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Professor Of Pediatrics,

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Title: Professor Of Pediatrics,


1
Pneumonia
  • By
  • Professor Of Pediatrics,
  • Head of Allergy Clinical Immunology Unit -
    Mansoura University
  • Egypt

Magdy Zedan.
2
Out Line
  • (1) Definition and Pathophysiolgoy of
    pneumomnia
  • (2) Does the patient have a pneumonia?
  • (3) What is the microbial etiology?
  • (4) Where you treat?
  • (5) How to treat?

3
Definition
  • Its an infection in alveolar spaces
  • (pulmonary parenchyma) leading to their
  • Consolidation.
  • Consolidation means the alveoli are
  • filled with exudates and inflammatory
  • cells with loss of their gaseous content.

4
Pathophysiology
  • A- Development of Pneumonia
  • Virulent organism.
  • Immune compromised host Local

  • Systemic
  • B- Pulmonary host defenses
  • (1)Mechanical and structural
  • Cough.
  • Mucocilliary clearance
  • Airway branching (configuration)
  • continue

5

Pathophysiology
  • Pulmonary host defenses
  • (2) Cellular defenses
  • Resident alveolar macrophages
  • Recruited Neutrophils occures when alveolar
    macrophages are over whelmed in lower respiratory
    tract infections.
  • continue

6
Pathophysiology
  • (3)Humoral defenses
  • IgA in upper airway
  • IgG in lower airway
  • (4) Inflammatory and molecular defenses
  • Airway epithelium through secretion of peptides
    called defensins, and chemokines.
  • Cytokines as IL-10,GM- CSF.
  • continue

7
Pathophysiology
  • Bacteria or virus gain access to respiratory
    tract from
  • Inhalation of contaminated air
  • Microaspiration
  • Hematogenous seeding of the lung.
  • Whether Pneumonia is the result of such
    bacterial entry depends on interaction between
    the bacterium (load, Virulence) and pulmonary
    defense mechanism.
  • continue

8
Pathophysiology
  • The usual out come is ingestion of bacteria or
    virus by alveolar macrophages, an alternative but
    less common is complement mediated bacterial
    lyses
  • When these mechanisms dont destroy alveolar
    bacteria,polymorph nuclear leukocytes with their
    phagocytic capability are required with the
    result inflammatory response results
    in Pneumonia passing in 3 stages.

9
Pathology of Pneumonia
  • 1- Stage of congestion (red hepatization)
  • Due to antigen antibody reaction no
  • radiological findings.
  • 2- Stage of gray hepatiztion
  • Respiratory distress and homogenous
  • opacity in chest rdiography.
  • 3- Stage of resolution
  • When immune system takes upper
  • hand, resolution and convalescence.

10
Pathology
11
Classification of Pneumonia
  • Two types typical And atypical.
  • (1) Typical pneumonia
  • (2) Atypical pneumonia
  • Another Classification
  • (1) Community- acquired pneumonia ( CAP)
  • (2) hospital acquired pneumonia (
    nosocomial
  • pneumonia)

12
Out Line
  • (1) Definition and Pathophysiolgoy of pneumomnia
  • (2) Does the patient have a pneumonia?
  • (3) What is the microbial etiology?
  • (4) Where you treat?
  • (5) How to treat?

13
Clinical and Radiological Diagnosis of Pneumonia
  • (1) Respiratory distress
  • (2) Bronchial breathing or fine
  • consonating creptation by
  • auscultation
  • (3) Homogenous opacity is a cardinal
  • radiological sign

14
Clinical and Radiological Diagnosis of Pneumonia
  • To differentiate between Bacterial and viral
    etiology
  • Look for
  • - preceding symptoms
  • - Fever
  • - Para pneumonic effusion
  • - Wheezes
  • - Distribution size of homogenous
  • opacity

15
Radiology
16
Radiology
17
Out Line
  • (1) Definition and Pathophysiolgoy of pneumomnia
  • (2) Does the patient have a pneumonia?
  • (3) What is the microbial etiology?
  • (4) Where you treat?
  • (5) How to treat?

