Literature DB >> 35014748

Sequence preference and scaffolding requirement for the inhibition of human neutrophil elastase by ecotin peptide.

Tanaya Bagga1, Su Ning Loh1, J Sivaraman1, Srihari Shankar1.   

Abstract

Human neutrophil elastase (hNE) is an abundant serine protease that is a major constituent of lung elastolytic activity. However, when secreted in excess, if not properly attenuated by selective inhibitor proteins, it can have detrimental effects on host tissues, leading to chronic lung inflammation and non-small cell lung cancer. To improve upon the design of inhibitors against hNE for therapeutic applications, here, we report the crystal structure of hNE in complex with an ecotin (ET)-derived peptide inhibitor. We show that the peptide binds in the nonprime substrate binding site. Unexpectedly, compared with full-length (FL) ET, we find that our short linear peptides and circular amide backbone-linked peptides of ET are incapable of efficient hNE inhibition. Our structural insights point to a preferred amino acid sequence and the potential benefit of a scaffold for optimal binding and function of the peptide inhibitor, both of which are retained in the FL ET protein. These findings will aid in the development of effective peptide-based inhibitors against hNE for targeted therapy.
© 2022 The Protein Society.

Entities:  

Keywords:  elastase; inhibition; peptide; serine protease; structure

Mesh:

Substances:

Year:  2022        PMID: 35014748      PMCID: PMC8927871          DOI: 10.1002/pro.4274

Source DB:  PubMed          Journal:  Protein Sci        ISSN: 0961-8368            Impact factor:   6.725


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  1 in total

1.  Sequence preference and scaffolding requirement for the inhibition of human neutrophil elastase by ecotin peptide.

Authors:  Tanaya Bagga; Su Ning Loh; J Sivaraman; Srihari Shankar
Journal:  Protein Sci       Date:  2022-01-22       Impact factor: 6.725

  1 in total

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