Download
1 / 28
E N D
1. Antibiotics (anti-microbials) Dr Gareth Noble (and Dr Sue Jordan)
3. Overview Antibiotics are a large and diverse group of drugs which combat infections by suppressing the growth and reproduction of bacteria.
However, many bacteria are now resistant to antibiotics and some are resistant to all known agents.
New drugs are continually being introduced to combat evolving patterns of resistance.
4. Antibiotics exploit the differences between bacterial and human cells.
They prevent the renewal of the bacterial cell wall and inhibit protein formation.
Note: bacteria are 'gram negative' or 'gram positive'.
Gram negative bacteria have a tough wall
5. Classification Bacteriostatic (inhibit growth without death) or Bactericidial (Kill)
Dosage related?
Mechanism of action (see later)
Spectrum of Activity:
Broad or Narrow
Chemical Structure
6. Bacteriostatic vs Bactericidal Bacteriostatic allows for natural immunity to deal with the microbe
Antibodies, Phagocytosis etc
Bactericidial may lead to release of toxins and microbial contents leading to subsequent illness and inflammatory responses.
7. Spectrum of Activity Relates to the number of microbes that are susceptible to the action of the drug
Narrow (limited number) / Broad (wide)
Penicillin G is a narrow spectrum drug as it is only effective against gram-positive microbe
Tetracyclines are effective against gram-positive and gram-negative microbes (Broad)
Note: Never confusion these terms with potency levels of the drugs or efficacy (ie. Narrow are weak, Broad are strong)
9. Inhibition of Cell Wall Synthesis Most bacteria possess a cell wall to protect from osmotic pressures
Microbe divides – needs to create a new cell wall
Interrupt this leads to new microbes being susceptible to external influences
Cell ruptures ? Microbe death
Eg. Penicillinsm cephalosporins, vancomycin and bacitracin
10. Disruption of the microbial cell membrane Essentially, affect cell membrane transportation in and out
Increases permeability of membrane
External influences have greater effect
Microbe death
Eg. Polymyxin, Colistin
Note: These agents are more toxic systemically than those agents that inhibit cell wall synthesis.
11. Inhibition of Protein Synthesis Proteins vital for growth and repair
Act either at:
Site of protein synthesis (ribosome)
Within the nucleus by inhibiting synthesis of nucleic acids
DNA replication / RNA synthesis = TRANSCRIPTION
Eg. Tetracyclines, aminoglycosides and macrolides (erythromycin)
Exploit structural differences between microbial and human cells
High dose can lead to toxicity
12. Interference with metabolic processes Agents are structurally similar to Para-aminobensoic acid (PABA) – component of folic acid
Essential for nucleic acid synthesis, without it microbes can not produce the proteins for growth
Exploits: microbes need to create their own folic acid, whilst we get it in our diets.
Eg Sulphonamides, Trimethoprim
15. Indications for antibiotics include:
Treating bacterial infections in accordance with culture and sensitivity testing or (second best) knowledge of prevalent organisms.
Prophylaxis:
surgery e.g. gastro-intestinal surgery, joint replacement.
meningitis contacts
surgical/ dental procedures in patients with artificial heart valves or heart valve lesions.
16. Administration:
Dose depends on many factors:
nature and severity of infection; weight, age and renal function of patient.
Some doses (e.g. gentamicin, vancomycin) are determined by therapeutic monitoring of venous blood samples, extracted prior to dosing.
Severe infections require intravenous infusion.
Observe veins carefully for signs of phlebitis, particularly with penicillins and vancomycin.
17. Intramuscular injections are painful and avoided, unless essential, in children. A warm compress may reduce pain.
Food affects absorption (table 2).
For other routes, see individual products (BNF).
18. Table 2. Oral Administration of antibiotics
19. Adverse effects of antibiotics can be considered as:
those occurring with all antibiotics (table 3);
those restricted to specific agents (table 4).