18
Etiological Diagnosis
  • It is difficult to determine the causative
    organism of Pneumonia. So the treatment usually
    empirical based on Predicting factors for the
    causative organism as the following.
  • a) Age of the patient.
  • b) Immune status,
  • c) Extra pulmonary manifestations.
  • It can be confirmed by
  • Culture Specific tests.
  • continue

19
Etiological Diagnosis
  • Age as a predictor for eteological diagnosis
  • A- In CAP
  • Neonates
  • Common- Group B B- hemolytic streptococci
  • Gram negative enteric bacilli
    such as Escherichia coli and Klepsella pneumoniae
  • Less frequent
  • Staph-auras
  • P.aeruginosa
  • continue

20
  • Etiological Diagnosis
  • Children Past neonatal period
  • 1- 5 month age Chlamydia trachomatis
  • gt 5 years Atypical (intracellular)
    micro-organisms as mycoplasma pneumoniae,
    legonella, chlamydia SPP are the commonest
    etiological agents.
  • All ages
  • Frequent S. pneumoniae
  • Infrequent causes as
  • - H. influenza (vaccine)
  • - S, aureus but it needs
    special consideration for
  • rapid progression of the
    disease.
  • - Group A B hemolytic
    streptococci are uncommon
  • cause of pneumonia
  • continue

21
Etiological Diagnosis
  • In hospital acquired pneumonia
  • Common
  • Gram negative organism such as
  • K. pneumonia, Pseudomonas aurugnosia and serrata
    spaces
  • Gram positive organisms such as
  • S. Aureus most frequent leogionella pneumoniae is
    rare

22
Investigation of Pneumonia
  • Routine Investigation
  • X ray
  • CBC with differential
  • SaO2,
  • Blood culture
  • Specific Investigation
  • Bronchoscopy and C.T for unresolved pneumonia
  • Serology ( IgM, IgE, IgG)
  • Sputum and pleural evaluation

23
Out Line
  • (1) Definition and Pathophysiolgoy of pneumomnia
  • (2) Does the patient have a pneumonia?
  • (3) What is the microbial etiology?
  • (4) Where you treat?
  • (5) How to treat?

24
Indication for Hospitalization in Pneumonia
  • 1) Patients with tacchypnea, toxic
  • appearance, poor feeding , dehyration
  • 2) Infant lt 2 months of age
  • 3) Massive para pneumonic affusion
  • 4) Associated co-morbidty
  • 5) Immundeficiency.

25
Staphylococcal Pneumonia
  • It is an infrequent cause of pneumonia
  • Age under one year , it occurs either community
    acquired following influenza or at nosocomial
    setting
  • Characters-
  • 1) At the onset, chest radiographs may be
    normal
  • However. S. aureus pneumonia is more
  • commonly bronchopneumonia with a patchy
  • central infiltrate. Usually unilateral
  • Continue
  • continue

26
Staphylococcal Pneumonia
  • 2) Rapid progression of the disease from
  • Patchy cansolidation to cavity, pneumatocele
    or
  • tension pneumothorax should raise the
    possibility of S. aureus pneumonia, when it
    occurs
  • 3) Effusion or empyema
  • Develops in about 90 of patients
  • Spontaneous pneumothorax or pyopneumothorax
  • Occur in about 25-50 of cases
  • Pneumatocele
  • Occur in gt 50 of cases and may change
    hourly in number or size in acute phase.
  • continue

27
Staphylococcal Pneumonia
  • This previous radiographic picture of S. aureus
    pneumonia is not pathognomonic as it occurs with
  • Pneumonia caused by
  • Klebsiella species, other gram negative
    bacteria group A streptococci and occasionally
    pneumococci
  • OR it may mimic congenital diaphragmatic hernia.
  • 4) Staphylococcal pneumenia
  • It should be suspected in hospitalized
    infants (particularly those in ICU) who develop
    parenchymal unexplained opaque shadows.
  • continue

28
Staphylococcal Pneumonia
  • 5) Species of staphylococci
  • A) S. aureus
    coagulase positive
  • B) S. albus
  • C) Staphylococcus epidermidis ?
    coagulase
  • negative
  • Morphologically all staphylococci are gram
    positive
  • Coagulase does not reflect virulence
  • Virulence of S. aureus related to secretion of
    different toxins as hemolysins and leukocidin
    that kills neutrophils.

