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Daniel Otzen

Bacterial amphiphiles as amyloid inducers: Effect of Rhamnolipid and Lipopolysaccharide on FapC fibrillation

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Bacterial amphiphiles as amyloid inducers : Effect of Rhamnolipid and Lipopolysaccharide on FapC fibrillation. / Najarzadeh, Zahra; Pedersen, Jannik Nedergaard; Christiansen, Gunna et al.

In: B B A - Proteins and Proteomics, Vol. 1867, No. 11, 140263, 01.11.2019.

Research output: Contribution to journal/Conference contribution in journal/Contribution to newspaper › Journal article › Research › peer-review

Vancouver

Najarzadeh Z, Pedersen JN, Christiansen G, Shojaosadati SA, Pedersen JS , Otzen DE. Bacterial amphiphiles as amyloid inducers: Effect of Rhamnolipid and Lipopolysaccharide on FapC fibrillation. B B A - Proteins and Proteomics. 2019 Nov 1;1867(11):140263. doi: 10.1016/j.bbapap.2019.140263

Author

Najarzadeh, Zahra ; Pedersen, Jannik Nedergaard ; Christiansen, Gunna et al. / Bacterial amphiphiles as amyloid inducers : Effect of Rhamnolipid and Lipopolysaccharide on FapC fibrillation. In: B B A - Proteins and Proteomics. 2019 ; Vol. 1867, No. 11.

Bibtex

@article{f7012ffeddb8418a9f47afb56bca39cd,

title = "Bacterial amphiphiles as amyloid inducers: Effect of Rhamnolipid and Lipopolysaccharide on FapC fibrillation",

abstract = "Pseudomonas species export the amyloid-forming protein FapC to strengthen bacterial biofilm. P. species also produce the biosurfactant rhamnolipid (Rhl) and its outer membrane contains lipopolysaccharide (LPS). Given the possible contacts between FapC, Rhl and LPS, we here investigate how Rhl and LPS affect FapC fibrillation compared with SDS, known to promote fibrillation of proteins at sub-micellar concentrations. Micelles of all three surfactants help FapC bypass the nucleation lag phase, leading to rapid fibrillation, which persists even at high concentrations of micelles and incorporates almost all available FapC monomers. Fibrils formed at high micellar concentrations of Rhl and SDS seed fibrillation at low surfactant concentrations while retaining the original fibril structure. FapC interacts strongly with SDS to form a dense network of narrow fibrils. Small angle X-ray scattering (SAXS) analyses reveal that surfactants reduce the population of intermediates in the fibrillation process and detect a fast aggregation step over the first 2-4 h which precedes the main fibrillation monitored by Thioflavin T. An additional SAXS-detected rearrangement of early aggregates occurs after 4-10 h. At high Rhl concentrations, the micelles are decorated with protein fibrils. SDS induces FapC fibrillation so efficiently that epigallocatechin-3-gallate (EGCG) is unable to inhibit this process. However, EGCG stimulates FapC oligomer formation and inhibits fibrillation both on its own and in the presence of Rhl and LPS. This oligomer could be modelled as a compact core with a flexible shell. This suggests that EGCG can override the natural amyloid-stimulatory properties of these biosurfactants and thus target biofilm.",

keywords = "FapC protein, Functional amyloid, Pseudomonas aeruginosa, Rhamnolipid, Surfactant",

author = "Zahra Najarzadeh and Pedersen, {Jannik Nedergaard} and Gunna Christiansen and Shojaosadati, {Seyed Abbas} and Pedersen, {Jan Skov} and Otzen, {Daniel E}",

