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Antimycobacterial drugs
 First line of drugs:
 Isoniazid (INH)
 Rifampicin
 Ethambutol
 Streptomycin
 Pyrazinamide
Never use a single drug therapy
 Isoniazid –rifampicin combination administered
for 9 months will cure 95-98% of cases .
 Addition of pyrazinamide for this combination for
the first 2 months allows total duration to be
reduced to 6 months.
Isoniazid
 Bacteriostatic at low conc. & bacteriocidal at high
conc. Especially against actively growing bacteria.
 Inhibits synthesis of mycolic acid is an essential
components of mycobacterial cell wall.
Pharmacokinetics
 Readily absorbed from GIT.
 Diffuse into all body fluids and tissues
 Penetrates caseous material and macrophages so it
is effective against intra and extracellular
organisms.
 Metabolized in liver by acetylation
 Excreted mainly in urine
Clinical uses
 Mycobacterial infections (it is recommended to be
given with pyridoxine to avoid neuropathy).
 Latent tuberculosis in patients with positive
tuberculin skin test
 Prophylaxis against active TB in individuals who
are in great risk as very young or
immunocompromised individuals.
Adverse effects
 Peripheral neuritis
 Optic neuritis.
 Allergic reactions ( fever,skin rash,systemic lupus
erythematosus )
 Hepatitis
 Gastric upset
 Haemolytic anaemia
 Enzyme inhibitor
 CNS toxicity.
Rifampicin
 Bactericidal ,binds strongly to β subunit of
bacterial DNA-dependent RNA polymerase
leading to inhibition of RNA synthesis .
Pharmacokinetics
 Well absorbed orall.
 Excreted mainly through liver into bile.
 Highly protein bind .
 Penetrates macrophages so affect extra and
intracellular organisms.
 Adequate CSF conc. Only in meningeal
inflammation.
Clinical uses
 Mycobacterial infections
 Prophylaxis in contacts of children with
Haemophilus influenzae type b disease.
 Treatment of serious staphylococcal infections as
osteomyelitis and endocarditis.
 Meningitis by highly resistant penicillin
pneumococci
Adverse effects
 Harmless red-orange colour to urine,sweat,tears,contact
lenses.
 Rashes
 Thrombocytopenia
 Nephritis
 Cholestatic jaundice,hepatitis
 Flu-like syndrome
 Induce cytochrome p-450
Ethambutol
 Inhibits mycobacterial cell wall synthesis by inhibiting
arabinosyl transferase .
 Bacteriostatic
 Active against intra&extracellular bacilli .
 Well absorbed from gut.
 20% excreted in feces and 50% in urine in unchanged
form.
 Crosses BBB in meningitis
 Used only in mycobacterial infections.
Adverse effects
 Retrobulbar (optic) neuritis causing loss of visual
acuity and red-green colour blindness.
 It is relatively contraindicated in children.
 GIT .upset .
 Hyperuricemia
Pyrazinamide
 It is converted to pyrazinoic acid ,the active form
(prodrug)
 Mechanism is unknown.
 Bactericidal
 Acting on intracellular organisms.
 Well absorbed orally ,metabolized in liver
,excreted mainly through kidney .
Clinical uses
 Mycobacterial infections (TB) mainly in multidrug
resistance cases.
 It is important in short –course (6 months)
regimens with isoniazid and rifampicin.
 Prophylaxis of TB in combination with
ciprofloxacin.
Adverse effects
 Hepatotoxic
 Hyperuricemia( provoke acute gouty arthritis )
 Nausea & vomiting
 Drug fever & skin rash
Streptomycin
 Life threating forms of TB ( meningitis,
dissiminated disease).
 Resistant cases (Multidrug resistance tuberculosis
at least to INH & rifampicin ) .
 Amikacin can be used as alternative to
streptomycin.
 Both active mainly against extracellular bacilli.
Indication of 2nd line treatment
 Resistance to the drugs of 1st line.
 Failure of clinical response
 Increase of risky effects.
 Patient is not tolerating the drugs first line drugs.
Ethionamide
 As isoniazid blocks synthesis of mycolic acid .
 Available only in oral form.
 Metabolized by the liver ,excreted by kidney.
 It is poorly tolerated because of :
 -intense gastric irritation
 -neurologic symptoms
 -hepatotoxicity
 Used in TB & leprosy.
Capreomycin
 It is an important injectable agent for treatment of
drug-resistant tuberculosis.
 It is nephrotoxic and ototoxic.
 Local pain & sterile abscesses may occur.
Cycloserine
 Inhibitor of cell wall synthesis
 Cleared renally
 The most serious side effects are peripheral
neuropathy and CNS dysfunction, including
depression & psychotic reaction.
 Pyridoxine should be given.
 Contraindicated in epileptic patients.
Amikacin
 Used as alternative to streptomycin.
 Used in multidrug- resistance tuberculosis.
 No cross resistance between streptomycin and
amikacin.
Ciprofloxacin & levofloxacin
 Effective against typical and atypical
mycobacteria.
 Used against resistant strains.
