗塞,心包积液,中风
稀有(小于0.1%):心包炎,房室传导阻滞,脑血管意外,动脉硬化,雷诺现象,网状网纹,毛细血管扩张
上市后报告:系统性血管炎[参考]
常见(1%至10%):上呼吸道感染,鼻咽炎,咽炎,急性支气管炎,肺炎,炎症
罕见(0.1%至1%):哮喘,胸腔积液,呼吸道充血,下呼吸道感染,口咽干燥,咳嗽
罕见(少于0.1%):间质性肺疾病,肺炎[参考]
普通(1%至10%):皮疹
罕见(0.1%至1%):脱发,牛皮癣新发或恶化(包括掌plant脓疱型牛皮癣)和相关疾病,皮炎和湿疹,汗腺疾病,皮肤溃疡,光敏性,痤疮,皮肤变色,皮肤干燥,指甲和指甲床疾病皮肤损伤
稀有(少于0.1%):皮肤脱落和脱皮,大疱状况,头发质地异常
未报告频率:蜂窝织炎,结节性红斑,荨麻疹,瘙痒
上市后报道:史蒂文斯-约翰逊综合征,中毒性表皮坏死溶解,多形性红斑[参考]
常见(1%至10%):尿路感染,肾盂肾炎
罕见(0.1%至1%):月经周期和子宫出血疾病(包括闭经),乳房疾病,血尿,膀胱症状,尿道症状
罕见(少于0.1%):性功能障碍[参考]
常见(1%至10%):嗜酸性粒细胞减少,白细胞减少(包括中性粒细胞减少,淋巴细胞减少)
罕见(0.1%至1%):贫血,淋巴结病,血小板减少症,血小板增多症,血液碱性磷酸酶增加,凝血时间延长
罕见(少于0.1%):全血细胞减少,脾肿大,红细胞增多,白细胞形态异常,血细胞减少(包括再生障碍性贫血),红细胞增多
未报告频率:血友病,出血,高凝,血肿,血尿酸增加,血胆红素增加[参考]
常见(1%至10%):肝炎(包括肝酶升高)
罕见(0.1%至1%):肝病(包括肝硬化),胆汁淤积
稀有(小于0.1%):乙肝病毒(HBV)活化,包括死亡
未报告频率:肝酶升高[参考]
罕见(0.1%至1%):药物超敏反应(包括过敏性休克),过敏性疾病,自身抗体阳性,血管性水肿,过敏性皮炎,头晕(姿势),呼吸困难,潮红,低血压,(血管迷走性)晕厥,自身抗体阳性[参考]
常见(1%至10%):结膜炎
罕见(0.1%至1%):视觉障碍(包括视力下降),眼和眼睑炎症,流泪障碍,视神经炎
未报告频率:视网膜出血,葡萄膜炎[参考]
罕见(0.1%至1%):血液和淋巴系统恶性肿瘤(包括淋巴瘤和白血病),实体器官肿瘤,非黑素瘤皮肤癌,癌前病变(包括口腔白斑,黑素细胞痣),良性肿瘤,囊肿(包括皮肤乳头状瘤)
罕见(少于0.1%):胃肠道肿瘤,黑色素瘤
未报告频率:默克尔细胞癌[参考]
罕见(0.1%至1%):焦虑,情绪障碍(包括相关症状),躁动不安
罕见(少于0.1%):自杀未遂,ir妄,精神障碍,躁郁症[参考]
罕见(0.1%至1%):肾功能不全
罕见(少于0.1%):肾病(包括肾炎) [参考]
常见(1%至10%):背痛,关节痛,肌肉痉挛,四肢疼痛
罕见(0.1%至1%):肌肉疾病,血肌酸磷酸激酶升高[参考]
常见(1%至10%):腹痛(包括上腹痛),腹泻,消化不良,胃炎,恶心
罕见(0.1%至1%):腹水,胃肠道感染,腹胀,胃肠道瘘管,吞咽困难,口咽干燥,运动过度,脾肿大,胰腺炎,牙齿感染,胃肠道溃疡和穿孔,胃肠道炎症(任何部位),
稀有(小于0.1%):胃肠道狭窄,胃肠道阻塞[参考]
常见(1%至10%):头痛(包括偏头痛),感觉异常
罕见(0.1%至1%):周围神经病变,头晕,震颤,眩晕,听觉神经炎,三叉神经痛,雷诺现象,颅神经发炎,颅神经损伤,感觉异常,感觉异常
罕见(少于0.1%):癫痫发作,临床症状加重和/或中枢神经系统脱髓鞘疾病(包括多发性硬化症)以及周围性脱髓鞘疾病(包括格林-巴利综合征)的放射学证据[参考]
常见(1%至10%):发热,疲劳,疼痛(任何部位),乏力,瘙痒(任何部位)
罕见(0.1%至1%):耳鸣,眩晕,发冷,温度感知改变,盗汗,潮红,愈合不良,不适,耳朵感染
罕见(小于0.1%):瘘(任何部位) [参考]
罕见(0.1%至1%):注射部位反应(红斑,瘙痒,血肿,疼痛,肿胀,瘀伤) [Ref]
罕见(0.1%至1%):电解质失衡,血脂异常,食欲不振,体重变化,电解质失衡,碱性磷酸酶水平升高
稀有(小于0.1%):血吸虫病[参考]
罕见(少于0.1%):甲状腺疾病[参考]
最常见的副作用是上呼吸道感染(18%),尿路感染(18%)和皮疹(9%) [参考]
1.“产品信息。Cimzia(certolizumab)。”乔治亚州士麦那市UCB Pharma Inc.
