(LE2) Antimicrobial Drugs

Question 1

Describe antibiotics

Answer 1

• naturally occurring
• common in soil, fungi, and bacteria (competitive environment)

Question 2

Describe synthetic Drugs. Give an example

Answer 2

• Laboratory derived
  e.g. sulfa

Question 3

Describe semisynthetic drugs

Answer 3

Antibiotics that are modified in the lab

Question 4

What is selective toxicity?

Answer 4

Harms or kills the pathogen without causing significant harm to the host (magic bullet)

Question 5

What properties are required for antimicrobial agents?

Answer 5

• selective toxicity
• soluble in body fluids
• biological half-life

Question 6

Why is body fluid solubility important for antimicrobial agents?

Answer 6

Needs water-soluble molecules so that it can be used by the body

Question 7

Why is half-life important for antimicrobial agents?

Answer 7

affects dosing

Question 8

What is a broad spectrum drug?

Answer 8

Works on two or more groups of bacteria

Question 9

What is a narrow spectrum drug?

Answer 9

Works on less than or equal to one group of bacteria

Question 10

What is the spectrum of activity for Penicillin?

Answer 10

G+, narrow spectrum

Question 11

What is the spectrum of activity for Isoniazid?

Answer 11

Very narrow spectrum
- Works on M. tuberculosis only

Question 12

What is the spectrum of activity for Tetracycline?

Answer 12

Very broad spectrum
G+, G-, intracellular bacteria

Question 13

What is the spectrum of activity for Streptomycin?

Answer 13

broad spectrum, acid-fast and G-

Question 14

What is the mode of action for the following drugs: penicillins, cephalosporins, bacitracin, and vancomycin?

Answer 14

Inhibition of cell wall synthesis (peptidoglycan, mycolic acid)
-antibacterial

Question 15

What is the mode of action for the following drugs: chloramphenicol, erythromycin, tetracyclines, and streptomycin?

Answer 15

Inhibition of protein synthesis (70S ribosomes)
- antibacterial

Question 16

What is the mode of action for the following drugs: quinolones and rifampin?

Answer 16

Inhibition of nucleic acid replication and transcription (DNA or RNA)
- antibacterial (DNA gyrase)
- mostly antivirals

Question 17

What is the mode of action for polymyxin B?

Answer 17

Injury to plasma membrane (ergosterol)
- antifungal

Question 18

What is the mode of action for the following drugs: sulfanilamide and trimethoprim?

Answer 18

Inhibition of essential metabolite synthesis (competitive or non-competitive inhibitors)
- synthetic antibacterials

Question 19

What category of side effects is most crucial to understand when developing an antimicrobial drug?

Answer 19

1. Toxicity - determined by selective toxicity of drug (e.g. vancomycin req monitoring of liver & kidney function)
2. Allergies - more common in some drugs than others (e.g. penicillin and sulfa)
3. Disruption of normal microflora - problem with broad-spectrum drugs
   • can lead to yeast infections and C. diff infections

Question 20

What are ideal antimicrobial attributes?

Answer 20

1. water-soluble
2. selective toxicity
3. biological half-life
4. narrow spectrum
5. low allergenicity
6. tissue stability
7. long shelf-life
8. low cost
9. low/no resistance acquisition

Question 21

Sulfonamides & Trimethoprim

Answer 21

Type: Synthetic
MOA: competitive protein inhibition. PABA analog
Preferred use: broad spectrum
Side effects:
Interesting features:

Question 22

Isoniazid (INH)

Answer 22

Type: Synthetic
MOA: inhibits mycolic acid in AF cell wall
Preferred use: Narrow spectrum; M. tuberculosis
Side effects: X
Interesting features: req 6 mo to 2 yr regiment compliance

Question 23

Quinolones (e.g. Ciprofloxacin)

Answer 23

Type: Synthetic
MOA: inhibits DNA gyrase used in DNA replication
Preferred use: Gram broad spectrum
Side effects: weakening of tendons
Interesting features: newer drug -> no resistance yet

Question 24

Penicillins

Answer 24

Type: Antibacterial
MOA: Cell wall inhibitor
Preferred use: narrow spectrum G+ Staphylococcus, Streptococcus, and some spirochetes (syphilis)
Side effects: X
Interesting features: Penicillin G (requires injection), Penicillin V (Orally, resists stomach acid)
Susceptible to beta-lactamase produced by MRSA. (carried on R plasmid)

Question 25

Semi-Synthetic Penicillins

Answer 25

Type: antibacterial
MOA: cell wall inhibitor
Preferred use: Broader spectrum than penicillin
Side effects: X
Interesting features: Still has beta-lactam ring. Combined with Clavulanate to inhibit beta-lactamase
e.g. Augmenten = Amoxicillin + Clavulanate, Methicillin

Question 26

Cephalosporins

Answer 26

Type: Antibacterial
MOA: cell wall inhibitor
Preferred use: broad spectrum
Side effects: X
Interesting features: more resistant to beta-lactamase; beta-lactam ring protected by 6-point ring structure

Question 27

Vancomycin

Answer 27

Type: antibacterial
MOA: cell wall inhibitor
Preferred use: last resort; Broad spectrum MRSA & TB
Side effects: High toxicity, req kidney & liver function monitored
Interesting features: VISA - Vancomycin intermediate S. aureus
VRSA
VRE - Vancomycin-resistant Enterococcus