29
Treatment of Staphylococcal pneumonia
  • The production of B- lactamase by nearly all S.
    aureus isolates rendered ineffective any drug
    bydrolysed by this enzyme.
  • First line therapy is Hospital admission,
  • B lactamase resistant penicillin
  • such as Methicillin ? no longer in use
  • its modern analogs i.e oxacillin, cloxacillin,
    Flucloxacillin, nafcillin
  • MRSA ( methicillin resistant S. aureus) which
    was found to be resistant to all B lactams and
    all cephalosporin compounds.

30
Treatment of Staphylococcal Pneumonia
  • MRSA infections that are nosocomially acquired
    was found to be sensitive to Vancomycin
  • Now MRSA infection became community acquired
  • Clindamycin indicated in MRSA infection in
    patients allergic to B-lactams
  • Duration of treatment 2-3 weeks, but 6 weeks
    recommended to decrease the risk of relapse
  • Supportive therapy o2, maintenance of, fluid,
    electrolyte and hemoglobin levels
  • continue
  • continue

31
Treatment of Staphylococcal Pneumonia
  • The most important complication is
  • Empyema and lung abscess, pneumothorax each
  • has a special treatment

Treatment in summary B. lactamase resistant penicillins or first generation cephalosporin for 2-3 weeks MRSA ? vancomycin Clindamycin MRSA patient allergic to B lactams
32
HaemophilusInfluenzaType b
  • H. influenza is gram - negative bacilli
  • H. influenza can lead to invasive infectious
    in pediatrics as pneumonia, meningitis,
    cellulites, epiglottites, septic arthritis,
    osteomyelitis percarditis and bacteremia
  • Incidance of H. influenza pneumonia decrease
    after administration of Hib canjugate vaccine
  • The virulence of serotype b is related to
    serotype b capsular polysaccharide

33
Haemophilus Influenza Type b
  • Radiographic findings of H. influenza pneumonia
    vary from-
  • 1) Bronchiolctic type with central linear
  • infiltrates and over inflation
  • 2)Bronchopneumonia with patchy
  • consolidation with no lobar affection

34
Treatment of H. Influenza Pneumonia
  • we have two clinical situations
  • 1) pneumonia complicated with bacteremia,
  • pleural effusion usually occur in
    children less
  • than 12 months. Those group needs
    Hospital
  • admission with I.V treatment for 7-10
    days
  • continue

35
Treatment of H. Influenza Pneumonia
  • 2) Pneumonia and the patient is not appears
    severely ill those group treated at home with
    oral antimicrobial
  • Oral therapy in mild H. influenza infection TMP/
    SMX or amoxicillin / clavulanate Erythromycin has
    poor activity
  • Invasive infections IV treatment by
    cephalosporin (cefotaxime or ceftriaxone)
    Alternatively chloramphencol with ampicillin,

36
Mycoplasma Pneumonia
  • Mycoplasma pneumoniae causes
  • Non classic bacterial pneumonias. They are small
    organisms that are able to live outside the host
    cell. Because they have no cell wall, they are
    not killed by cell wall- active agents such as
    penicillins and cephalosporins.
  • Mycoplasma pneumonia is common cause
  • of CAP that occurs gt 5 years of age

37
Pathogenesis of Pulmonary Infections
  • Infection with M. pneumoniae are acquired via
    respiratory route from droplet infection.
  • The organism attaches to a receptor on
    respiratory epithelium and remains extra cellular
    causing cellular damage.
  • Specific cell mediated immune responses increase
    with age so it tends to be milder in children
    than in adults and also severe in reinfection.

38
Diagnosis of Mycoplasma Pneumonia
  • The diagnostic clue Is the poor correlation
    between clinical symptoms which are severe, with
    minimal pulmonary physical and radiological
    findings. This poor correlation present all
    through the course of the disease and this is the
    hall mark of diagnosis of M.pneumonia.