2. Cerner Multum,Inc.“澳大利亚产品信息”。 00
3.“ Certolizumab(Cimzia)用于克罗恩病” Med Lett Drugs Ther 50(2008):81-2
4. Cerner Multum,Inc.“英国产品特性摘要”。 00
某些副作用可能没有报道。您可以将其报告给FDA。
最初,第2周和第4周,成人银屑病关节炎患者的CIMZIA推荐剂量为400 mg(两次皮下注射,每次200 mg),然后每两周200 mg。对于维持剂量,可以考虑每4周服用CIMZIA 400 mg [请参阅临床研究(14.3)] 。
对于成年性强直性脊柱炎患者,CIMZIA的推荐剂量为最初(第2周和第4周)400 mg(两次皮下注射,每次200 mg),然后每2周200 mg或每4周400 mg。
的Cimzia冻干粉应做好准备,并通过卫生保健专业人士管理。 CIMZIA以包装形式提供,其中包含重构和注射药物所需的一切。下面提供了逐步的准备和管理说明。 CIMZIA冻干粉应由医疗保健专业人员制备和管理。 CIMZIA是在包装中提供的,其中包含重构和注射药物所需的一切[请参阅如何提供/存储和处理(16) ]。下面提供了逐步的准备和管理说明。
制备和储存
管理
接受皮下注射技术的适当培训后,如果医生确定合适的话,患者可以自行注射CIMZIA预填充注射器。
应指导患者使用CIMZIA预填充注射器,并按照《使用说明》手册中的说明将全部剂量的注射器(1 mL)注入注射器。
在开始使用CIMZIA治疗之前,必须对所有患者进行活动性和非活动性(潜伏性)结核感染评估。从结核病高发国家移民或旅行或与活动性结核病患者密切接触的患者应考虑未发现潜伏性结核病的可能性。所有患者均应进行适当的筛查检查(例如结核菌素皮肤检查和胸部X光检查)。
CIMZIA可用作单一疗法,或与非生物疾病改良抗风湿药(DMARD)并用。
不建议将CIMZIA与生物DMARD或其他肿瘤坏死因子(TNF)阻断剂联合使用。
严重感染
接受Cimzia治疗的患者发生严重感染的风险增加,可能导致住院或死亡[请参阅警告和注意事项(5.1)和不良反应(6.1) ] 。发生这些感染的大多数患者都在服用免疫抑制剂,例如甲氨蝶呤或皮质类固醇。
如果患者出现严重感染或败血症,应停止服用Cimzia。
报告的感染包括:
对于患有慢性或反复感染的患者,在开始治疗之前应仔细考虑使用Cimzia进行治疗的风险和益处。
在用Cimzia治疗期间和之后,应密切监测患者的感染迹象和症状的发展,包括在开始治疗前对潜伏性结核感染呈阴性的患者可能发生的结核病。 [请参阅警告和注意事项(5.1)和不良反应(6.1) ]。
犯罪
据报道,接受TNF受体阻滞剂治疗的儿童和青少年患者中淋巴瘤和其他恶性肿瘤具有致命性,其中Cimzia是其中的一员[见警告和注意事项(5.2) ]。 Cimzia未指定用于儿科患者。
Cimzia用于减轻克罗恩氏病的症状和体征,并维持对常规疗法反应不足的中度至重度活动性疾病成年患者的临床反应。
Cimzia适用于治疗中度至重度活动性类风湿关节炎(RA)的成人。
Cimzia用于治疗患有活动性银屑病关节炎(PsA)的成年患者。
Cimzia适用于治疗患有活动性强直性脊柱炎(AS)的成人。 [请参阅临床研究(14.4) ]
Cimzia通过皮下注射给药。应当旋转注射部位,并且不应将注射部位注入皮肤嫩,青肿,发红或坚硬的区域。当需要400 mg剂量时(两次皮下注射200 mg),应在大腿或腹部的不同部位进行注射。
给药前应仔细检查溶液中的颗粒物和变色。溶液应为无色至黄色透明液体,基本上无颗粒,如果混浊或存在异物,则不应使用。 Cimzia不包含防腐剂;因此,应将残留在注射器或小瓶中的未使用药物部分丢弃。
建议的初始成人Cimzia初始剂量为400 mg(两次皮下注射200 mg),并在第2周和第4周开始。对于获得临床反应的患者,推荐的维持方案为每四周400 mg。
成年类风湿关节炎患者的Cimzia推荐剂量最初为400毫克(两次皮下注射200毫克,在第2周和第4周注射),然后每两周200 mg。对于维持剂量,可以考虑每4周服用Cimzia 400 mg [请参阅临床研究(14.2) ] 。
成年银屑病关节炎患者的推荐Cimzia剂量为最初(第2周和第4周)400 mg(两次皮下注射,每次200 mg),然后每两周200 mg。对于维持剂量,可以考虑每4周服用Cimzia 400 mg [请参阅临床研究(14.3) ] 。
成年强直性脊柱炎患者的Cimzia推荐剂量为最初(第2周和第4周)400 mg(两次皮下注射,每次200 mg),然后每2周200 mg或每4周400 mg。
Cimzia冻干粉应由医疗保健专业人员制备和使用。 Cimzia装在包装中,其中包含重构和注射药物所需的一切。下面提供了逐步的准备和管理说明。 Cimzia冻干粉应由医疗保健专业人员制备和使用。 Cimzia是在包装中提供的,其中包含重构和注射药物所需的一切[请参阅供应/储存和处理方式(16) ]。下面提供了逐步的准备和管理说明。
准备和储存
行政
接受皮下注射技术的适当培训后,如果医生认为合适,患者可以自行注射Cimzia预填充注射器。
应指导患者使用Cimzia预填充注射器,并按照《使用说明》手册中的说明将全部量的注射器(1 mL)注入注射器。
在开始使用Cimzia进行治疗之前,必须对所有患者的活动性和非活动性(潜伏性)结核感染进行评估。从结核病高发国家移民或旅行或与活动性结核病患者密切接触的患者应考虑未发现潜伏性结核病的可能性。所有患者均应进行适当的筛查检查(例如结核菌素皮肤检查和胸部X光检查)。
Cimzia可用作单一疗法,或与非生物疾病改良抗风湿药(DMARDs)一起使用。
不建议将Cimzia与生物DMARD或其他肿瘤坏死因子(TNF)阻断剂联合使用。
注射用:冻干粉
无菌的白色冻干粉剂,可复原后皮下给药。每个一次性小瓶可提供约200毫克的Cimzia。
进样:预填充注射器