note = "Copyright {\textcopyright} 2019. Published by Elsevier B.V.",

year = "2019",

month = nov,

day = "1",

doi = "10.1016/j.bbapap.2019.140263",

language = "English",

volume = "1867",

journal = "B B A - Proteins and Proteomics",

issn = "1570-9639",

publisher = "Elsevier BV",

number = "11",

}

RIS

TY - JOUR

T1 - Bacterial amphiphiles as amyloid inducers

T2 - Effect of Rhamnolipid and Lipopolysaccharide on FapC fibrillation

AU - Najarzadeh, Zahra

AU - Pedersen, Jannik Nedergaard

AU - Christiansen, Gunna

AU - Shojaosadati, Seyed Abbas

AU - Pedersen, Jan Skov

AU - Otzen, Daniel E

PY - 2019/11/1

Y1 - 2019/11/1

N2 - Pseudomonas species export the amyloid-forming protein FapC to strengthen bacterial biofilm. P. species also produce the biosurfactant rhamnolipid (Rhl) and its outer membrane contains lipopolysaccharide (LPS). Given the possible contacts between FapC, Rhl and LPS, we here investigate how Rhl and LPS affect FapC fibrillation compared with SDS, known to promote fibrillation of proteins at sub-micellar concentrations. Micelles of all three surfactants help FapC bypass the nucleation lag phase, leading to rapid fibrillation, which persists even at high concentrations of micelles and incorporates almost all available FapC monomers. Fibrils formed at high micellar concentrations of Rhl and SDS seed fibrillation at low surfactant concentrations while retaining the original fibril structure. FapC interacts strongly with SDS to form a dense network of narrow fibrils. Small angle X-ray scattering (SAXS) analyses reveal that surfactants reduce the population of intermediates in the fibrillation process and detect a fast aggregation step over the first 2-4 h which precedes the main fibrillation monitored by Thioflavin T. An additional SAXS-detected rearrangement of early aggregates occurs after 4-10 h. At high Rhl concentrations, the micelles are decorated with protein fibrils. SDS induces FapC fibrillation so efficiently that epigallocatechin-3-gallate (EGCG) is unable to inhibit this process. However, EGCG stimulates FapC oligomer formation and inhibits fibrillation both on its own and in the presence of Rhl and LPS. This oligomer could be modelled as a compact core with a flexible shell. This suggests that EGCG can override the natural amyloid-stimulatory properties of these biosurfactants and thus target biofilm.

AB - Pseudomonas species export the amyloid-forming protein FapC to strengthen bacterial biofilm. P. species also produce the biosurfactant rhamnolipid (Rhl) and its outer membrane contains lipopolysaccharide (LPS). Given the possible contacts between FapC, Rhl and LPS, we here investigate how Rhl and LPS affect FapC fibrillation compared with SDS, known to promote fibrillation of proteins at sub-micellar concentrations. Micelles of all three surfactants help FapC bypass the nucleation lag phase, leading to rapid fibrillation, which persists even at high concentrations of micelles and incorporates almost all available FapC monomers. Fibrils formed at high micellar concentrations of Rhl and SDS seed fibrillation at low surfactant concentrations while retaining the original fibril structure. FapC interacts strongly with SDS to form a dense network of narrow fibrils. Small angle X-ray scattering (SAXS) analyses reveal that surfactants reduce the population of intermediates in the fibrillation process and detect a fast aggregation step over the first 2-4 h which precedes the main fibrillation monitored by Thioflavin T. An additional SAXS-detected rearrangement of early aggregates occurs after 4-10 h. At high Rhl concentrations, the micelles are decorated with protein fibrils. SDS induces FapC fibrillation so efficiently that epigallocatechin-3-gallate (EGCG) is unable to inhibit this process. However, EGCG stimulates FapC oligomer formation and inhibits fibrillation both on its own and in the presence of Rhl and LPS. This oligomer could be modelled as a compact core with a flexible shell. This suggests that EGCG can override the natural amyloid-stimulatory properties of these biosurfactants and thus target biofilm.

KW - FapC protein

KW - Functional amyloid

KW - Pseudomonas aeruginosa

KW - Rhamnolipid

KW - Surfactant

U2 - 10.1016/j.bbapap.2019.140263

DO - 10.1016/j.bbapap.2019.140263

M3 - Journal article

C2 - 31421227

VL - 1867

JO - B B A - Proteins and Proteomics

JF - B B A - Proteins and Proteomics

SN - 1570-9639

IS - 11

M1 - 140263

ER -