Hepatitis B Core-Related Antigen to Indicate High Viral Load: Systematic Review and Meta-Analysis of 10,397 Individual Participants

Kyoko Yoshida; Alice Desbiolles; Sarah F. Feldman; Sang Hoon Ahn; Enagnon K. Alidjinou; Masanori Atsukawa; Laurence Bocket; Maurizia R. Brunetto; Maria Buti; Ivana Carey; Gian Paolo Caviglia; En Qiang Chen; Markus Cornberg; Masaru Enomoto; Masao Honda; Christoph Höner Zu Siederdissen; Masatoshi Ishigami; Harry L.A. Janssen; Benjamin Maasoumy; Takeshi Matsui; Akihiro Matsumoto; Shuhei Nishiguchi; Mar Riveiro-Barciela; Akinobu Takaki; Pisit Tangkijvanich; Hidenori Toyoda; Margo J.H. van Campenhout; Bo Wang; Lai Wei; Hwai I. Yang; Yoshihiko Yano; Hiroshi Yatsuhashi; Man Fung Yuen; Eiji Tanaka; Maud Lemoine; Yasuhito Tanaka; Yusuke Shimakawa

doi:10.1016/j.cgh.2020.04.045

Hepatitis B Core-Related Antigen to Indicate High Viral Load: Systematic Review and Meta-Analysis of 10,397 Individual Participants

Kyoko Yoshida, Alice Desbiolles, Sarah F. Feldman, Sang Hoon Ahn, Enagnon K. Alidjinou, Masanori Atsukawa, Laurence Bocket, Maurizia R. Brunetto, Maria Buti, Ivana Carey, Gian Paolo Caviglia, En Qiang Chen, Markus Cornberg, Masaru Enomoto, Masao Honda, Christoph Höner Zu Siederdissen, Masatoshi Ishigami, Harry L.A. Janssen, Benjamin Maasoumy, Takeshi MatsuiAkihiro Matsumoto, Shuhei Nishiguchi, Mar Riveiro-Barciela, Akinobu Takaki, Pisit Tangkijvanich, Hidenori Toyoda, Margo J.H. van Campenhout, Bo Wang, Lai Wei, Hwai I. Yang, Yoshihiko Yano, Hiroshi Yatsuhashi, Man Fung Yuen, Eiji Tanaka, Maud Lemoine, Yasuhito Tanaka, Yusuke Shimakawa

Research output: Contribution to journal › Article › peer-review

23 Citations (Scopus)

Abstract

Background & Aims: To eliminate hepatitis B virus (HBV) infection, scale-up of testing and treatment in resource-limited countries is crucial. However, access to nucleic acid testing to quantify HBV DNA, an essential test to examine treatment eligibility, remains severely limited. We assessed the performance of a novel immunoassay, HBV core-related antigen (HBcrAg), as a low-cost (less than US $15/assay) alternative to nucleic acid testing to indicate clinically important high viremia in chronic HBV patients infected with different genotypes. Methods: We searched Medline, Embase, Scopus, and Web of Science databases through June 27, 2018. Three reviewers independently selected studies measuring HBV DNA and HBcrAg in the same blood samples. We contacted authors to provide individual participant data (IPD). We randomly allocated each IPD to a derivation or validation cohort. We applied optimal HBcrAg cut-off values derived from the derivation set to the validation set to estimate sensitivity/specificity. Results: Of 74 eligible studies, IPD were obtained successfully for 60 studies (81%). Meta-analysis included 5591 IPD without antiviral therapy and 4806 treated with antivirals. In untreated patients, the pooled area under the receiver operating characteristic curve and optimal cut-off values were as follows: 0.88 (95% CI, 0.83–0.94) and 3.6 log U/mL to diagnose HBV DNA level of 2000 IU/mL or greater; and 0.96 (95% CI, 0.94–0.98) and 5.3 log U/mL for 200,000 IU/mL or greater, respectively. In the validation set, the sensitivity and specificity were 85.2% and 84.7% to diagnose HBV DNA level of 2000 IU/mL or greater, and 91.8% and 90.5% for 200,000 IU/mL or greater, respectively. The performance did not vary by HBV genotypes. In patients treated with anti-HBV therapy the correlation between HBcrAg and HBV DNA was poor. Conclusions: HBcrAg might be a useful serologic marker to indicate clinically important high viremia in treatment-naïve, HBV-infected patients.