一次性使用的1 mL预填充玻璃注射器,带有固定的25号½英寸英寸薄壁针,每1 mL Cimzia提供200 mg。
没有。
[请参阅带框警告]
用Cimzia治疗的患者发生严重感染的风险增加,涉及各种器官系统和部位,可能导致住院或死亡。
TNF阻滞剂已报道由细菌,分枝杆菌,侵入性真菌,病毒,寄生虫或其他机会性病原体引起的机会性感染,包括曲霉菌病,芽孢杆菌病,念珠菌病,球虫病,组织胞浆菌病,军团病,李斯特菌病,肺囊虫病和结核病。患者经常表现为传播性疾病而非局部性疾病。
患有活动性感染(包括临床上重要的局部感染)的患者不应开始使用Cimzia进行治疗。年龄大于65岁的患者,合并症患者和/或同时服用免疫抑制剂(例如皮质类固醇或甲氨蝶呤)的患者感染的风险可能更高。在开始对患者进行治疗之前,应考虑治疗的风险和益处:
结核
在接受Cimzia的患者中,包括先前或同时接受过潜伏性或活动性肺结核治疗的患者中,已经观察到结核病重新激活或新的结核感染的病例。报告包括肺结核和肺外(即弥散性)结核病例。在开始Cimzia之前和治疗期间定期评估患者的结核病危险因素并进行潜伏性感染的研究。在接受Cimzia的患者中,包括先前或同时接受过潜伏性或活动性治疗的患者,发现了结核病重新激活或新发结核病的案例结核。报告包括肺结核和肺外(即弥散性)结核病例。在开始Cimzia之前和治疗期间定期评估患者的结核病危险因素并测试潜伏感染。
已显示在用TNF阻断剂治疗之前治疗潜伏性结核感染可降低治疗过程中结核再激活的风险。开始Cimzia之前,请评估是否需要治疗潜伏性结核;并考虑结核菌素皮肤试验阳性结果的硬结5 mm或更大,即使对于先前已接种Bacille Calmette-Guerin(BCG)的患者。
对于过去有潜伏性或活动性肺结核病史且无法确定适当治疗方案的患者,以及对于潜伏性结核病呈阴性反应但存在结核病感染危险因素的患者,考虑在开始Cimzia之前考虑抗结核治疗。尽管先前或同时进行过潜伏性结核治疗,但使用Cimzia治疗的患者仍发生活动性结核病。一些已经成功治疗活动性肺结核的患者在接受Cimzia治疗的同时又重新发展了结核病。建议咨询具有结核治疗专业知识的医生,以帮助决定是否开始抗结核治疗适合个别患者。
对于在Cimzia治疗期间发生新感染的患者,尤其是以前或最近去过结核病高发国家或与活动性结核病患者有密切接触的患者,强烈考虑结核病。在Cimzia治疗期间发生新感染的人,尤其是以前或最近去过结核病高发国家或与活动性结核病患者密切接触的患者。
监控方式
在用Cimzia治疗期间和之后,应密切监测患者的感染迹象和症状的发展,包括在开始治疗前对潜伏性结核感染测试呈阴性的患者的结核病发展。在用Cimzia进行治疗时,潜伏性结核感染的检测结果也可能是假阴性的。
如果患者出现严重感染或败血症,应停止服用Cimzia。在用Cimzia治疗期间发生新感染的患者应受到密切监测,并应针对免疫功能低下的患者进行迅速而全面的诊断检查,并应开始适当的抗菌治疗。
侵袭性真菌感染
对于在霉菌病流行地区居住或旅行的患者,如果他们发展为严重的全身性疾病,则应怀疑为侵袭性真菌感染。在进行诊断性检查时,应考虑采用适当的经验性抗真菌治疗。在某些活动性感染患者中,用于组织胞浆菌病的抗原和抗体检测可能为阴性。在可行的情况下,应对这些患者进行经验性抗真菌治疗的决定应咨询具有侵入性真菌感染的诊断和治疗经验的专业医生,并应考虑到严重真菌感染的风险和抗真菌治疗的风险。
在某些TNF阻滞剂的临床研究的对照部分中,与对照患者相比,在接受TNF阻滞剂的患者中观察到了更多的恶性肿瘤病例。在Cimzia的克罗恩氏病和其他疾病的对照和开放标签研究中,观察到的恶性肿瘤(不包括非黑素瘤皮肤癌)每100病人年中的恶性肿瘤(95%置信区间)为0.5(0.4,0.7)在1,319名接受安慰剂治疗的患者中,接受Cimzia治疗的患者为4,650名,而每100名患者-年的比率为0.6(0.1,1.7)。对照组的大小和受控部分的持续时间有限,因此无法得出肯定的结论。在某些TNF受体阻滞剂的临床研究的受控部分中,与相比,接受TNF阻滞剂的患者观察到更多的恶性肿瘤病例。控制病人。在Cimzia的克罗恩氏病和其他疾病的对照和开放标签研究中,观察到的恶性肿瘤(不包括非黑素瘤皮肤癌)每100病人年中的恶性肿瘤(95%置信区间)为0.5(0.4,0.7)在1,319名接受安慰剂治疗的患者中,接受Cimzia治疗的患者为4,650名,而每100名患者-年的比率为0.6(0.1,1.7)。对照组的大小和受控部分的持续时间有限,因此无法得出明确的结论。
据报导,接受Cimzia治疗的TNF阻断剂(治疗开始≤18岁)的儿童,青少年和年轻人恶性肿瘤是致命的。大约一半的病例是淋巴瘤,包括霍奇金淋巴瘤和非霍奇金淋巴瘤。其他病例代表各种不同的恶性肿瘤,包括通常与免疫抑制相关的罕见恶性肿瘤和儿童和青少年通常不观察到的恶性肿瘤。中位治疗30个月(范围1到84个月)后发生恶性肿瘤。大多数患者正在接受伴随的免疫抑制剂。这些案件是在上市后报告的,并来自各种来源,包括注册管理机构和自发的上市后报告。尚无Cimzia用于儿童患者的研究。据报道,接受TNF阻断剂治疗(开始治疗≤18岁)的儿童,青少年和年轻人中的恶性肿瘤是致命的。会员。大约一半的病例是淋巴瘤,包括霍奇金淋巴瘤和非霍奇金淋巴瘤。其他病例代表各种不同的恶性肿瘤,包括通常与免疫抑制相关的罕见恶性肿瘤和儿童和青少年通常不观察到的恶性肿瘤。中位治疗30个月(范围1到84个月)后发生恶性肿瘤。大多数患者正在接受伴随的免疫抑制剂。这些案例是在上市后报告的,并且来自各种来源,包括注册管理机构和自发的上市后报告。 Cimzia未指定用于儿科患者。
在所有TNF阻断剂的临床试验的对照部分中,与对照患者相比,在接受TNF阻断剂的患者中观察到更多的淋巴瘤病例。在针对Cimzia的克罗恩病和其他研究用途的对照研究中,在2657名接受Cimzia治疗的患者中有1例淋巴瘤,在1319例安慰剂治疗的患者中有1例霍奇金淋巴瘤。在所有TNF阻滞剂临床试验的对照部分中与对照组相比,在接受TNF阻滞剂治疗的患者中观察到更多的淋巴瘤病例。在针对Cimzia的克罗恩病和其他研究用途的对照研究中,在2657名接受Cimzia治疗的患者中有1例淋巴瘤,在1319例安慰剂治疗的患者中有1例霍奇金淋巴瘤。