 Used in combination with other drugs.
Rifapentine
 As rifampicin , it is RNA polymerase inhibitor.
 Cross resistance with rifampicin.
 Potent inducer of cytochrome p450.
 Effective against typical and atypical
mycobacteria.
Aminosalicylic Acid (PAS).
 Similar in structure to sulfonamide and p-aminobenzoic
acid.
 Folate synthesis inhibitor.
 Well absorbed from GIT.
 Widely distributed in tissues except CSF.
 Excreted in urine as active and as metabolic products.
 Causes crystalluria,anorexia,nausea,diarrhea,epigastric
pain.
 Peptic ulcer and haemorrhage can occur.
 Hypersensitivity reactions.
Drugs used in leprosy
Dapsone
 Inhibits folate synthesis.
 Well absorbed orally,widely distributed .
 Half-life 1-2 days,tends to be retained in
skin,muscle,liver and kidney.
 Excreted into bile and reabsorbed in the intestine.
 Excreted in urine as acetylated.
 It is well tolerated.
Clinical uses
 Tuberculoid leprosy.
 Lepromatous leprosy in combination with rifampin
& clofazimine.
 To prevent & treat Pneumocystis pneumonia in
AIDS caused by Pneumocystis jiroveci (
Pneumocystis carinii).
Adverse effects
 Haemolytic anaemia
 Methemoglobinemia
 Gastrointestinal intolerance
 Fever,pruritus,rashes.
 Erythema nodosum leprosum
Clofazimine
 It is a phenazine dye.
 Unknown mechanism of action ,may be DNA binding.
 Antiinflammatory effect.
 Absorption from the gut is variable.
 Given orally , once daily.
 Excreted mainly in feces.
 Stored mainly in reticuloendothelial tissues and skin.
 Half-life 2 months.
 Delayed onset of action (6 weeks).
Clinical uses
 Multidrug resistance TB.
 Lepromatous leprosy
 Tuberculoid leprosy in :
 patients intolerant to sulfones
 dapsone-resistant bacilli.
 Chronic skin ulcers caused by M.ulcerans.
Adverse effects
 Skin discoloration ranging from red-brown to black.
 Gastrointestinal intolerance.
 Red colour urine.
 Eosinophilic enteritis
Treatment of TB in pregnant women
 INH ( pyridoxine should be given ),
 Rifampicin , ethambutol
 Pyrazinamide is given only if :
 Resistant to other drugs is documented
 Streptomycin is contraindicated.
 Breast feeding is not contraindication to receive
drugs , but caution should be observed.

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Antimycobacterial drugs.ppt

  • 1. Antimycobacterial drugs  First line of drugs:  Isoniazid (INH)  Rifampicin  Ethambutol  Streptomycin  Pyrazinamide
  • 2. Never use a single drug therapy  Isoniazid –rifampicin combination administered for 9 months will cure 95-98% of cases .  Addition of pyrazinamide for this combination for the first 2 months allows total duration to be reduced to 6 months.
  • 3. Isoniazid  Bacteriostatic at low conc. & bacteriocidal at high conc. Especially against actively growing bacteria.  Inhibits synthesis of mycolic acid is an essential components of mycobacterial cell wall.
  • 4. Pharmacokinetics  Readily absorbed from GIT.  Diffuse into all body fluids and tissues  Penetrates caseous material and macrophages so it is effective against intra and extracellular organisms.  Metabolized in liver by acetylation  Excreted mainly in urine
  • 5. Clinical uses  Mycobacterial infections (it is recommended to be given with pyridoxine to avoid neuropathy).  Latent tuberculosis in patients with positive tuberculin skin test  Prophylaxis against active TB in individuals who are in great risk as very young or immunocompromised individuals.
  • 6. Adverse effects  Peripheral neuritis  Optic neuritis.  Allergic reactions ( fever,skin rash,systemic lupus erythematosus )  Hepatitis  Gastric upset  Haemolytic anaemia  Enzyme inhibitor  CNS toxicity.
  • 7. Rifampicin  Bactericidal ,binds strongly to β subunit of bacterial DNA-dependent RNA polymerase leading to inhibition of RNA synthesis .
  • 8. Pharmacokinetics  Well absorbed orall.  Excreted mainly through liver into bile.  Highly protein bind .  Penetrates macrophages so affect extra and intracellular organisms.  Adequate CSF conc. Only in meningeal inflammation.
  • 9. Clinical uses  Mycobacterial infections  Prophylaxis in contacts of children with Haemophilus influenzae type b disease.  Treatment of serious staphylococcal infections as osteomyelitis and endocarditis.  Meningitis by highly resistant penicillin pneumococci
  • 10. Adverse effects  Harmless red-orange colour to urine,sweat,tears,contact lenses.  Rashes  Thrombocytopenia  Nephritis  Cholestatic jaundice,hepatitis  Flu-like syndrome  Induce cytochrome p-450
  • 11. Ethambutol  Inhibits mycobacterial cell wall synthesis by inhibiting arabinosyl transferase .  Bacteriostatic  Active against intra&extracellular bacilli .  Well absorbed from gut.  20% excreted in feces and 50% in urine in unchanged form.  Crosses BBB in meningitis  Used only in mycobacterial infections.
