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Samiyathunnisa P
First year m pharm
 Tuberculosis (TB) remains a leading infectious
disease caused by Mycobacterium tuberculosis,
which can produce either a silent, latent infection
or a progressive, active disease.
 Transmission usually takes place through the
airborne spread of droplet nuclei produced by
patients with infectious pulmonary tuberculosis
ETIOLOGY
 M. tuberculosis preferentially infects
humans, and the closely related
Mycobacterium bovis causes a similar
disease in cattle and other livestock.
humans frequently developed TB by
drinking milk contaminated with M. bovis.
 The complex includes M. africanum, M.
microti and M. canettii
 M. tuberculosis is an aerobic ,slender
bacillus with a waxy outer layer.
 under the microscope, it is either straight or
slightly curved in shape.
 It does not stain well with Gram stain, so the
Ziehl-Neelsen stain.
 After Ziehl-Neelsen staining with carbol-
fuchsin, mycobacteria retain the red color
despite acid–alcohol washes. Hence they
are called acid-fast bacilli
EPIDEMIOLOGY
 Tuberculosis is the second most common
cause of death from an infectious disease in
the world
 In 2009, there were an estimated 9.4 million
incident cases (range, 8.9 million–9.9 million)
of TB globally
 There were an estimated 14 million prevalent
cases(range 12 million–16 million) of TB in
2009
 There were an estimated 440 000 cases of
multi-drug resistant TB (MDR-TB) in 2008
CLASSIFICATION
1)pulmonary TB
2)Extrapulmonary TB:
It occurs in places other than the lungs,
including the larynx, the lymph nodes, the
pleura, the brain, the kidneys, or the bones
and joints. In HIV-infected persons,
extrapulmonary TB disease is often
accompanied by pulmonary TB.
 Lymphadenopathy
 Tubercular meningitis
 Miliary TB
 Bone/joint TB
 Additional sites
 lymphadenopathy
 Trials have shown that 6 months of treatment are just as
effective as 9 months for fully susceptible bacilli.
 The standard 6-month treatment regimen is recommended
 Meningeal TB
 Patients with active meningeal TB (tuberculous
meningitis)should be treated with rifampicin and isoniazid
for 12 months together with pyrazinamide, and normally
ethambutol, for the first 2 months.
 Bone and joint TB
 The spine is the most common site for bone TB.
 treated effectively with standard agents such as isoniazid
and rifampicin for 6 months, together with pyrazinamide
and a fourth drug, usually ethambutol in the initial phase
(for 2 months).
 Miliary TB
 Miliary TB occurs when tubercle bacilli enter the
bloodstream and disseminate to all parts of the
body, where they grow and cause disease in
multiple sites. This condition is rare but serious.
“
 Miliary” refers to the radiograph appearance of
millet seeds scattered throughout the lung. It is
most common in infants and children younger
than 5 years of age, and in severely
immunocompromised persons.
 The standard 6-month regimen containing both
 isoniazid and rifampicin, with pyrazinamide and
ethambutol in
 the first 2 months, is used.
PATHOPHYSIOLOGY
 Primary infection usually results from inhaling
airborne particles that contain M.
tuberculosis.These particles, called droplet
nuclei, contain one to three bacilli and are small
enough (1 to 5 mm)to reach the alveolar
surface.
 The progression to clinical disease depends on
three factors:
 (a) the number of M. tuberculosis organisms
inhaled
 (b) the virulence of these organisms
 (c) the host’s cell-mediated immune response.
 Droplet nuclei
containing tubercle
bacilli are inhaled,
enter the lungs, and
travel to the alveoli.
 Tubercle bacilli
multiply in the alveoli.
ALVEOLI
 Within 2 to 8 weeks, special
immune cells
(macrophages) ingest and
surround the tubercle
bacilli. The cells form a
barrier shell, called a
granuloma, that keeps the
bacilli contained and under
control (LTBI).
 If the immune system
cannot keep the tubercle
bacilli under control, the
bacilli begin to multiply
rapidly (TB disease).
 A small number of
tubercle bacilli enter
the bloodstream and
spread throughout
the body. The bacilli
may reach any part
of the body, including
areas where TB
disease is more
likely to develop.
