Post on 30-Jul-2018
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Bacteriocins as alternatives to antibiotics : the case of enterocins DD14 AND DD28
OIE headquarters, Paris, FranceDecember 13th 2016
Pr. Djamel DRIDERLille University Sciences and Technologies
E-mail : djamel.drider@univ-lille1.frTwitter @DjamelDrider
I would like to thank- Dr. Cyril G. Gay (USDA)- Dr. Bruce Seal (Oregon State University)
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What are bacteriocins ?Bacteriocins are AMPs :
- ribosomally synthesized- proteinaceous nature- non-cytotoxic (usually)- active against bacteria which are closely related to the
producing strains but…- stable at extreme pHs and temperatures- produced by both Gram-negative and Gram-positive bacteria
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> 2756 AMPs registered in APDhttp://aps.unmc.edu/AP/main.php
Nebraska University – USA.
- 276 Bacteriocins- 337 Plants- 04 Archaea- 08 Protists- 13 Fungi- 2070 Animals
Antimicrobial Peptides Database content on December, 12th 2016
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BACTERIOCINS OR REAL SWISS KNIFE
Functions allocated to bacteriocins- Antimicrobial Agents- Antibiotics-Improving Complementary Agents- Antiviral Agents- Microbiota Regulators- Anticancer Agents- Plant Growth Promotors- Emerging functions (immuno-stimulating agents, virulence factor)
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BACTERIOCINS
Gram-negative bacteriaEnterobacteriaceae Bacilli
Lactic acid bacteriaColicins
Microcins (> 40 representatives) Bacteriocins – hundreds -
COMMON POINTSStability at extreme pHs and temperatures
MW < 10 kDa
Microcins (class I) 1 < MW < 3 KDa Post-translational modifications
(lasso-peptides)
Microcins (classe II) 6 < MW < 10 KDaSiderophores peptides
Gram-positive bacteria
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Mode of action of LAB bacteriocins
Pore forming Cell – membrane target
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MODE OF ACTION THROUGH PORE-FORMING
Intracellularside K+, amino-acids, inorganic phosphate, ATP
+ --+
Extracellularside
8NAGHMOUCHI, DRIDER and FLISS. (2007). Journal of Applied Microbiology 102:1508-1517.
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Cell-membrane targetFigure two
Lipid II : Concentration “nanomolar”
Figure credit Dr. Paul CotterUniversity college, Cork. Ireland
Class IIa bacteriocin
Interaction with docking protein on the cell membrane (MptC)
2. Pore-formation andpermeabilization of the cellmembrane
Figure from Drider et al. Mic Mol Biol Reviews (2006)
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uracil phosphoribosyl transferase
AnimalsHumans
LAB bacteriocins inputs – Management of antibiotics
- Replacement of fading antibiotics (in some cases !)- Antibiotics-Improving Complementary Agents ! (potentialization of antibiotics)
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- 6 samples of meconium from six blind donors (Roubaix hospital, France) - Isolation on MRS medium- Selection of Gram-positive and devoid of catalase activity (Lactic Acid Bacteria)
Distribution of LAB isolates
107 bacterial isolates
0
5
10
15
20
25
30
1 2 3 4 5 6
num
bers
of b
acte
ria in
sam
ples
Samples
20 20
12 12
26
17
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Identification of bacterial isolatesClassical and molecular methods
Enterococcus faecalis
141414
0
5
10
15
20
25
30
1 2 3 4 5 6
num
bers
of b
acte
ria in
sam
ples
Samples
(Ef 14, Ef 28, Ef 90, Ef 97 and Ef 101) (Ef 93)
Ef 14
Ef 28 Ef 90
Ef 93
Ef 97Ef 101
Antimicrobial activity by welldiffusion method against Listeria
innocua
Screening of antibacterial activity
