Clinical Aspects of Tuberculosis - PowerPoint PPT Presentation

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Clinical Aspects of Tuberculosis

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Clinical Aspects of Tuberculosis Professor Mike McKendrick Lead Physician Department of Infection and Tropical Medicine Royal Hallamshire Hospital – PowerPoint PPT presentation

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Title: Clinical Aspects of Tuberculosis


1
Clinical Aspects of Tuberculosis
  • Professor Mike McKendrick
  • Lead Physician
  • Department of Infection and Tropical Medicine
  • Royal Hallamshire Hospital
  • Sheffield
  • Honorary Professor
  • Division of Genomic Medicine
  • University of Sheffield

2
Clinical aspects of TB
  • Pathogenisis
  • Clinical diagnosis
  • Treatment and monitoring and control
  • New issues

3
Clinical Aspects of Tuberculosis
  • Pathogenesis of tuberculosis
  • Infection versus disease
  • Host factors
  • Pathogen factors

4
Pathogenesis
  • Host factors include
  • Social e.g.
  • Poverty
  • alcoholism
  • Age e.g.
  • Baby
  • Teenage girl
  • Old age
  • Immunity e.g.
  • HIV
  • Gamma interferon
  • SCID

5
Pathogenesis
  • Organism factors e.g.
  • Virulence factors
  • Drug resistance

6
Pathogenesis
  • MTB into lungs (or to cervical nodes or abdo.
    nodes)
  • Replication of organisms
  • Primary complex (lung and mediastinal lymph
    nodes)
  • Mycobacteraemia with potential for seeding
  • Consequence of tuberculous infection
  • Symptomatic illness disease (minority)
  • immunological control (majority) with Ghon focus
    on Xray. Infection is contained by granuloma
    but not eliminated

7
Pathogenesis
  • Tuberculous disease is a consequence of
  • Primary infection e.g. in baby
  • Reactivation
  • natural
  • Associated with immunosupression
  • Re infection

8
Clinical features
  • Clinical illness
  • Pulmonary
  • Extrapulmonary

9
Clinical illness
  • Chest
  • Pulmonary
  • Pleural
  • Mediastinal nodes
  • pericardium
  • Extra pulmonary
  • skin and soft tissues (including lymph nodes)
  • Bone
  • Abdominal
  • Intra cranial
  • other

10
Clinical clues for TB
  • Clinical symptoms usually chronic rather than
    acute
  • Fever
  • Sweats
  • Weight loss
  • Focal symptoms
  • Epidemiology
  • History of TB, HIV
  • Country of origin, recent travel/work
  • Contact with TB
  • England, Wales NI 2004
  • 7,176 notifications, 414 children
  • 70 foreign born population groups

11
TB guidelines for the clinician
  • Great mimicker
  • Low index of suspicion
  • Pulmonary TB usually easy to consider
  • Non pulmonary often requires lateral thinking

12
Clinical TB
  • Laboratory samples
  • In the current era every effort must be made to
    obtain adequate samples likely to lead to a
    microbiological diagnosis before treatment is
    started (sometimes difficult with surgical
    specimens!)

13
What can the laboratory do to help the clinician?
  • Awareness of TB e.g. in the patient with
    recurrent sputum samples for chronic bronchitis
  • Rapid diagnosis of infection and resistance
  • Culture and sensitivities the clinician wants
    answers immediately if possible
  • PCR further opportunities for development
  • Gamma interferon based tests??
  • other

14
What samples? Depends on clinical scenario
  • Chest
  • Sputum if productive
  • Induced sputum
  • Bronchoscopic alveolar lavage (BAL)
  • Pleural biopsy
  • Pleural fluid
  • Other
  • E.g. Lymph node, aspiration of abscess,
    mesenteric biopsy, stool, bone marrow etc.
  • What about EMSU? - should be done selectively
    where it is likely to be helpful

15
Induced sputum
  • Hypertonic saline nebuliser in negative pressure
    room with HEPA filter and well trained
    physiotherapist
  • Study of 27 confirmed positive patients
  • 13 ve induced sputum only
  • 1 ve bronchoscopy only
  • 13 ve induced sputum and bronchoscopy
  • McWilliams T et al Thorax 2002 57 1010-1014

