Analysis of Data on Adverse Drug Events Reported to the Food and Drugs Administration of the United States of America

Background: The Spontaneous Reporting System (SRS) of the Food and Drugs Administration (FDA) of the United States of America (US), known as the FDA Adverse Event Reporting System (FAERS), is a mechanism for collecting information on safety concerns associated with the use of drugs for redress, as they are used on large scale. The data which is the subject of this paper came from the FAERS database. This paper reports on the analysis of data covering 2013 to 2018 period, but compares the observed trends in the variables during this period with that of the 2007 to 2012 period to ascertain whether the trends change over time;as this paper is, in a sense, a sequel to an earlier one with a similar title as this but covering the period 2007 to 2012. Objectives: The objectives of the study reported in this paper were to: i) explore the trends in the variables involved with the adverse events problem in the 2013 to 2018 period and compare these trends with that found in the study covering the 2007 to 2012 period;ii) determine whether or not the level of missing variable values in the 2013 to 2018 period is lower than, the same or higher than it was in the 2007 to 2012 period;iii) find out how the first twenty principal suspect drugs most cited to be involved in adverse events occurring during drug use in the 2013 to 2018 period compare with that of the 2007 to 2012 period. Methods: The Food and Drugs Administration (FDA) makes extracts from the FAERS database freely available to the public on quarterly basis. Fourteen (14) out of over fifty (50) variables contained in these extracts were reckoned to be connected with the objectives of the study and were examined using the tools of frequencies, proportions and averages, on account of the nature of the data. Results: For the period 2013 to 2018, adverse events reports submitted to the FDA (US) more than doubled (2.1 times), accounting for an annual average growth rate of 15.8 %, which is considerably lower than the annual average growth rate of 22.1% for the 2007 to 2012 period. However, the reported number of cases for 2015 was 53.8% more than that of 2014. Consistent with the results for 2007 to 2012 period, the 2013 to 2018 period saw Female subjects accounting for over 60% of the annual and the overall number of reports. Overall, non-health professionals appear to have a slight edge over health professionals in reporting adverse drug events in the 2013 to 2018 period, with an indication that reports from non-health professionals are on the decline and that from health professionals is on the rise. Non-health professionals and health professionals were almost equally likely to report adverse events in the 2007 to 2012 period. Also, the findings for the 2013 to 2018 period suggest that the older one gets the more vulnerable one becomes to adverse events associated with drug use, which is consistent with the findings for the 2007 to 2012 period. Conclusion: The dangers that come with the use of drugs is an evolving one and therefore there is the need to examine SRS data from time to time so that emerging drug safety concerns can be dealt with timeously.

Analysis of Adverse Drug Reactions Caused by Chinese Patent Medicine Treatment Based on Kidney Damp-heat Syndrome and Damp-turbidity Syndrome

[Objectives]To determine relationship of the adverse drug reaction(ADR)occurrence of the single use and combined use of Huangkui Capsule and Haikun Shenxi Capsule.[Methods]To determine relationship of the ADR occurrence of the single use and combined use of Huangkui Capsule and Haikun Shenxi Capsule.[Results]The main adverse drug reactions of the single use of Huangkui Capsule or Haikun Shenxi Capsule was severe diarrhea(n=7,n=9),however the combined use of the two resulted in more occurrence of adverse drug reactions(n=23)with significant difference in contrast to the single use group(P=0.0015,P=0.0069).[Conclusions]When traditional Chinese patent medicines are used in combination to treat kidney damp-heat syndrome and damp-turbid syndrome,it is necessary to pay close attention to the occurrence of adverse drug reactions,especially the digestive system.

Analysis of the adverse reactions of atezolizumab: A real-world study based on FAERS database