Question 28

Streptomycin

Answer 28

Type: Antibacterial
MOA: Protein synthesis inhibitors
Preferred use: Broad spectrum; last resort for G- and TB
Side effects: Fairly toxic
Interesting features: Neomycin (Neosporin) topical variant

Question 29

Tetracycline

Answer 29

Type: Antibacterial
MOA: protein synthesis inhibitor
Preferred use: broad spectrum; G+, G-, intracellular pathogens (chlamydia)
Side effects: High toxicity
Interesting features: Doxycycline common for acne, STDs, and malaria (intracellular protozoan) prophylactic

Question 30

Chloramphenicol

Answer 30

Type: antibacterial
MOA: protein synthesis inhibitor
Preferred use: broad spectrum (G+/-)
Side effects: high toxicity. high penetrating power can enter bone marrow causing aplastic anemia, a type of leukemia
Interesting features: Topical use only for diabetic ulcers

Question 31

Erythromycin

Answer 31

Type: antibacterial
MOA: protein synthesis inhibitor
Preferred use: narrow spectrum, G+
Side effects: X
Interesting features: -macrocyclic ring blocked by G- cell wall
- best alternative to penicillin

Question 32

Rifampin

Answer 32

Type: antibacterial
MOA: Nucleic acid synthesis inhibitor
Preferred use: broad spectrum (G+/-)
Side effects: red/orange body fluid secretions
Interesting features: not super common

Question 33

Amphotericin B

Answer 33

Type: antifungal
MOA: cell membrane inhibition
Preferred use: Systemic fungal infections
Side effects: fairly toxic
Interesting features: polyene ring disrupts ergosterol

Question 34

Imidazoles

Answer 34

Type: antifungal
MOA: cell membrane inhibition
Preferred use: topical use; cutaneous fungal infections (athlete’s foot, yeast infection)
Side effects: X
Interesting features: Lamisil (pill form)

Question 35

Griseofulvin

Answer 35

Type: antifungal
MOA: mitosis inhibition (targets microtubule formation)
Preferred use: under-the-nail fungal infections
Side effects:
Interesting features: targets keratinized tissues only

Question 36

Acylovir

Answer 36

Type: antiviral
MOA: Inhibit viral DNA replication (nucleotide analog)
Preferred use: Herpes (HSV, shingles, etc.)
Side effects: non-selectively toxic
Interesting features: e.g. Valtrex

Question 37

Anti-HIV drugs

Answer 37

Type: antiviral

1. MOA: reverse transcription inhibitor (AZT)
   Preferred use: HIV
   Side effects: high mutation rate, toxic in high doses
   Interesting features: nucleotide analog (adenine)
2. MOA: protease inhibitor. inhibit last step of HIV maturation
   Preferred use: HIV
   Side effects: high mutation rate
   Interesting features: used in combination with AZT to reduce HIV replication

Question 38

Quinine derivatives

Answer 38

Type: anti-protozoan
MOA: Toxin buildup
Preferred use: antimalarial
Side effects: vivid dreams
Interesting features: Chloroquine and Mefloquine; given as prophylactic prior to travel to high-risk areas

Question 39

Metronidazole (Flagyl)

Answer 39

Type: anti-protozoan
MOA: interferes with anaerobic metabolism
Preferred use: Trichomonas (intestinal protozoan) & C. diff
Side effects:
Interesting features:

Question 40

Mebendazole (Vermox)

Answer 40

Type: anti-helminth
MOA: inhibits microtubules -> motility
Preferred use: Ascaris and pinworm
Side effects: X
Interesting features: not absorbed by our cells

Question 41

Niclosamide

Answer 41

Type: anti-helminth
MOA: inhibits aerobic respiration
Preferred use: tapeworms
Side effects: X
Interesting features: X

Question 42

Pyrantel Pamoate (Antiminth)

Answer 42

Type: anti-helminth
MOA: causes paralysis of worm
Preferred use: hookworm, pinworm, Ascaris
Side effects: X
Interesting features: X

Question 43

Antibiotic resistance is selected for by exposure to the drug. What habits/actions facilitate this?

Answer 43

1. non-compliance
2. incorrect dosage (self-medication)
3. Use in animal foods
4. Lack of prescription control
5. use for non-bacterial infections
6. overuse of broad-spectrum drugs

Question 44

What mechanism of drug resistance is shown? Give an example

Answer 44

Inactivate the drug with enzyme
e.g. beta-lactamase for penicillin resistance

Question 45

What mechanism of drug resistance is shown? Give an example

Answer 45

Alterations in membrane permeability
e.g. Tetracycline kept out and can’t reach target

Question 46

What mechanism of drug resistance is shown? Give an example

Answer 46

Alterations in drug target
e.g. Erythromycin - AA change in ribosome

Question 47

What mechanism of drug resistance is shown? Give an example

Answer 47

Active transport of drug back out of the cell
e.g. Pseudomonas

Question 48

What mechanism of drug resistance is shown?

Answer 48

Horizontal gene transfer
- R plasmid

Question 49

How can we limit drug resistance?

Answer 49

• effective drug concentrations: compliance and no drug “holidays”
• simultaneous drug administration (synergism/antagonism)
• restricting drug prescriptions