16
Audit of induced sputum in Department of
Infection in Sheffield
  • Criteria for procedure
  • Past history TB or contact with TB in last year
  • Respiratory symptoms of one or more of
  • Non-productive cough
  • Fever, Night sweats, weight loss
  • Haemoptysis
  • 114 procedures, 12 positive for TB
  • Cohort followed up for 12 months, no cases missed
  • - Bell et al. J Infection 2003 47 317-321

17
Clinical cases
  • Cases of
  • pulmonary infection
  • Non pulmonary infection
  • Examples of spectrum of disease produced by TB

18
Pulmonary and non pulmonary TB disease
Sheffield 2005
  • Equal numbers of patients with pulmonary and non
    pulmonary tuberculosis

19
Clinical presentation 1
  • 35 year old African lady with fever and dry cough
    for 3 weeks.
  • Mildly unwell
  • Night sweats
  • Weight loss 4 pounds
  • No history of contact with TB
  • CXR

20
Case 1 miliary tuberculosis
21
Pulmonary TB typically affects the upper zones of
the lung
22
Case 1
  • Investigation
  • FBC normal
  • ESR 53
  • U and E normal
  • LFT albumen 31
  • CRP 40
  • Induced sputum smear negative

23
Case 1
  • Progress
  • Clinical diagnosis of TB
  • 4 drug treatment
  • Clinical improvement
  • TB culture
  • positive at week 3
  • fully sensitive (week 5)
  • Modified anti TB drug regime in light of lab
    results

24
Case 1
  • What about HIV testing? who to test?
  • Strong association between HIV and TB
  • Universal testing or selective testing?
  • What about testing for vitamin D?
  • Vitamin D has role in activating macrophages to
    destroy mycobacteria
  • Vitamin D deficiency in ethnic populations in UK
    often low

25
Case 1
  • Cured after standard 6 months therapy

26
Clinical presentation 2
  • 28 year old African lady with backache for 6
    weeks
  • Diagnosed initially as non specific
  • Developed fever no obvious cause
  • ID opinion sought
  • Investigation with MRI scan

27
Clinical case 2
  • Diagnosis
  • Vertebral osteomyelitis with soft tissue mass
    impinging on the cord
  • Investigation
  • Biopsy and culture
  • Treatment
  • 4 anti TB drugs and antibiotic therapy

28
Clinical case 2
  • What will happen if diagnosis or treatment for TB
    spinal osteomyelitis is delayed?

29
What will happen if treatment delayed? gibbus
formation (acute angulation of spine with or
without neurological damage)
30
The physical appearance Potts disease of spine
- gibbus
31
Clinical case 2
  • Progress
  • Increasing back pain and neurological symptoms
    mild leg weakness
  • Repeat MRI changes similar
  • Treatment
  • Continue therapy
  • consider surgical decompression

32
Clinical case 2
  • Further progress
  • Weakness of legs
  • Neurosurgery and internal splinting
  • Other considerations - clinical
  • Has she got HIV?
  • Is her vitamin D level normal?
  • Other considerations - epidemiological
  • From where has she got infection?
  • To whom might she have given it?

33
  • TB may affect any tissue of the body including
  • Skin and soft tissue
  • Lymph nodes
  • Bones and joints
  • Intra abdominal structures including
  • peritoneum
  • Kidneys
  • Adrenal glands
  • Lymph nodes
  • Central nervous system
  • Tuberculoma
  • meningitis

34
  • Skin and soft tissue

35
25 male African. Expanding non painful lesion in
neck - Cervical lymph node TB progressing to
abscess (beware deep extension collar stud
abscess)
36
TB node in neck with deep extension
37
35 female African systemically well - hand and
foot lesions present for 6 months MTB grown on
biopsy by plastic surgeons (HIV neg)
38
  • Bony tuberculosis

39
Astute radiologist should enable the appropriate
further investigation
40
Often associated with delay in diagnosis any
chronic discharging lesion must be considered
possibly TB
41
  • Abdominal Tuberculosis

