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Childhood tuberculosis

Childhood tuberculosis. Dr. Magdy Fawzy NTP, Egypt PAL coordinator. Introduction: . One third of the world’s population is infected with Mycobacterium tuberculosis . Each year, about 9 million people develop TB, of whom 2 millions die

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Childhood tuberculosis

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  1. Childhood tuberculosis Dr. Magdy Fawzy NTP, Egypt PAL coordinator

  2. Introduction: • One third of the world’s population is infected with Mycobacterium tuberculosis. • Each year, about 9 million people develop TB, of whom 2 millions die • Of the 9 million annual TB cases, about 1 million (11%) occur in children (under 15 years of age). • Of these childhood cases, 75% occur annually in 22 high-burden countries that together account for 80% of the world’s estimated incident cases. • In countries worldwide, the reported percentage of all TB cases occurring in children varies from 3% to more than 25%.

  3. 22 high-burden countries: 80% of all new cases 10000 1000 Estimated new TB cases ('000s) 100 10 India China Brazil Kenya Nigeria Ethiopia Uganda Pakistan Thailand Viet Nam Myanmar Cambodia Indonesia DR Congo Philippines Zimbabwe Bangladesh Mozambique UR Tanzania Afghanistan South Africa Russian Federation

  4. Which factors influence children to become infected? Mostly “Environmental” • Exposure - Never exposed = never infected - Duration of exposure • Bacterial load in source case • Closeness of contact

  5. Only Adults Transmit TB Number of bacilli in sputum Adult Child 108 104 Need about 105 organisms/ml for positive smear

  6. Transitions in Childhood Tuberculosis Contact with smear positive index case Not infected (50-70%) Infected (30-50%) Diseased (10-30%) Within 2 years (50%) Lifelong (50%)

  7. Exposure, infection and evolution: • The source of infection of most children is an infectious adult in their close environment (usually the household). • This exposure leads to the development of a primary parenchymal lesion (Ghon focus) in the lung with spread to the regional lymph node(s). • The immune response (delayed hypersensitivity and cellular immunity) develops about 4–6 weeks after the primary infection.

  8. Exposure, infection and evolution, cont.: • In most cases, the immune response stops the multiplication of M. tuberculosis bacilli at this stage. • However, a few dormant bacilli may persist. • A positive tuberculin skin test (TST) would be the only evidence of infection. • In some cases, the immune response is not strong enough to contain the infection and disease occurs within a few months.

  9. Exposure, infection and evolution, cont.: • Risk of progression to disease is increased when primary infection occurs particularly in the very young (0–4 years). • Children who develop disease usually do so within 2 years following exposure and infection, i.e. they develop primary TB. • A small proportion of children (generally older children) develop post-primary TB either due to: • Reactivation, after a latent period, of dormant bacilli acquired from a primary infection or • By reinfection.

  10. The key risk factors for TB are: • Household contact with a newly diagnosed smear-positive case. • Age less than 5 years. • HIV infection. • Severe malnutrition.

  11. Diagnosis of TB in children

  12. Key features suggestive of TB The presence of three or more of the following should strongly suggest a diagnosis of TB: • Chronic symptoms suggestive of TB • Physical signs highly of suggestive of TB • A positive tuberculin skin test • ChestX-ray suggestive of TB.

  13. Recommended approach to diagnose TB in children

  14. Careful history including history of TB contact and symptoms consistent with TB.

  15. history of Contact • Close contact is defined as living in the same household as or in frequent contact with a source case (e.g. the child’s caregiver) with sputum smear-positive pulmonary TB. • Smear-negative but culture-positive cases are also infectious, but to a much lesser degree.

  16. Important points • All symptomatic children who have been in close contact with a smear-positive TB case, must be screened for TB. • When any child is diagnosed with TB, an effort should be made to detect the source case and any other undiagnosed cases in the household. • Children should be regarded as infectious if they have sputum smear-positive pulmonary TB or cavitary TB on CXR and child contacts must be sought and screened.