Objective In this study,we aimed to determine the incidence of adverse drug reactions(ADRs)of atezolizumab,identify ADR signals that are significantly related to atezolizumab,and provide a reference for the rational use of atezolizumab in the clinic through the statistical analysis of its adverse drug events(ADEs)reported in the American Food and Drug Administration(FDA)Adverse Event Reporting System(FAERS)database.Methods In total,4796 cases of atezolizumab ADEs reported in the American FAERS database from 2017 to 2019 were retrospectively analyzed.Results The top three ADEs were febrile neutropenia(3.7%),anemia(2.9%),and acute renal failure(2.3%).In addition,the incidence rates of some ADEs were significantly different according to sex and age.The systematic organ classification of atezolizumab ADEs involved 32 systems,among which the top three were blood and lymphatic system disorders(585 cases,12.2%),gastrointestinal disorders(433 cases,9.0%),and infections and infestations(401 cases,8.4%).The reporting odds ratio(ROR)method was used to detect the ADR signals of atezolizumab.The ROR(95%confidence interval)of the top ADE,febrile neutropenia,was 39.236(33.757–45.604).In addition,we found 121 cases of complications associated with immune-related ADEs.Conclusion The ADRs of atezolizumab reported in the FAERS database were consistent with those mentioned in the instructions for atezolizumab use,suggesting that atezolizumab has an acceptable and controllable drug effect.

Systematic review on the adverse reactions of oral administration of Indigo Naturalis and its preparations

Objective:This article systematically analyses the effects of adverse drug events/adverse drug reactions(ADEs/ADRs)of oral Indigo Naturalis(Qingdai)preparations in order to provide references for its rational clinical application.Methods:All clinical studies reporting ADE/ADR related to the oral administration of Qingdai preparations were searched through electronic databases,including PubMed,the Cochrane Library,Embase,China National Knowledge Infrastructure(CNKI),China Biology Medicine disc(CBM),VIP Information Chinese Journal Service Platform(VIP),and Wanfang database,from inception to September 27,2020.Information were extracted from these literatures,including primary disease,type of adverse reactions,dose,treatment,outcomes and so on.Incidence of ADE/ADR was estimated,as well as distribution of primary diseases and victim organs and systems were analyzed.Results:A total of 682 articles were included,with 651 clinical population studies and 31 case reports.Among them,604 detailed ADR/AE involving 33459 patients using oral Qingdai preparations,and a total of 5061 cases were found to present adverse events,including 2827 cases of digestive system(abdominal pain,diarrhea,etc.),469 cases of blood system damage(thrombocytopenia,leukopenia,anemia,etc.),313 cases of liver damage(abnormal liver function,liver toxicity,elevated liver enzymes,etc.),327 cases of nervous system reactions(headache,dizziness,poor sleep,etc.)and 1186 cases of other systems and organs.Severe adverse events(SAEs)mainly were liver damage,and could be relived after symptomatic treatment.Conclusion:From the systematic information retrieval and analysis,it is found that oral Qingdai preparations application may clinically cause ADEs/ADRs in terms of gastrointestinal tract and liver damage.Therefore,when using oral Qingdai preparations,liver and stomach protection should be done.At the same time,pay close attention to various biochemical indicators and the patient's drug response during the treatment process,and,if necessary,deal with it in time so as not to deteriorate the condition.Moreover,active surveillance system should be conducted to monitor ADE/ADR,so as to establish a clearer causal relationship between the drug and the adverse event.

基于FAERS数据库的奥马珠单抗不良事件信号挖掘

目的运用数据挖掘的方法检测奥马珠单抗上市后的不良反应信号,为临床安全合理用药提供参考。方法本研究采用报告比值比法(ROR)和贝叶斯判别可信区间递进神经网络法(BCPNN)对美国FDA不良事件报告系统(FAERS)中2004年第1季度至2023年第2季度的奥马珠单抗相关不良事件(ADE)报告进行数据挖掘和信号检测。结果通过数据挖掘和信号检测,涉及奥马珠单抗的ADE报告中提取了186,353份报告,涉及45,383例患者。在这些报告中,女性(65.31%)比例远高于男性(24.97%)。主要报告国家为美国(64.93%)和加拿大(11.96%)。报告者中以消费者(41.35%)和医师(36.97%)为主要群体。研究发现了621个ADE阳性信号,涉及25个系统器官分类(SOC),主要包括呼吸系统、胸部和纵隔疾病(21.29%)以及感染和侵染类疾病(10.91%)。其中,183个信号被评定为高风险信号,其中包括57个新的高风险信号,如血压升高、易醒型失眠和心律失常等。这些发现有助于更全面地了解奥马珠单抗的安全性和潜在风险。结论在奥马珠单抗的临床应用过程中,除了要注意药品说明中提到的已知不良反应外,还需特别警惕潜在的不良药物事件,如血压升高、心率升高、中间易醒型失眠、体位性心动过速综合征等。