在Cimzia RA临床试验(安慰剂对照和开放标签)中,在2367名患者中共观察到3例淋巴瘤。这比一般人群的预期值高约2倍。患有RA的患者,特别是患有高度活跃疾病的患者,罹患淋巴瘤的风险更高。在Cimzia RA临床试验中(安慰剂对照和开放标签),在2367名患者中共观察到三例淋巴瘤。这比一般人群的预期值高约2倍。 RA患者,特别是患有高活性疾病的患者,罹患淋巴瘤的风险更高。
Cimzia的临床研究比率无法与其他TNF阻滞剂的临床试验比率进行比较,并且可能无法预测将Cimzia用于更广泛的患者群体时观察到的比率。需要长期暴露于免疫抑制剂治疗的克罗恩病患者,即使没有TNF阻断剂治疗,其发生淋巴瘤的风险也可能比一般人群更高。 TNF阻断剂治疗在成人恶性肿瘤发展中的潜在作用尚不清楚。 Cimzia的临床研究比率无法与其他TNF阻滞剂的临床试验比率进行比较,并且可能无法预测将Cimzia用于更广泛的患者群体时观察到的比率。需要长期暴露于免疫抑制剂治疗的克罗恩病患者,即使没有TNF阻断剂治疗,其发生淋巴瘤的风险也可能比一般人群更高[见不良反应(6.1) ] 。 TNF阻断剂治疗在成人恶性肿瘤发展中的潜在作用尚不清楚。
据报道,使用Cimzia进行TNF受体阻滞剂治疗的患者,有肝脾T细胞淋巴瘤(HSTCL)上市后病例,这是一种罕见的T细胞淋巴瘤,具有很强的病程,通常是致命的。大部分报道的TNF阻滞剂病例发生在患有克罗恩氏病或溃疡性结肠炎的青春期和成年男性中。在诊断之前或诊断之前,几乎所有这些患者均接受了免疫抑制剂硫唑嘌呤和/或6-巯基嘌呤(6-MP)以及TNF阻断剂的治疗。尚不确定HSTCL的发生是否与TNF阻滞剂或TNF阻滞剂与这些其他免疫抑制剂联合使用有关。应慎重考虑将TNF阻滞剂与硫唑嘌呤或6-MP组合使用的潜在风险。肝脾T细胞淋巴瘤(HSTCL)的上市后案例是一种罕见的T细胞淋巴瘤,具有很强的病程,是在包括Cimzia在内的TNF受体阻滞剂治疗的患者中,通常会致命。大部分报道的TNF阻滞剂病例发生在患有克罗恩氏病或溃疡性结肠炎的青春期和成年男性中。在诊断之前或诊断之前,几乎所有这些患者均接受了免疫抑制剂硫唑嘌呤和/或6-巯基嘌呤(6-MP)以及TNF阻滞剂的治疗。尚不确定HSTCL的发生是否与TNF阻滞剂或TNF阻滞剂与这些其他免疫抑制剂联合使用有关。应仔细考虑将TNF阻滞剂与硫唑嘌呤或6-MP组合使用的潜在风险。
据报道,在RA和其他适应症中,上市后使用TNF-受体阻滞剂可导致急性和慢性白血病。即使没有TNF受体阻滞剂治疗,RA患白血病的风险也可能比一般人群高(约2倍)。据报道,上市后有急性和慢性白血病案例TNF阻滞剂用于RA和其他适应症。即使没有TNF受体阻滞剂治疗,RA患白血病的风险也可能比一般人群高(约2倍)。
在包括Cimzia在内的TNF拮抗剂治疗的患者中,已有黑色素瘤和默克尔细胞癌的报道。建议对所有患者进行定期皮肤检查,尤其是那些有皮肤癌危险因素的患者。
包括Cimzia在内的TNF阻滞剂已报道了充血性心力衰竭(CHF)和新发性CHF恶化的病例。 Cimzia尚未在CHF患者中进行正式研究。然而,在对患有另一种TNF阻滞剂的CHF患者的临床研究中,发现充血性心力衰竭(CHF)恶化且CHF导致死亡率增加。心力衰竭患者要格外小心,并仔细监测[见不良反应(6.1) ]。
服用Cimzia后很少报告以下可能与超敏反应相适应的症状:血管性水肿,呼吸困难,低血压,皮疹,血清病和荨麻疹。其中一些反应是在首次服用Cimzia之后发生的。如果发生此类反应,请停止进一步给予Cimzia并采取适当的治疗方法。目前尚无关于对另一种TNF阻断剂发生严重超敏反应的患者使用Cimzia的风险的数据。在这些患者中,需要谨慎[见不良反应(6.1) ] 。
TNF阻滞剂(包括Cimzia)的使用与慢性乙型肝炎病毒携带者的乙肝病毒(HBV)活化有关。在某些情况下,与TNF受体阻滞剂疗法联合发生的HBV再激活是致命的。大多数报告发生在同时接受抑制免疫系统的其他药物的患者中,这也可能有助于HBV的重新激活。
开始用Cimzia治疗之前,先测试患者的HBV感染情况。对于测试为HBV感染呈阳性的患者,建议咨询专业的乙肝治疗医生。关于抗病毒治疗结合TNF阻断剂治疗来预防HBV激活的HBV携带者患者的安全性或有效性,尚无足够的数据。 HBV携带者且需要Cimzia治疗的患者应在整个治疗过程中以及治疗终止后的几个月内密切监测活动性HBV感染的临床和实验室迹象。
在发生HBV激活的患者中,应停止Cimzia并开始进行有效的抗病毒治疗以及适当的支持治疗。在控制HBV激活后恢复TNF阻断剂治疗的安全性尚不清楚。因此,在这种情况下考虑恢复Cimzia治疗时应谨慎行事,并密切监视患者。
使用Cimzia成员的TNF阻滞剂与罕见的新发病例或临床症状的新发作或加重和/或中枢神经系统脱髓鞘疾病(包括多发性硬化症)和放射影像学证据,以及周围性脱髓鞘疾病(包括Guillain)有关-巴雷综合症。在已有或近期发作的中枢或周围神经系统脱髓鞘疾病的患者中考虑使用Cimzia时应谨慎行事。据报道,接受Cimzia治疗的患者很少见神经系统疾病,包括癫痫发作,视神经炎和周围神经病变[见不良反应(6.1) ] 。
TNF阻滞剂报道了罕见的全血细胞减少症,包括再生障碍性贫血。 Cimzia很少报道血液系统的不良反应,包括医学上重要的血细胞减少症(如白细胞减少症,全血细胞减少症,血小板减少症) [见不良反应(6.1) ] 。这些事件与Cimzia的因果关系仍不清楚。
尽管尚未确定高危人群,但在接受Cimzia治疗的患有持续性血液病或有明显血液学异常史的患者中要谨慎行事。劝告所有患者在服用Cimzia时出现迹象表明血液异常或感染(例如持续发烧,瘀伤,出血,苍白),应立即就医。对于已确认患有严重血液学异常的患者,请考虑停止Cimzia治疗。
