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Consensus sequence L/PKSSLL mimics crucial epitope on Loop III of Taiwan cobra cardiotoxin.

作者信息

Wang Ping-Chieh, Loh Kah-Sin, Lin Shih-Ting, Chien Tzu-Ling, Chiang Jen-Ron, Hsieh Wen-Chin, Miao Bor-Lin, Su Cheng-Fu, Yang Wen-Jen

机构信息

Institute of Biotechnology, National University of Kaohsiung, Kaohsiung 811, Taiwan.

出版信息

Biochem Biophys Res Commun. 2009 Sep 25;387(3):617-22. doi: 10.1016/j.bbrc.2009.07.097. Epub 2009 Jul 24.

Abstract

Phage display is effective in screening peptides that mimic venom's neutralizing epitopes. A phage display cyclized heptapeptide library (C7C library) was panned with purified divalent antivenin IgG, which neutralizes Naja naja atra venom (NAV) and Bungarus multicinctus venom (BMV). The selected heptapeptide sequences were aligned with known protein sequences of NAV and BMV in GenBank. One of the four consensus sequences, L/PKSSLL, mimicked the crucial epitope on Loop III of Taiwan cobra cardiotoxin that is associated with the venom's lethal potency. In dot blot analysis, several clones showed varying reactivities for NAV monovalent antivenin and lesser cross-reactions with BMV monovalent antivenin. The KSSLLRN-carrying phage occurred four times in selected clones and showed the strongest reactivity to NAV monovalent antivenin. Furthermore, the QDSLLPS-carrying phage also presented significant dot blot signal, indicating that the SLL sequence shared by these two clones may be a crucial antibody-binding site.

摘要

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