Original language	English
Pages (from-to)	46-60.e8
Journal	Clinical Gastroenterology and Hepatology
Volume	19
Issue number	1
DOIs	https://doi.org/10.1016/j.cgh.2020.04.045
Publication status	Published - Jan 2021

Keywords

Diagnosis
Hepatitis B Core-Related Antigen
Meta-Analysis
Sensitivity
Specificity
Systematic Review

ASJC Scopus subject areas

Hepatology
Gastroenterology

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.cgh.2020.04.045

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Yoshida, K., Desbiolles, A., Feldman, S. F., Ahn, S. H., Alidjinou, E. K., Atsukawa, M., Bocket, L., Brunetto, M. R., Buti, M., Carey, I., Caviglia, G. P., Chen, E. Q., Cornberg, M., Enomoto, M., Honda, M., Zu Siederdissen, C. H., Ishigami, M., Janssen, H. L. A., Maasoumy, B., ... Shimakawa, Y. (2021). Hepatitis B Core-Related Antigen to Indicate High Viral Load: Systematic Review and Meta-Analysis of 10,397 Individual Participants. Clinical Gastroenterology and Hepatology, 19(1), 46-60.e8. https://doi.org/10.1016/j.cgh.2020.04.045

Yoshida, K, Desbiolles, A, Feldman, SF, Ahn, SH, Alidjinou, EK, Atsukawa, M, Bocket, L, Brunetto, MR, Buti, M, Carey, I, Caviglia, GP, Chen, EQ, Cornberg, M, Enomoto, M, Honda, M, Zu Siederdissen, CH, Ishigami, M, Janssen, HLA, Maasoumy, B, Matsui, T, Matsumoto, A, Nishiguchi, S, Riveiro-Barciela, M, Takaki, A, Tangkijvanich, P, Toyoda, H, van Campenhout, MJH, Wang, B, Wei, L, Yang, HI, Yano, Y, Yatsuhashi, H, Yuen, MF, Tanaka, E, Lemoine, M, Tanaka, Y & Shimakawa, Y 2021, 'Hepatitis B Core-Related Antigen to Indicate High Viral Load: Systematic Review and Meta-Analysis of 10,397 Individual Participants', Clinical Gastroenterology and Hepatology, vol. 19, no. 1, pp. 46-60.e8. https://doi.org/10.1016/j.cgh.2020.04.045

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title = "Hepatitis B Core-Related Antigen to Indicate High Viral Load: Systematic Review and Meta-Analysis of 10,397 Individual Participants",

abstract = "Background & Aims: To eliminate hepatitis B virus (HBV) infection, scale-up of testing and treatment in resource-limited countries is crucial. However, access to nucleic acid testing to quantify HBV DNA, an essential test to examine treatment eligibility, remains severely limited. We assessed the performance of a novel immunoassay, HBV core-related antigen (HBcrAg), as a low-cost (less than US $15/assay) alternative to nucleic acid testing to indicate clinically important high viremia in chronic HBV patients infected with different genotypes. Methods: We searched Medline, Embase, Scopus, and Web of Science databases through June 27, 2018. Three reviewers independently selected studies measuring HBV DNA and HBcrAg in the same blood samples. We contacted authors to provide individual participant data (IPD). We randomly allocated each IPD to a derivation or validation cohort. We applied optimal HBcrAg cut-off values derived from the derivation set to the validation set to estimate sensitivity/specificity. Results: Of 74 eligible studies, IPD were obtained successfully for 60 studies (81%). Meta-analysis included 5591 IPD without antiviral therapy and 4806 treated with antivirals. In untreated patients, the pooled area under the receiver operating characteristic curve and optimal cut-off values were as follows: 0.88 (95% CI, 0.83–0.94) and 3.6 log U/mL to diagnose HBV DNA level of 2000 IU/mL or greater; and 0.96 (95% CI, 0.94–0.98) and 5.3 log U/mL for 200,000 IU/mL or greater, respectively. In the validation set, the sensitivity and specificity were 85.2% and 84.7% to diagnose HBV DNA level of 2000 IU/mL or greater, and 91.8% and 90.5% for 200,000 IU/mL or greater, respectively. The performance did not vary by HBV genotypes. In patients treated with anti-HBV therapy the correlation between HBcrAg and HBV DNA was poor. Conclusions: HBcrAg might be a useful serologic marker to indicate clinically important high viremia in treatment-na{\"i}ve, HBV-infected patients.",

