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QUINOLONES
INTRODUCTION
• These are synthetic antimicrobial having a quinolones
structure.
• These are active against most of the gram negative
bacteria.
• In 1960s the first membered of this group, Nalidixic acid,
was introduced .
• Flouroquinolones have:
High potency
Expanded antimicrobial spectrum
Better tissue penetration
Good tolerability profile
Very low resistance development
1. NALIDIXIC ACID
• It was the first member in quinolones. It was active against
gram negative bacteria. It acts by inhibiting bacterial DNA
gyrase. It is bacterial in nature.
• It is given orally. It attains good concentration in gut,
lumen, hence useful in diarrhea.
•
NALIDIXIC ACID CONTD…
• It is most commonly seen in children. And causes
neurological toxicity present as headache, drowsiness
and vertigo and contraindicated in infants and G6PD
deficient patients.
• It is given in a dose of 0.5-1g TDS/QID
2. FLUOROQUINOLONES
• Fluoroquinolones are quinolones antimicrobials having one
or more fluorine substituitions.
• The first generation fluoroquinolones have one fluoro
substitution and were developed in 1980s.
• The second generation fluoroquinolones have additional
fluoroquinolones have additional fluoro substitution, which
extended the antimicrobial activity and were developed in
1990s.
MECHANISM OF ACTION
• The fluoroquinolones inhibits the enzyme DNA gyrase in
Gram-negative micro-organism and topoisomerase IV in
gram positive micro-organism. This lead to the bactericidal
effects of fluoroquinolones.
RESISTANCE
• The resistance to fluoroquinolones develops when the
bacteria produce a DNA gyrase or topoisomerase IV
which have reduced affinity for fluoroquinolones or
the bacteria produce efflux pumps across bacterial
memberane which shunt out the fluoroquinolones
from the bacterial cells.
CLASSIFICATION
• FIRST GENERATION
FLOUROQUINOLONES :
1. Norfloxacin
2. Ofloxacin
3. Ciprofloxacin
4. Pefloxacin
• SECOND GENERATION
FLUOROQUINOLONES:
1. Levofloxacin
2. Moxifloxacin
3. Lomefloxacin
4. Gemifloxacin
5. Sparfloxacin
6. Prulifloxacin
PHARMACOKINETICS
• These are given both by oral and intravenous route.
• These have good absorption, when given empty stomach
and food delays the absorption. These drugs have good
tissue penetrability.
• These are excreted in urine by glomerular filtration as well
as tubular secretion.
INDICATIONS
• Bacterial gastroenteritis
• Typhoid fever
• UTI
• Gonorrhoea
• Chancroid
• Bone, Soft tissue and gynaecological infections
• Respiratory infections
• Tuberculosis
• Gram negative septicemia and meningitis
• Conjuctivitis
COMMON ADVERSE EFFECTS
• GI SYSTEM: Nausea, vomiting, bad taste and anorexia
• CNS: Headache, anxiety, insomnia, restlessness and
impairment of concentrations.
• Skin: Rash, photosensitivity
• Contraindicated in pregnancy.
• They should be used in caution in children as a few cases of
joint pain and swelling have been reported and a risk of
cartilage damage is suspended.
FIRST GENERATION
FLUROQUINOLONES
DRUG HALF LIFE ROUTE DOSE
CIPROFLOXACIN 3-5 ORAL, IV, TOPICAL 250-750 mg BD
100-200mg BD
0.3% EYE DROPS
NORFLOXACIN 4-6 ORAL 400mg BD
OFLOXACIN 5-8 ORAL, IV, TOPICAL 200-400 mg BD
200mg BD
0.3% EYE DROPS
PEFLOXACIN 8-14 ORAL OR IV 400mg BD (oral, IV)
SECOND GENERATION
FLUROQUINOLONES
DRUG HALF LIFE ROUTE DOSE
LEVOFLOXACIN 8 ORL,IV,TOPICAL 500mg OD
0.5% EYE DROPS
LOMEFLOXACIN 9 ORAL TOPICAL 400mG OD
0.3% EYE DROPS
SPARFLOXACIN 16-30 ORAL, TOPICAL 200-400mg OD
0.3% eye drops
MOXIFLOXACIN 10-15 ORAL, IV, TOPICAL 400 mg OD
0.5% eye drops
GEMIFLOXACIN 7 ORAL 320 mg OD
PRULIFLOXACIN 10-12 ORAL 600mg OD
GATIFLOXACIN 7-14 ORAL,TOPICAL 400 mg OD
0.5% eye drops.
DRUG INTERACTIONS
• Antacids decrease the absorption of fluoroquinolones.
• Ciprofloxacin inhibits the metabolism of caffeine,
theophylline and warfarin and leads to serious
toxicity.
NURSING IMPLICATIONS
• Patient should be advised to avoid direct sun light.
• Patient should be advised to take plenty of water
during the course.
• Patient should be advised to take medicine in empty
stomach or with little meals for better absorption.
• Patient should be regularly enquired about any side
effects.

