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乙型肝炎核心相关抗原的检测可识别高病毒载量的患者:个 [复制链接]

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发表于 2020-5-5 15:04 |只看该作者 |倒序浏览 |打印
Clin Gastroenterol Hepatol. 2020 Apr 29. pii: S1542-3565(20)30590-5. doi: 10.1016/j.cgh.2020.04.045. [Epub ahead of print]
Assay for Hepatitis B Core-related Antigen Identify Patients With High Viral Load: Systematic Review and Meta-analysis of Individual Participant Data.
Yoshida K1, Desbiolles A2, Feldman SF2, Ahn SH3, Alidjinou EK4, Atsukawa M5, Bocket L4, Brunetto MR6, Buti M7, Carey I8, Caviglia GP9, Chen EQ10, Cornberg M11, Enomoto M12, Honda M13, Zu Siederdissen CH11, Ishigami M14, Janssen H15, Maasoumy B11, Matsui T16, Matsumoto A17, Nishiguchi S18, Riveiro-Barciela M7, Takaki A19, Tangkijvanich P20, Toyoda H21, van Campenhout MJ22, Wang B8, Wei L23, Yang HI24, Yano Y25, Yatsuhashi H26, Yuen MF27, Tanaka E28, Lemoine M1, Tanaka Y29, Shimakawa Y30.
Author information

1
    Department of Surgery and Cancer, Liver Unit, Imperial College London, Praed St, Paddington, London W2 1NY, UK.
2
    Unité d'Épidémiologie des Maladies Émergentes, Institut Pasteur, 25-28 Rue du Dr Roux, 75015 Paris, France.
3
    Department of Internal Medicine, Yonsei University College of Medicine, 50-1 Yonsei-ro, Seodaemun-gu, Seoul 120-752, Korea.
4
    Laboratoire de Virologie, Centre de Biologie Pathologie, CHU de Lille, Boulevard du Professeur Jules Leclercq, 59037 Lille, France.
5
    Division of Gastroenterology, Department of Internal Medicine, Nippon Medical School Chiba Hokusoh Hospital, 1715 Kamakari, Inzai, Chiba 270-1694, Japan.
6
    Hepatology Unit and Laboratory of Molecular Genetics and Pathology of Hepatitis Viruses, University Hospital of Pisa, Lungarno Antonio Pacinotti, 43, 56126 Pisa PI, Italy.
7
    Liver Unit, Department of Internal Medicine, Hospital Universitari Vall d'Hebron and Universitat Autònoma de Barcelona, Passeig Vall Hebron, 119-129, 08035, Barcelona, Spain.
8
    Institute of Liver Studies, King's College Hospital, Denmark Hill, Brixton, London SE5 9RS, UK.
9
    Department of Medical Sciences, University of Turin, Corso Dogliotti 14, Turin 10126, Italy.
10
    Center of Infectious Diseases, West China Hospital, Sichuan University, No. 37 Guo Xue Xiang, Wuhou District, Chengdu 610041, China.
11
    Department of Gastroenterology, Hepatology and Endocrinology, Hannover Medical School, Carl-Neuberg Strasse 1, 30625 Hannover, Germany.
12
    Department of Hepatology, Graduate School of Medicine, Osaka City University Medical School, 1-4-3 Asahimachi, Abeno-ku, Osaka 545-8585, Japan.
13
    Department of Gastroenterology, and Department of Advanced Medical Technology, Kanazawa University Graduate School of Health Medicine, 13-1 Takara-Machi, Kanazawa, Ishikawa 920-8641, Japan.
14
    Department of Gastroenterology and Hepatology, Nagoya University Graduate School of Medicine, 65 Tsuruma-cho, Showa-ku, Nagoya 466-8550, Japan.
15
    Toronto Centre for Liver Disease, Toronto General Hospital, University Of Toronto, 200 Elizabeth Street, Eaton Building 9th floor Room 234 (9EB234), Toronto, ON, Canada.
16
    Center for Gastroenterology, Teine-Keijinkai Hospital, 12-1-40 Maeda-ichijo, Teine, Sapporo, Hokkaido 006-0811, Japan.
17
    Department of Internal Medicine, Shinshu University School of Medicine, 3-1-1 Asahi, Matsumoto 390-8621, Japan.
18
    Division of Hepatobiliary and Pancreatic Disease, Department of Internal Medicine, Hyogo College of Medicine, 1-1 Mukogawacho, Nishinomiya, Hyogo 663-8501, Japan.
19
    Department of Gastroenterology and Hepatology, Okayama University Graduate School of Medicine, Dentistry and Pharmaceutical Sciences, 2-5-1 Shikata-cho, Okayama 700-8558, Japan.
20
    Center of Excellence in Hepatitis and Liver cancer, Faculty of Medicine, Chulalongkorn University, 1873 Rama IV Rd, 10330, Bangkok, Thailand.
21
    Department of Gastroenterology and Hepatology, Ogaki Municipal Hospital, 4-86 Minaminokawa, Ogaki, Gifu 503-8502, Japan.
22
    Department of Gastroenterology and Hepatology, Erasmus MC University Medical Center, Doctor Molewaterplein 40, 3015 GD Rotterdam, The Netherlands.
23
    Peking University Hepatology Institute, Beijing Key Laboratory of Hepatitis C and Immunotherapy for Liver Diseases, Peking University People's Hospital, No. 11 Xizhimen South Street, Beijing 100044, China.
24
    Genomics Research Center, Academia Sinica, 128 Academia Road, Nankang, Taipei 11529, Taiwan.
25
    Center for Infectious Diseases, Department of Gastroenterology, Kobe University Graduate School of Medicine, 7-5-1 Kusunoki-cho, Chuo-ku, Kobe 650-0017, Japan.
26
    Clinical Research Center, National Hospital Organization (NHO), Nagasaki Medical Center, 2-1001-1, Kubara, Omura, Nagasaki 856-8562, Japan.
27
    Department of Medicine, The University of Hong Kong, Queen Mary Hospital, 102 Pokfulam Road, Hong Kong, China.
28
    Department for the Promotion of Regional Medicine, Shinshu University School of Medicine, 3-1-1 Asahi, Matsumoto 390-8621, Japan.
29
    Department of Virology and Liver Unit, Nagoya City University Graduate School of Medical Sciences, 1 Kawasumi, Mizuho, Nagoya 467-8601, Japan.
30
    Unité d'Épidémiologie des Maladies Émergentes, Institut Pasteur, 25-28 Rue du Dr Roux, 75015 Paris, France. Electronic address: [email protected].