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Indicator strains Ef 14 Ef 28 Ef 90 Ef 93 Ef 97 Ef 101
BN AN BN AN BN AN BN AN BN AN BN ANListeria monocytogenes +++* ++ +++ ++ ++ ++ +++ ++ +++ ++ +++ +Listeria innocua F +++ +++ +++ + ++ ++ ++ ++ +++ ++ +++ ++Bacillus subtilis +++ +++ +++ ++ +++ ++ +++ ++ ++ + +++ ++Staphylococcus aureus ATCC33862
++* ++ ++ ++ +++ ++ ++ ++ ++ ++ ++ ++Staphylococcus aureus (MRSA) +* - ++ - + - + - + - + -Enterococcus faecalis +++ +++ ++ ++ ++ ++ ++ ++ ++ ++ ++ ++E. coli CIPI103982 +++ - ++ - ++ - ++ - ++ - ++ -Klebisella oxytoca +++ - ++ - ++ - ++ + ++ - ++ +Proteus mirabilis ++ - ++ - +++ - + - ++ - ++ -Salmonella heidbelberg ++ - ++ - ++ - ++ - ++ - ++ -Pseudomonas fluorescens
++ - ++ - ++ ++ ++ - ++ - +++ +Candida albicans - - - - - - - - - - - -Saccharomyces cerevisiae
- - - - - - - - - - - -
SPECTRUM OF THE ANTAGONISTIC STRAINS
* : + (1-3 mm), ++ (3-6 mm), +++ ( > 6 mm)
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S. aureus ATCC 33862 vs E. faecalis 28
S. aureus ATCC 33862 vs E. faecalis 93
S. aureus ATCC 33862 vs E. faecalis ATCC 29212
- Drop in S. aureus ATCC 33862 counts in the presence of E. faecalis 28 or E. faecalis 93- Stability in S. aureus ATCC 33862 counts in the presence of E. faecalis ATCC 29212
CHALLENGE TESTS S. aureus vs. E. faecalis
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DD28
DD93
MW= 5204.21 Da
MW= 5203.89 Da
Purification of enterocins DD28 and DD93
Mass spectrometryRP-HPLC of Enterocins DD28 and DD93
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Antibiotics MIC (mg/L) Antibiotics MIC (mg/L)
Benzylpenicillin R 0.25 Linezolid S 2Oxacillin R 1 Teicoplanin S ≤ 0.5Gentamicin S ≤ 0.5 Vancomycin S 1Kanamycin R 32 Tetracyclin S ≤ 1Tobramycin R ≥ 16 Fosfomycin S ≤ 8Ofloxacin S ≤ 0.5 Nitrofurantoin S ≤ 16Erythromycin R ≥ 8 Fusidic acid S ≤ 0.5Lincomycin R ≥ 16 Rifampin S ≤ 0.03Pristinamycin S 1 Trimethoprim-sulfamethoxazole S ≤ 10
Antibiotic susceptibility of MRSA-S1 (clinical isolate)
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Effects of antimicrobials combinations against MRSA-S1Ch
ecke
rboa
rd as
says
Kill-
curv
es ex
perim
ents
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Effect of antimicrobials on MRSA-S1 biofilm formation on AISI 304L stainless steel
Epifluorescence microscopy
Time (h) 0h 3h 6h 24h
Control 5.55±0.08 7.25±0.15 7.81±0.18 8.85±0.11
Erythromycin (8 µg/ml) 5.25±0.25 7.09±0.19 7.39±0.29 8.57±0.12
Ofloxacin (0.5 µg/ml) 3.12±0.12 5.24±0.22 5.58±0.18 6.45±0.13
Vancomycin (1 µg/ml) 3.10±0.08 5.29±0.19 5.20±0.14 6.10±0.03
Rifampin (0.03 µg/ml) 3.11±0.10 5.17±0.11 5.28±0.17 6.06±0.04
Enterocin DD28 (200 µg/ml) 3.29±0.1 5.51±0.1 5.62±0.13 6.54±0.12
Enterocin DD93(200 µg/ml) 3.35±0.21 5.59±0.1 5.58±0.19 6.58±0.17
Erythromycin / DD28 (1/50 µg/ml) 3.35±0.1 5.32±0.17 5.15±0.25 6.13±0.1
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SEM of biofilms formation by MRSA-S1 on glass slides
CVancomycin
A Control B DD28
D DD28 + Erythromycin
Key information
Enterocins DD28 and DD93 but also DD14, DD90, DD97 and DD101 displayed 100% identical sequences to enterocin 7 (strain isolated from meat in Canada) and enterocin MR10 (strain isolated from bird in Spain)
The resulting sequences were blasted on blastn pubmed database and showed complete alignment with the sequences of enterocin MR10A and MR10B
International Journal of Antimicrobial Agents (In press)
The French National Research Agency Projects for scienceProject SINCOLISTIN (2015-2018).
Phileo Lesaffre Animal CareProjects Clostrisaf I and Clostrisaf II
Financial supports
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Thank you for your attention