Class II bacteriocin

Class IIb bacteriocin
Class IIb bacteriocin
Identifiers
Symbol	Antimicrobial17
Pfam	PF08129
Pfam clan	CL0400
InterPro	IPR012950
TCDB	1.C.25
OPM superfamily	219
OPM protein	2jpj
Pfam
Available protein structures:
Pfam	structures / ECOD
PDB	RCSB PDB; PDBe; PDBj
PDBsum	structure summary

Available protein structures:
Pfam	structures / ECOD
PDB	RCSB PDB; PDBe; PDBj
PDBsum	structure summary

Class II bacteriocin
Class II bacteriocin
	Three-dimensional structure of leucocin A, a type IIa bacteriocin.
Identifiers
Symbol	Bacteriocin_II
Pfam	PF01721
InterPro	IPR002633
PROSITE	PDOC60030
SCOP2	3leu / SCOPe / SUPFAM
TCDB	1.C.24
OPM superfamily	141
OPM protein	1ohm
Pfam
Available protein structures:
Pfam	structures / ECOD
PDB	RCSB PDB; PDBe; PDBj
PDBsum	structure summary

Last updated January 26, 2023

Class II bacteriocins are a class of small peptides that inhibit the growth of various bacteria.

Class IIa

One important and well studied class of bacteriocins is the class IIa or pediocin-like bacteriocins produced by lactic acid bacteria. All class IIa bacteriocins are produced by food-associated strains, isolated from a variety of food products of industrial and natural origins, including meat products, dairy products and vegetables. Class IIa bacteriocins are all cationic, display anti- Listeria activity, and kill target cells by permeabilizing the cell membrane.^[2]^[3]^[4]

Class IIa bacteriocins contain between 37 and 48 residues.^[5] Based on their primary structures, the peptide chains of class IIa bacteriocins may be divided roughly into two regions: a hydrophilic, cationic and highly conserved N-terminal region, and a less conserved hydrophobic/amphiphilic C-terminal region. The N-terminal region contains the conserved Y-G-N-G-V/L 'pediocin box' motif and two conserved cysteine residues joined by a disulfide bridge. It forms a three-stranded antiparallel beta-sheet supported by the conserved disulfide bridge. This cationic N-terminal beta-sheet domain mediates binding of the class IIa bacteriocin to the target cell membrane. The C-terminal region forms a hairpin-like domain that penetrates into the hydrophobic part of the target cell membrane, thereby mediating leakage through the membrane. The two domains are joined by a hinge, which enables movement of the domains relative to each other.^[3]^[4]

Some proteins known to belong to the class IIa bacteriocin family are listed below:

Pediococcus acidilactici pediocin PA-1.^[6]
Leuconostoc mesenteroides mesentericin Y105.
Carnobacterium piscicola carnobacteriocin B2.
Lactobacillus sakei sakacin P.
Enterococcus faecium enterocin A.
Enterococcus faecium enterocin P.
Leuconostoc gelidum leucocin A.
Lactobacillus curvatus curvacin A.^[7]
Listeria innocua listeriocin 743A.

Class IIb

The class IIb bacteriocins (two-peptide bacteriocins) require two different peptides for activity. It includes the alpha enterocins and lactococcin G peptides. These peptides have some antimicrobial properties; they inhibit the growth of Enterococcus spp. and a few other Gram-positive bacteria. These peptides act as pore-forming toxins that create cell membrane channels through a barrel-stave mechanism and thus produce an ionic imbalance in the cell ^[8]

Class IIc

Bacteriocin_IIc

x-ray structure of bacteriocin as-48 at ph 4.5. sulphate bound form

Identifiers

Symbol

Bacteriocin_IIc

Pfam

PF09221

InterPro

IPR009086

SCOP2

1o82 / SCOPe / SUPFAM

TCDB

1.C.28

OPM superfamily

77

OPM protein

1o82

Available protein structures:
Pfam	structures / ECOD
PDB	RCSB PDB; PDBe; PDBj
PDBsum	structure summary

Other class II bacteriocins can be grouped together as Class IIc (circular bacteriocins). These have a wide range of effects on membrane permeability, cell wall formation and pheromone actions of target cells. In particular, Bacteriocin AS-48 is a cyclic peptide antibiotic produced by the eubacteria Enterococcus faecalis (Streptococcus faecalis) that shows a broad antimicrobial spectrum against both Gram-positive and Gram-negative bacteria. Bacteriocin AS-48 is encoded by the pheromone-responsive plasmid pMB2, and acts on the plasma membrane in which it opens pores leading to ion leakage and cell death.^[9] The globular structure of bacteriocin AS-48 consists of five alpha helices enclosing a hydrophobic core. The mammalian NK-lysin effector protein of T and natural killer cells has a similar structure, though it lacks sequence homology with bacteriocins AS-48.

