antibacterials 2 a

Question 1

how do antibacterials get into bacteria (gram +ve)?

Answer 1

a have active peptide transporters
– dipeptide, tripeptide and OligoPePtide transporters (Opp)
– transport most hydrophilic antibacterials directly into the cytoplasm
– hydrophobic antibacterials can use passive diffusion

Question 2

how do antibacterials get into gram negative bacteria?

Answer 2

Gram negative bacteria have Outer Membrane Proteins (porins, Omp) that act as
molecular sieves
– e.g. main porins in E. coli: OmpC and OmpF – allow hydrophilic molecules up to about 600 Da (1.1 – 1.2 nm diameter) to pass into periplasmic space

Question 3

who targets the cell wall?

Answer 3

b-lactams
vancomycin
teicoplanin
isoniazid

Question 4

what are b-lactam antibiotics?

Answer 4

Broad spectrum bactericidal activity against – both G+ve (except aztreonam) and G-ve bacteria

Question 5

what are the characteristics of b-lactam antibiotics?

Answer 5

time dependent action
good distribution:
- increased with greater lipophilicity
-remember polarity
must have low PAE
largely renal excretion

Question 6

why do we usually not use b-lactams for UTIs?

Answer 6

largely renal excreted
– not often used for UTIs to reduce increase in resistance
* treat with other suitable agents, if possible
* can be used for complicated UTIs, if necessary

Question 7

what is the penicillin SAR?

Answer 7

• Amide and carboxylic acid are involved in binding
• Carboxylic acid binds as the carboxylate ion (pKa ~ 2.5 – 3.0)
• Mechanism of action involves the b-lactam ring
• Activity related to b-lactam ring strain
  (subject to stability factors)
• Bicyclic system increases b-lactam ring strain
• Not much variation in structure is possible
• Variations are limited to the side chain (R)

Question 8

what are some areas for developements for b-lactams?

Answer 8

1* to increase chemical stability for oral administration (stomach acid)
* addition of electron withdrawing groups (R)
* prodrugs (-CO2H)
2* to increase resistance to b-lactamases
* addition of bulky groups (R)
3* to increase the range of activity
* addition of ionisable groups (R)
* addition of ureido groups (R)

Question 9

what happens to b-lactam structure at physiological ph?

Answer 9

All have >99.9% ionised ‘acid’ at physiological pH

Question 10

what is the MOA of b-lactams?

Answer 10

Act upon synthesis of bacterial cell membrane
b-Lactams interfere with peptidoglycan (components of call wall) formation through their interaction with the transpeptidase enzyme [penicillin binding proteins (PBPs)]

Question 11

what is the consequence of b-lactams inhibiting the formation of cross-links in cell wall?

Answer 11

– reduces integrity and strength, eventually leads to cell lysis / death
* high osmotic pressure inside bacterial cells
* when cell wall weakened, easily bursts

Question 12

what is prokaryotic cell wall composed of?

Answer 12

peptidoglycan
– polymer
– sugar units (NAG/NAM)
– cross-linked by peptide uni

Question 13

what are 3 reasons for potential acid sensitivity?

Answer 13

• (1) Ring strain – acid-catalysed ring opening relieves ring of β-lactam ring
• (2) Highly reactive β-lactam carbonyl group – resonance stabilisation is not possible for β-lactam ring
• (3) Influence of the acyl side chain (neighbouring group participation)

Question 14

what is a solution to acid sensitivity?

Answer 14

• β-lactam ring is vital for antibacterial activity and only the third factor can be
  addressed
  – reduce amount of neighbouring group participation
  – use electron-withdrawing group in side chain to draw electrons away from the
  carbonyl oxygen and reduce its nucleophilicity
  – stability improvements can allow oral administration

Question 15

what are the 4 mechanisms of resistance to B-lactam agents?

Answer 15

• Most resistance to b-lactam antibiotics due to specific enzymes
  – b-lactamases
  – break open b-lactam ring, which is essential to activity
  – b-lactamase resistance to penicillin first seen in 1940, before clinical use started!
• Modification of the target protein (PBP)
  – most common in G+ve bacteria, e.g. Haemophilus and Neisseria strains
  – less common in G-ve bacteria
• Limited uptake into the bacterial cell, especially G-ve bacteria
  – polar molecules, so poor passive diffusion, use porins
  – mutations to porins reduce uptake and confer resistance
• Increased efflux pump activity
  – up-regulation of efflux pumps causes multi-drug resistance
• affects many antibiotics (e.g. fluroquinolones, aminoglycosides)

Question 16

what are the 4 classes b-lactamases are divided into?

Answer 16

– active-site serine β-lactamases (SBLs; classes A, C and D)
– zinc-dependent or metallo-β-lactamases (MBLs; class B

Question 17

how do extended spectrum b-lactamases (ESBLs) work?

Answer 17

• hydrolyse even third generation cephalosporins, but not usually carbapenems

Question 18

how do carbapenemases work?

Answer 18

• confer resistance to carbapenemases, alongside almost all clinical b-lactam
  antibiotics

Question 19

how do metallo b-lactamases work?

Answer 19

• broad range of b-lactam substrates, including carbapenems (but not aztreonam)

Question 20

what are b-lactamases in gram +ve bacteria?

Answer 20

Beta-lactamases are inducible in G+ve bacteria – produced in response to presence of b-lactam antibiotic

Question 21

what are b-lactamases in gram -ve bacteria?

Answer 21

constitutive in G-ve bacteria – they produce the enzyme all the time, whether or not beta-lactam antibiotics are present
– but, only if the G-ve bacterium has the b-lactamase gene
– located in periplasmic space

Question 22

how do b-lactamases work?