keywords = "Diagnosis, Hepatitis B Core-Related Antigen, Meta-Analysis, Sensitivity, Specificity, Systematic Review",

author = "Kyoko Yoshida and Alice Desbiolles and Feldman, {Sarah F.} and Ahn, {Sang Hoon} and Alidjinou, {Enagnon K.} and Masanori Atsukawa and Laurence Bocket and Brunetto, {Maurizia R.} and Maria Buti and Ivana Carey and Caviglia, {Gian Paolo} and Chen, {En Qiang} and Markus Cornberg and Masaru Enomoto and Masao Honda and {Zu Siederdissen}, {Christoph H{\"o}ner} and Masatoshi Ishigami and Janssen, {Harry L.A.} and Benjamin Maasoumy and Takeshi Matsui and Akihiro Matsumoto and Shuhei Nishiguchi and Mar Riveiro-Barciela and Akinobu Takaki and Pisit Tangkijvanich and Hidenori Toyoda and {van Campenhout}, {Margo J.H.} and Bo Wang and Lai Wei and Yang, {Hwai I.} and Yoshihiko Yano and Hiroshi Yatsuhashi and Yuen, {Man Fung} and Eiji Tanaka and Maud Lemoine and Yasuhito Tanaka and Yusuke Shimakawa",

note = "Funding Information: Conflicts of interest These authors disclose the following: Maurizia R. Brunetto has received grants and personal fees from AbbVie and Gilead, grants from BMS, and research support from Fujirebio; Maria Buti has received grants and personal fees from Gilead; Gian Paolo Caviglia has received grants from Fujirebio Europe; Markus Cornberg has received personal fees from AbbVie, Bristol-Myers Squibb, Gilead Sciences, Janssen-Cilag, Roche , Merck , MSD, Biogen, Falk Foundation, Boehringer Ingelheim, Siemens, and Spring Bank, and grants from Roche; Christoph H{\"o}ner Zu Siederdissen has received grants from Novartis Pharma and Gilead Sciences; Harry L. A. Janssen has received grants and personal fees from AbbVie, Bristol Myers Squibb, Gilead Sciences, Janssen, MedImmune, Merck, and Roche, and personal fees from Benitec, Arbutus, and Vir Biotechnology, Inc; Benjamin Maasoumy has received grants from Fujirebio, Roche Diagnostics, Abbott Diagnostics, Fujirebio Europe, and Altona Diagnostics, personal fees from Abbott Diagnostics, Merck/MSD, AbbVie, Falk Foundation, and Astellas, and research support from Merck/MSD, Gilead, and AbbVie; Hidenori Toyoda has received personal fees from AbbVie and MSD; Margo J. H. van Campenhout has received personal fees from Fujirebio Europe; and Yasuhito Tanaka has received grants and personal fees from Fujirebio. The remaining authors disclose no conflicts. Publisher Copyright: {\textcopyright} 2021 AGA Institute",

year = "2021",

month = jan,

doi = "10.1016/j.cgh.2020.04.045",

language = "English",

volume = "19",

pages = "46--60.e8",

journal = "Clinical Gastroenterology and Hepatology",

issn = "1542-3565",

publisher = "W.B. Saunders Ltd",

number = "1",

}

TY - JOUR

T1 - Hepatitis B Core-Related Antigen to Indicate High Viral Load

T2 - Systematic Review and Meta-Analysis of 10,397 Individual Participants

AU - Yoshida, Kyoko

AU - Desbiolles, Alice

AU - Feldman, Sarah F.