Related Research Articles

Bacteriocins are proteinaceous or peptidic toxins produced by bacteria to inhibit the growth of similar or closely related bacterial strain(s). They are similar to yeast and paramecium killing factors, and are structurally, functionally, and ecologically diverse. Applications of bacteriocins are being tested to assess their application as narrow-spectrum antibiotics.

Lantibiotics are a class of polycyclic peptide antibiotics that contain the characteristic thioether amino acids lanthionine or methyllanthionine, as well as the unsaturated amino acids dehydroalanine, and 2-aminoisobutyric acid. They belong to ribosomally synthesized and post-translationally modified peptides.

<span class="mw-page-title-main">Polymyxin</span>

Polymyxins are antibiotics. Polymyxins B and E are used in the treatment of Gram-negative bacterial infections. They work mostly by breaking up the bacterial cell membrane. They are part of a broader class of molecules called nonribosomal peptides.

Streptococcus salivarius is a species of spherical, gram-positive, facultative anaerobic lactic acid bacteria that is both catalase and oxidase negative. S. salivarius colonizes the oral cavity and upper respiratory tract of humans just a few hours after birth, making further exposure to the bacteria harmless in most circumstances. The bacteria is considered an opportunistic pathogen, rarely finding its way into the bloodstream, where it has been implicated in cases of sepsis in people with neutropenia,.

Antimicrobial peptides (AMPs), also called host defence peptides (HDPs) are part of the innate immune response found among all classes of life. Fundamental differences exist between prokaryotic and eukaryotic cells that may represent targets for antimicrobial peptides. These peptides are potent, broad spectrum antibiotics which demonstrate potential as novel therapeutic agents. Antimicrobial peptides have been demonstrated to kill Gram negative and Gram positive bacteria, enveloped viruses, fungi and even transformed or cancerous cells. Unlike the majority of conventional antibiotics it appears that antimicrobial peptides frequently destabilize biological membranes, can form transmembrane channels, and may also have the ability to enhance immunity by functioning as immunomodulators.

Lactobacillales are an order of gram-positive, low-GC, acid-tolerant, generally nonsporulating, nonrespiring, either rod-shaped (bacilli) or spherical (cocci) bacteria that share common metabolic and physiological characteristics. These bacteria, usually found in decomposing plants and milk products, produce lactic acid as the major metabolic end product of carbohydrate fermentation, giving them the common name lactic acid bacteria (LAB).

In molecular biology, the Signal Peptide Peptidase (SPP) is a type of protein that specifically cleaves parts of other proteins. It is an intramembrane aspartyl protease with the conserved active site motifs 'YD' and 'GxGD' in adjacent transmembrane domains (TMDs). Its sequences is highly conserved in different vertebrate species. SPP cleaves remnant signal peptides left behind in membrane by the action of signal peptidase and also plays key roles in immune surveillance and the maturation of certain viral proteins.

Lysins, also known as endolysins or murein hydrolases, are hydrolytic enzymes produced by bacteriophages in order to cleave the host's cell wall during the final stage of the lytic cycle. Lysins are highly evolved enzymes that are able to target one of the five bonds in peptidoglycan (murein), the main component of bacterial cell walls, which allows the release of progeny virions from the lysed cell. Cell-wall-containing Archaea are also lysed by specialized pseudomurein-cleaving lysins, while most archaeal viruses employ alternative mechanisms. Similarly, not all bacteriophages synthesize lysins: some small single-stranded DNA and RNA phages produce membrane proteins that activate the host's autolytic mechanisms such as autolysins.

Alpha defensins are a family of mammalian defensin peptides of the alpha subfamily. In mammals they are also known as cryptdins and are produced within the small bowel. Cryptdin is a portmanteau of crypt and defensin.

<span class="mw-page-title-main">Beta defensin</span>

Beta defensins are a family of vertebrate defensins. The beta defensins are antimicrobial peptides implicated in the resistance of epithelial surfaces to microbial colonization.

Sakacins are bacteriocins produced by Lactobacillus sakei. They are often clustered with the other lactic acid bacteriocins. The best known sakacins are sakacin A, G, K, P, and Q. In particular, sakacin A and P have been well characterized.

