Antibiotics 3 a Flashcards
Diaminopyrimidines and flouro quinolones
Diaminopyrimidines (trimethoprim)
Group of antibiotics acting on tetrahydrofolate synthesis pathway
Mechanism of action of diaminopyrimidines (Trimethroprim)
- Inhibits dihydrofolate in the later stages of the tetrahydrofolate biosynthesis pathway
- Trimethoprim: Inhibits activity of hydro folate reductase by binding to the enzyme and preventing binding of substrate dihydrofolate.
- structurally different from bacterial dihydrofolate reductase: has a lower affinity for the isozyme meaning its not a significant target of this antibiotic.
- has a higher affinity for the bacterial enzyme making the drug selectively toxic to bacterial cells and not toxic to mammalian cells.
Diaminopyrimidine side effects (trimethoprim)
- Broad-spectrum bacteriostatic antibiotic
- Side effects are rare
Co-therapy; trimethoprim and sulphamethoxazole
- Trimethoprim mostly used in treatment of urinary tract infections someitmes in combination with a sulphonamide to act on two locations of the tetrahydrobiosnthesis pathway
- Trimethoprim can be just as effective alone and has fewer side effects.
Co-therapy; trimethoprim and sulphamethoxazole - CO-TRIMOXAZOLE
trimethorpim administered in the same tablet as sulphamethoxazole in a 1:5 ratio
- not active against Pseudomonas sp.
- rarely used due to potential toxicity.
- used as an alternative when resistance to B-lactam antibiotics and ciprofloxacin have occurred.
- used to treat and prevent pneumocystis pneumonia (fungal infection) in HIV/AIDS
Diaminopyrimidine resistance - acquisition of dihydrofolate reductase isozymes
- Occurs via horizontal gene transfer
- over 30 dihydrofolate reductase isozymes identified causing resistance, often carried on integrons
- integrons found on E.coli cause resistance to sulphonamides and trimethoprim.
Other mechanisms of diaminopyrimidine resistance
Reduced permeability of the drug into the cell.
Enhanced efflux of antibiotic from the cell
Flouoro quinolones
- Family of synthetically made or naturally occurring broad-spectrum antibiotics.
- ## Prevent bacterial DNA from unwinding and replicating.
Flouoro quinolones structure
- R groups are variable depending on which quinolone is being shown
- Known are a fluroquinolone if the fluorine sites in the circled position
- Side chains vary at several positions giving rise to quinolones with different activities.
Examples of qiunolones
alidixic acid, norfloxacin and ciprofloxacin
Examples of fluoroquinolones
Ciprofloxacin and moxifloxacin
Nalidixic acid
- First quinolone antibiotic discovered
- Good activity against gram negative bacteria: notable exception is Pseudmonas aeruginosa.
- Well absorbed when taken orally
- Extensively metabolised in the body prior to excretion via urine
- used exclusively to treat urinary tract infections
Fluoroquinolones
- Active against broader ranfe of organisms than quinolones; active against gram negative and positive bacteria including P.aerugiosa
- Largely replaced quinolones
What are ciprofloxacin and moxifloxacin used for?
- Treatment of anaerobes of Bacteroides fragilis group ( commensal gut microbes causing blood infections when displaced due to surgery or trauma)
Fluoroquinolone administration
- generally orally.
- dosages can remain low due to the drugs good distribution throughout the tissues of the body and their concentration within mammalian cells: particularly useful on fighting intracellular pathogens such as chlamydia, legionella and some mycobacteria.
