Post on 31-Jan-2016
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Lecture 5
Enzymatic destruction (ESBL)
Enzymatic modification (erm )
Mechanisms of resistance
1. Modifying enzymes• erm
2. Degrading enzymes• ESBL
3. Target Change
4. Efflux pumps
ESBL
Extendened Spectrum β-lactamases
Resistance in Gram negative bacteria
• β-lactamases – the most important mechanism of resistance to β-lactam Ab (in Gr-).
• ESBLs (Extended spectrum β-lactamases)
• Carbapenemase
Gram Negative Rods/Bacilli (GNR)
V. choleraeC. jejuni
Helicobacter pylori
EnterobacteriaceaePseudomonas
aeruginosa
Stenotrophomonas maltophilia
Acinetobacter spp.
Many other
(H. influenza, etc..)
Enterobactericea(E. coli, Klebsiela, Enterobacter)
• Gram negative rods
• Colonize GI tract
• Clinical manifestations:– Urinary tract infections– Nosocomial pneumoniae– Bacteremia / Sepsis– Other
Mechanism of resistance
β-lactamases
Enzymes that inactivate β -lactams by hydrolyzing the amide bond of the β -lactam ring.
β-lactamase inhibitors• Clavulonic acid: derived from Streptomyces clavuligerus• Little antibiotic effect in itself• Given in combination with a β -lactam Ab• Function: by binding the β -lactamase enzyme more
efficiently than the actual β -lactam• Thus protect the β -lactam Ab from hydrolysis• Not efficient against cephalosporinases
History of GNR resistance
1928
Fleming
1941
Penicillin use
1940 Penicillinase detected in
E. coli
1959
β -lactamase resistant penicillins: Methicillin
1960s
Broad spectrum/ extended spectrum
penicillins
1964
Cefalotin use
1965
Broad spectrum β –lactamases (TEM-1 in E. coli) 1983
Extended spectrum β-lactamases
1950 1960 1970 1980 1990 2000
1985
Carbapenem (Imipenem)
Early 1980s
3rd generation ceph.
Carbapenemases
TEM-1 widespread
2005
Tigecycline
ESBL outbreaks in
France
1976
β –lactamases inhibitors
β-lactamases classification
• Molecular class:– A:
• TEM• SHV• other
– B: • Metalloenzymes
(carbapenemases)– C:
• Prototype: chromosomal ampC
– D: • OXA (oxacillin
hydrolyzing enzymes)
• Enzyme type (by substrate profile):– Penicillinase– Broad-spectrum– Extended Spectrum– Carbapenemase
• Genetic classification:– plasmids mediated– Chromosomal
http://www.lahey.org/studies/webt.asp
Types of β-lactamases
• β-lactamases– Penicillinase: gene blaZ ,
inducible, on transposon (can move between chromosome and plasmid).
• Broad spectrum β-lactamases – (plasmid encoded)– TEM– SHV – OXA (mainly in pseudomonas)
• ESBLs – TEM related– SHV related– OXA related– CTX-M – Other
• ampC β-lactamases– Resistant to β-lactamase
inhibitors– chromosomal
• Carbapenemases– Metallo- β-lactamases– Serine carbapenemases
Genetic Mechanism
Transformation
Penicillinase blaZ
Plasmidtransfer
Broad spectrum b-lactamase
(blaTEM)
&
Mutation
ESBL(TEM related)
&
ESBL• Confer resistance to 1st , 2nd, 3rd cef.
– Most are susceptible to β-lactamase inhibitors– Most are susceptible to 4th cef.– All are susceptible to carbapenems
• Diversity of ESBL– SHV (widespread)– TEM (>100 types)– OXA
• Predominantly in Pseudomonas• less susceptible to β-lactamase inhibitors
– CTX-M• Probably independent evolution• Highly resistant to 3rd generation cephalosporines• initially in South America, Far East & Eastern Europe• Probably most frequent worldwide• Clonal spread has been documented
CarbapenemasesPan-resistance
• Carbapenem: “the magic bullet” very broad spectrum
• Metallo-β-lactamases (class B)– Not susceptible to clavulonate
• Serine-carbapenemases (class A+ D)• KPC (Klebsiela pneumonia carbapenemase)-
plasmid associated
AmpC β-lactamase
• Chromosomal
• Inducible
• Fully resistant to β-lactamase inhibitors
Further complicating matters:
• More than one gene of β-lactamase / ESBL / ampC / carbapenemase can be carried on the same plasmid.
