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Directed Evolution of an LBP/CD14 Inhibitory Peptide and Its Anti-Endotoxin Activity

21

Citations

29

References

2014

Year

Abstract

By in vitro directed evolution of peptide analogs for the LBP/CD14 binding site, we established a new polypeptide (P1) with a threonine (T)-to-methionine (M) mutation in amino acid 287 of LBP. This polypeptide had high anti-endotoxin activity in vitro and in vivo, which suggested that amino acid 287 in the C-terminus of LBP may play an important role in LBP binding with CD14.

References

YearCitations

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