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Childhood tb

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Title: Childhood tb

1
Childhood tuberculosis

Dr. Salvatory .F.M
Lecture
PDCH

2
Introduction

One third of the worlds population is infected
with Mycobacterium tuberculosis.
In 2015,estimated of incidence cases were
10.4millions,whereby 10 were children below 15
years
In 2015,WHO estimated 1.4m deaths due to TB
Of these childhood cases, 75 occur annually in
22 high-burden countries that together account
for 80 of the worlds estimated incident cases.
The magnitude of childhood TB in Tanzania is
difficult to ascertain due to challenges in
diagnosis and reporting

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

4
Only Adults Transmit TB

Number of bacilli in sputum
Adult Child
108
104
Need about 105 organisms/ml for positive smear

5
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.

6
Natural history and pathogenesis

Caused by Mycobacterium tuberculosis
Inhalation of bacilli form a smear positive adult
or adolescent
Bacilli are deposited in the lungs and multiply
in terminal alveoli(Ghon focus)
Some bacilli are carried by macrophages through
lymphatic channels to regional lymph nodes
especially hillar lymph nodes

Lymphatic and haematogeneous spread the bacilli
to other part of the body leading to
disserminated TB
In majority of infected children the immune
system stops multiplication of bacilli and the
infection remain latent for many years

gtReactivation of infection may occur in children
with weak immune system eg malnutrition and
HIV-AIDS

9
Diagnosis of TB in children
10
Key features suggestive of TB

The presence of three or more of the following
should strongly suggest a diagnosis of TB
History of close contact with an infectious
case(smear ve)
Physical signs highly suggestive of TB
A positive tuberculin skin test
Suggestive findings of TB in X RAY,FNAC .

11
Recommended approach to diagnose TB in children

Careful history
including history of TB contact and symptoms
consistent with TB.
Coughgt 2 or more weeks
failure to thrive
night sweats
fevergt2 weeks or more
Wait loss or faltering

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

Some signs are highly suggestive and 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).

3.Tuberculin skin test
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.

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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.

17
TST
18
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.

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.

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

21
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..

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24
Extra-pulmonary TB
25

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.

26
Scoring system
27
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.

28
score 4 3 2 1 0 feature
General General General General General General General
4wlt 2-4w 2wgt Duration of illness
60gt 60-80 80lt Weight for age
Proved VE Reported -VE Family history
positive Tuberculin test
Not improving After 4 w Malnutrition
No response to nonspecific treatment Unexplained fever and night sweats
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Local Local Local Local Local Local Local
Lymph nodes
Joint or bone swelling
Abd. mass or ascites
CNS findings
Angle deformity of the spine
Total score Total score Total score Total score Total score Total score
30
TB treatment
31

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.

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.

33
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.

34
First-line anti-tuberculosis drugs, action and
side effects
35
DRUG RECOMMENDED DAILY DOSAGE (DOSE RANGE),mg/kg
Isoniazide (H) 5 (46)
Rifampicin (R) 10 (812)
Pirazinamide (Z) 25 (2030)
Ethambutol (E) 15 (1520)
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Treatment regimens
Continuation Initial Patient Category Treatment category
4/HR 2/SHRZ OR 2/EHRZ New smear ve PTB. New smear ve New forms of extra-Pulmonary TB. I
HRZE means isoniazid rifampicin pyrazinamide
ethambutol.
38
Treatment regimens, cont
Continuation Initial Patient Category Treatment category
5/HRE 2/SHRZE then 1/HRZE Sputum smear ve Relapse. Treatment after failure. Treatment after interruption. II
39