在临床研究中发现严重感染是同时使用anakinra(一种白介素1拮抗剂)和另一种TNF阻断剂etanercept,与单独使用etanercept相比,没有其他好处。 TNF阻滞剂与阿巴西普和利妥昔单抗联合使用时,还发现了发生严重感染的较高风险。由于这种联合疗法所见的不良事件的性质,在这种联合疗法中使用辛西娅也可能产生类似的毒性。因此,不建议将Cimzia与其他生物DMARD组合使用[见药物相互作用(7.1) ]。
用Cimzia治疗可能会导致自身抗体的形成,很少会导致狼疮样综合征的发展。如果患者在用Cimzia治疗后出现暗示狼疮样综合征的症状,请停止治疗[见不良反应(6.1) ] 。
除活疫苗或减毒活疫苗外,接受奇姆齐亚治疗的患者都可以接种疫苗。尚无关于接受Cimzia的患者对活疫苗反应或活疫苗继发感染的反应的数据。
在风湿性关节炎患者的安慰剂对照临床试验中,当肺炎球菌多糖疫苗和流感疫苗与Cimzia并用时,Cimzia与安慰剂治疗组之间对疫苗的抗体反应未发现差异。 Cimzia和安慰剂治疗组之间有相似比例的患者产生了抗疫苗抗体的保护水平;然而,与仅接受Cimzia的患者相比,接受Cimzia和伴随的甲氨蝶呤的患者的体液反应较低。其临床意义尚不清楚。
由于TNF介导炎症并调节细胞免疫反应,因此包括Cimzia在内的TNF阻断剂可能会影响宿主抵抗感染和恶性肿瘤的防御能力。治疗与的Cimzia的开发,当然恶性肿瘤的影响,以及主动和/或慢性感染,尚不完全清楚[见警告和注意事项(5.1 , 5.2 , 5.5)和不良反应(6.1) ]。尚未正式评估Cimzia在免疫抑制患者中的安全性和有效性。
最严重的不良反应是:
由于临床研究是在广泛变化和可控制的条件下进行的,因此不能将在某种药物的临床研究中观察到的不良反应率直接与另一种药物的临床研究中观察到的不良反应率相比较,并且可能无法预测在更广泛的临床人群中观察到的不良反应率实践。
在所有患者人群的上市前对照试验中,最常见的不良反应(≥8%)是上呼吸道感染(18%),皮疹(9%)和尿路感染(8%)。
不良反应最常见的是导致在上市前对照试验中终止治疗
在对照的临床研究中,因不良反应而终止治疗的克罗恩病患者比例为Cimzia为8%,安慰剂为7%。导致Cimzia终止的最常见不良反应(至少2例患者,发生率高于安慰剂)是腹痛(Cimzia为0.4%,安慰剂为0.2%),腹泻(Cimzia为0.4%,安慰剂为0%)和肠梗阻(0.4%Cimzia,0%安慰剂)。
在对照的临床研究中,由于不良反应而停止治疗的类风湿关节炎患者的比例为Cimzia为5%,安慰剂为2.5%。导致Cimzia中断的最常见不良反应是结核感染(0.5%);和发热,荨麻疹,肺炎和皮疹(0.3%)。
克罗恩病对照研究
下文所述数据反映了在克罗恩氏病患者的研究中,皮下给药400 mg后对Cimzia的暴露。在对照研究的安全人群中,总共620名克罗恩病患者接受400 mg剂量的Cimzia,614名受试者接受安慰剂(包括在第0、2周接受Cimzia开放标签给药后随机分配至研究CD2中的安慰剂的受试者) ,4)。在对照和非对照研究中,有1,564名患者接受了一定剂量的Cimzia,其中1,350名患者接受了400 mg Cimzia。大约55%的受试者是女性,45%是男性,94%是白种人。活动组中的大多数患者年龄在18至64岁之间。
During controlled clinical studies, the proportion of patients with serious adverse reactions was 10% for Cimzia and 9% for placebo. The most common adverse reactions (occurring in ≥ 5% of Cimzia-treated patients, and with a higher incidence compared to placebo) in controlled clinical studies with Cimzia were upper respiratory infections (eg nasopharyngitis, laryngitis, viral infection) in 20% of Cimzia-treated patients and 13% of placebo-treated patients, urinary tract infections (eg bladder infection, bacteriuria, cystitis) in 7% of Cimzia-treated patients and in 6% of placebo-treated patients, and arthralgia (6% Cimzia, 4% placebo).
Other Adverse Reactions
The most commonly occurring adverse reactions in controlled trials of Crohn's disease were described above. Other serious or significant adverse reactions reported in controlled and uncontrolled studies in Crohn's disease and other diseases, occurring in patients receiving Cimzia at doses of 400 mg or other doses include:
Blood and lymphatic system disorders: Anemia, leukopenia, lymphadenopathy, pancytopenia, and thrombophilia.
