Advances in Molecular Understanding of α-helical
Membrane-Active Peptides.

KABELKA, Ivo a Robert VÁCHA. Advances in Molecular Understanding of α-helical Membrane-Active Peptides. Accounts of chemical research. American Chemical Society, 2021, roč. 54, č. 9, s. 2196-2204. ISSN 0001-4842. Dostupné z: https://dx.doi.org/10.1021/acs.accounts.1c00047.

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TY  - JOUR
ID  - 1773100
AU  - Kabelka, Ivo - Vácha, Robert
PY  - 2021
TI  - Advances in Molecular Understanding of α-helical Membrane-Active Peptides.
JF  - Accounts of chemical research
VL  - 54
IS  - 9
SP  - 2196-2204
EP  - 2196-2204
PB  - American Chemical Society
SN  - 00014842
KW  - ANTIMICROBIAL PEPTIDESPORE FORMATIONMAGAININ 2LIPID-BILAYERSBUFORIN IISIMULATIONSMECHANISMTRANSLOCATIONSPECTROSCOPYALAMETHICIN
UR  - https://pubs.acs.org/doi/10.1021/acs.accounts.1c00047
N2  - CONSPECTUS: Biological membranes separate the interior of cells or cellular compartments from their outer environments. This barrier function of membranes can be disrupted by membrane-active peptides, some of which can spontaneously penetrate through the membranes or open leaky transmembrane pores. However, the origin of their activity/toxicity is not sufficiently understood for the development of more potent peptides. To this day, there are no design rules that would be generally valid, and the role of individual amino acids tends to be sequence-specific. In this Account, we describe recent progress in understanding the design principles that govern the activity of membrane-active peptides. We focus on alpha-helical amphiphilic peptides and their ability to (1) translocate across phospholipid bilayers, (2) form transmembrane pores, or (3) act synergistically, i.e., to produce a significantly more potent effect in a mixture than the individual components. We refined the description of peptide translocation using computer simulations and demonstrated the effect of selected residues. Our simulations showed the necessity to explicitly include charged residues in the translocation description to correctly sample the membrane perturbations they can cause. Using this description, we calculated the translocation of helical peptides with and without the kink induced by the proline/glycine residue. The presence of the kink had no effect on the translocation barrier, but it decreased the peptide affinity to the membrane and reduced the peptide stability inside the membrane. Interestingly, the effects were mainly caused by the peptide's increased polarity, not the higher flexibility of the kink. Flexibility plays a crucial role in pore formation and affects distinct pore structures in different ways. The presence of a kink destabilizes barrel-stave pores, because the kink prevents the tight packing of peptides in the bundle, which is characteristic of the barrel-stave structure. In contrast, the kink facilitates the formation of toroidal pores, where the peptides are only loosely arranged and do not need to closely assemble. The exact position of the kink in the sequence further determines the preferred arrangement of peptides in the pore, i.e., an hourglass or U-shaped structure. In addition, we demonstrated that two self-associated (via termini) helical peptides could mimic the behavior of peptides with a helix-kink-helix motif. Finally, we review the recent findings on the peptide synergism of the archetypal mixture of Magainin 2 and PGLa peptides. We focused on a bacterial plasma membrane mimic that contains negatively charged lipids and lipids with negative intrinsic curvature. We showed that the synergistic action of peptides was highly dependent on the lipid composition. When the lipid composition and peptide/lipid ratios were changed, the systems exhibited more complex behavior than just the previously reported pore formation. We observed membrane adhesion, fusion, and even the formation of the sponge phase in this regime. Furthermore, enhanced adhesion/partitioning to the membrane was reported to be caused by lipid-induced peptide aggregation. In conclusion, the provided molecular insight into the complex behavior of membrane-active peptides provides clues for the design and modification of antimicrobial peptides or toxins.
ER  -

Základní údaje
Originální název	Advances in Molecular Understanding of α-helical Membrane-Active Peptides.
Autoři	KABELKA, Ivo (203 Česká republika, domácí) a Robert VÁCHA (203 Česká republika, garant, domácí).
Vydání	Accounts of chemical research, American Chemical Society, 2021, 0001-4842.