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QUINOLONES.pptx

  • 2. INTRODUCTION • These are synthetic antimicrobial having a quinolones structure. • These are active against most of the gram negative bacteria. • In 1960s the first membered of this group, Nalidixic acid, was introduced . • Flouroquinolones have: High potency Expanded antimicrobial spectrum Better tissue penetration Good tolerability profile Very low resistance development
  • 3. 1. NALIDIXIC ACID • It was the first member in quinolones. It was active against gram negative bacteria. It acts by inhibiting bacterial DNA gyrase. It is bacterial in nature. • It is given orally. It attains good concentration in gut, lumen, hence useful in diarrhea. •
  • 4. NALIDIXIC ACID CONTD… • It is most commonly seen in children. And causes neurological toxicity present as headache, drowsiness and vertigo and contraindicated in infants and G6PD deficient patients. • It is given in a dose of 0.5-1g TDS/QID
  • 5. 2. FLUOROQUINOLONES • Fluoroquinolones are quinolones antimicrobials having one or more fluorine substituitions. • The first generation fluoroquinolones have one fluoro substitution and were developed in 1980s. • The second generation fluoroquinolones have additional fluoroquinolones have additional fluoro substitution, which extended the antimicrobial activity and were developed in 1990s.
  • 6. MECHANISM OF ACTION • The fluoroquinolones inhibits the enzyme DNA gyrase in Gram-negative micro-organism and topoisomerase IV in gram positive micro-organism. This lead to the bactericidal effects of fluoroquinolones.
  • 7. RESISTANCE • The resistance to fluoroquinolones develops when the bacteria produce a DNA gyrase or topoisomerase IV which have reduced affinity for fluoroquinolones or the bacteria produce efflux pumps across bacterial memberane which shunt out the fluoroquinolones from the bacterial cells.
  • 8. CLASSIFICATION • FIRST GENERATION FLOUROQUINOLONES : 1. Norfloxacin 2. Ofloxacin 3. Ciprofloxacin 4. Pefloxacin • SECOND GENERATION FLUOROQUINOLONES: 1. Levofloxacin 2. Moxifloxacin 3. Lomefloxacin 4. Gemifloxacin 5. Sparfloxacin 6. Prulifloxacin
  • 9. PHARMACOKINETICS • These are given both by oral and intravenous route. • These have good absorption, when given empty stomach and food delays the absorption. These drugs have good tissue penetrability. • These are excreted in urine by glomerular filtration as well as tubular secretion.
  • 10. INDICATIONS • Bacterial gastroenteritis • Typhoid fever • UTI • Gonorrhoea • Chancroid • Bone, Soft tissue and gynaecological infections • Respiratory infections • Tuberculosis • Gram negative septicemia and meningitis • Conjuctivitis
  • 11. COMMON ADVERSE EFFECTS • GI SYSTEM: Nausea, vomiting, bad taste and anorexia • CNS: Headache, anxiety, insomnia, restlessness and impairment of concentrations. • Skin: Rash, photosensitivity • Contraindicated in pregnancy. • They should be used in caution in children as a few cases of joint pain and swelling have been reported and a risk of cartilage damage is suspended.
  • 12. FIRST GENERATION FLUROQUINOLONES DRUG HALF LIFE ROUTE DOSE CIPROFLOXACIN 3-5 ORAL, IV, TOPICAL 250-750 mg BD 100-200mg BD 0.3% EYE DROPS NORFLOXACIN 4-6 ORAL 400mg BD OFLOXACIN 5-8 ORAL, IV, TOPICAL 200-400 mg BD 200mg BD 0.3% EYE DROPS PEFLOXACIN 8-14 ORAL OR IV 400mg BD (oral, IV)
  • 13. SECOND GENERATION FLUROQUINOLONES DRUG HALF LIFE ROUTE DOSE LEVOFLOXACIN 8 ORL,IV,TOPICAL 500mg OD 0.5% EYE DROPS LOMEFLOXACIN 9 ORAL TOPICAL 400mG OD 0.3% EYE DROPS SPARFLOXACIN 16-30 ORAL, TOPICAL 200-400mg OD 0.3% eye drops MOXIFLOXACIN 10-15 ORAL, IV, TOPICAL 400 mg OD 0.5% eye drops GEMIFLOXACIN 7 ORAL 320 mg OD PRULIFLOXACIN 10-12 ORAL 600mg OD GATIFLOXACIN 7-14 ORAL,TOPICAL 400 mg OD 0.5% eye drops.
  • 14. DRUG INTERACTIONS • Antacids decrease the absorption of fluoroquinolones. • Ciprofloxacin inhibits the metabolism of caffeine, theophylline and warfarin and leads to serious toxicity.
  • 15. NURSING IMPLICATIONS • Patient should be advised to avoid direct sun light. • Patient should be advised to take plenty of water during the course. • Patient should be advised to take medicine in empty stomach or with little meals for better absorption. • Patient should be regularly enquired about any side effects.