Cardiac disorders: Angina pectoris, arrhythmias, atrial fibrillation, cardiac failure, hypertensive heart disease, myocardial infarction, myocardial ischemia, pericardial effusion, pericarditis, stroke and transient ischemic attack.
Eye disorders: Optic neuritis, retinal hemorrhage, and uveitis.
General disorders and administration site conditions: Bleeding and injection site reactions.
Hepatobiliary disorders : Elevated liver enzymes and hepatitis.
Immune system disorders : Alopecia totalis.
Psychiatric disorders: Anxiety, bipolar disorder, and suicide attempt.
Renal and urinary disorders: Nephrotic syndrome and renal failure.
Reproductive system and breast disorders: Menstrual disorder.
Skin and subcutaneous tissue disorders: Dermatitis, erythema nodosum, and urticaria.
Vascular disorders: Thrombophlebitis, vasculitis.
Controlled Studies with Rheumatoid Arthritis
Cimzia was studied primarily in placebo-controlled trials and in long-term follow-up studies. The data described below reflect the exposure to Cimzia in 2,367 RA patients, including 2,030 exposed for at least 6 months, 1,663 exposed for at least one year and 282 for at least 2 years; and 1,774 in adequate and well-controlled studies. In placebo-controlled studies, the population had a median age of 53 years at entry; approximately 80% were females, 93% were Caucasian and all patients were suffering from active rheumatoid arthritis, with a median disease duration of 6.2 years. Most patients received the recommended dose of Cimzia or higher.
Table 1 summarizes the reactions reported at a rate of at least 3% in patients treated with Cimzia 200 mg every other week compared to placebo (saline formulation), given concomitantly with methotrexate.
不良反应 (Preferred Term) | Placebo+ MTX * (%) N =324 | Cimzia 200 mg EOW + MTX(%) N =640 |
---|---|---|
| ||
Upper respiratory tract infection | 2 | 6 |
头痛 | 4 | 5 |
高血压 | 2 | 5 |
鼻咽炎 | 1个 | 5 |
背疼 | 1个 | 4 |
发热 | 2 | 3 |
咽炎 | 1个 | 3 |
皮疹 | 1个 | 3 |
Acute bronchitis | 1个 | 3 |
疲劳 | 2 | 3 |
Hypertensive adverse reactions were observed more frequently in patients receiving Cimzia than in controls. These adverse reactions occurred more frequently among patients with a baseline history of hypertension and among patients receiving concomitant corticosteroids and non-steroidal anti-inflammatory drugs.
Patients receiving Cimzia 400 mg as monotherapy every 4 weeks in rheumatoid arthritis controlled clinical trials had similar adverse reactions to those patients receiving Cimzia 200 mg every other week.
Other Adverse Reactions
Other infrequent adverse reactions (occurring in less than 3% of RA patients) were similar to those seen in Crohn's disease patients.
Psoriatic Arthritis Clinical Study
Cimzia has been studied in 409 patients with psoriatic arthritis (PsA) in a placebo-controlled trial. The safety profile for patients with PsA treated with Cimzia was similar to the safety profile seen in patients with RA and previous experience with Cimzia .
Ankylosing Spondylitis Clinical Study
Cimzia has been studied in 325 patients with axial spondyloarthritis of whom the majority had ankylosing spondylitis (AS) in a placebo-controlled study (AS-1). The safety profile for patients in study AS-1 treated with Cimzia was similar to the safety profile seen in patients with RA.
传染病
The incidence of infections in controlled studies in Crohn's disease was 38% for Cimzia-treated patients and 30% for placebo-treated patients. The infections consisted primarily of upper respiratory infections (20% for Cimzia, 13% for placebo). The incidence of serious infections during the controlled clinical studies was 3% per patient-year for Cimzia-treated patients and 1% for placebo-treated patients. Serious infections observed included bacterial and viral infections, pneumonia, and pyelonephritis.
The incidence of new cases of infections in controlled clinical studies in rheumatoid arthritis was 0.91 per patient-year for all Cimzia-treated patients and 0.72 per patient-year for placebo-treated patients. The infections consisted primarily of upper respiratory tract infections, herpes infections, urinary tract infections, and lower respiratory tract infections. In the controlled rheumatoid arthritis studies, there were more new cases of serious infection adverse reactions in the Cimzia treatment groups, compared to the placebo groups (0.06 per patient-year for all Cimzia doses vs. 0.02 per patient-year for placebo). Rates of serious infections in the 200 mg every other week dose group were 0.06 per patient-year and in the 400 mg every 4 weeks dose group were 0.04 per patient-year. Serious infections included tuberculosis, pneumonia, cellulitis, and pyelonephritis. In the placebo group, no serious infection occurred in more than one subject. There is no evidence of increased risk of infections with continued exposure over time [see Warnings and Precautions (5.1) ] .
Tuberculosis and Opportunistic Infections
In completed and ongoing global clinical studies in all indications including 5,118 Cimzia-treated patients, the overall rate of tuberculosis is approximately 0.61 per 100 patient-years across all indications.
The majority of cases occurred in countries with high endemic rates of TB. Reports include cases of miliary, lymphatic, peritoneal, as well as pulmonary TB. The median time to onset of TB for all patients exposed to Cimzia across all indications was 345 days. In the studies with Cimzia in RA, there were 36 cases of TB among 2,367 exposed patients, including some fatal cases. Rare cases of opportunistic infections have also been reported in these clinical trials [see Warnings and Precautions (5.1) ].
恶性肿瘤
In clinical studies of Cimzia, the overall incidence rate of malignancies was similar for Cimzia-treated and control patients. For some TNF blockers, more cases of malignancies have been observed among patients receiving those TNF blockers compared to control patients [see Warnings and Precautions (5.2) ].
心脏衰竭
In placebo-controlled and open-label rheumatoid arthritis studies, cases of new or worsening heart failure have been reported for Cimzia-treated patients. The majority of these cases were mild to moderate and occurred during the first year of exposure [see Warnings and Precautions (5.3) ].
Autoantibodies
In clinical studies in Crohn's disease, 4% of patients treated with Cimzia and 2% of patients treated with placebo that had negative baseline ANA titers developed positive titers during the studies. One of the 1,564 Crohn's disease patients treated with Cimzia developed symptoms of a lupus-like syndrome.