  • 12. Adverse effects  Retrobulbar (optic) neuritis causing loss of visual acuity and red-green colour blindness.  It is relatively contraindicated in children.  GIT .upset .  Hyperuricemia
  • 13. Pyrazinamide  It is converted to pyrazinoic acid ,the active form (prodrug)  Mechanism is unknown.  Bactericidal  Acting on intracellular organisms.  Well absorbed orally ,metabolized in liver ,excreted mainly through kidney .
  • 14. Clinical uses  Mycobacterial infections (TB) mainly in multidrug resistance cases.  It is important in short –course (6 months) regimens with isoniazid and rifampicin.  Prophylaxis of TB in combination with ciprofloxacin.
  • 15. Adverse effects  Hepatotoxic  Hyperuricemia( provoke acute gouty arthritis )  Nausea & vomiting  Drug fever & skin rash
  • 16. Streptomycin  Life threating forms of TB ( meningitis, dissiminated disease).  Resistant cases (Multidrug resistance tuberculosis at least to INH & rifampicin ) .  Amikacin can be used as alternative to streptomycin.  Both active mainly against extracellular bacilli.
  • 17. Indication of 2nd line treatment  Resistance to the drugs of 1st line.  Failure of clinical response  Increase of risky effects.  Patient is not tolerating the drugs first line drugs.
  • 18. Ethionamide  As isoniazid blocks synthesis of mycolic acid .  Available only in oral form.  Metabolized by the liver ,excreted by kidney.  It is poorly tolerated because of :  -intense gastric irritation  -neurologic symptoms  -hepatotoxicity  Used in TB & leprosy.
  • 19. Capreomycin  It is an important injectable agent for treatment of drug-resistant tuberculosis.  It is nephrotoxic and ototoxic.  Local pain & sterile abscesses may occur.
  • 20. Cycloserine  Inhibitor of cell wall synthesis  Cleared renally  The most serious side effects are peripheral neuropathy and CNS dysfunction, including depression & psychotic reaction.  Pyridoxine should be given.  Contraindicated in epileptic patients.
  • 21. Amikacin  Used as alternative to streptomycin.  Used in multidrug- resistance tuberculosis.  No cross resistance between streptomycin and amikacin.
  • 22. Ciprofloxacin & levofloxacin  Effective against typical and atypical mycobacteria.  Used against resistant strains.  Used in combination with other drugs.
  • 23. Rifapentine  As rifampicin , it is RNA polymerase inhibitor.  Cross resistance with rifampicin.  Potent inducer of cytochrome p450.  Effective against typical and atypical mycobacteria.
  • 24. Aminosalicylic Acid (PAS).  Similar in structure to sulfonamide and p-aminobenzoic acid.  Folate synthesis inhibitor.  Well absorbed from GIT.  Widely distributed in tissues except CSF.  Excreted in urine as active and as metabolic products.  Causes crystalluria,anorexia,nausea,diarrhea,epigastric pain.  Peptic ulcer and haemorrhage can occur.  Hypersensitivity reactions.
  • 25. Drugs used in leprosy Dapsone  Inhibits folate synthesis.  Well absorbed orally,widely distributed .  Half-life 1-2 days,tends to be retained in skin,muscle,liver and kidney.  Excreted into bile and reabsorbed in the intestine.  Excreted in urine as acetylated.  It is well tolerated.
  • 26. Clinical uses  Tuberculoid leprosy.  Lepromatous leprosy in combination with rifampin & clofazimine.  To prevent & treat Pneumocystis pneumonia in AIDS caused by Pneumocystis jiroveci ( Pneumocystis carinii).
  • 27. Adverse effects  Haemolytic anaemia  Methemoglobinemia  Gastrointestinal intolerance  Fever,pruritus,rashes.  Erythema nodosum leprosum
  • 28. Clofazimine  It is a phenazine dye.  Unknown mechanism of action ,may be DNA binding.  Antiinflammatory effect.  Absorption from the gut is variable.  Given orally , once daily.  Excreted mainly in feces.  Stored mainly in reticuloendothelial tissues and skin.  Half-life 2 months.  Delayed onset of action (6 weeks).
  • 29. Clinical uses  Multidrug resistance TB.  Lepromatous leprosy  Tuberculoid leprosy in :  patients intolerant to sulfones  dapsone-resistant bacilli.  Chronic skin ulcers caused by M.ulcerans.
  • 30. Adverse effects  Skin discoloration ranging from red-brown to black.  Gastrointestinal intolerance.  Red colour urine.  Eosinophilic enteritis
  • 31. Treatment of TB in pregnant women  INH ( pyridoxine should be given ),  Rifampicin , ethambutol  Pyrazinamide is given only if :  Resistant to other drugs is documented  Streptomycin is contraindicated.  Breast feeding is not contraindication to receive drugs , but caution should be observed.