 Patients typically
present with weight
loss, fatigue, a
productive cough,
fever, and night sweats
 Frank hemoptysis
SIGNS AND SYMPTOMS
DIAGNOSIS
Physical Examination
 Dullness to chest percussion, rales, and
increased vocal fremitus are observed frequently
on auscultation
Laboratory Tests
 Moderate elevations in the WBC count with a
lymphocyte predominance
TUBERCULIN /MANTOUX TEST
 The standard 5-
tuberculin-unit PPD dose
is placed intracutaneously
in the forearm.
 Produce wheal 6 mm to
10 mm in diameter
 Represent DTH (delayed
type hypersensitivity)
 read the test in 48 to 72
hours.
 Measure only induration
 Record reaction in mm
 AFB Microscopy
 A presumptive diagnosis
is based on the finding of
AFB on microscopic
examination of a
diagnostic specimen such
as a smear of
expectorated sputum or of
tissue.
 three sputum specimens,
preferably collected early
in the morning.
 Strongly consider TB in
patients with smears
containing acid-fast bacilli
(AFB)
Mycobacterium tuberculosis (stained
red) in sputum
Chest Radiograph
 Patchy or nodular
infiltrates in the
apical areas of the
upper lobes or the
superior segment of
the lower lobes
 Cavitation that may
show air-fluid levels
as the infection
progresses
GENERAL APPROACHES TO TREATMENT
 Drug treatment is the cornerstone of TB management.
 Monotherapy can be used only for infected patients
who do not have active TB.
 Once active disease is present, a minimum of two
drugs, and generally 3 or 4 drugs, must be used
simultaneously.
 The duration of treatment depends on the condition of
the host, extent of disease, presence of drug
resistance, and tolerance of medications.
 The shortest duration of treatment generally is 6
months, and 2 to 3 years of treatment may be
necessary for cases of multidrug-resistant TB (MDR-
TB).
 The DOTS strategy has emerged as a
possible solution to the rising number of TB
cases in different parts of the world and has
been incorporated in India’s Revised
National Tuberculosis Control Programme
(RNTCP)as well.
 The strategy assures a compulsory and free
availability of good quality drugs to all TB
cases and necessitates drug administration
under direct supervision, thereby ensuring
the requisite regimen-compliance.
Grouping Drugs
Group 1:
First-line oral anti-TB agents
Isoniazid (H); Rifampicin (R);
Ethambutol (E); Pyrazinamide
(Z)
Group 2:
Injectable anti-TB agents
Streptomycin (S); Kanamycin (Km);
Amikacin (Am);
Capreomycin (Cm); Viomycin
(Vm).
Group 3:
Flouroquinolones
Ciprofloxacin (Cfx); Ofloxacin (Ofx);
Levofloxacin (Lvx); Moxifloxacin
(Mfx); Gatifloxacin (Gfx)
Group 4:
Oral second-line anti-TB agents
Ethionamide (Eto); Prothionamide
(Pto); Cycloserine (Cs);
Terizadone (Trd);
para-aminosalycilic acid (PAS);
FIRST-LINE DRUGS
DRUG 3 times
per week
dose(ad
ult)
Dose in
mg per kg
(thrice a
week) in
children
SIDE EFFECTS
Isoniazid (H) 900mg
10 – 15mg
clinical hepatitis,peripheral
neuropathy, CNS effects, lupus-
like syndrome, hypersensitivity
Rifampicin(R) 600mg 10mg Pruritis, rash,hepatotoxicity, GI
Symptoms, flu-like
syndrome,thrombocytopenia, renal
failure
Pyrazinamide(Z) 1500mg 35mg Hepatotoxicity,nausea,anorexia,po
lyarthralgia, rash, hyperuricemia,
dermatitis
Ethambutol(E) 1200mg 30mg Optic neuritis, skin rash
LATENT TB INFECTION
 Isoniazid preferred drug for treating LTBI.
 Generally, isoniazid alone is given for 9 months.
 The treatment of LTBI reduces a person’s lifetime
risk of active TB.
 adult doses are usually 300mg daily
 Isoniazid should be given on an empty stomach,
and antacids should be avoided within 2 hours of
dosing.