Další údaje
Originální jazyk	angličtina
Typ výsledku	Článek v odborném periodiku
Obor	10608 Biochemistry and molecular biology
Stát vydavatele	Spojené státy
Utajení	není předmětem státního či obchodního tajemství
WWW	URL
Impakt faktor	Impact factor: 24.466
Kód RIV	RIV/00216224:14740/21:00118992
Organizační jednotka	Středoevropský technologický institut
Doi	http://dx.doi.org/10.1021/acs.accounts.1c00047
UT WoS	000648508400014
Klíčová slova anglicky	ANTIMICROBIAL PEPTIDESPORE FORMATIONMAGAININ 2LIPID-BILAYERSBUFORIN IISIMULATIONSMECHANISMTRANSLOCATIONSPECTROSCOPYALAMETHICIN
Štítky	rivok
Příznaky	Mezinárodní význam, Recenzováno
Změnil	Změnila: Mgr. Pavla Foltynová, Ph.D., učo 106624. Změněno: 26. 2. 2022 15:16.

Anotace

CONSPECTUS: Biological membranes separate the interior of cells or cellular compartments from their outer environments. This barrier function of membranes can be disrupted by membrane-active peptides, some of which can spontaneously penetrate through the membranes or open leaky transmembrane pores. However, the origin of their activity/toxicity is not sufficiently understood for the development of more potent peptides. To this day, there are no design rules that would be generally valid, and the role of individual amino acids tends to be sequence-specific. In this Account, we describe recent progress in understanding the design principles that govern the activity of membrane-active peptides. We focus on alpha-helical amphiphilic peptides and their ability to (1) translocate across phospholipid bilayers, (2) form transmembrane pores, or (3) act synergistically, i.e., to produce a significantly more potent effect in a mixture than the individual components. We refined the description of peptide translocation using computer simulations and demonstrated the effect of selected residues. Our simulations showed the necessity to explicitly include charged residues in the translocation description to correctly sample the membrane perturbations they can cause. Using this description, we calculated the translocation of helical peptides with and without the kink induced by the proline/glycine residue. The presence of the kink had no effect on the translocation barrier, but it decreased the peptide affinity to the membrane and reduced the peptide stability inside the membrane. Interestingly, the effects were mainly caused by the peptide's increased polarity, not the higher flexibility of the kink. Flexibility plays a crucial role in pore formation and affects distinct pore structures in different ways. The presence of a kink destabilizes barrel-stave pores, because the kink prevents the tight packing of peptides in the bundle, which is characteristic of the barrel-stave structure. In contrast, the kink facilitates the formation of toroidal pores, where the peptides are only loosely arranged and do not need to closely assemble. The exact position of the kink in the sequence further determines the preferred arrangement of peptides in the pore, i.e., an hourglass or U-shaped structure. In addition, we demonstrated that two self-associated (via termini) helical peptides could mimic the behavior of peptides with a helix-kink-helix motif. Finally, we review the recent findings on the peptide synergism of the archetypal mixture of Magainin 2 and PGLa peptides. We focused on a bacterial plasma membrane mimic that contains negatively charged lipids and lipids with negative intrinsic curvature. We showed that the synergistic action of peptides was highly dependent on the lipid composition. When the lipid composition and peptide/lipid ratios were changed, the systems exhibited more complex behavior than just the previously reported pore formation. We observed membrane adhesion, fusion, and even the formation of the sponge phase in this regime. Furthermore, enhanced adhesion/partitioning to the membrane was reported to be caused by lipid-induced peptide aggregation. In conclusion, the provided molecular insight into the complex behavior of membrane-active peptides provides clues for the design and modification of antimicrobial peptides or toxins.

Návaznosti
GA20-20152S, projekt VaV	Název: Proteinová přitažlivost a selektivita pro buněčné membrány
GA20-20152S, projekt VaV	Investor: Grantová agentura ČR, Protein Affinity and Selectivity to Cellular Membranes
LL2007, projekt VaV	Název: Peptidoví zabijáci bakterií (Akronym: PeptideKillers)
LL2007, projekt VaV	Investor: Ministerstvo školství, mládeže a tělovýchovy ČR, Peptide Killers of Bacteria

VytisknoutZobrazeno: 25. 7. 2024 12:34

Advances in Molecular Understanding of α-helical Membrane-Active Peptides.

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