39
Clinical Picture
  • Typically the patients present with gradual
    onset of malaise, headache and fever over 1 week.
    Cough dry or productive associated with symptoms
    as vomiting, diarrhea, chest pain, sore throat.
  • Physical findings are relatively minimal early
    in the course of illness no finding on chest
    examination later on bronchial breathing crackles
    or wheezes can be heard.
  • 3- Radiologic findings
  • Usually unilateral in 87 and involves lower
    lobes
  • In the early stages the pattern is reticular and
    interstitial
  • Later patchy or segmental areas of consolidation
    are
  • noted.
  • Continue

40
Clinical Picture
  • 4- Extra pulmonary manifestation
  • They are the second hallmark of M. pneumonia.
  • Such complications commonly occur 1-21 days
    after the onset of respiratory symptoms. Most of
    the diagnosis have been based on the result of
    serology (four fold rise in complement fixation
    titres) rather than no culture confirmation.
  • Neurological manifestations.
  • Dermatologic manifestations.
  • Cardiac manifestations.
  • continue

41
Clinical Picture
  • 4- Extra pulmonary manifestation
  • GIT manifestations.
  • Hematologic manifestations.
  • Musculoskeletal manifestations.
  • Genitourinary manifestations.
  • Immunologic manifestations.

42
Diagnostic Criteria of Mycoplasma Infection
  • Serologic assays are the mainstay for diagnosing
    mycoplasma infection-
  • 1.Cold agglutinin identification
  • Cold agglutinins usually appear by the end of
    first week and disappear by 2-3 months
  • Cold agglutinin responses are non specific and
    consistent mostly IgM
  • So IgM lacks specificity and sensitivity
  • continue

43
Diagnostic Criteria of Mycoplasma Infection
  • Specific serological test-
  • Complement fixation test has been used as
  • standared for diagnosis with titer gt 132
  • The test measures IgM antibodies
  • This test has 90 sensitivity and 94
  • specificity
  • Polymerase chain Reaction(PCR)
  • PCR diagnosis M. pneumonia in both throat
    swab and CSF.

44
Treatment of M. Pneumonia
  • Macrolides are the drug of choice as-
  • Erythromycins, Azithromycin are specific
  • treatment.
  • Because M. pneumonia has no cell wall, it is
  • resistant to penicillins, cephalosporins and
  • other cell wall active agents.

45
Pneumococcal Pneumonia
  • Pneumococcus (Streptococcus Pneumoniae)
  • It is the most common cause of bacterial
    pneumonia in children. The organism is gram
    positive cocci.The virulence of the pneumococci
    is related to there capsule.
  • It affects all ages.
  • Continue

46
  • Pneumococcal Pneumonia
  • Diagnosis
  • It is typical pneumonia with sudden onset of
    fever, cough, chest pain and dyspnea.
  • Physical examination
  • Pleurtic chest pain my be referred to abdomen
    with misleading suspicion of acute appendicitis.
  • Symptoms and signs of meningismus may be present
    with upper lobe pneumonia.
  • Continue

47
Pneumococcal Pneumonia
  • 2) Physical examination
  • Dullness on percussion denotes empyema because
    the
  • lesion usually patchy in distribution
  • Fine rales difficult to be heard.

48
Pneumococcal Pneumonia
  • Treatment
  • Penicillins are the drugs of choice in treatment
    of pneumococcal infection.
  • If the patient is resistant to penicillins,
    cephalosporin is indicated.
  • If the patient is allergic to penicillins
    vancomycin clindamycin or chloramphenecol are the
    drugs of choice .

49
Recurrent or Unresolved Pneumonia
  • I- Multiple lobe affection
  • Congential heart disease with excess pulmonary
    blood flow.
  • Immune deficiency either local or general.
  • Specific infection as T.B and fungal infection
    (Aspergillus)
  • II- Singal lobe affection
  • Obstruction Intraluminal, Extraluminal.
  • Structural abnormalities as pulmonary
    sequestration.

50
Differential Diagnosis of Pneumonias
  • 1) Between 4 common types of pneumonia
  • Staph pneumonia
  • Mycoplasma Pneumonia
  • H. influenza pneumonia
  • Pneumococcal pneumonia
  • 2) From other causes of
  • Respiratory distress
  • Pulmonory inflitrates.

51
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