 Pregnant women, alcoholics,and patients with poor
diets who are treated with isoniazid should receive
pyridoxine 10 -50 mg daily to reduce the incidence
of peripheral neuropathy.
 Rifampin 600 mg daily for 4 months can be used
when isoniazid resistance is suspected or when the
patient cannot tolerate isoniazid.
Diagnosti
c
category
People with TB
disease
Initial phase 3
times weekly
Continuation
Daily or 3
times weekly
1 New sputum smear
positive
2 HRZE 4 HR
or
6 HE daily
2 Previously treated
sputum smear
positive: relapse
2 HRZES
followed by 1
HRZE
5 HRE
3 Sputum smear-
negative Not
seriously ill, extra-
pulmonary
2 HRZE 4 HR
or 6 HE daily
4 Chronic and multi-
drug-resistant TB
Specially designed standardized
or individualized regimens
ACTIVE TB
DRUG-RESISTANT TB DISEASE (CAT 4)
 can develop in two different ways, called
primary and secondary resistance.
 Primary resistance occurs in persons who are
initially exposed to and infected with resistant
organisms.
 Secondary resistance, or acquired resistance,
develops during TB therapy, either because the
patient was treated with an inadequate regimen
or did not take the prescribed regimen
appropriately, or because of other conditions
such as drug malabsorption or drug-drug
interactions that led to low serum levels.
2 TYPE
 1. Multi-drug resistant TB
 2.Extensively resistant TB
1.MDR TB is caused by organisms resistant to
both isoniazid and rifampin, which are the two
most effective anti-TB drugs. These drugs are
considered first-line drugs and are used to treat
most persons with TB disease.
Standardized RNTCP regimen for MDR TB
Intensive phase(6-9
months)
Kanamycin
Ofloxacin Or
levofloxacin
Ethionamide
Cycloserine
Pyrazinamide
Ethambutol
Continuation
phase(18months)
Ofloxacin or levofloxacin
Ethionamide
Cycloserine
ethambutol
+pyridoxine 100mg/day
 2.XDR TB is resistant to both isoniazid and
rifampin, plus any fluoroquinolone and at least
one of three injectable second-line drugs (i.e.,
amikacin, kanamycin, or capreomycin). Because
XDR TB disease is resistant to first-line and
second-line drugs, patients are left with
treatment options that are more toxic, more
expensive, and much less effective.
SPECIAL POPULATIONS
 Streptomycin should be avoided, while other
drugs can be used safely during pregnancy.
 Lactation:-
 Mother and baby should stay together and the
baby should continue to breastfeed.
 After active TB in the baby is ruled out, the
baby should be given 6 months of isoniazid
preventive therapy, followed by BCG
vaccination
 In the presence of renal disease, H, R and Z are
relatively safe for administration, while S and E
are avoided.
 In liver disease, the reverse procedure is
followed i.e. S and E are considered to be
safe, whereas H, R and Z should be
stopped.
 Children under 6 years of age, having a
family member with smear-positive TB,
should be screened for symptoms.
BCG VACCINE
 It is a live vaccine bearing an attenuated
bovine strain of M. tuberculosis
 It is supplied as 0.5-1 mg dry powder in
ampules to be suspended in 1 ml of
sterilewater
 DOSE: 0.05 ml (in neonate) 0.1 ml (older
individuals) is injected intracutaneously in
the left deltoid region atbirth.