Abstract
BACKGROUND & AIMS:

Scale-up of tests and treatments is needed to eliminate hepatitis B virus (HBV) infection from resource-limited countries. However, access to nucleic acid tests that quantify HBV DNA, to determine treatment eligibility, is severely limited. We performed a systematic review and meta-analysis to assess the performance of the hepatitis B core-related antigen (HBcrAg) immunoassay, a low-cost (less than $15/assay) alternative to the nucleic acid test, to identify highly viremic patients, infected with any HBV genotype.
METHODS:

We searched Medline, Embase, Scopus, and Web of Science through June 27, 2018 for studies that measured HBV DNA and HBcrAg in the same blood samples. We contacted study authors to obtain data from each study participant, and randomly assigned each participant to the derivation or validation cohorts. We applied optimal HBcrAg cut-off values derived from the derivation set to the validation set to estimate sensitivity and specificity of HBcrAg to indicate high viremia.
RESULTS:

Of 74 eligible studies found in the systematic review, we obtained individual participant data from 60 studies (81%). We performed a meta-analysis of individual participant data of 5591 HBV-infected patients who did not receive antiviral therapy and 4806 HBV-infected patients who received antiviral agents. In untreated patients, the pooled area under the receiver operating characteristic curve and the optimal cut-off value for the HBcrAg assay were 0.88 (95% CI, 0.83-0.94) and 3.6 log U/ml for identifying patients with a level of HBV DNA ≥2000 IU/ml, and 0.96 (95% CI, 0.94-0.98) and 5.3 log U/ml for identifying patients with a level of HBV DNA ≥200,000 IU/ml, respectively. In the validation set, the HBcrAg assay identified patients with ≥2000 IU/ml HBV DNA with 85.2% sensitivity and 84.7% specificity; the assay identified patients with ≥200,000 IU/ml HBV DNA with 91.8% sensitivity and 90.5% specificity. Performance did not vary among HBV genotypes. In patients receiving anti-HBV therapy, there was no correlation between levels of HBcrAg and HBV DNA.
CONCLUSIONS:

In a systematic review and meta-analysis of individual participant data, we found that the assay for HBcrAg identifies treatment-naïve patients with high levels of HBV DNA with high sensitivity and specificity, regardless of genotype. The HBcrAg assay is a good, low-cost alternative to the nucleic acid test to identify highly viremic patients infected with different genotypes.