基于FAERS数据库的维泊妥珠单抗不良反应信号挖掘

目的:评价和分析维泊妥珠单抗上市后的药物不良反应(adverse drug reaction,ADR)信号,为临床安全性管理提供参考。方法:通过开放性OpenVigil数据平台,收集2019年6月10日(美国FDA批准上市时间)至2023年3月31日美国FDA不良事件报告系统(FAERS)数据库中维泊妥珠单抗的ADR报告。采用比例失衡法中的报告比值比(ROR)和比例报告比(PRR)进行信号挖掘。为提高阈值,得到信号较强、较常出现的ADR,将信号进行二次筛选。结果:共检索到维泊妥珠单抗相关ADR报告2408份,经过二次筛选得到83个ADR信号。其中,脊柱磁共振成像异常、骨吸收增加、骨质溶解、天门冬氨酸氨基转移酶降低、丙氨酸氨基转移酶降低、低纤维蛋白原血症、肺栓塞等26个ADR信号在药品说明书中未提及。信号数或累积例数较多的系统器官分类包含感染及侵染类疾病(24个信号、632例),各类检查(17个信号、675例),血液及淋巴系统疾病(11个信号、734例),各类神经系统疾病(7个信号、153例),免疫系统疾病(3个信号、95例),全身性疾病及给药部位各种反应(2个信号、145例),代谢及营养类疾病(2个信号、87例)等。结论:除说明书提示的常见ADR外,本研究发现了维泊妥珠单抗新的ADR风险信号。建议临床在关注感染、骨髓抑制、周围神经病、输液相关反应、肝功能异常等已知常见ADR的同时,予以脊柱磁共振成像异常、骨吸收增加等新的风险信号更多关注。

Clinical decision support for drug related events: Moving towards better prevention

Clinical decision support(CDS) systems with automated alerts integrated into electronic medical records demonstrate efficacy for detecting medication errors(ME) and adverse drug events(ADEs). Critically ill patients are at increased risk for ME, ADEs and serious negative outcomes related to these events. Capitalizing on CDS to detect ME and prevent adverse drug related events has the potential to improve patient outcomes. The key to an effective medication safety surveillance system incorporating CDS is advancing the signals for alerts by using trajectory analyses to predict clinical events, instead of waiting for these events to occur. Additionally, incorporating cutting-edge biomarkers into alert knowledge in an effort to identify the need to adjust medication therapy portending harm will advance the current state of CDS. CDS can be taken a step further to identify drug related physiological events, which are less commonly included in surveillance systems. Predictive models for adverse events that combine patient factors with laboratory values and biomarkers are being established and these models can be the foundation for individualized CDS alerts to prevent impending ADEs.

基于美国FAERS数据库的右佐匹克隆不良事件信号挖掘与分析

目的:分析右佐匹克隆上市后的药品不良反应(ADR)信号,为临床用药安全提供参考。方法:利用美国食品药品监督管理局不良事件报告系统(FAERS)数据库,使用OpenVigil 2.1数据平台,收集右佐匹克隆从美国上市至2023年3月31日的ADR报告。采用频率法检测右佐匹克隆的ADR信号,并分别按照发生频次和信号强度进行排序。结果:获得右佐匹克隆相关的ADR报告9131份,检测到ADR信号分别为77个。按发生频次排序,发生最多的ADR是味觉障碍(3162例),可见于其药品说明书,自杀意念在药品说明书中未出现;按信号强度排序,右佐匹克隆的入睡困难(报告比值比为225.402)位列首位,毛发稀少未被其药品说明书提及。结论:建议临床不仅应关注药物最常见的精神系统系统ADR,还应关注药品说明书中未报道的ADR。

