Ann Heawon, Lee Yil Seob, Kim Yeon Sook, Jung Sook In, Lee Sun Hee, Lee Chang Seop, Lee Jin Soo, Choi Won Suk, Choi Young Hwa, Kim Shin Woo
GlaxoSmithKline Korea, Seoul, Korea.
Department of Internal Medicine, Yonsei University College of Medicine, Seoul, Korea.
Infect Chemother. 2019 Jun;51(2):150-160. doi: 10.3947/ic.2019.51.2.150.
Lamivudine and abacavir sulfate are widely used nucleoside/tide reverse transcriptase inhibitors (NRTI) backbone agents, which are recommended in major international treatment guidelines. The fixed-dose combination of lamivudine and abacavir sulfate has been developed to contribute to low pill burden of antiretroviral therapy (ART) regimen and patient adherence. A mandatory post-marketing surveillance was conducted in Korea to monitor the safety of Kivexa (lamivudine 300 mg/abacavir 600 mg).
An open label, multi-center, non-interventional post-marketing surveillance was conducted to monitor the safety of Kivexa from July 2011 to July 2017 in 23 hospitals in Korea. Subjects over 12 years old taking Kivexa per prescribing information were enrolled. The primary outcome was defined as the occurrence of any adverse events during the study period. Secondary outcomes included the occurrence of adverse drug reaction, the occurrence of serious adverse events and the effectiveness of Kivexa.
A total of 600 patients from 23 hospitals were enrolled within the 6 years of study. The total observation period was 1,004 person-years. Three hundred and ten patients reported 674 adverse events. The incidence of upper respiratory infection (65 cases, 10.9%) was the highest, followed by diarrhea (20 cases, 3.3%), and nausea (18 cases, 3.0%). 109 subjects reported 71 events of adverse drug reactions, and the most common reaction was nausea in 2.33% of the subjects. Thirty-one subjects reported serious adverse events, none of them were considered drug related. From the total of 600 subjects, excluding 48 subjects who were 'effectiveness unassessable' by investigators, 552 patients were eligible for the subjective effectiveness analysis. 459 (83.2%) were evaluated as 'improved'. Proportion of subjects whose human immunodeficiency virus-RNA is <50 copies/ml was 61.2% (309/505) at the beginning of observation and increased to 91.9% (464/505) at the end of study period.
The post-marketing surveillance showed the safety of Kivexa in HIV-1 patients in Korea. Ischemic cardiovascular events and hypersensitivity associated with Kivexa were few. There was no significant new safety information. This data may be helpful in implementing Kivexa and lamivudine/abacavir sulfate containing drugs in Korea.
拉米夫定和硫酸阿巴卡韦是广泛使用的核苷/核苷酸逆转录酶抑制剂(NRTI)骨干药物,在主要国际治疗指南中均有推荐。拉米夫定和硫酸阿巴卡韦的固定剂量复方制剂已研发出来,有助于降低抗逆转录病毒治疗(ART)方案的服药负担并提高患者依从性。韩国开展了一项上市后强制监测,以监测Kivexa(拉米夫定300毫克/阿巴卡韦600毫克)的安全性。
2011年7月至2017年7月,在韩国23家医院开展了一项开放标签、多中心、非干预性的上市后监测,以监测Kivexa的安全性。纳入年龄超过12岁且按照处方信息服用Kivexa的受试者。主要结局定义为研究期间发生的任何不良事件。次要结局包括药物不良反应的发生、严重不良事件的发生以及Kivexa的有效性。
在6年的研究期间,23家医院共纳入600例患者。总观察期为1004人年。310例患者报告了674例不良事件。上呼吸道感染的发生率最高(65例,10.9%),其次是腹泻(20例,3.3%)和恶心(18例,3.0%)。109名受试者报告了71例药物不良反应事件,最常见的反应是恶心,占受试者的2.33%。31名受试者报告了严重不良事件,其中无一例被认为与药物有关。在600名受试者中,排除48名被研究者判定为“有效性不可评估”的受试者后,552例患者符合主观有效性分析的条件。459例(83.2%)被评估为“改善”。观察开始时,人类免疫缺陷病毒RNA<50拷贝/毫升的受试者比例为61.2%(309/505);研究期末,这一比例增至91.9%(464/505)。
上市后监测显示了Kivexa在韩国HIV-1患者中的安全性。与Kivexa相关的缺血性心血管事件和超敏反应较少。未发现重大新的安全信息。这些数据可能有助于在韩国使用Kivexa以及含拉米夫定/硫酸阿巴卡韦的药物。