REFERENCE
 Pharmacotherapy - A Pathophysiologic
approach, 7th edition by Joseph. T. Dipiro,
 Applied therapeutics – Marry Anne koda-
kimble
 Medical pharmacology by K.D.Tripathi

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tuberulosis ppt

  • 2.  Tuberculosis (TB) remains a leading infectious disease caused by Mycobacterium tuberculosis, which can produce either a silent, latent infection or a progressive, active disease.  Transmission usually takes place through the airborne spread of droplet nuclei produced by patients with infectious pulmonary tuberculosis
  • 3. ETIOLOGY  M. tuberculosis preferentially infects humans, and the closely related Mycobacterium bovis causes a similar disease in cattle and other livestock. humans frequently developed TB by drinking milk contaminated with M. bovis.  The complex includes M. africanum, M. microti and M. canettii
  • 4.  M. tuberculosis is an aerobic ,slender bacillus with a waxy outer layer.  under the microscope, it is either straight or slightly curved in shape.  It does not stain well with Gram stain, so the Ziehl-Neelsen stain.  After Ziehl-Neelsen staining with carbol- fuchsin, mycobacteria retain the red color despite acid–alcohol washes. Hence they are called acid-fast bacilli
  • 5. EPIDEMIOLOGY  Tuberculosis is the second most common cause of death from an infectious disease in the world  In 2009, there were an estimated 9.4 million incident cases (range, 8.9 million–9.9 million) of TB globally  There were an estimated 14 million prevalent cases(range 12 million–16 million) of TB in 2009  There were an estimated 440 000 cases of multi-drug resistant TB (MDR-TB) in 2008
  • 6. CLASSIFICATION 1)pulmonary TB 2)Extrapulmonary TB: It occurs in places other than the lungs, including the larynx, the lymph nodes, the pleura, the brain, the kidneys, or the bones and joints. In HIV-infected persons, extrapulmonary TB disease is often accompanied by pulmonary TB.  Lymphadenopathy  Tubercular meningitis  Miliary TB  Bone/joint TB  Additional sites
  • 7.  lymphadenopathy  Trials have shown that 6 months of treatment are just as effective as 9 months for fully susceptible bacilli.  The standard 6-month treatment regimen is recommended  Meningeal TB  Patients with active meningeal TB (tuberculous meningitis)should be treated with rifampicin and isoniazid for 12 months together with pyrazinamide, and normally ethambutol, for the first 2 months.  Bone and joint TB  The spine is the most common site for bone TB.  treated effectively with standard agents such as isoniazid and rifampicin for 6 months, together with pyrazinamide and a fourth drug, usually ethambutol in the initial phase (for 2 months).
  • 8.  Miliary TB  Miliary TB occurs when tubercle bacilli enter the bloodstream and disseminate to all parts of the body, where they grow and cause disease in multiple sites. This condition is rare but serious. “  Miliary” refers to the radiograph appearance of millet seeds scattered throughout the lung. It is most common in infants and children younger than 5 years of age, and in severely immunocompromised persons.  The standard 6-month regimen containing both  isoniazid and rifampicin, with pyrazinamide and ethambutol in  the first 2 months, is used.
  • 9. PATHOPHYSIOLOGY  Primary infection usually results from inhaling airborne particles that contain M. tuberculosis.These particles, called droplet nuclei, contain one to three bacilli and are small enough (1 to 5 mm)to reach the alveolar surface.
  • 10.  The progression to clinical disease depends on three factors:  (a) the number of M. tuberculosis organisms inhaled  (b) the virulence of these organisms  (c) the host’s cell-mediated immune response.
  • 11.  Droplet nuclei containing tubercle bacilli are inhaled, enter the lungs, and travel to the alveoli.  Tubercle bacilli multiply in the alveoli. ALVEOLI
  • 12.  Within 2 to 8 weeks, special immune cells (macrophages) ingest and surround the tubercle bacilli. The cells form a barrier shell, called a granuloma, that keeps the bacilli contained and under control (LTBI).  If the immune system cannot keep the tubercle bacilli under control, the bacilli begin to multiply rapidly (TB disease).
  • 13.  A small number of tubercle bacilli enter the bloodstream and spread throughout the body. The bacilli may reach any part of the body, including areas where TB disease is more likely to develop.
