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Identification of the critical regions in hepatitis B virus preS required for its stability

โœ Scribed by Min Lian; Xu Zhou; Bin Chen; Chan Li; Xiaocheng Gu; Ming Luo; Xiaofeng Zheng

Publisher
John Wiley and Sons
Year
2008
Tongue
English
Weight
531 KB
Volume
14
Category
Article
ISSN
1075-2617

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โœฆ Synopsis

Abstract

As a hepatitis B virus (HBV) envelope domain, preS plays significant roles in receptor recognition and viral infection. However, the regions critical for maintaining a stable and functional conformation of preS are still unclear and require further investigation. In order to unravel these regions, serially truncated fragments of preS were constructed and expressed in Escherichia coli. Their solubility, stability, secondary structure, and affinity to polyclonal antibodies and hepatocytes were examined. The results showed that amino acids 31โ€“36 were vital for its stable conformation, and the absence of 10โ€“36 amino acids significantly reduced its binding to polyclonal antibodies as well as hepatocytes. The most stable fragment 1โ€“120 (preS1 + Nโ€terminal 12 amino acids of preS2), perhaps the core of preS, was discovered, which bound to HepG2 cells most tightly. Moreover, the availability of large amounts of wellโ€folded and stable preS1โ€120 enables us to carry out further structural determination and mechanistic study on HBV infection. Copyright ยฉ 2007 European Peptide Society and John Wiley & Sons, Ltd.

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