AU - Ahn, Sang Hoon

AU - Alidjinou, Enagnon K.

AU - Atsukawa, Masanori

AU - Bocket, Laurence

AU - Brunetto, Maurizia R.

AU - Buti, Maria

AU - Carey, Ivana

AU - Caviglia, Gian Paolo

AU - Chen, En Qiang

AU - Cornberg, Markus

AU - Enomoto, Masaru

AU - Honda, Masao

AU - Zu Siederdissen, Christoph Höner

AU - Ishigami, Masatoshi

AU - Janssen, Harry L.A.

AU - Maasoumy, Benjamin

AU - Matsui, Takeshi

AU - Matsumoto, Akihiro

AU - Nishiguchi, Shuhei

AU - Riveiro-Barciela, Mar

AU - Takaki, Akinobu

AU - Tangkijvanich, Pisit

AU - Toyoda, Hidenori

AU - van Campenhout, Margo J.H.

AU - Wang, Bo

AU - Wei, Lai

AU - Yang, Hwai I.

AU - Yano, Yoshihiko

AU - Yatsuhashi, Hiroshi

AU - Yuen, Man Fung

AU - Tanaka, Eiji

AU - Lemoine, Maud

AU - Tanaka, Yasuhito

AU - Shimakawa, Yusuke

N1 - Funding Information: Conflicts of interest These authors disclose the following: Maurizia R. Brunetto has received grants and personal fees from AbbVie and Gilead, grants from BMS, and research support from Fujirebio; Maria Buti has received grants and personal fees from Gilead; Gian Paolo Caviglia has received grants from Fujirebio Europe; Markus Cornberg has received personal fees from AbbVie, Bristol-Myers Squibb, Gilead Sciences, Janssen-Cilag, Roche , Merck , MSD, Biogen, Falk Foundation, Boehringer Ingelheim, Siemens, and Spring Bank, and grants from Roche; Christoph Höner Zu Siederdissen has received grants from Novartis Pharma and Gilead Sciences; Harry L. A. Janssen has received grants and personal fees from AbbVie, Bristol Myers Squibb, Gilead Sciences, Janssen, MedImmune, Merck, and Roche, and personal fees from Benitec, Arbutus, and Vir Biotechnology, Inc; Benjamin Maasoumy has received grants from Fujirebio, Roche Diagnostics, Abbott Diagnostics, Fujirebio Europe, and Altona Diagnostics, personal fees from Abbott Diagnostics, Merck/MSD, AbbVie, Falk Foundation, and Astellas, and research support from Merck/MSD, Gilead, and AbbVie; Hidenori Toyoda has received personal fees from AbbVie and MSD; Margo J. H. van Campenhout has received personal fees from Fujirebio Europe; and Yasuhito Tanaka has received grants and personal fees from Fujirebio. The remaining authors disclose no conflicts. Publisher Copyright: © 2021 AGA Institute