Answer 22

Generally, have a similar mechanism of action, cleaving the b-lactam ring leading to inactivation of b-lactam antibiotics

Question 23

how are SBLS related to PBPs?

Answer 23

– share a similar SER-based amino acid sequence
– Use serine as the nucleophile to hydrolyse β-lactams

Question 24

how do MBLs work?

Answer 24

MBLs (class B) have a different hydrolytic mechanism
– use a metal-activated water nucleophile to to hydrolyse β-lactams

Question 25

what are the catalytic important residues of serine b-lactamases in serine?

Answer 25

SER64/70

Question 26

what additional mechanism do b-lactamases have?

Answer 26

• Additionally, are hydrolysed to recycle the b-lactamase enzyme
  – not irreversibly bound to b-lactam
  – this continues activity

Question 27

what are carbapenemases?

Answer 27

• Carbapenems: important class of antibiotics
  – stable to most b-lactamases due to the hydroxyl-containing group
  – active against most clinically relevant bacteria (especially Gram-ve bacteria)

Question 28

what is the real threat to carbapenemases?

Answer 28

Real threat from pan-drug resistant G-ve bacteria

Question 29

what does NDM-1 do?

Answer 29

NDM-1 hydrolyses and inactivates all b-lactam antibiotics, except aztreonam

Question 30

what should be done for an NDM expressing bacterial infection?

Answer 30

– no b-lactam antibiotic can treat
– few, if any, other agents that can treat
– resistant to (almost) all clinical antibacterials
– currently, colistin active against most NDM
-expressing G-ve bacteria
– colistin resistance is increasing
– examples of otherwise healthy (and young) patients dying from a pan
-drug resistant bacterial infection are increasing (very few in UK so far)

Question 31

how do b-lactamase resistant penicillins occur?

Answer 31

Steric shields used to block the penicillin derivative from accessing the penicillinase
or β-lactamase active site
* Introduce a bulky group on the side chain

Question 32

how do steric shields work?

Answer 32

• β-lactam ring interacts with both β-lactamase and transpeptidase target enzyme in the
  same way – difficult problem
  – If steric shield is too bulky, then also prevents the penicillin derivative from
  interacting with transpeptidase target enzyme
  – large enough to not react with b-lactamase enzyme
  – small enough to allow reaction with target enzyme

Question 33

what factors affect whether a particular strain is susceptible to a penicillin?

Answer 33

– structure
– ability to cross the cell membrane of Gram-negative bacteria
– susceptibility to β-lactamases
– affinity for the transpeptidase target enzyme – rate at which it is pumped back out of cells b

Question 34

how do the hydrophobic groups affect spectrum of activity?

Answer 34

– favour activity against G+ve bacteria
– poor activity against G-ve bacteria
– as hydrophobic character increases, little effect on G+ve activity, but drops
against G-ve bacteria

Question 35

how do hydrophilic groups affect spectrum of activity?

Answer 35

– little (or reduce) effect on G+ve activity
– increase activity against G-ve bacteria
– enhancement of G-ve activity greatest if hydrophilic group (e.g. NH2, OH,
CO2H) is attached to carbon α to the carbonyl group on side chain

Question 36

give examples of carbapenems/ penems

Answer 36

• Biapenem
• Doripenem
• Ertapenem
• Imipenem
• Meropenem
  Penems
• Faropenem
• Ritipenem

Question 37

what is currently the only monobactam in clinical use?

Answer 37

Aztreonam IV use only
strong against gram -ve bacteria
no activity against gram +ve
resistant to many b-lactamase enzymes including NDM
inactivated by extended spectrum b-lactamases and carbapenemases

Question 38

what are b-lactamase inhibitors traditionally based on?

Answer 38

b-lactam core

Question 39

what are the properties of sulbactam?

Answer 39

Sulbactam – a penam
– not active vs P. aeruginosa or AmpC cephalosporinases – ampicillin and sulbactam (US)

Question 40

what are the properties of tazobactam?

Answer 40

• Tazobactam – a penam
  – used to inhibit ESBL-expressing bacteria in combination with Piperacillin – piperacillin and tazobactam
  – ceftolozane and tazobactam

Question 41

how do b-lactamase inhibitors also attack?

Answer 41

• Are also attacked by b-lactamase enzyme….
  – BUT, form stable covalently bonded complex – enzyme not released to inactivate other b
  -lactams
  – suicide inhibitors of b-lactamase enz

Question 42

what is diazabicycloocyanones?

Answer 42

– bicyclic core structure that still reacts at serine of β-lactamases – ceftazidime and avibactam
– imipenem, cilastatin and relebactam

Question 43

what are boronate-based compounds?

Answer 43

– boron can adopt a tetrahedral geometry
– interacts at serine of β-lactamases as transition state inhibitor mimicking the
transient tetrahedral species formed during hydrolytic reaction
– meropenem and vaborbacta

Question 44

what is imipenem?

Answer 44

– largely excreted unchanged into kidneys
– metabolised by dehydropeptidase-I in kidneys – metabolite is toxic to kidneys

Question 45

what is cilastatin?

Answer 45

• Cilastatin is a dehydropeptidase-I inhibitor – protective to kidneys and works as a booster of imipenem (also boosted with
  relebactam)

Question 46

why do we use prodrugs?

Answer 46

Prodrugs used to improve oral stability and uptake
– penicillins particularly acid sensitive, decreased bioavailability
– many zwitterionic / very polar and poor uptake
– ester groups help to increase logP and uptake