Drugs for leprosy
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Aug 05, 2020
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About This Presentation
Antileprosy drugs have been described with their pharmacology also this topic covers Multidrug treatment for leprosy including paucibacillary and multibacillary leprosy and lepra reactions
Slide Content
Dr Naser Ashraf Tadvi
Objectives
•Classify anti-leprosy drugs
•Discuss the Mechanism of action, relevant
pharmacokinetics, adverse effects and
contraindications of antileprosy drugs
•Describe the treatment of Paucibacillary and
multibacillary leprosy
•Describe the treatment of type 1 and 2 lepra
reaction
•Classify anti-leprosy drugs
•Discuss the Mechanism of action, relevant
pharmacokinetics, adverse effects and
contraindications of antileprosy drugs
•Describe the treatment of Paucibacillary and
multibacillary leprosy
•Describe the treatment of type 1 and 2 lepra
reaction
Leprosy
•Dapsone
SULFONES
•Clofazimine
PHENAZINE DERIVATIVES
•Rifampicin
ANTITUBERCULAR DRUGS
•FLUOROQUINOLONES : Ofloxacin, Moxifloxacin
•MACROLIDES : Clarithromycin
•TETRACYCLINES : Minocycline
OTHER ANTIBIOTICS :
SULFONES
•Clofazimine
PHENAZINE DERIVATIVES
•Rifampicin
ANTITUBERCULAR DRUGS
•FLUOROQUINOLONES : Ofloxacin, Moxifloxacin
•MACROLIDES : Clarithromycin
•TETRACYCLINES : Minocycline
OTHER ANTIBIOTICS :
•Chemically related to sulfonamides & shares a
common mechanism of action
•Leprostatic at very low concentration
•Not used for other pyogenic infections
•Not used alone always used with rifampicin and/or
clofazimine in MDT for leprosy
Dapsone'schemical name is 4,4'-diamino diphenylsulfone
common mechanism of action
•Leprostatic at very low concentration
•Not used for other pyogenic infections
•Not used alone always used with rifampicin and/or
clofazimine in MDT for leprosy
Dapsone'schemical name is 4,4'-diamino diphenylsulfone
•Slowly and completely absorbed from GIT
•70% plasma protein bound
•Produces ten times more concentration
in diseased skin than in normal skin
•t ½ -24 hrs
•70-80% excreted in urine
•Drug is excreted in milk
Pharmacokinetics
DAPSONE
•70% plasma protein bound
•Produces ten times more concentration
in diseased skin than in normal skin
•t ½ -24 hrs
•70-80% excreted in urine
•Drug is excreted in milk
Pharmacokinetics
DAPSONE
•ActascompetitiveinhibitoroftheenzymeDIHYDROPTEROATESYNTHETASE
(DHPS).
Mechanism of Action
DAPSONE
(DHPS).
Mechanism of Action
DAPSONE
Mechanism of Action
•Folateisnecessaryforthecelltosynthesizenucleicacidsand
initsabsencecellswillbeunabletodivide.
•Hencethesulfonamideantibacterialexhibitabacteriostatic
effect
•Folateisnotsynthesizedinmammaliancells,butisinsteada
dietaryrequirement.Thisexplainstheselectivetoxicityto
bacterialcellsofthesedrugs.
DAPSONE
•Folateisnecessaryforthecelltosynthesizenucleicacidsand
initsabsencecellswillbeunabletodivide.
•Hencethesulfonamideantibacterialexhibitabacteriostatic
effect
•Folateisnotsynthesizedinmammaliancells,butisinsteada
dietaryrequirement.Thisexplainstheselectivetoxicityto
bacterialcellsofthesedrugs.
DAPSONE
Resistance
❑Secondaryresistanceusuallyisseeninlepromatous(multibacillary)
patientstreatedwithasingledrug.
RESISTANCE
PRIMARY
Untreated
Patients
SECONDARY
Patients on
treatment
❑mutationinfolP1ofM.leprae
DAPSONE
❑Secondaryresistanceusuallyisseeninlepromatous(multibacillary)
patientstreatedwithasingledrug.
RESISTANCE
PRIMARY
Untreated
Patients
SECONDARY
Patients on
treatment
❑mutationinfolP1ofM.leprae
DAPSONE
•Mild hemolytic anemia in G6PD deficiency
•Methemoglobinemia
Adverse effect
DAPSONE
Dapsone to be avoided if Hb is < 7 gm/dl
•Methemoglobinemia
Adverse effect
DAPSONE
Dapsone to be avoided if Hb is < 7 gm/dl
•Gastric intolerance: nausea , vomiting
anorexia.
•Cutaneous reactions:
•Hepatitis & agranulocytosis
•CNS: headache parasthesia, tinnitus
•Fever
•Sulfone (Dapsone) syndrome
Adverse Effects
DAPSONE
anorexia.