  • 14.  Patients typically present with weight loss, fatigue, a productive cough, fever, and night sweats  Frank hemoptysis SIGNS AND SYMPTOMS
  • 15. DIAGNOSIS Physical Examination  Dullness to chest percussion, rales, and increased vocal fremitus are observed frequently on auscultation Laboratory Tests  Moderate elevations in the WBC count with a lymphocyte predominance
  • 16. TUBERCULIN /MANTOUX TEST  The standard 5- tuberculin-unit PPD dose is placed intracutaneously in the forearm.  Produce wheal 6 mm to 10 mm in diameter  Represent DTH (delayed type hypersensitivity)  read the test in 48 to 72 hours.  Measure only induration  Record reaction in mm
  • 17.  AFB Microscopy  A presumptive diagnosis is based on the finding of AFB on microscopic examination of a diagnostic specimen such as a smear of expectorated sputum or of tissue.  three sputum specimens, preferably collected early in the morning.  Strongly consider TB in patients with smears containing acid-fast bacilli (AFB) Mycobacterium tuberculosis (stained red) in sputum
  • 18. Chest Radiograph  Patchy or nodular infiltrates in the apical areas of the upper lobes or the superior segment of the lower lobes  Cavitation that may show air-fluid levels as the infection progresses
  • 19.
  • 20. GENERAL APPROACHES TO TREATMENT  Drug treatment is the cornerstone of TB management.  Monotherapy can be used only for infected patients who do not have active TB.  Once active disease is present, a minimum of two drugs, and generally 3 or 4 drugs, must be used simultaneously.  The duration of treatment depends on the condition of the host, extent of disease, presence of drug resistance, and tolerance of medications.  The shortest duration of treatment generally is 6 months, and 2 to 3 years of treatment may be necessary for cases of multidrug-resistant TB (MDR- TB).
  • 21.  The DOTS strategy has emerged as a possible solution to the rising number of TB cases in different parts of the world and has been incorporated in India’s Revised National Tuberculosis Control Programme (RNTCP)as well.  The strategy assures a compulsory and free availability of good quality drugs to all TB cases and necessitates drug administration under direct supervision, thereby ensuring the requisite regimen-compliance.
  • 22. Grouping Drugs Group 1: First-line oral anti-TB agents Isoniazid (H); Rifampicin (R); Ethambutol (E); Pyrazinamide (Z) Group 2: Injectable anti-TB agents Streptomycin (S); Kanamycin (Km); Amikacin (Am); Capreomycin (Cm); Viomycin (Vm). Group 3: Flouroquinolones Ciprofloxacin (Cfx); Ofloxacin (Ofx); Levofloxacin (Lvx); Moxifloxacin (Mfx); Gatifloxacin (Gfx) Group 4: Oral second-line anti-TB agents Ethionamide (Eto); Prothionamide (Pto); Cycloserine (Cs); Terizadone (Trd); para-aminosalycilic acid (PAS);
  • 23. FIRST-LINE DRUGS DRUG 3 times per week dose(ad ult) Dose in mg per kg (thrice a week) in children SIDE EFFECTS Isoniazid (H) 900mg 10 – 15mg clinical hepatitis,peripheral neuropathy, CNS effects, lupus- like syndrome, hypersensitivity Rifampicin(R) 600mg 10mg Pruritis, rash,hepatotoxicity, GI Symptoms, flu-like syndrome,thrombocytopenia, renal failure Pyrazinamide(Z) 1500mg 35mg Hepatotoxicity,nausea,anorexia,po lyarthralgia, rash, hyperuricemia, dermatitis Ethambutol(E) 1200mg 30mg Optic neuritis, skin rash
  • 24. LATENT TB INFECTION  Isoniazid preferred drug for treating LTBI.  Generally, isoniazid alone is given for 9 months.  The treatment of LTBI reduces a person’s lifetime risk of active TB.  adult doses are usually 300mg daily  Isoniazid should be given on an empty stomach, and antacids should be avoided within 2 hours of dosing.  Pregnant women, alcoholics,and patients with poor diets who are treated with isoniazid should receive pyridoxine 10 -50 mg daily to reduce the incidence of peripheral neuropathy.  Rifampin 600 mg daily for 4 months can be used when isoniazid resistance is suspected or when the patient cannot tolerate isoniazid.
