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- Title
A Novel Peptide Can Mimic Extracellular Fibrinogen-Binding Protein to Block the Activation of Complement System.
- Authors
Gao, Ya-ping; Dong, Jie; Zhang, Xin; Liu, Yu; Lu, Qiang; Feng, Jian-nan; Tan, Xiao-rong; Yang, Guang
- Abstract
Extracellular fibrinogen-binding protein (Efb) of Staphylococcus aureus ( S. aureus) is a bi-functional protein, which can specifically bind fibrinogen with its N terminus and inhibit deposition of C3b on the surface of S. aureus with its C terminus. Here, we screened the epitopes of Efb using phage display. Four peptides with consensus motif were screened. This consensus motif was identical to C terminus (161-164) of Efb. In the further investigation, it was found the synthesized peptide EC1 (154-165aa of Efb) could specifically bind C3/C3b and subsequently to block the activation of complement. Meanwhile, EC1 could inhibit the interaction between Efb and C3/C3b. Moreover, the interaction between the mutant protein of EmC1 (Efb without EC1) and C3 was decreased. And, the effect on the complement system of the mutant protein was dramatically declined compared with Efb. Our finding suggested that the peptide EC1 could mimic Efb to block complement system activation via binding C3.
- Subjects
STAPHYLOCOCCUS aureus; FIBRINOGEN-binding proteins; PROTEINS; EPITOPES; BACTERIOPHAGES
- Publication
Cell Biochemistry & Biophysics, 2013, Vol 66, Issue 3, p753
- ISSN
1085-9195
- Publication type
Article
- DOI
10.1007/s12013-013-9520-0