•Cutaneous reactions:
•Hepatitis & agranulocytosis
•CNS: headache parasthesia, tinnitus
•Fever
•Sulfone (Dapsone) syndrome
Adverse Effects
DAPSONE
•Severe anemia
•G6PD deficiency
•Hypersensitivity reactions
Contraindications
DAPSONE
•G6PD deficiency
•Hypersensitivity reactions
Contraindications
DAPSONE
•Leprosy
•With pyrimethamine
–Resistant Falciparum malaria
–P Jirovecii Infection
–Toxoplasmosis
Indications
DAPSONE
•With pyrimethamine
–Resistant Falciparum malaria
–P Jirovecii Infection
–Toxoplasmosis
Indications
DAPSONE
•Phenazine dye
•Leprostatic
•Anti-inflammatory action:
–Major advantage used in ENL
•BIOLOGICAL LAG 6-7 weeks
•Clinical improvement visible by 6
th
month
CLOFAZIMINE
•Leprostatic
•Anti-inflammatory action:
–Major advantage used in ENL
•BIOLOGICAL LAG 6-7 weeks
•Clinical improvement visible by 6
th
month
CLOFAZIMINE
Mechanism of Action
CLOFAZIMINE
•Preferentialybinds to mycobacterial DNA
•Interferes with template function of the DNA
•Alteration of membrane structure and
transport function
CLOFAZIMINE
•Preferentialybinds to mycobacterial DNA
•Interferes with template function of the DNA
•Alteration of membrane structure and
transport function
Pharmacokinetics
CLOFAZIMINE
▪Absorption : 40-70%
▪Lipophilic taken up by macrophages
▪t 1/2 –70 days
CLOFAZIMINE
▪Absorption : 40-70%
▪Lipophilic taken up by macrophages
▪t 1/2 –70 days
Adverse Effects
CLOFAZIMINE
•Reddish black discoloration of nonexposed
skin
•Discoloration of hair and body secretions
•Dryness of skin, itching & scaling
•Abdominal pain
SMALL BOWEL
SYNDROME
Persistent diarrhea
Abdominal pain
Weight loss
CLOFAZIMINE
•Reddish black discoloration of nonexposed
skin
•Discoloration of hair and body secretions
•Dryness of skin, itching & scaling
•Abdominal pain
SMALL BOWEL
SYNDROME
Persistent diarrhea
Abdominal pain
Weight loss
1. Pregnancy
2. Liver and kidney disease
3. GI symptoms
Contraindications
CLOFAZIMINE
2. Liver and kidney disease
3. GI symptoms
Contraindications
CLOFAZIMINE
•Most potent cidaldrug for M Leprae
•Rifampicin kills 99.99 %of organisms in 3-7 days
•Free from cross resistance from other organisms.
•The drug has a particular effect in relieving nasal
symptoms and healing of foot ulcers
•Dose–600 mg once a month
•Rifampicin kills 99.99 %of organisms in 3-7 days
•Free from cross resistance from other organisms.
•The drug has a particular effect in relieving nasal
symptoms and healing of foot ulcers
•Dose–600 mg once a month
FLUOROQUINOLONES
•Ofloxacin, Pefloxacin, Sparfloxacin, Moxifloxacin
•BACTERICIDAL & highly effective
•22 doses of Ofloxacin ( 400mg/day) -killed 99.99%
•Used as an alternate drug
•Ofloxacin, Pefloxacin, Sparfloxacin, Moxifloxacin
•BACTERICIDAL & highly effective
•22 doses of Ofloxacin ( 400mg/day) -killed 99.99%
•Used as an alternate drug
•Only macrolide having significant activity against M.
Leprae
•Clarithromycin is less BACTERICIDALthan Rifampicin.
•500mg /day in Lepromatous Leprosy patients killed
99.9% bacteria in 8 WEEKS
•Included in alternative regimens
CLARITHROMYCIN
CLARITHROMYCIN
Leprae
•Clarithromycin is less BACTERICIDALthan Rifampicin.