基于FAERS的阿替利珠单抗与度伐利尤单抗不良反应信号挖掘与分析

目的为临床安全使用阿替利珠单抗和度伐利尤单抗提供参考。方法利用OpenVigil 2.1平台,从美国食品和药物管理局不良事件报告系统(FAERS)中提取2016年1月1日至2023年9月30日有关阿替利珠单抗和度伐利尤单抗的药品不良事件(ADE)报告;采用《监管活动医学词典》(MedDRA 24.0)对首选语进行系统器官分类(SOC)匹配;采用报告比值比(ROR)法和比例报告比值(PRR)法挖掘药品不良反应(ADR)信号。结果共获得ADE报告19835份(涉及患者19835例),其中阿替利珠单抗13420份(13420例),度伐利尤单抗6415份(6415例);ADR信号,阿替利珠单抗814个,度伐利尤单抗315个,其中未在药品说明书中提及的均为49个,分别为自身免疫性心肌炎、暴发性1型糖尿病,放射性食管炎、支气管瘘等。共获得192个重叠ADR信号,其中胃肠系统疾病21个,呼吸系统、胸及纵隔疾病21个,各类检查18个,皮肤及皮下组织类疾病18个;阿替利珠单抗发生周围感觉神经病的信号强度远大于度伐利尤单抗(ROR值相差近5倍),度伐利尤单抗发生放射性肺炎、胆道感染、美国东部肿瘤协作组体能状态下降、浅表血栓性静脉炎的信号强度远大于阿替利珠单抗(ROR值相差5~77倍)。结论临床应加强对阿替利珠单抗和度伐利尤单抗主要ADR及差异ADR的认识,重点关注药品说明书中未提及但信号强且易导致不良后果的ADR,从而促进该类药物的临床安全使用。

基于FAERS数据库分析波生坦药物不良事件

目的:基于美国食品药品监督管理局不良事件报告系统(FAERS),挖掘波生坦不良事件信号,判断其安全性,以期临床安全用药提供参考。方法:选取FAERS数据库2016年1季度~2022年2季度数据信息,比照MedDRA不良事件编码处理数据,提取以波生坦为首要怀疑药品的不良事件报告,采取比例报告比值法(PRR)和报告比值法(ROR)对信号进行分析。结果:以波生坦为首要怀疑药品的不良事件报告中,女性占比(61.51%)高于男性(21.40%);通过对器官系统分类(SOC)分析发现波生坦产生不良反应主要集中在全身性疾病及给药部位各种反应、呼吸系统、胸及纵隔疾病、感染及侵染类疾病;对首选语(PT)分析发现呼吸困难、死亡、感染性肺炎的发生排在前3位;对低位语(LLT)分析发现波生坦易导致死亡、基因突变、肺水肿等不良事件的发生。结论:通过对FAERS数据库中波生坦不良反应的挖掘,从SOC、PT、LLT 3个层次分析了不良事件特点,为波生坦在临床中的安全使用提供了参考依据。

基于美国FAERS和日本JADER数据库的内皮素受体拮抗剂不良事件信号分析

目的 分析马昔腾坦、安立生坦和波生坦不良事件发生特点,为临床选择内皮素受体拮抗剂提供参考。方法 基于美国食品药品监督管理局(FDA)不良事件报告系统(adverse event reporting system, FAERS)和日本药品不良事件报告数据库(Japanese adverse drug event report database,JADER)中2013年10月1日至2023年12月31日以马昔腾坦、安立生坦、波生坦为首要怀疑药品的所有不良事件报告,采用ROR法和IC法对内皮素受体拮抗剂相关不良事件信号进行计算,筛选阳性信号进行对比分析。采用Log-rank检验和非参数检验比较内皮素受体拮抗剂相关不良事件诱发时间差异性。结果 基于2个数据库共获得马昔腾坦不良事件报告35 150例、安立生坦75 177例、波生坦22707例。马昔腾坦、安立生坦的诱发贫血在JADER中报告数量最多,马昔腾坦、安立生坦、波生坦诱发液体潴留在FAERS中报告数量最多。波生坦肝功能异常相关信号强度显著高于马昔腾坦和安立生坦。马昔腾坦贫血相关不良事件信号强度显著高于安立生坦和波生坦。安立生坦液体潴留相关信号强度显著高于马昔腾坦和波生坦。对未成年患者进行不良事件信号挖掘发现,波生坦相较其他内皮素受体拮抗剂更容易诱发未成年患者肝功能检验异常,安立生坦更容易诱发未成年患者鼻咽不适。未成年患者使用马昔腾坦应重点关注贫血、血小板降低、肝功能指标异常、鼻衄、血压降低、低钾血症。马昔腾坦联合一氧化氮受体拮抗剂[173(IQR 40~544)]不良事件诱发时间最短,波生坦联合前列环素受体拮抗剂[632.5(IQR 222.75~1225.5)]不良事件诱发时间最长。结论 不同内皮素受体拮抗剂不良事件风险信号强度和不良事件诱发时间可能存在差异。对患者应开展个体化用药和监护,减少可能的不良反应,保障患者用药安全。

