Manipulation of charged residues within the two-peptide lantibiotic lacticin 3147

Lucy H. Deegan; Srinivas Suda; Elaine M. Lawton; Lorraine A. Draper; Floor Hugenholtz; Andreas Peschel; Colin Hill; Paul D. Cotter; R. Paul Ross

doi:https://doi.org/10.1111/j.1751-7915.2009.00145.x

Manipulation of charged residues within the two-peptide lantibiotic lacticin 3147

Lucy H. Deegan, Srinivas Suda, Elaine M. Lawton, Lorraine A. Draper, Floor Hugenholtz, Andreas Peschel, Colin Hill, Paul D. Cotter, R. Paul Ross

Amsterdam UMC

Research output: Contribution to journal › Article › Academic › peer-review

20 Citations (Scopus)

Abstract

Lantibiotics are antimicrobial peptides which contain a high percentage of post-translationally modified residues. While most attention has been paid to the role of these critical structural features, evidence continues to emerge that charged amino acids also play a key role in these peptides. Here 16 'charge' mutants of the two-peptide lantibiotic lacticin 3147 [composed of Ltnα (2+, 2-) and Ltnβ (2+)] were constructed which, when supplemented with previously generated peptides, results in a total bank of 23 derivatives altered in one or more charged residues. When examined individually, in combination with a wild-type partner or, in some instances, in combination with one another, these mutants reveal the importance of charge at specific locations within Ltnα and Ltnβ, confirm the critical role of the negatively charged glutamate residue in Ltnα and facilitate an investigation of the contribution of positively charged residues to the cationic Ltnβ. From these investigations it is also apparent that the relative importance of the overall charge of lacticin 3147 varies depending on the target bacteria and is most evident when strains with more negatively charged cell envelopes are targeted. These studies also result in, for the first time, the creation of a derivative of a lacticin 3147 peptide (LtnβR27A) which displays enhanced specific activity

Original language	English
Pages (from-to)	222-234
Journal	Microbial biotechnology
Volume	3
Issue number	2
DOIs	https://doi.org/10.1111/j.1751-7915.2009.00145.x
Publication status	Published - 2010

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https://doi.org/10.1111/j.1751-7915.2009.00145.x

Cite this

@article{5ef248ea64cf466d967ebd41c85acd7f,

title = "Manipulation of charged residues within the two-peptide lantibiotic lacticin 3147",

abstract = "Lantibiotics are antimicrobial peptides which contain a high percentage of post-translationally modified residues. While most attention has been paid to the role of these critical structural features, evidence continues to emerge that charged amino acids also play a key role in these peptides. Here 16 'charge' mutants of the two-peptide lantibiotic lacticin 3147 [composed of Ltnα (2+, 2-) and Ltnβ (2+)] were constructed which, when supplemented with previously generated peptides, results in a total bank of 23 derivatives altered in one or more charged residues. When examined individually, in combination with a wild-type partner or, in some instances, in combination with one another, these mutants reveal the importance of charge at specific locations within Ltnα and Ltnβ, confirm the critical role of the negatively charged glutamate residue in Ltnα and facilitate an investigation of the contribution of positively charged residues to the cationic Ltnβ. From these investigations it is also apparent that the relative importance of the overall charge of lacticin 3147 varies depending on the target bacteria and is most evident when strains with more negatively charged cell envelopes are targeted. These studies also result in, for the first time, the creation of a derivative of a lacticin 3147 peptide (LtnβR27A) which displays enhanced specific activity",

author = "Deegan, {Lucy H.} and Srinivas Suda and Lawton, {Elaine M.} and Draper, {Lorraine A.} and Floor Hugenholtz and Andreas Peschel and Colin Hill and Cotter, {Paul D.} and Ross, {R. Paul}",

year = "2010",

doi = "https://doi.org/10.1111/j.1751-7915.2009.00145.x",

language = "English",

volume = "3",

pages = "222--234",

journal = "Microbial biotechnology",

issn = "1751-7915",

publisher = "Wiley",

number = "2",

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TY - JOUR

T1 - Manipulation of charged residues within the two-peptide lantibiotic lacticin 3147

AU - Deegan, Lucy H.

AU - Suda, Srinivas

AU - Lawton, Elaine M.

AU - Draper, Lorraine A.

AU - Hugenholtz, Floor

AU - Peschel, Andreas

AU - Hill, Colin

AU - Cotter, Paul D.

AU - Ross, R. Paul

PY - 2010

Y1 - 2010

N2 - Lantibiotics are antimicrobial peptides which contain a high percentage of post-translationally modified residues. While most attention has been paid to the role of these critical structural features, evidence continues to emerge that charged amino acids also play a key role in these peptides. Here 16 'charge' mutants of the two-peptide lantibiotic lacticin 3147 [composed of Ltnα (2+, 2-) and Ltnβ (2+)] were constructed which, when supplemented with previously generated peptides, results in a total bank of 23 derivatives altered in one or more charged residues. When examined individually, in combination with a wild-type partner or, in some instances, in combination with one another, these mutants reveal the importance of charge at specific locations within Ltnα and Ltnβ, confirm the critical role of the negatively charged glutamate residue in Ltnα and facilitate an investigation of the contribution of positively charged residues to the cationic Ltnβ. From these investigations it is also apparent that the relative importance of the overall charge of lacticin 3147 varies depending on the target bacteria and is most evident when strains with more negatively charged cell envelopes are targeted. These studies also result in, for the first time, the creation of a derivative of a lacticin 3147 peptide (LtnβR27A) which displays enhanced specific activity

AB - Lantibiotics are antimicrobial peptides which contain a high percentage of post-translationally modified residues. While most attention has been paid to the role of these critical structural features, evidence continues to emerge that charged amino acids also play a key role in these peptides. Here 16 'charge' mutants of the two-peptide lantibiotic lacticin 3147 [composed of Ltnα (2+, 2-) and Ltnβ (2+)] were constructed which, when supplemented with previously generated peptides, results in a total bank of 23 derivatives altered in one or more charged residues. When examined individually, in combination with a wild-type partner or, in some instances, in combination with one another, these mutants reveal the importance of charge at specific locations within Ltnα and Ltnβ, confirm the critical role of the negatively charged glutamate residue in Ltnα and facilitate an investigation of the contribution of positively charged residues to the cationic Ltnβ. From these investigations it is also apparent that the relative importance of the overall charge of lacticin 3147 varies depending on the target bacteria and is most evident when strains with more negatively charged cell envelopes are targeted. These studies also result in, for the first time, the creation of a derivative of a lacticin 3147 peptide (LtnβR27A) which displays enhanced specific activity

U2 - https://doi.org/10.1111/j.1751-7915.2009.00145.x

DO - https://doi.org/10.1111/j.1751-7915.2009.00145.x

M3 - Article

C2 - 21255322

SN - 1751-7915

VL - 3

SP - 222

EP - 234

JO - Microbial biotechnology

JF - Microbial biotechnology

IS - 2

ER -