Antibiotic Resistance Flashcards

1
Q

Antibiotic resistance effects

A

Antibiotic resistance:

Increases mortality
challenges control of infectious diseases
threatens a return to the pre-antibiotic era
increases the costs of health care
jeopardizes health-care gains to society

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2
Q

Enterococci - define

A

large genus of lactic acid bacteria of the phylum Firmicutes.

gut vancomycin R+ (VREs)
G+ve origin - chickens ?

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3
Q

Acinetobacter - define

A

Acinetobacter is a genus of Gram-negative bacteria belonging to the wider class of Gammaproteobacteria

gut multiply resistant (can use carbapenems)
G-ve wound infections
hospital acquired infection

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4
Q

MRSA - define

A

Methicillin-resistant Staphylococcus aureus (MRSA) is a bacterium that causes infections in different parts of the body.

MRSA G+ve gut, wounds reserve drug - vancomycin

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5
Q

Mechanisms of antibiotic resistance - list with examples

A

Drug inactivation
e.g. beta-lactamase

Metabolic by-pass
e.g. vancomycin
D-ala-D-lac

Efflux pump

Overproduction
of target

Intrinsic
impermeability

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6
Q

Altered or new target if resistance shown

A
Altered or new target
e.g. 
Ribosome
Porin
PBPs – 
peptidoglycan synthesis
DNA gyrase
RNA polymerase
Mcr1 & colistin
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7
Q

Paths to Resistance - describe each

A

Directed at antibiotic itself -
Degrading the drug
Modifying the drug

New or Altered target
antibiotic no longer binds
e.g. PBPs - PBP2a in MRSA

Altered transport
Actively pumping drug out - efflux pump porins no longer influx drug

Metabolic by-pass
metabolic change D-ala-D-lac and vancomycin

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8
Q

Mechanisms of Resistance - types

A

Natural resistance

Genetic Mechanisms - acquired

Non-Genetic Mechanisms (growth phases)

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9
Q

Describe natural resistance

A

Drug must reach target - natural barriers, porins, export pump

G+ve peptidoglycan - highly porus - no barrier to diffusion

G-ves outer membrane - barrier resistance advantage

Porins single mutation - multiple resistance

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10
Q

Describe types of genetic mechanisms

A
Chromosome-mediated
Due to spontaneous mutation: 
in the target molecule 
in the drug uptake system
Mutants are SELECTED ; they  are NOT induced

Plasmid-mediated
Common in Gram-negative rods
Transferred via conjugation
Multidrug resistance

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11
Q

Resistance to Beta-Lactams compare gram +ve vs gram -ve

A

Gram + ve

ß-lactamase (Penicillinase)

Alteration of the transpeptidase enzyme
(PBP)

Gram - ve

ß -Lactamase (Penicillinase)

Alteration of porins

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12
Q

Penicillinase function

A

Penicillinase destroys active part of penicillin molecule

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13
Q

Augmentin/co-amoxiclav - structure and action

A

Clavulanic acid + amoxicillin

Binds to and inactivates beta-lactamases
No anti-bacterial activity of its own

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14
Q

Beta-lactam Resistance in Gram –ve bacteria - describe events

A
1. Porin mutates or new porin type
Multi-resistant 
2. PBP - mutates or bacteria 
acquires a new PBP
3. bacteria acquires a 
beta-lactamase enzyme
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15
Q

PBP =

A
PBP =
	Penicillin 
	binding 
	Protein or
transpeptidase
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16
Q

Mechanisms by which bacteria become resistant to penicillin - describe all 4

A

Any of:-

Produce penicillinases / beta lactamases that cleave the beta lactam ring
- penicillin is inactivated

Acquire alternative forms of / or mutations in penicillin binding proteins (PBPs)
- penicillin can’t bind

Acquire alternative forms of / mutations in porins,
- penicillin cannot get into cell

Acquire alternative forms of / mutations in efflux pumps
- penicillins are pumped out faster

17
Q

Treatment of MRSA

A

Only effective treatment is vancomycin, a 1.5 kDa glycopeptide

18
Q

Vancomycin Resistance - describe events and effect

A

Acquisition of van operon by transposition

          Makes D-ala-D-lactate   - prevents vancomycin binding
19
Q

Non-Genetic Mechanism - describe

A

Inaccessibility to drugs
(e.g., abscess, TB lesion)

Stationary phase/vegetations and biofilms
(non-susceptible to inhibitors of cell wall synthesis)

20
Q

Disc diffusion test for

A

Disc diffusion test for antibiotic susceptibility testing of S. pneumoniae

21
Q

How to prevent/overcome antibiotic resistance

A

Control use

not in animal feeds
complete course [DOTS for TB]
appropriate prescribing

New or modified drugs few in past 25 years

Combination therapy different targets
overcome mutation rates

Infection control individual - ward - society

22
Q

Neisseria gonorrhoeae - gonorrhoea

treatmen

A

Neisseria gonorrhoeae - gonorrhoea
treatment - a single I/M penicillin
↓rates; ↑penicillin R+ ~15%

Then we used new front line drug - Ciprofloxacin

23
Q

Treatment if cipro R+ N. gonorrhoeae

A

Switched to single oral dose – cefixime
Now i/m ceftriaxone + 1g Azithromycin
125mg increased to 250mg due to increasing MIC

24
Q

Carbapenems - define

A

Carbapenems – broad spectrum antibiotics
of last resort for Gram negative bacteria
e.g. E.coli or Klebsiella (CREs)