PY - 2021/1

Y1 - 2021/1

N2 - Background & Aims: To eliminate hepatitis B virus (HBV) infection, scale-up of testing and treatment in resource-limited countries is crucial. However, access to nucleic acid testing to quantify HBV DNA, an essential test to examine treatment eligibility, remains severely limited. We assessed the performance of a novel immunoassay, HBV core-related antigen (HBcrAg), as a low-cost (less than US $15/assay) alternative to nucleic acid testing to indicate clinically important high viremia in chronic HBV patients infected with different genotypes. Methods: We searched Medline, Embase, Scopus, and Web of Science databases through June 27, 2018. Three reviewers independently selected studies measuring HBV DNA and HBcrAg in the same blood samples. We contacted authors to provide individual participant data (IPD). We randomly allocated each IPD to a derivation or validation cohort. We applied optimal HBcrAg cut-off values derived from the derivation set to the validation set to estimate sensitivity/specificity. Results: Of 74 eligible studies, IPD were obtained successfully for 60 studies (81%). Meta-analysis included 5591 IPD without antiviral therapy and 4806 treated with antivirals. In untreated patients, the pooled area under the receiver operating characteristic curve and optimal cut-off values were as follows: 0.88 (95% CI, 0.83–0.94) and 3.6 log U/mL to diagnose HBV DNA level of 2000 IU/mL or greater; and 0.96 (95% CI, 0.94–0.98) and 5.3 log U/mL for 200,000 IU/mL or greater, respectively. In the validation set, the sensitivity and specificity were 85.2% and 84.7% to diagnose HBV DNA level of 2000 IU/mL or greater, and 91.8% and 90.5% for 200,000 IU/mL or greater, respectively. The performance did not vary by HBV genotypes. In patients treated with anti-HBV therapy the correlation between HBcrAg and HBV DNA was poor. Conclusions: HBcrAg might be a useful serologic marker to indicate clinically important high viremia in treatment-naïve, HBV-infected patients.

AB - Background & Aims: To eliminate hepatitis B virus (HBV) infection, scale-up of testing and treatment in resource-limited countries is crucial. However, access to nucleic acid testing to quantify HBV DNA, an essential test to examine treatment eligibility, remains severely limited. We assessed the performance of a novel immunoassay, HBV core-related antigen (HBcrAg), as a low-cost (less than US $15/assay) alternative to nucleic acid testing to indicate clinically important high viremia in chronic HBV patients infected with different genotypes. Methods: We searched Medline, Embase, Scopus, and Web of Science databases through June 27, 2018. Three reviewers independently selected studies measuring HBV DNA and HBcrAg in the same blood samples. We contacted authors to provide individual participant data (IPD). We randomly allocated each IPD to a derivation or validation cohort. We applied optimal HBcrAg cut-off values derived from the derivation set to the validation set to estimate sensitivity/specificity. Results: Of 74 eligible studies, IPD were obtained successfully for 60 studies (81%). Meta-analysis included 5591 IPD without antiviral therapy and 4806 treated with antivirals. In untreated patients, the pooled area under the receiver operating characteristic curve and optimal cut-off values were as follows: 0.88 (95% CI, 0.83–0.94) and 3.6 log U/mL to diagnose HBV DNA level of 2000 IU/mL or greater; and 0.96 (95% CI, 0.94–0.98) and 5.3 log U/mL for 200,000 IU/mL or greater, respectively. In the validation set, the sensitivity and specificity were 85.2% and 84.7% to diagnose HBV DNA level of 2000 IU/mL or greater, and 91.8% and 90.5% for 200,000 IU/mL or greater, respectively. The performance did not vary by HBV genotypes. In patients treated with anti-HBV therapy the correlation between HBcrAg and HBV DNA was poor. Conclusions: HBcrAg might be a useful serologic marker to indicate clinically important high viremia in treatment-naïve, HBV-infected patients.

KW - Diagnosis

KW - Hepatitis B Core-Related Antigen

KW - Meta-Analysis

KW - Sensitivity

KW - Specificity

KW - Systematic Review

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U2 - 10.1016/j.cgh.2020.04.045

DO - 10.1016/j.cgh.2020.04.045

M3 - Article

C2 - 32360825

AN - SCOPUS:85090062751

SN - 1542-3565

VL - 19

SP - 46-60.e8

JO - Clinical Gastroenterology and Hepatology

JF - Clinical Gastroenterology and Hepatology

IS - 1

ER -

Hepatitis B Core-Related Antigen to Indicate High Viral Load: Systematic Review and Meta-Analysis of 10,397 Individual Participants

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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