Copyright © 2020 AGA Institute. Published by Elsevier Inc. All rights reserved.
KEYWORDS:

developing nation; diagnosis; diagnostic test; real-world

PMID:
    32360825
DOI:
    10.1016/j.cgh.2020.04.045

Rank: 8Rank: 8

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才高八斗

2
发表于 2020-5-5 15:06 |只看该作者
Castro Gastroenterol Hepatol。 2020年4月29日。pii:S1542-3565(20)30590-5。 doi:10.1016 / j.cgh.2020.04.045。 [Epub提前发行]
乙型肝炎核心相关抗原的检测可识别高病毒载量的患者:个体参与者数据的系统评价和荟萃分析。
吉田K1,Desbiolles A2,Feldman SF2,Ahn SH3,Alidjinou EK4,Atsukawa M5,Bocket L4,Brunetto MR6,Buti M7,Carey I8,Caviglia GP9,Chen EQ10,Cornberg M11,Enomoto M12,Honda M13,Zu Siederdissen CH11 M14,Janssen H15,Maasoumy B11,Matsui T16,Matsumoto A17,Nishiguchi S18,Riveiro-Barciela M7,Takaki A19,Tangkijvanich P20,Toyoda H21,van Campenhout MJ22,Wang B8,Wei L23,Yang HI24,Yano Y25,Yatsuhashi H26元MF27,田中E28,Lemoine M1,田中Y29,岛川Y30。
作者信息

1个
    英国伦敦帕丁顿Praed St伦敦帝国理工学院肝脏科外科和癌症系,纽约W2 1NY。
2
    法兰西共和国巴斯德研究所,埃德蒙蒂斯疟疾联合会,75015年,鲁克斯博士,法国巴黎。
3
    延世大学医学院内科,首尔市西大门区延世路50-1,韩国首尔120-752。
4
    法国里约热内卢生物生物学中心病毒学实验室,朱利勒·勒克莱尔克大道教授,59037里尔,法国。
5
    日本医科大学千叶北寿医院内科消化内科,千叶县印西市镰仓市1715,日本千叶270-1694。
6
    比萨大学医院肝病科和肝炎病毒分子遗传学和病理学实验室,意大利伦萨诺Lungarno Antonio Pacinotti,43,56126。
7
    巴塞罗那希伯伦大学医院和巴塞罗那自治大学内科医院肝脏科,Passeig Vall Hebron,119-129,08035,西班牙巴塞罗那。
8
    国王学院医院肝病研究所,丹尼斯希尔,布里克斯顿,伦敦SE5 9RS,英国。
9
    都灵大学医学系,意大利都灵10126 Corso Dogliotti 14。
10
    四川大学华西医院传染病中心,四川省武侯区郭学巷37号,四川成都610041。
11
    汉诺威医学院胃肠病学,肝病学和内分泌学系,德国汉诺威Carl-Neuberg Strasse 1,30625。
12
    大阪市立大学医学院大学院医学系肝病科,日本大阪市阿倍野区旭町1-4-3,邮编545-8585。
13
    日本金泽大学健康医学研究生院胃肠病学系和先进医学技术系,石川县金泽市宝町13-1,石川920-8641,日本。
14
    名古屋大学医学研究科胃肠病学和肝病学系,日本名古屋市昭和区鹤马町65号466-8550。
15
    多伦多大学多伦多总医院多伦多肝病中心,伊丽莎白街200号,伊顿大厦9楼234室(9EB234),加拿大安大略省多伦多市。
16
    日本北海道札幌市手稻市前田一条町12-1-40前手稻京津会医院胃肠病学中心006-0811
17
    信州大学医学院内科学系,朝日3-1-1,日本松本390-8621。
18岁
    兵库大学内科肝胆胰疾病科,日本西宫市木河町町1-1,兵库663-8501。
19
    冈山大学医学研究科,胃肠病学和肝病学系,冈山县涩谷町2-5-1,日本冈山700-8558。
20
    朱拉隆功大学医学院肝炎和肝癌卓越研究中心,泰国曼谷1330 Rama IV Rd,10330。
21
    大垣市立医院消化内科,大垣市南野川4-86,日本岐阜503-8502。
22
    Erasmus MC大学医学中心胃肠病学和肝病学系,荷兰鹿特丹Molewaterplein博士40,3015。
23
    北京大学肝病研究所,北京大学人民医院北京市丙型肝炎和肝病免疫治疗重点实验室,北京西直门南大街11号,北京100044。
24
    台湾台北市南港市学术路128号中央研究院基因组学研究中心,台湾11529
25
    日本神户市中央区Ku之木町7-5-1,神户大学医学研究生院消化病学中心传染病中心,日本650-0017。
26
    日本长崎市立医院长崎医疗中心国家医院组织(NHO)临床研究中心,长崎856-8562,大村久原市2-1001-1。
27
    香港大学香港薄扶林道102号玛丽医院香港大学医学系。
28
    信州大学医学院局部医学促进系,朝日3-1-1,日本松本390-8621。
29
    名古屋市立大学医学研究科病毒与肝病学系,日本名古屋瑞穗川澄1,名古屋市467-8601。
30
    法兰西共和国巴斯德研究所,埃德蒙蒂斯疟疾联合会,75015年,鲁克斯博士,法国巴黎。电子地址:[email protected]