  17. b. Symptoms The commonest are: • Prolonged cough An unremitting cough that is not improving and has been present for more than 21 days. • Fever Body temperature of >38 °C for 14 days, after common causes such as malaria or pneumonia...etc have been excluded. • Weight loss or failure to thrive

  18. Clinical examination (including growth assessment). • There are no specific features on clinical examination that confirm pulmonary TB.

  19. Some signs are highly suggestiveand requiring investigation to exclude extra-pulmonary TB: • gibbus, especially of recent onset (resulting from vertebral TB) • non-painful enlarged cervical lymphadenopathy with sinus formation; • Meningitis not responding to antibiotic treatment, with a sub-acute onset or raised intracranial pressure with early affection of the cranial nerves. • Pleural effusion • Pericardial effusion • Distended abdomen with ascites • Non-painful enlarged joint • Signs of tuberculin hypersensitivity (e.g. phlyctenular conjunctivitis, erythema nodosum).

  20. Documented weight loss or failure to gain weight, especially after being treated in a nutritional rehabilitation program, is a good indicator of chronic disease in children, of which TB may be the cause.

  21. Tuberculin skin test • A TST is the intradermal injection of a combination of mycobacterial antigens which elicit an immune response (delayed-type hypersensitivity), represented by induration, which can be measured in millimeters. • TST using the Mantoux method is the standard method of identifying people infected with M. tuberculosis. • Multiple puncture tests should not be used to determine whether a person is infected, as these tests are unreliable (because the amount of tuberculin injected intradermally cannot be precisely controlled).

  22. A positive TST occurs when a person is infected with M. tuberculosis, but does not necessarily indicate disease. • TST can be used as an adjunct in diagnosing TB in children with signs and symptoms of TB and in conjunction with other diagnostic tests. • Use 5 tuberculin units (TU) / 0.1 ml of tuberculin PPD-S or 2 TU / 0.1 of tuberculin PPD RT23. • The results should be read between 48 and 72 hours after administration. A patient who does not return within 72 hours will probably need to be rescheduled for another TST.

  23. Interpretation of the test Diameter of induration of ≥5 mm is considered positive in: • HIV-infected children • Severely malnourished children (with clinical evidence of marasmus or kwashiorkor). Diameter of induration of ≥10 mm is considered positive in: • Children more than 5 years or not vaccinated with BCG.

  24. Bacteriological confirmation whenever possible • Among younger children, especially under 5 years, sputum is difficult to obtain. • Most children are sputum smear-negative. • Children who are able to produce a specimen, it is worth sending it for smear microscopy and mycobacterial culture if available. • Bacterial yields are higher in older children (more than 5 years of age) and adolescents, and in children of all ages with severe disease.

  25. Appropriate clinical samples include: • Sputum, • Gastric aspirates • Laryngeal swaps • Certain other material e.g. lymph node biopsy or other biopsies. • Fine-needle aspiration of enlarged lymph glands – for both staining of acid-fast bacilli and histology – has been shown to be a useful investigation, with a high bacteriological yield.

  26. Role of culture • Increase the yield of confirmed TB cases, • Differentiate M. tuberculosis from other non-tuberculous mycobacteria. • determine the resistance pattern.

  27. Common ways of obtaining samples for smear microscopy and culture

  28. Expectoration • Older children (10 years of age or older). • As with adult TB suspects, three sputum specimens should be obtained: an on-the-spot specimen, an early morning specimen and a second on-the-spot specimen.

  29. b. Gastric aspirate • Gastric aspiration using a naso-gastric feeding tube can be performed in young children who are unable expectorate sputum. • A gastric aspirate should be obtained on each of three consecutive mornings. • The diagnostic yield (positive culture) of a set of three gastric aspirates is only about 25–50% of children with active TB.

  30. Gastric aspirate, cont. Precautions • Fasting for at least 4 hours (3 hours for infants) prior to the procedure. • Children with a low platelet count or bleeding tendency should not undergo the procedure.