基于美国FAERS数据库的利培酮不良事件信号挖掘与分析

目的 为利培酮的临床安全使用提供参考。方法 采用报告比值比法与英国药品和保健品管理局综合标准法,对美国FDA不良事件报告系统(FAERS)数据库中2017年第1季度至2021年第3季度共19个季度的利培酮相关药品不良事件(ADE)报告进行数据挖掘与分析。结果 获得以利培酮为首要怀疑药物的ADE报告共计101 181份,涉及患者33 179例。所统计的报告中,男女比约为6.21∶1;以<18岁的患者居多(占15.01%);上报ADE者主要为消费者(占69.74%),上报国家主要为美国(占79.72%);使用口服剂型的患者最多(占83.71%)。共产生ADE信号409个,包括男性乳腺发育、假性男性乳房发育症、体质量异常增加、高催乳素血症和Wellens综合征等;涉及26个系统器官分类,主要为生殖系统及乳腺疾病,各类损伤、中毒及操作并发症,精神病类,代谢及营养类疾病,各类神经系统疾病等。结论 利培酮常见ADE信号及其累及系统器官与说明书基本一致,但也要警惕其说明书中未记载的ADE,如Wellens综合征、纤维增生性心内膜炎、门静脉海绵样变性、兔子综合征等。

地舒单抗的肌肉骨骼相关毒性:基于FAERS对地舒单抗不良反应信号的挖掘与分析

目的 评价地舒单抗的安全警戒信号,为临床安全用药提供参考。方法 调取美国FDA不良事件报告系统(FAERS)中地舒单抗在美国上市后连续46个季度的数据,采用报告比值比法(ROR)和比例报告比值法(PRR)进行信号挖掘,以分析其不良反应的发生情况。结果 得到的602个不良反应信号表明,肌肉骨骼疾病是发生频率和强度最高的不良反应类型,对SOC项下“肌肉骨骼及结缔组织疾病”进行了分析,结果显示主要的不良反应包括颌骨骨坏死、关节痛、肢体疼痛、背痛、肌痛、骨痛等,这些都有在说明书中记录,同时还发现了一些未被记录在说明书中的不良反应,例如颌骨外生性骨疣、颌部瘘管、动脉瘤样骨囊肿,颌骨疼痛、肌痉挛等。结论 临床上常应用地舒单抗治疗骨质疏松和骨肿瘤等骨骼相关疾病,但是该药的骨骼相关不良反应发生的强度最高,因此在临床使用过程中,需要特别关注与肌肉骨骼疾病相关的不良反应,并区分原发疾病及不良反应。

基于FAERS的比伐芦定不良反应信号挖掘与分析

目的 挖掘并分析比伐芦定不良反应(ADR)信号,为临床合理用药提供参考。方法 收集2004年1月至2021年12月美国食品和药物管理局(FDA)药品不良事件报告系统(FAERS)中的比伐芦定药品不良事件(ADE)报告,采用报告比值比法(ROR)和比例报告比法(PRR)进行数据挖掘,采用Spearman秩相关进行相关性分析。结果 共收集首要怀疑药物为比伐芦定的ADE报告1 549份,涉及患者1 549例,其中男641例,女482例,性别不详426例;平均年龄(63.71±15.42)岁;报告数居首的国家为美国(81.79%)。经ROR法和PRR法筛选得到143个ADR信号,累及15个系统器官分类(SOC)。相关性分析显示,年龄与比伐芦定出血、栓塞的发生和结局严重程度均呈显著正相关(P <0.05)。结论 临床使用比伐芦定时应密切关注出血和栓塞,尤其应加强高龄人群的临床用药监测。

