Improving Antigenicity of the Recombinant Hepatitis C Virus Core Protein via Random Mutagenesis

Author:

Huang Chen-Ji1,Peng Hwei-Ling1,Cheng Chih-Yu2

Affiliation:

1. Department of Biological Science and Technology, National Chiao Tung University, Hsinchu 30010, Taiwan

2. Department of Marine Biotechnology, National Kaohsiung Marine University, Kaohsiung 81143, Taiwan

Abstract

In order to enhance the sensitivity of diagnosis, a recombinant clone containing domain I of HCV core (amino acid residues 1 to 123) was subjected to random mutagenesis. Five mutants with higher sensitivity were obtained by colony screening of 616 mutants using reverse ELISA. Sequence analysis of these mutants revealed alterations focusing on W84, P95, P110, or V129. The inclusion bodies of these recombinant proteins overexpressed inE. coliBL21(DE3) were subsequently dissolved using 6 M urea and then refolded by stepwise dialysis. Compared to the unfolded wild-type antigen, the refolded M3b antigen (W84S, P110S and V129L) exhibited an increase of 66% antigenicity with binding capacity of 0.96 and affinity of 113 μM−1. Moreover, the 33% decrease of the production demand suggests that M3b is a potential substitute for anti-HCV antibody detection.

Funder

National Science Council

Publisher

Hindawi Limited

Subject

Health, Toxicology and Mutagenesis,Genetics,Molecular Biology,Molecular Medicine,General Medicine,Biotechnology

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