42
Renal tuberculosis (may have few or no symptoms)
leading to autonephrectomy
43
30 middle eastern asylum seeker - abdo pain,
fever, sweats CT scan - peritoneal TB confirmed
on biopsy may mimic malignancy
44
  • Intracranial TB

45
miliary TB on MRI scantuberclomas on CT scan
46
meningitis diagnosis usually made on clinical
grounds
  • Clinical
  • Acute or subacute
  • Prognosis related to severity of disease at onset
    of treatment
  • Commonly delay between presentation and diagnosis
  • Common in children
  • c100 cases per year in England
  • CSF
  • Cell count 50-500 (50 lymphs, 50 polys)
  • High protein
  • Low glucose
  • Micro often negative (PCR/culture important)

47
  • Treatment of TB

48
  • BTS guidelines 1999 Thorax 2000 55 210-218
  • NICE guidelines 2006
  • Sensitive TB 4 drugs for 2 months 2 drugs
    for 4 months
  • Resistant TB - 6 drugs for 24 months (second
    line drugs are not so effective)
  • Eng, Wales NI 2004, 6.8 Isoniazid resistant,
    1 MDR TB (R to Isoniazid and rifampicin)

49
Problems of TB therapy
  • Toxicity e.g. liver
  • Multiple therapy
  • Prolonged treatment
  • Drug interactions e.g. anti HIV drugs

50
Compliance
  • Treatment will not work if not taken
  • DOTS (Directly Observed Therapy) if
  • Likely poor compliance
  • MDRTB

51
Outcome
  • WHO target (1991)
  • detect 70 infectious cases of TB and cure at
    least 85 by 2005
  • Eng, Wales and NI
  • Probably detect 70 cases infectious TB
  • Cure rate uncertain
  • Among all TB patients with a known outcome the
    proportion of cases that have completed treatment
  • 79 in 2003
  • 78 in 2002
  • 79 in 2001 CDR 23 March 2006

52
Why failure?
  • Patient non compliance
  • Deliberate
  • Failure to understand e.g. language, culture
  • Social e.g. alcohol
  • Patient movement e.g. lost to follow up
  • Lack of medical/nursing support
  • others

53
public health - avoiding transmission
  • TB is statutorily notifiable disease
  • Multidisciplinary approach medical, TB nurses,
    CCDC etc.
  • Identify and manage possible sources of infection
    and contacts
  • Considerations
  • treat as OP where possible
  • multi occupancy housing, social deprivation
  • negative pressure rooms in hospitals (limited
    facility)
  • beware transmission in OP setting e.g. waiting
    area

54
New challenges in TB

55
Challenges in TB
  • Anti TNF therapy (Eg infliximab, etanercept)
  • May promote breakdown of granulomas and
    reactivation of TB
  • How to screen
  • Clinical history
  • CXR (? With induced sputum)
  • Skin testing
  • ?? Value of gamma interferon tests

56
Challenges in TB
  • What will be the place of Quantiferon and
    Elispot type tests in clinical practice?

57
  • Clinical need for new and better anti TB drugs

58
  • Objective - to lead to more effective shorter
    course regimen
  • Better pharmacokinetics
  • longer half life
  • better penetration to cavities
  • Better activity
  • kill TB in dormant phase
  • Active against resistant strains
  • Safer and easier
  • Lack of interaction with anti HIV therapy
  • Less toxic
  • Low cost

59
Will there be new affordable therapy for TB?
  • Global Alliance for TB Drug Development
  • TB development drug discovery research unit
  • Astra Zenica
  • Glaxo SmithKline
  • Novartis
  • WHO links with pharma
  • TB trials consortium (US CDC)

60
Will there be new affordable therapy for TB?
  • Moxifloxacin
  • TMC 207
  • OPC-67683
  • PA-824
  • LL3858

61
Summary
  • TB is a challenging disease for the clinician
  • Must have microbiology before starting treatment
    more rapid lab tests?
  • Need to encourage compliance
  • Need for multidisciplinary approach to diagnosis
    and management and control
  • Need shorter, better, cheap anti TB regimes
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