• Genes of ESBL are carried on plasmids that usually carry additional resistant genes: frequently MDR
• Laboratory diagnosis confusing: susceptibility profiles sometimes misleading: “hidden resistance” -> CLSI guidelines are changing.
• CTX-M clones appearing in the community (Canada, Greece, Spain, Italy).
Treatment of Gram negative infections:
• Penicillins• Cephalosporines (1st, 2nd)• Extended spectrum
Cephalosporines (3rd, 4th)• Quinolones• β-lactam-β-lactamase
inhibitors• Carbapenems• Colistin…Tigecycline
• β-lactamase (penicillinase)• Broad spectrum β -lactamase• ESBL
• Quinolone resistance • ESBL (OXA) • ampC• Carbapenemases
•We are running out of treatment options!
The evolution of ESBL
• In a single patient: – SHV-1-> 3rd Cef Rx. -> SHV-8– ESBL TEM-24 from:
Enterobacter aerogenes -> E. coli -> proteus mirabilis -> Pseudomonas aeruginosa
• Mutations + efficient horizontal transmission
• K. pneumoniae the major ESBL producer
Klebsiela resistant to 3rd generation cephalosporines (CDC)
0
2
4
6
8
10
12
14
1989
1990
1991
1992
1993
1994
1995
1996
1997
1998
1999
2000
Year
Per
cent
Res
ista
nce
MDR (qnl, aminoglycoside 3rd ceph.) in Klebsiella pneumoniae in Europe (EARSS) 2005
Risk factors
• Critically ill patients
• Long hospitalization (median 11-67 d)
• Invasive medical devices
• Heavy Ab treatment – 3rd generation cephalosporines– Also other: quinolones, TMP-SMX,
aminoglycosides, metronidazole
Control of ESBL outbreaks
Monoclonal• Indicates
transmission from patient to patient.
• Probably induced by lack of IC measures
• Infection Control
Polyclonal• Indicates multiple
events of evolving resistance.
• Probably induced by selective Ab pressure
• Antibiotic control
Enzymatic modification
The case of macrolides
Enzymatic modification:
• Aminoglycosides– Acetyltransferases– Phosphotransferases– nucleotidyltransferases
• MLS (macrolides, lincosamides, streptogramin B)– erm (erythromycin resistance methylase) (most
common)– Other: hydrolases, esterases, glycosylases,
phosphotransferases, nucleotidyl-transferases and acetyltransferases
Mechanism animation
Macrolide resistance
• Macrolides are used to treat Gram+ bacteria and atypical bacteria (mycoplasma, legionella,
chlamidia).
• Bacteriostatic
• Macrolides act by inhibiting protein synthesis, by binding to 50S subunit of the ribosome of the bacteria.
Macrolide resistance
• Phenotypes of macrolide resistance:– MLSB– M
• Genotypes of macrolide resistance:– erm (erythromycin ribosomal methylase)– mef (specific macrolide effulx pump )
erm Erythromycin ribosomal methylase:
• The predominant macrolide resistance mechanism.
• 34 different classes of Erm proteins.
• Each functions by methylating a single adenine residue of the 23S rRNA.
• Methylation results in MLSB pheontype (resistance to most macrolides).
• Can be either inducible or constitutive.
Macrolide resistance in S. pneumoniae
• ermB • predominant in most of the world• High level resistance (MIC>64)
• mefA• most common in some areas (USA)• low level resistance (MIC 4-8)• Increasing level of resistance
• Changing epidemiology– Strains containing both mefA + ermB emerging (from 10% to 18%
in last 4 y)– mefA + ermB usually clonally related to MDR (19A – non-vaccine
type)
• Correlation between increasing consumption of mac and Mac R in SP
Macrolide resistance in S. pneumoniae (2001-2005) / Flemingham et al. J. Infection
2000-2004
PROTEKT US 2008 (2000-2004)
Mac-R in S. pneumoniae in Finland / Bergman et al. 2006 AAC
Macrolide resistance in GAS
• Uncommon: US<5%• Single outbreak in Pittsburg (up to 48% Mac-
R, single clone)• Mechanisms:
– ermA (ErmA subclass TR)– ermB– mefA
• All associated with mobile genetic elements
Mac-R is GAS in Finland / Bergman et al. CID 2004
Macrolide R in S. aureus
• Clindamycin resistance – an important treatment issue.
• Mechanism of resistance:– Target modification (MLSBi) (ermA, ermC)
– Efflux pumps (MS phenotype:
not clinda R) (msrA)
– Inactivation