  • 25. Diagnosti c category People with TB disease Initial phase 3 times weekly Continuation Daily or 3 times weekly 1 New sputum smear positive 2 HRZE 4 HR or 6 HE daily 2 Previously treated sputum smear positive: relapse 2 HRZES followed by 1 HRZE 5 HRE 3 Sputum smear- negative Not seriously ill, extra- pulmonary 2 HRZE 4 HR or 6 HE daily 4 Chronic and multi- drug-resistant TB Specially designed standardized or individualized regimens ACTIVE TB
  • 26. DRUG-RESISTANT TB DISEASE (CAT 4)  can develop in two different ways, called primary and secondary resistance.  Primary resistance occurs in persons who are initially exposed to and infected with resistant organisms.  Secondary resistance, or acquired resistance, develops during TB therapy, either because the patient was treated with an inadequate regimen or did not take the prescribed regimen appropriately, or because of other conditions such as drug malabsorption or drug-drug interactions that led to low serum levels.
  • 27. 2 TYPE  1. Multi-drug resistant TB  2.Extensively resistant TB
  • 28. 1.MDR TB is caused by organisms resistant to both isoniazid and rifampin, which are the two most effective anti-TB drugs. These drugs are considered first-line drugs and are used to treat most persons with TB disease. Standardized RNTCP regimen for MDR TB Intensive phase(6-9 months) Kanamycin Ofloxacin Or levofloxacin Ethionamide Cycloserine Pyrazinamide Ethambutol Continuation phase(18months) Ofloxacin or levofloxacin Ethionamide Cycloserine ethambutol +pyridoxine 100mg/day
  • 29.  2.XDR TB is resistant to both isoniazid and rifampin, plus any fluoroquinolone and at least one of three injectable second-line drugs (i.e., amikacin, kanamycin, or capreomycin). Because XDR TB disease is resistant to first-line and second-line drugs, patients are left with treatment options that are more toxic, more expensive, and much less effective.
  • 30. SPECIAL POPULATIONS  Streptomycin should be avoided, while other drugs can be used safely during pregnancy.  Lactation:-  Mother and baby should stay together and the baby should continue to breastfeed.  After active TB in the baby is ruled out, the baby should be given 6 months of isoniazid preventive therapy, followed by BCG vaccination  In the presence of renal disease, H, R and Z are relatively safe for administration, while S and E are avoided.
  • 31.  In liver disease, the reverse procedure is followed i.e. S and E are considered to be safe, whereas H, R and Z should be stopped.  Children under 6 years of age, having a family member with smear-positive TB, should be screened for symptoms.
  • 32. BCG VACCINE  It is a live vaccine bearing an attenuated bovine strain of M. tuberculosis  It is supplied as 0.5-1 mg dry powder in ampules to be suspended in 1 ml of sterilewater  DOSE: 0.05 ml (in neonate) 0.1 ml (older individuals) is injected intracutaneously in the left deltoid region atbirth.
  • 33. REFERENCE  Pharmacotherapy - A Pathophysiologic approach, 7th edition by Joseph. T. Dipiro,  Applied therapeutics – Marry Anne koda- kimble  Medical pharmacology by K.D.Tripathi

Hinweis der Redaktion

  1. Miliary TB Miliary TB occurs when tubercle bacilli enter the bloodstream and disseminate to all parts of the body, where they grow and cause disease in multiple sites. This condition is rare but serious. “Miliary” refers to the radiograph appearance of millet seeds scattered throughout the lung. It is most common in infants and children younger than 5 years of age, and in severely immunocompromised persons.
  2. Good T-lymphocyte responses are essential to controlling M. tuberculosis infections. The TH1 response is the preferred response to TB. T-lymphocytes activate macrophages that, in turn, engulf and kill mycobacteria. They also destroy immature macrophages that harbor M. tuberculosis but are unable to kill the invaders. CD4+ cells are the primary T cells involved, with contributions by T cells and CD8+ T cells.
  3. The area of induration (the “bump”)is the important end point, not the area of redness.
  4. Persons unable to cough up sputum induce sputum bronchoscopy gastric aspiration Follow infection control precautions during specimen collection
  5. The keys to successful treatment of LTBI are (a) infection by an isoniazid-susceptible isolate, (b) adherence to the 9-month regimen, and (c) no exogenous reinfection.2 Isoniazid adult doses are usually 300 mg daily (5 to 10 mg/kg of body weight)55 (see Table 116–2). Lower doses are less effective.2,52 Isoniazid should be given on an empty stomach, and antacids should be avoided within 2 hours of dosing