In clinical trials of TNF blockers, including Cimzia, in patients with RA, some patients have developed ANA. Four patients out of 2,367 patients treated with Cimzia in RA clinical studies developed clinical signs suggestive of a lupus-like syndrome. The impact of long-term treatment with Cimzia on the development of autoimmune diseases is unknown [see Warnings and Precautions (5.9) ].
Immunogenicity
Patients with Crohn's disease were tested at multiple time points for antibodies to certolizumab pegol during Studies CD1 and CD2. In patients continuously exposed to Cimzia,the overall percentage of patients who were antibody positive to Cimzia on at least one occasion was 8%; approximately 6% were neutralizing in vitro . No apparent correlation of antibody development to adverse events or efficacy was observed. Patients treated with concomitant immunosuppressants had a lower rate of antibody development than patients not taking immunosuppressants at baseline (3% and 11%, respectively). The following adverse events were reported in Crohn's disease patients who were antibody-positive (N = 100) at an incidence at least 3% higher compared to antibody-negative patients (N = 1,242): abdominal pain, arthralgia, edema peripheral, erythema nodosum, injection site erythema, injection site pain, pain in extremity, and upper respiratory tract infection.
In two long-term (up to 7 years of exposure), open-label Crohn's disease studies, overall 23% (207/903) of patients developed antibodies against certolizumab pegol on at least one occasion. Of the 207 patients who were antibody positive, 152 (73%) had a persistent reduction of drug plasma concentration, which represents 17% (152/903) of the study population. The data from these two studies do not suggest an association between the development of antibodies and adverse events.
The overall percentage of patients with antibodies to certolizumab pegol detectable on at least one occasion was 7% (105 of 1,509) in the rheumatoid arthritis placebo-controlled trials. Approximately one third (3%, 39 of 1,509) of these patients had antibodies with neutralizing activity in vitro . Patients treated with concomitant immunosuppressants (MTX) had a lower rate of antibody development than patients not taking immunosuppressants at baseline. Patients treated with concomitant immunosuppressant therapy (MTX) in RA-I, RA-II, RA-III had a lower rate of neutralizing antibody formation overall than patients treated with Cimzia monotherapy in RA-IV (2% vs. 8%). Both the loading dose of 400 mg every other week at Weeks 0, 2 and 4 and concomitant use of MTX were associated with reduced immunogenicity.
Antibody formation was associated with lowered drug plasma concentration and reduced efficacy. In patients receiving the recommended Cimzia dosage of 200 mg every other week with concomitant MTX, the ACR20 response was lower among antibody positive patients than among antibody-negative patients (Study RA-I, 48% versus 60%; Study RA-II 35% versus 59%, respectively). In Study RA-III, too few patients developed antibodies to allow for meaningful analysis of ACR20 response by antibody status. In Study RA-IV (monotherapy), the ACR20 response was 33% versus 56%, antibody-positive versus antibody-negative status, respectively [see Clinical Pharmacology (12.3) ]. No association was seen between antibody development and the development of adverse events.
The data reflect the percentage of patients whose test results were considered positive for antibodies to certolizumab pegol in an ELISA, and are highly dependent on the sensitivity and specificity of the assay. The observed incidence of antibody (including neutralizing antibody) positivity in an assay is highly dependent on several factors, including assay sensitivity and specificity, assay methodology, sample handling, timing of sample collection, concomitant medications, and underlying disease. For these reasons, comparison of the incidence of antibodies to certolizumab pegol with the incidence of antibodies to other products may be misleading.
过敏反应
The following symptoms that could be compatible with hypersensitivity reactions have been reported rarely following Cimzia administration to patients: angioedema, dermatitis allergic, dizziness (postural), dyspnea, hot flush, hypotension, injection site reactions, malaise, pyrexia, rash, serum sickness, and (vasovagal) syncope [see Warnings and Precautions (5.4) ] .
The following adverse reactions have been identified during post-approval use of Cimzia.由于这些反应是从不确定大小的人群中自愿报告的,因此并非总是能够可靠地估计其发生频率或建立与药物暴露的因果关系。
Vascular disorder : systemic vasculitis has been identified during post-approval use of TNF blockers.
Skin : case of severe skin reactions, including Stevens-Johnson syndrome, toxic epidermal necrolysis, erythema multiforme, and new or worsening psoriasis (all sub-types including pustular and palmoplantar) have been identified during post-approval use of TNF blockers.
Immune System Disorders : sarcoidosis
Neoplasms benign, malignant and unspecified (including cysts and polyps): Melanoma, Merkel cell carcinoma (neuroendocrine carcinoma of the skin) [see Warnings and Precautions (5.2) ].
An increased risk of serious infections has been seen in clinical studies of other TNF-blocking agents used in combination with anakinra or abatacept, with no added benefit. Formal drug interaction studies have not been performed with rituximab or natalizumab. Because of the nature of the adverse events seen with these combinations with TNF blocker therapy, similar toxicities may also result from the use of Cimzia in these combinations. There is not enough information to assess the safety and efficacy of such combination therapy. Therefore, the use of Cimzia in combination with anakinra, abatacept, rituximab, or natalizumab is not recommended [see Warnings and Precautions (5.8) ] .
Avoid use of live (including attenuated) vaccines concurrently with Cimzia [see Warnings and Precautions (5.10) ] .
Interference with certain coagulation assays has been detected in patients treated with Cimzia. Certolizumab pegol may cause erroneously elevated activated partial thromboplastin time (aPTT) assay results in patients without coagulation abnormalities. This effect has been observed with the PTT-Lupus Anticoagulant (LA) test and Standard Target Activated Partial Thromboplastin time (STA-PTT) Automate tests from Diagnostica Stago, and the HemosIL APTT-SP liquid and HemosIL lyophilized silica tests from Instrumentation Laboratories. Other aPTT assays may be affected as well. Interference with thrombin time (TT) and prothrombin time (PT) assays has not been observed. There is no evidence that Cimzia therapy has an effect on in vivo coagulation.
