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Vol. 15. Issue 6.
Pages 560-566 (November - December 2011)
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Vol. 15. Issue 6.
Pages 560-566 (November - December 2011)
Original article
Open Access
Simultaneous detection of hepatitis B virus genotypes and mutations associated with resistance to lamivudine, adefovir, and telbivudine by the polymerase chain reaction-ligase detection reaction
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Yong-Zhong Wang1,
Corresponding author
wyz213003@163.com

Correspondence to: Yong-Zhong Wang 300 North Lanling Road Changzhou 213001 – Jiangsu Province China.
, Jun-Hua Xiao2, Long-Gen Liu3, Chun-Yan Ye4, Hong-Yu Shen5, Tian-Min Xu4, Ke-Zhuan Zhu4
1 Institute for the Study of Liver Diseases, The Third People's Hospital of Changzhou, China
2 College of Chemistry, Chemical Engineering and Biotechnology, Donghua University, China
3 Third People's Hospital of Changzhou; Professor, Department of Infectious Diseases, Institute for the Study of Liver Diseases, The Third People's Hospital of Changzhou, China
4 Professors, Department of Infectious Diseases, Institute for the Study of Liver Diseases, The Third People's Hospital of Changzhou, China
5 Supervising Laboratorian, Institute for the Study of Liver Diseases, The Third People's Hospital of Changzhou, China
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Abstract
Objectives

Detection of mutations associated to nucleos(t)ide analogs and hepatitis B virus (HBV) genotyping are essential for monitoring treatment of HBV infection. We developed a multiplex polymerase chain reaction-ligase detection reaction (PCR-LDR) assay for the rapid detection of HBV genotypes and mutations associated with lamivudine, adefovir, and telbivudine resistance in HBV-infected patients.

Methods

HBV templates were amplified by PCR, followed by LDR and electrophoresis on a sequencer. The assay was evaluated using plasmids that contained wild-type or mutant HBV sequences and 216 clinical samples.

Results

The PCR-LDR assay and sequencing gave comparable results for 158 of the 216 samples (73.1%) with respect to mutation detection and genotyping. Complete agreement between the two methods was observed for all the samples (100%) at codon 180 and codon 204. Concordant results were observed for 99.4% of the 158 samples at codon 181 and 98.7% at codon 236. The genotyping results were completely concordant between the PCR-LDR assay and sequencing. The PCR-LDR assay could detect a proportion of 1% mutant plasmid in a background of wild-type plasmid.

Conclusion

The PCR-LDR assay is sensitive and specific for detection of HBV genotypes and drug resistance mutations, and could be helpful for decision making in the treatment of HBV infection.

Keywords:
hepatitis B
drug resistance
mutation
genotype
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