Enterococcus gallinarum is a species of Enterococcus. E. gallinarum demonstrates an inherent, low-level resistance to vancomycin. Resistance is due to a chromosomal gene, vanC, which encodes for a terminal D-alanine-D-serine instead of the usual D-alanine-D-alanine in cell wall peptidoglycan precursor proteins. That is a separate mechanism than the vancomycin resistance seen in VRE isolates of E. faecium and E. faecalis which is mediated by vanA or vanB. This species is known to cause clusters of infection, although it considered very rare. It is the only other known enterococcal species besides E. faecium and E. faecalis known to cause outbreaks and spread in hospitals.

<span class="mw-page-title-main">Sortase</span> Group of prokaryotic enzymes

Sortase refers to a group of prokaryotic enzymes that modify surface proteins by recognizing and cleaving a carboxyl-terminal sorting signal. For most substrates of sortase enzymes, the recognition signal consists of the motif LPXTG (Leu-Pro-any-Thr-Gly), then a highly hydrophobic transmembrane sequence, followed by a cluster of basic residues such as arginine. Cleavage occurs between the Thr and Gly, with transient attachment through the Thr residue to the active site Cys residue, followed by transpeptidation that attaches the protein covalently to cell wall components. Sortases occur in almost all Gram-positive bacteria and the occasional Gram-negative bacterium or Archaea, where cell wall LPXTG-mediated decoration has not been reported. Although sortase A, the "housekeeping" sortase, typically acts on many protein targets, other forms of sortase recognize variant forms of the cleavage motif, or catalyze the assembly of pilins into pili.

Polymers with the ability to kill or inhibit the growth of microorganisms such as bacteria, fungi, or viruses are classified as antimicrobial agents. This class of polymers consists of natural polymers with inherent antimicrobial activity and polymers modified to exhibit antimicrobial activity. Polymers are generally nonvolatile, chemically stable, and can be chemically and physically modified to display desired characteristics and antimicrobial activity. Antimicrobial polymers are a prime candidate for use in the food industry to prevent bacterial contamination and in water sanitation to inhibit the growth of microorganisms in drinking water.

Bacteriocin AS-48 is a cyclic peptide antibiotic produced by the eubacteria Enterococcus faecalis that shows a broad antimicrobial spectrum against both Gram-positive and Gram-negative bacteria. Bacteriocin AS-48 is encoded by the pheromone-responsive plasmid pMB2, and acts on the plasma membrane in which it opens pores leading to ion leakage and cell death. The globular structure of bacteriocin AS-48 is composed of five alpha helices enclosing a hydrophobic core. The mammalian NK-lysin effector protein of T and natural killer cells has a similar structure, though it lacks sequence homology with bacteriocins AS-48.

<span class="mw-page-title-main">Trimeric autotransporter adhesin</span> Proteins found on the outer membrane of Gram-negative bacteria

In molecular biology, trimeric autotransporter adhesins (TAAs), are proteins found on the outer membrane of Gram-negative bacteria. Bacteria use TAAs in order to infect their host cells via a process called cell adhesion. TAAs also go by another name, oligomeric coiled-coil adhesins, which is shortened to OCAs. In essence, they are virulence factors, factors that make the bacteria harmful and infective to the host organism.

Virtual colony count (VCC) is a kinetic, 96-well microbiological assay originally developed to measure the activity of defensins. It has since been applied to other antimicrobial peptides including LL-37. It utilizes a method of enumerating bacteria called quantitative growth kinetics, which compares the time taken for a bacterial batch culture to reach a threshold optical density with that of a series of calibration curves. The name VCC has also been used to describe the application of quantitative growth kinetics to enumerate bacteria in cell culture infection models. Antimicrobial susceptibility testing (AST) can be done on 96-well plates by diluting the antimicrobial agent at varying concentrations in broth inoculated with bacteria and measuring the minimum inhibitory concentration that results in no growth. However, these methods cannot be used to study some membrane-active antimicrobial peptides, which are inhibited by the broth itself. The virtual colony count procedure takes advantage of this fact by first exposing bacterial cells to the active antimicrobial agent in a low-salt buffer for two hours, then simultaneously inhibiting antimicrobial activity and inducing exponential growth by adding broth. The growth kinetics of surviving cells can then be monitored using a temperature-controlled plate reader. The time taken for each growth curve to reach a threshold change in optical density is then converted into virtual survival values, which serve as a measure of antimicrobial activity.