怀孕暴露登记
There is a pregnancy exposure registry that monitors pregnancy outcomes in women exposed to Cimzia during pregnancy. For more information, healthcare providers or patients can contact:
MotherToBaby Pregnancy Studies conducted by the Organization of Teratology Information Specialists (OTIS). The OTIS AutoImmune Diseases Study at 1-877-311-8972 or visit http://mothertobaby.org/pregnancy-studies/
风险摘要
Limited data from the ongoing pregnancy registry on use of Cimzia in pregnant women are not sufficient to inform a risk of major birth defects or other adverse pregnancy outcomes. Certolizumab pegol plasma concentrations obtained from 10 women treated with Cimzia during pregnancy and their newborn infants demonstrated low placental transfer of certolizumab pegol. Cimzia may be eliminated at a slower rate in exposed infants than in adult patients [see Data ] . There are risks to the mother and fetus associated with active rheumatoid arthritis or Crohn's disease. The theoretical risks of administration of live or live-attenuated vaccines to the infants exposed in utero to Cimzia should be weighed against the benefits of vaccinations [see Clinical Considerations ] . No adverse developmental effects were observed in animal reproduction studies during which pregnant rats were administered intravenously a rodent anti-murine TNFα pegylated Fab' fragment (cTN3 PF) similar to certolizumab pegol during organogenesis at up to 2.4 times the recommended human dose of 400 mg per month.
The estimated background risk of major birth defects and miscarriage for the indicated population(s) are unknown.所有怀孕都有出生缺陷,流产或其他不良后果的背景风险。 In the US general population, the estimated background risks of major birth defects and miscarriage in clinically recognized pregnancies are 2-4% and 15-20%, respectively.
临床注意事项
与疾病相关的孕产妇和/或胚胎/胎儿风险
Published data suggest that the risk of adverse pregnancy outcomes in women with rheumatoid arthritis or Crohn's disease is correlated with maternal disease activity and that active disease increases the risk of adverse pregnancy outcomes, including fetal loss, preterm delivery (before 37 weeks of gestation), low birth weight (<2500 g) and small for gestational age birth.
胎儿/新生儿不良反应
Due to its inhibition of TNFα, Cimzia administered during pregnancy could affect immune responses in the in utero -exposed newborn and infant. Although certolizumab pegol levels were low in 12 infants exposed to Cimzia in utero , the clinical significance of these low levels is unknown. Additional data available from one exposed infant suggests that Cimzia may be eliminated at a slower rate in infants than in adults [see Data ]. The safety of administering live or live-attenuated vaccines in exposed infants is unknown.
数据
人数据
A limited number of pregnancies have been reported in the ongoing pregnancy exposure registry. Due to the small number of Cimzia-exposed pregnancies with known outcomes (n=23), no meaningful comparisons between the exposed group and control groups may be conducted to determine an association with Cimzia and major birth defects or adverse pregnancy outcomes.
In an independent clinical study conducted in 10 pregnant women with Crohn´s disease treated with Cimzia, certolizumab pegol concentrations were measured in maternal blood as well as in cord and infant blood (n=12) at the day of birth. The last dose of Cimzia (400 mg for every mother) was given on average 19 days prior to delivery (range 5-42 days). Plasma certolizumab pegol concentrations were <0.41 –1.66 μg/mL in cord blood, <0.41 – 1.58 μg/mL in infant blood, and 1.87–59.57 μg/mL in maternal blood. Plasma certolizumab pegol concentrations were lower (by at least 75%) in the infants than in mothers suggesting low placental transfer of certolizumab pegol. In one infant, the plasma certolizumab pegol concentration declined from 1.02 to 0.84 μg /mL over 4 weeks suggesting that Cimzia may be eliminated at a slower rate in infants than adults.
动物资料
Because certolizumab pegol does not cross-react with mouse or rat TNFα, reproduction studies were performed in rats using a rodent anti-murine TNFα pegylated Fab' fragment (cTN3 PF) similar to certolizumab pegol. Animal reproduction studies have been performed in rats during organogenesis at intravenous doses up to 100 mg/kg (about 2.4 times the recommended human dose of 400 mg, based on the surface area) and have revealed no evidence of harm to the fetus due to cTN3 PF.
风险摘要
No data are available regarding the presence of certolizumab pegol in human milk, the effects on the breast fed infant, or the effects on milk production. Published data suggest that the systemic exposure to a breastfed infant is expected to be low because certolizumab pegol is a large molecule and is degraded in the gastrointestinal tract. However, if certolizumab pegol is transferred into human milk, effects of local exposure in the gastrointestinal tract are unknown.
The developmental and health benefits of breastfeeding should be considered along with the mother's clinical need for Cimzia and any potential adverse effects on the breastfed child from Cimzia or from the underlying maternal condition.
儿科患者的安全性和有效性尚未确定。 Due to its inhibition of TNFα, Cimzia administered during pregnancy could affect immune responses in the in utero -exposed newborn and infant [see Use in Specific Populations (8.1) ].
Clinical studies of Cimzia did not include sufficient numbers of patients aged 65 and over to determine whether they respond differently from younger subjects.其他报告的临床经验尚未发现老年患者和年轻患者在反应方面的差异。 Population pharmacokinetic analyses of patients enrolled in Cimzia clinical studies concluded that there was no apparent difference in drug concentration regardless of age. Because there is a higher incidence of infections in the elderly population in general, use caution when treating the elderly with Cimzia [see Warnings and Precautions (5.1) ] .
The maximum tolerated dose of certolizumab pegol has not been established. Doses of up to 800 mg subcutaneous and 20 mg/kg intravenous have been administered without evidence of dose-limiting toxicities. In cases of overdosage, it is recommended that patients be monitored closely for any adverse reactions or effects, and appropriate symptomatic treatment instituted immediately.
Cimzia (certolizumab pegol) is a TNF blocker. Cimzia is a recombinant, humanized antibody Fab' fragment, with specificity for human tumor necrosis factor alpha (TNFα), conjugated to an approximately 40kDa polyethylene glycol (PEG2MAL40K). The Fab' frag
已知共有382种药物与Cimzia(certolizumab)相互作用。
查看Cimzia(certolizumab)与下列药物的相互作用报告。
与Cimzia(certolizumab)有7种疾病相互作用,包括:
具有高度临床意义。避免组合;互动的风险大于收益。 | |
具有中等临床意义。通常避免组合;仅在特殊情况下使用。 | |
临床意义不大。降低风险;评估风险并考虑使用替代药物,采取措施规避相互作用风险和/或制定监测计划。 | |
没有可用的互动信息。 |