基于美国FAERS数据库的培唑帕尼不良事件信号挖掘与分析

目的 挖掘并分析培唑帕尼上市后的药物不良事件(ADE)信号,为临床安全用药提供参考。方法 通过OpenVigil 2.1数据平台对美国FDA药物不良事件报告系统(FAERS)数据库进行信号挖掘,收集培唑帕尼2009年10月-2022年6月的ADE报告,采用比例失衡法中的比例报告比值(PRR)法和报告比值比(ROR)法检测该药的ADE信号并进行分析。结果 共筛选出以培唑帕尼为首要怀疑药物的ADE报告16 655份,经ROR法、PRR法挖掘出ADE信号220个,涉及19个系统器官分类。信号频度排前10位的ADE信号在该药的药品说明书中均有记载;发现了88个新的ADE信号,主要分布在胃肠系统、各种检查、肾脏和泌尿系统。嗜碱细胞数减少、甲床出血、肿瘤破裂、阴道瘘既是新的ADE信号,也是信号强度排前10位的ADE信号。结论 培唑帕尼在上市后应用中常见ADE(腹泻、毛发颜色改变、高血压等)的发生情况与其药品说明书基本一致;新的可疑风险信号(嗜碱细胞数减少、甲床出血、肿瘤破裂、阴道瘘等)报道例数较少,还需持续关注。

基于FAERS数据库的4种磷酸二酯酶5抑制剂安全性分析

目的对真实世界不良事件报告数据进行挖掘,分析4种磷酸二酯酶5(PDE5)抑制剂的上市后安全性特征。方法检索美国食品药品监督管理局(FDA)不良事件报告系统(FAERS),分别收集2012年第二季度至2022第三季度以西地那非、他达拉非、伐地那非和阿伐那非为首要怀疑药物的不良事件(ADE)报告数据,并进行系统-器官分类(SOC)和首选术语(PT)标准化映射分析,根据报告比值比(ROR)法和信息成分分析(IC)法筛选出药品不良反应(ADR)的有效不相称测定信号,并对高强度信号进行分析。结果共纳入西地那非ADE报告27695例、他达拉非16683例、伐地那非718例、阿伐那非222例,4种药物ADE报告的SOC主要类型较为类似。在高强度ADR信号方面,整体信号强度(按ROR值)为西地那非>他达拉非>伐地那非,未检测出阿伐那非的有效ADR信号。其中西地那非ADR信号主要集中于生殖系统并出现多个恶性皮肤肿瘤相关ADR信号,他达拉非的恶性皮肤肿瘤相关ADR信号强度明显高于其他药物、且其大部分高强度信号尚未被说明书收载,伐地那非则主要为生殖系统疾病和眼器官疾病。结论4种PDE5抑制剂的ADE整体分布具有一致性,但具体ADR信号特征方面存在一定差异,临床应用时应予以针对性关注,并重点建议对伐地那非和西地那非药品说明书中的ADR信息进行及时补充更新。

基于美国FAERS数据库的德曲妥珠单抗不良事件挖掘与分析

目的基于美国食品药品监督管理局不良事件报告系统(FAERS)及临床试验对德曲妥珠单抗(T-DXd,DS-8201)相关不良反应(ADR)进行数据挖掘,为其临床安全合理使用提供一定的参考。方法使用OpenVigil 2.1数据平台,收集FAERS数据库中德曲妥珠单抗从美国上市至2022年6月30日的相关ADR报告数据,采用报告比值比(ROR)法和比例报告比值(PRR)法对该药物相关报告进行数据挖掘分析。通过在PubMed、Medline和Ovid上搜索与德曲妥珠单抗安全性相关的临床试验,计算各级ADR的发生率评估药物安全性。结果纳入不良事件报告统计:德曲妥珠单抗735例,共得到ADR信号45个。按系统器官(SOC)分类,胃肠系统疾病和呼吸系统、胸及纵膈疾病中ADR信号最多;按发生频次排序,发生频次最多的ADR是恶心(104例)和间质性肺病(92例),与临床试验中发生率最高的ADR相同;按信号强度排序,粒缺性发热(ROR为278.181)和间质性肺病(ROR为84.534)为前2位。结合发生频次和信号强度排序,美国药品说明书中未提及的ADR包括:腹腔积液、细菌性肺炎、心功能不全、肠梗阻和胸腔积液。结论使用德曲妥珠单抗治疗前应做好患者的用药评估,治疗期间应密切监测患者肺功能、心功能指标,如发生ADR,应及时采取干预措施,避免因ADR导致的相关损伤。