•500mg /day in Lepromatous Leprosy patients killed
99.9% bacteria in 8 WEEKS
•Included in alternative regimens
CLARITHROMYCIN
CLARITHROMYCIN
•Semisynthetic derivative of tetracycline
•High lipophilicity
•Bactericidal
MINOCYCLINE
BACTERICIDAL ACTION
Rifampicin> Minocycline> Clarithromycin
•High lipophilicity
•Bactericidal
MINOCYCLINE
BACTERICIDAL ACTION
Rifampicin> Minocycline> Clarithromycin
Classification of Leprosy
Tuberculoid leprosy
•Anaesthetic patch
•CMI is normal
•Lepromin test positive
•Bacilli rarely found in
biopsies
•Prolonged remissions with
periodic exacerbation
Lepromatous leprosy
•Diffuse skin & mucus
membrane infiltration &
nodules
•Deficient
•Negative
•Skin & mucus membrane
lesions bacilli +
•Progresses to anesthesia of
distal parts, atrophy,
ulceration, absorption of
digits
Tuberculoid leprosy
•Anaesthetic patch
•CMI is normal
•Lepromin test positive
•Bacilli rarely found in
biopsies
•Prolonged remissions with
periodic exacerbation
Lepromatous leprosy
•Diffuse skin & mucus
membrane infiltration &
nodules
•Deficient
•Negative
•Skin & mucus membrane
lesions bacilli +
•Progresses to anesthesia of
distal parts, atrophy,
ulceration, absorption of
digits
Classification of Leprosy
Paucibacillary leprosy
•1-5 skin lesions
•No nerve or only 1 nerve
involvement
•Skin smear is negative at all
sites
•TT & BT
Multibacillary leprosy
•6 or more skin lesions
•> 1 nerve involvement
•Negative
•Skin smear positive at any
one site
•LL, BL, BB
Paucibacillary leprosy
•1-5 skin lesions
•No nerve or only 1 nerve
involvement
•Skin smear is negative at all
sites
•TT & BT
Multibacillary leprosy
•6 or more skin lesions
•> 1 nerve involvement
•Negative
•Skin smear positive at any
one site
•LL, BL, BB
Multidrug therapy for leprosy
Multibacillary Paucibacillary
Rifampicin 600 mg once
monthly supervised
600 mg once
monthly supervised
Dapsone 100 mg daily
supervised
100 mg daily
supervised
Clofazimine 300 mg/ month
supervised + 50 mg
daily supervised
-
Duration 12 months 6 months
Multibacillary Paucibacillary
Rifampicin 600 mg once
monthly supervised
600 mg once
monthly supervised
Dapsone 100 mg daily
supervised
100 mg daily
supervised
Clofazimine 300 mg/ month
supervised + 50 mg
daily supervised
-
Duration 12 months 6 months
Alternative regimens for leprosy
•Intermittent ROM
•Intermittent RMMx
•Ofloxacin or minocycline can be used in place
of clofazimine (if pt refuses Clofazimine)
•4 drug therapy
–Rifampicin 600 mg + sparfloxacin 200 mg +
clarithromycin 500 mg + Minocycline 100 mg daily
for 12 weeks
•Intermittent ROM
•Intermittent RMMx
•Ofloxacin or minocycline can be used in place
of clofazimine (if pt refuses Clofazimine)
•4 drug therapy
–Rifampicin 600 mg + sparfloxacin 200 mg +
clarithromycin 500 mg + Minocycline 100 mg daily
for 12 weeks
Treatment : Corticosteroids
Cutaneous ulcerations,multiple
nerve involvement
Type IV Hypersensitivity
(Delayed hypersensitivity response)
TYPE 1 /
REVERSAL REACTIONS
Treatment :
Clofazamine,corticosteroids,
Thalidomide
Existing lesions enlarge ,
become red, inflamed and
painful
Type III Hypersensitivity
(Humoral antibody response)
TYPE2 / ERYTHEMA
NODOSUM LEPROSUM
LEPRA REACTIONS
LepraReactions
DAPSONE
Cutaneous ulcerations,multiple
nerve involvement
Type IV Hypersensitivity
(Delayed hypersensitivity response)
TYPE 1 /
REVERSAL REACTIONS
Treatment :
Clofazamine,corticosteroids,
Thalidomide
Existing lesions enlarge ,
become red, inflamed and
painful
Type III Hypersensitivity
(Humoral antibody response)
TYPE2 / ERYTHEMA
NODOSUM LEPROSUM
LEPRA REACTIONS
LepraReactions
DAPSONE
REACTION PREDNISOLONE CLOFAZAMINE THALIDOMIDE
Reversal
reaction
(Type 1)
up to 1 mg/kg/d
then gradually
reduced
Erythema
Nodosum
Leprosum
(Type 2)
up to 1 mg/kg/d
then gradually
reduced
up to 300 mg up to 400 mg
•Maximum daily dose is shown when single use
•Combination therapy is recommended in ENL
Treatment of LepraReactions
DAPSONE
Reversal
reaction
(Type 1)
up to 1 mg/kg/d
then gradually
reduced
Erythema
Nodosum
Leprosum
(Type 2)
up to 1 mg/kg/d
then gradually
reduced
up to 300 mg up to 400 mg
•Maximum daily dose is shown when single use
•Combination therapy is recommended in ENL
Treatment of LepraReactions
DAPSONE
Drugs used for the Management of Reactions
•Thalidomide
•Corticosteroids
•Chloroquine
•Clofazamine
•NSAIDS
•Thalidomide
•Corticosteroids
•Chloroquine
•Clofazamine
•NSAIDS
Summary
•Drugs for leprosy
•MDT for leprosy
•Type 1 lepra reaction
•Type 2 lepra reaction
•Drugs for leprosy
•MDT for leprosy
•Type 1 lepra reaction
•Type 2 lepra reaction
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