  31. Gastric aspirate, cont. Procedure • Inpatient first thing in the morning when the child wakes up, • Position the child on his or her back or side. • Measure the distance between the nose and stomach, to estimate distance that will be required to insert the tube into the stomach. • Attach a syringe to the nasogastric tube. • Gently insert the nasogastric tube through the nose and advance it into the stomach. • Withdraw (aspirate) gastric contents (2–5 ml) using the syringe attached to the nasogastric tube.

  32. Gastric aspirate, cont. • To check the position of the tube is correct, test the gastric contents with litmus paper: • This can also be checked by pushing some air (e.g. 3–5 ml) from the syringe into the stomach and listening with a stethoscope over the stomach. • If no fluid is aspirated, insert 5–10 ml sterile normal saline and attempt to aspirate again.

  33. Gastric aspirate, cont. • If still unsuccessful, attempt this again (even if the nasogastric tube is in an incorrect position and water or normal saline is inserted into the airways, the risk of adverse events is still very small). • Do not repeat more than three times. • Withdraw the gastric contents (ideally at least 5–10 ml). • Transfer gastric fluid from the syringe into a sterile container (sputum collection cup). • Add an equal volume of sodium bicarbonate solution to the specimen to neutralize the acidic gastric contents.

  34. c. Sputum induction • safe and effective in children of all ages. • the bacterial yields are as good as or better than for gastric aspirates. • should be performed in an isolation room with adequate infection control precautions.

  35. Sputum induction, cont. Very few adverse events have been reported: • Coughing spells, • Mild wheezing • Nosebleeds.

  36. Sputum induction, cont. General approach • Examine child before the procedure to ensure he is well enough to undergo the procedure. • Children with the following characteristics should not undergo sputum induction. • Inadequate fasting: for at least 3 hours, • Respiratory distress (including rapid breathing, wheezing, hypoxia). • Intubated. • low platelet count, bleeding tendency, severe nosebleeds. • Reduced level of consciousness. • History of significant asthma

  37. Procedure • Administer a bronchodilator (e.g. salbutamol) to reduce the risk of wheezing. • Administer nebulized hypertonic saline (3% NaCl) for 15 minutes or until 5 cm3 of solution have been fully administered. • Chest physiotherapy is necessary; this is useful to mobilize secretions. • Older children now able to expectorate • young children, do suction of the nasopharynx to collect a suitable specimen.

  38. Chest radiography • The commonest picture is that of persistent opacification in the lung together with enlarged hilar or subcarinal lymph glands. • Adolescent patients with TB have CXR changes similar to adult patients..

  39. Extra-pulmonary TB

  40. Other tests • PCR Not currently recommended for routine diagnosis of childhood TB, as they have been inadequately studied in children and have performed poorly in the few studies which have been done.

  41. Scoring system

  42. SCORE SYSTEM FOR THE DIAGNOSIS OF TB IN CHILDREN • Has been rarely evaluated or validated • The basis of a score system is the careful and systematic collection of diagnostic information. • A score of 7 or more indicates a high likelihood of TB.

  43. TB treatment

  44. TB chemotherapy should be based on two important microbiological considerations: The combination of drugs to avoid the development of resistance. The need for prolonged chemotherapy to prevent disease relapse.

  45. All mono-therapeutic regimens (real or masked by combination with drugs to which bacilli are resistant) lead to treatment failure and to the development of resistance. When three or more drugs are administered, the risk of resistance is practically zero.

  46. Phases of treatment: The intensive phase • usually covers the first 2 months of treatment. • During this phase, most of the bacilli will be killed. • The sputum converts from positive to negative in more than 80 % of the new patients within the first 2 months of treatment. The continuation phase • usually lasts 4-6 months, depending on the treatment regimen. • This phase is intended to eliminate the remaining dormant bacilli. • These dormant bacilli decrease constantly as treatment intake progresses. • Since it is not possible to identify which patients still have dormant bacilli, all patients should continue their treatment until the end of the prescribed period, to limit the number of relapses.

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