<span class="mw-page-title-main">OmpT</span>

OmpT is an aspartyl protease found on the outer membrane of Escherichia coli. OmpT is a subtype of the family of omptin proteases, which are found on some gram-negative species of bacteria.

Ribosomally synthesized and post-translationally modified peptides (RiPPs), also known as ribosomal natural products, are a diverse class of natural products of ribosomal origin. Consisting of more than 20 sub-classes, RiPPs are produced by a variety of organisms, including prokaryotes, eukaryotes, and archaea, and they possess a wide range of biological functions.

<span class="mw-page-title-main">MP196</span>

MP196 is a synthetic antimicrobial peptide. It falls under the structural class: short cationic peptides. Since it is a short cationic peptide, it can be easily synthesized, derivatized and isolated. MP196 is rich in tryptophan, a hydrophobic amino acid and arginine residues, a positively charged amino acid. It has structure: RWRWRW-NH2. This a short linear peptide with minimal pharmacophore. MP196 is effective against gram-positive bacteria and moderately effective against gram-negative bacteria.

References

↑ Fregeau Gallagher NL, Sailer M, Niemczura WP, Nakashima TT, Stiles ME, Vederas JC (December 1997). "Three-dimensional structure of leucocin A in trifluoroethanol and dodecylphosphocholine micelles: spatial location of residues critical for biological activity in type IIa bacteriocins from lactic acid bacteria". Biochemistry. 36 (49): 15062–72. doi:10.1021/bi971263h. PMID 9398233.
↑ Ennahar S, Sonomoto K, Ishizaki A (1999). "Class IIa bacteriocins from lactic acid bacteria: antibacterial activity and food preservation". J. Biosci. Bioeng. 87 (6): 705–16. doi:10.1016/S1389-1723(99)80142-X. PMID 16232543.
1 2 Fimland G, Nissen-Meyer J, Johnsen L (2005). "The C-terminal domain of pediocin-like antimicrobial peptides (class IIa bacteriocins) is involved in specific recognition of the C-terminal part of cognate immunity proteins and in determining the antimicrobial spectrum". J. Biol. Chem. 280 (10): 9243–50. doi: 10.1074/jbc.M412712200 . PMID 15611086.
1 2 Dalhus B, Fimland G, Nissen-Meyer J, Johnsen L (2005). "Pediocin-like antimicrobial peptides (class IIa bacteriocins) and their immunity proteins: biosynthesis, structure, and mode of action". J. Pept. Sci. 11 (11): 688–96. doi:10.1002/psc.699. PMID 16059970. S2CID 38561151.
↑ Simon L, Fremaux C, Cenatiempo Y, Berjeaud JM (2002). "Sakacin g, a new type of antilisterial bacteriocin". Appl. Environ. Microbiol. 68 (12): 6416–20. doi:10.1128/AEM.68.12.6416-6420.2002. PMC 134399 . PMID 12450870.
↑ Zhu, Liyan; Zeng, Jianwei; Wang, Chang; Wang, Jiawei (2022-02-08). "Structural Basis of Pore Formation in the Mannose Phosphotransferase System by Pediocin PA-1". Applied and Environmental Microbiology. 88 (3): e0199221. doi:10.1128/AEM.01992-21. ISSN 1098-5336. PMC 8824269 . PMID 34851716.
↑ Zhu, Liyan; Zeng, Jianwei; Wang, Jiawei (2022-06-15). "Structural Basis of the Immunity Mechanisms of Pediocin-like Bacteriocins". Applied and Environmental Microbiology. 88 (13): e0048122. doi:10.1128/aem.00481-22. ISSN 1098-5336. PMC 9275228 . PMID 35703550.
↑ Balla E, Dicks LM, Du Toit M, Van Der Merwe MJ, Holzapfel WH (April 2000). "Characterization and cloning of the genes encoding enterocin 1071A and enterocin 1071B, two antimicrobial peptides produced by Enterococcus faecalis BFE 1071". Appl. Environ. Microbiol. 66 (4): 1298–304. doi:10.1128/aem.66.4.1298-1304.2000. PMC 91984 . PMID 10742203.
↑ González C, Langdon GM, Bruix M, Gálvez A, Valdivia E, Maqueda M, Rico M (October 2000). "Bacteriocin AS-48, a microbial cyclic polypeptide structurally and functionally related to mammalian NK-lysin". Proc. Natl. Acad. Sci. U.S.A. 97 (21): 11221–6. Bibcode:2000PNAS...9711221G. doi: 10.1073/pnas.210301097 . PMC 17181 . PMID 11005847.