基于FAERS数据库的达雷妥尤单抗相关药品不良反应信号挖掘

目的:利用美国食品药品监督管理局药品不良事件报告系统(FAERS)数据库,对达雷妥尤单抗的药品不良反应进行挖掘,为临床合理用药提供参考。方法:调取FAERS数据库中达雷妥尤单抗自2014年在美国上市后连续32个季度的数据,采用报告比值比法和比例报告比法进行药品不良反应信号检测。结果:共得到达雷妥尤单抗相关药品不良反应报告17757例,目标不良反应(死亡)报告772例;患者年龄主要在17~79岁,男性多于女性;报告例数排序居前3位的国家为美国、印度及法国;发生频次较高的不良反应主要集中于输液相关反应、肺炎、腹泻和中性粒细胞减少等。结论:临床使用达雷妥尤单抗时,不仅需要关注常见的不良反应,而且应对药品说明书中没有提到的不良反应加以重视,及时采取预防措施,减少不良反应发生。

基于美国FAERS数据库的阿巴西普不良事件信号挖掘与分析

目的 为阿巴西普的临床安全使用提供参考依据。方法 以美国FDA不良事件报告系统(FAERS)数据库为基础,以药品通用名“abatacept”与商品名“Orencia”作为检索关键词,检索首要怀疑药物为阿巴西普的药物不良事件(ADE)信号,并采用比例失衡法中的报告比值比法和比例报告比值法以及Excel 2020软件对信号进行挖掘与分析。结果 共检索出阿巴西普ADE报告93 189份,以女性病例(75.98%)为主,年龄主要集中于18~64岁(35.17%);数据上报的主要国家为美国(47.41%)与加拿大(30.59%),上报的数量总体呈逐年递增的趋势。共筛选出ADE信号3 092个,其中与阿巴西普的药品说明书描述相似的是与原发疾病相关的ADE信号,如类风湿性关节炎、关节痛、关节肿胀等;其次是与输液反应相关的ADE信号,包括疼痛、乏力、皮疹等。所有筛选出的ADE信号共涉及27个系统器官分类,主要为全身疾病及给药部位各种反应,肌肉骨骼和结缔组织疾病,伤害、中毒和手术并发症,感染和侵袭类疾病,胃肠疾病,神经系统疾病,呼吸、胸腔和纵隔疾病,心脏疾病,良性、恶性和未特指的肿瘤,生殖系统和乳腺疾病等。报告例数排前50位的ADE信号中未被阿巴西普药品说明书收录的共有22个,包括乏力、药物不耐受、腹部不适、肿胀、红斑狼疮、周围肿胀、天疱疮、腹泻、肝酶升高与下呼吸道感染等。结论 临床在使用阿巴西普的过程中应格外注意感染及其致癌性,同时评估患者的呼吸及心血管系统疾病风险,当患者合并这2类基础疾病时,应权衡利弊后谨慎选用;此外,该药在神经、胃肠及生殖系统的ADE也不容忽视。

基于FAERS的替格瑞洛及氯吡格雷相关出血事件信号挖掘

目的为替格瑞洛及氯吡格雷的临床合理应用提供指导与依据。方法利用美国食品和药物管理局(FDA)不良事件报告系统(FAERS)获取替格瑞洛和氯吡格雷从上市起至2021年9月30日的药品不良事件(ADE)报告数据,采用标准MedDRA查询(SMQ)检索其中的出血事件报告,采用报告比值比(ROR)法进行信号挖掘。结果分别获得两药相关出血报告3326例和25538例,严重不良事件(SAE)发生率均较高(66.36%,67.22%),均以住院/住院时间延长为主(40.56%,45.83%)。替格瑞洛[ROR=4.02,95%CI(3.86,4.18)]出血信号值低于氯吡格雷[ROR=6.32,95%CI(6.22,6.42)]。替格瑞洛相关出血事件涉及17个系统器官分类(SOC),85个可疑信号;氯吡格雷涉及18个SOC,198个可疑信号。出血事件多分布于胃肠系统(33.98%,43.08%)以及血管与淋巴管系统(20.42%,14.03%)。结论替格瑞洛与氯吡格雷均可诱发多个系统的出血事件,其中胃肠系统较多见,临床应加强对此两种药物的出血事件监护。