抽象
背景与目的:

需要扩大测试和治疗的范围,以消除资源有限国家的乙型肝炎病毒(HBV)感染。但是,严格限制了使用可以量化HBV DNA的核酸测试来确定治疗资格的方法。我们进行了系统的审查和荟萃分析,以评估乙型肝炎核心相关抗原(HBcrAg)免疫测定的性能,这是一种低成本的核酸检测方法(每次检测少于15美元),可鉴定出高病毒血症患者,感染了任何HBV基因型。
方法:

我们在2018年6月27日之前搜索Medline,Embase,Scopus和Web of Science,以研究测量相同血液样本中HBV DNA和HBcrAg的研究。我们与研究作者联系以从每个研究参与者那里获取数据,并将每个参与者随机分配到派生或验证队列中。我们将源自派生集的最佳HBcrAg临界值应用于验证集,以估计HBcrAg的敏感性和特异性,以指示高病毒血症。
结果:

在系统评价中发现的74项合格研究中,我们从60项研究中获得了个体参与者数据(81%)。我们对5591例未接受抗病毒治疗的HBV感染患者和4806例接受抗病毒药物的HBV感染患者的个体参与者数据进行了荟萃分析。在未经治疗的患者中,接受者工作特征曲线下的合并面积和HBcrAg测定的最佳临界值为0.88(95%CI,0.83-0.94)和3.6 log U / ml,以鉴定具有HBV DNA水平的患者≥2000 IU / ml和0.96(95%CI,0.94-0.98)和5.3 log U / ml分别用于鉴定HBV DNA≥200,000 IU / ml的患者。在验证组中,HBcrAg分析确定了≥2000 IU / ml HBV DNA的患者,敏感性为85.2%,特异性为84.7%;该检测方法鉴定出≥200,000 IU / ml HBV DNA的患者,灵敏度为91.8%,特异性为90.5%。 HBV基因型之间的表现没有差异。在接受抗HBV治疗的患者中,HBcrAg水平和HBV DNA之间没有相关性。
结论:

在对单个参与者数据的系统回顾和荟萃分析中,我们发现针对HBcrAg的检测方法可以识别出未接受过治疗的患者,无论其基因型如何,均具有高水平的HBV DNA敏感性和特异性。 HBcrAg检测是核酸检测的一种很好的低成本替代方法,可用于鉴定感染了不同基因型的高病毒血症患者。

版权所有©2020 AGA Institute。由Elsevier Inc.出版。保留所有权利。
关键字:

发展中国家诊断;诊断测试;真实世界

PMID:
    32360825
DOI:
    10.1016 / j.cgh.2020.04.045
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