External links

Class II bacteriocin and related families is variously recorded in Pfam and InterPro as:

Pfam	Pfam symbol	InterPro	InterPro symbol
PF08129	Antimicrobial17	InterPro : IPR012950	Alpha_enterocin/lactococcin
PF01721	Bacteriocin_II	InterPro : IPR002633	Bacteriocin_IIa
PF10439	Bacteriocin_IIc	InterPro : IPR019493	Bacteriocin_IIb_lactacin-rel
PF12173	BacteriocIIc_cy	InterPro : IPR020970	Bacteriocin_IIc
PF04369	Lactococcin	InterPro : IPR007464	Bacteriocin_IId
PF04604	L_biotic_typeA	InterPro : IPR007682	Lantibiotic_typ-A_Lactobact

The naming is inconsistent at times.

This article incorporates text from the public domain Pfam and InterPro: IPR002633

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[pmid9398233-1] Fregeau Gallagher NL, Sailer M, Niemczura WP, Nakashima TT, Stiles ME, Vederas JC (December 1997). "Three-dimensional structure of leucocin A in trifluoroethanol and dodecylphosphocholine micelles: spatial location of residues critical for biological activity in type IIa bacteriocins from lactic acid bacteria". Biochemistry. 36 (49): 15062–72. doi:10.1021/bi971263h. PMID 9398233.

[PUB00033828-2] Ennahar S, Sonomoto K, Ishizaki A (1999). "Class IIa bacteriocins from lactic acid bacteria: antibacterial activity and food preservation". J. Biosci. Bioeng. 87 (6): 705–16. doi:10.1016/S1389-1723(99)80142-X. PMID 16232543.

[PUB00033829-3] 1 2 Fimland G, Nissen-Meyer J, Johnsen L (2005). "The C-terminal domain of pediocin-like antimicrobial peptides (class IIa bacteriocins) is involved in specific recognition of the C-terminal part of cognate immunity proteins and in determining the antimicrobial spectrum". J. Biol. Chem. 280 (10): 9243–50. doi: 10.1074/jbc.M412712200 . PMID 15611086.

[PUB00033830-4] 1 2 Dalhus B, Fimland G, Nissen-Meyer J, Johnsen L (2005). "Pediocin-like antimicrobial peptides (class IIa bacteriocins) and their immunity proteins: biosynthesis, structure, and mode of action". J. Pept. Sci. 11 (11): 688–96. doi:10.1002/psc.699. PMID 16059970. S2CID 38561151.

[pmid12450870-5] Simon L, Fremaux C, Cenatiempo Y, Berjeaud JM (2002). "Sakacin g, a new type of antilisterial bacteriocin". Appl. Environ. Microbiol. 68 (12): 6416–20. doi:10.1128/AEM.68.12.6416-6420.2002. PMC 134399 . PMID 12450870.

[6] Zhu, Liyan; Zeng, Jianwei; Wang, Chang; Wang, Jiawei (2022-02-08). "Structural Basis of Pore Formation in the Mannose Phosphotransferase System by Pediocin PA-1". Applied and Environmental Microbiology. 88 (3): e0199221. doi:10.1128/AEM.01992-21. ISSN 1098-5336. PMC 8824269 . PMID 34851716.

[7] Zhu, Liyan; Zeng, Jianwei; Wang, Jiawei (2022-06-15). "Structural Basis of the Immunity Mechanisms of Pediocin-like Bacteriocins". Applied and Environmental Microbiology. 88 (13): e0048122. doi:10.1128/aem.00481-22. ISSN 1098-5336. PMC 9275228 . PMID 35703550.

[pmid10742203-8] Balla E, Dicks LM, Du Toit M, Van Der Merwe MJ, Holzapfel WH (April 2000). "Characterization and cloning of the genes encoding enterocin 1071A and enterocin 1071B, two antimicrobial peptides produced by Enterococcus faecalis BFE 1071". Appl. Environ. Microbiol. 66 (4): 1298–304. doi:10.1128/aem.66.4.1298-1304.2000. PMC 91984 . PMID 10742203.

[pmid11005847-9] González C, Langdon GM, Bruix M, Gálvez A, Valdivia E, Maqueda M, Rico M (October 2000). "Bacteriocin AS-48, a microbial cyclic polypeptide structurally and functionally related to mammalian NK-lysin". Proc. Natl. Acad. Sci. U.S.A. 97 (21): 11221–6. Bibcode:2000PNAS...9711221G. doi: 10.1073/pnas.210301097 . PMC 17181 . PMID 11005847.

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