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Rafael Laniado-Laborin MD, MPH, FCCP

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Title: Rafael Laniado-Laborin MD, MPH, FCCP


1
Tuberculosis and HIV/AIDS
  • Rafael Laniado-Laborin MD, MPH, FCCP
  • Universidad Autónoma de Baja California

2
Background
  • The World Health Organization (WHO) estimates
    that approximately one third of the total
    population of the world harbors tubercle bacilli
    in a latent form
  • A new infection occurs every second

Int J Tuberc Lung Dis 2003 7S328
3
Background
  • The WHO also estimates that each year more than 9
    million new cases of tuberculosis occur and
    approximately 2 million persons die from the
    disease
  • One case can infect from 10 to 15 people

IUTLD-NAR Meeting 2006
4
How frequent is the co-infection?
5
TB cases in persons with HIV co-infection, USA
1993-2003 (25-44 years old)
CDC Website, Sep 2006
6
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7
TB Border states USA Mexico
8.3
CA
2.2
4.7
NM
AZ
7.5
BC
TX
25.3
41.5
18.7
SON
11.7
CHI
COH
NL
31.1
21.9
TAM
SOURCE DGE MEXICO / CDC EUA
8
Bacteriology
  • MTB belongs to the genus Mycobaterium
  • Mycobacterium tuberculosis complex
  • M. tuberculosis
  • M. bovis
  • M. africanum
  • M. microti
  • M. canetti

9
Nontuberculous mycobacterium (MOTT)
  • In the US up 30 of the isolates are NTM (rate
    1.8 per 100,000 h.
  • The most common NTM are
  • Mycobacterium avium complex (60 )
  • Mycobacterium fortuitum (20 )
  • Mycobacterium kansasii (10 )

10
Pathogenesis
  • Tuberculosis is spread from person to person
    through the air by droplet nuclei, particles lt5
    mm in diameter that contain M. tuberculosis
    complex

11
Pathogenesis
  • 4 factors determine the risk of infection
  • the number of organisms being expelled into the
    air
  • the concentration of organisms in the air
    (volume of the space and its ventilation)
  • the length of time an exposed person breathes the
    contaminated air
  • the immune status of the exposed individual

12
  • HIV-infected persons and others with impaired
    cell-mediated immunity are thought to be more
    likely to become infected with M. tuberculosis
    after exposure than persons with normal immunity

13
  • Also, HIV-infected persons and others with
    impaired cell-mediated immunity are much more
    likely to develop disease if they are infected

14
Pathogenesis
  • Inhalation and deposition in the lungs of the
    tubercle bacillus leads to one of four possible
    outcomes
  • immediate clearance of the organism
  • chronic or latent infection
  • rapidly progressive disease (or primary disease)
  • active disease months to years after the
    infection (reactivation disease)

15
Pathogenesis
  • Only 5 to 10 percent of patients with no
    underlying medical problems who become infected
    develop active disease in their lifetime
  • The risk increases markedly in patients with AIDS

16
Pathogenesis
  • Once they are inhaled, the bacilli will reach
    the distal bronchioles and alveoli
  • Inside the alveolar macrophages M. tuberculosis
    will multiply slowly (once every 24-32 hours) and
    kill the cell

17
Pathogenesis
  • The infected macrophages produce cytokines that
    attract other phagocytic cells which eventually
    form a nodular granulomatous structure called the
    tubercle

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19
Pathogenesis
  • If the bacterial replication is not controlled,
    the tubercle enlarges and the bacilli enter the
    local draining lymph nodes
  • The lesion produced by the expansion of the
    tubercle into the lung parenchyma and lymph node
    involvement is called the Ghon complex

20
Primary complex (Gohns)
21
Pathogenesis
  • Failure by the host to mount an effective CMI
    response and tissue repair leads to progressive
    destruction of the lung
  • If the bacterial growth continues to remain
    unchecked, the bacilli may spread hematogenously
    to produce disseminated TB

22
  • HIV-infected persons, especially those with low
    CD4 cell counts, develop tuberculosis disease
    rapidly after becoming infected with M.
    tuberculosis
  • Up to 50 percent of such persons may do so in the
    first two years after infection with M.
    tuberculosis

23
  • Conversely, an individual who has a prior latent
    infection with M. tuberculosis (not treated) and
    then acquires HIV infection will develop
    tuberculosis disease at an approximate rate of 5
    to 10 percent per year

24
  • Voluntary HIV counseling and testing is
    recommended for all patients with TB and should
    be considered the standard of care

Am J Respir Crit Care Med 2005 1721169
25
  • Physicians who provide primary care to persons
    with HIV infection or populations at increased
    risk for HIV infection should maintain a high
    index of suspicion for TB
  • Every patient in whom HIV infection has been
    newly diagnosed should be assessed for the
    presence of TB or LTBI

Am J Respir Crit Care Med 2005 1721169
26
  • The risk depends, however, on the degree of
    immunosuppressionthe risk of a patient with AIDS
    developing tuberculosis is 170 times higher than
    a non immunosuppressed person

27
Reactivation disease
  • Reactivation TB results when the persistent
    bacteria in a host suddenly proliferate
  • While immunosuppression is clearly associated
    with reactivation TB, it is not clear what host
    factors specifically maintain the infection in a
    latent state for many years and what triggers the
    latent infection to become overt

28
Reactivation disease
  • Immunosuppressive conditions associated with
    reactivation TB include
  • HIV infection and AIDS
  • end-stage renal disease
  • diabetes mellitus
  • malignant lymphoma
  • corticosteroid use
  • old age

29
Clinical manifestations
30
Clinical manifestations
  • In immunocompetent individuals, 85 of the cases
    are exclusively pulmonary, and the rest have
    extrapulmonary manifestations
  • This distribution is modified in HIV patients
  • 38 exclusively pulmonary
  • 30 extrapulmonary
  • 32 pulmonary extrapulmonary

31
Systemic manifestations
  • Fever (37-80)
  • Weight loss
  • Night sweats
  • Loss of appetite
  • Malaise

32
Pulmonary TB
  • Cough is the most common symptom
  • Sputum, hemoptysis
  • Pleuritic pain
  • Dyspnea

33
Radiographic manifestations
34
Radiographic findings
  • PTB is almost associated to radiographic
    abnormalities
  • Patients with HIV and PTB might have a normal
    chest x-ray

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37
Radiographic findings
  • In patients with HIV infection, the nature of the
    x-ray findings depends to a certain extent on the
    degree of immunocompromise produced by the HIV
    infection
  • TB that occurs relatively early in the course of
    HIV infection tends to have the typical x-ray
    findings of the immunocompetent patient

38
Radiographic findings
  • With more advanced HIV disease the radiographic
    findings become more "atypical" cavitations is
    uncommon, and lower lung zone or diffuse
    infiltrates and intrathoracic adenopathy are
    frequent

39
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40
Disseminated tuberculosis
41
Disseminated tuberculosis
  • The term "miliary" is derived from the visual
    similarity of some disseminated lesions to millet
    seeds
  • Grossly, these lesions are 1- to 2-mm yellowish
    nodules that, histologically, are granulomas
  • Thus disseminated tuberculosis is sometimes
    called "miliary" tuberculosis

42
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45
Disseminated TB
  • Because of the multisystem involvement in
    disseminated tuberculosis, the clinical
    manifestations are protean
  • The presenting symptoms and signs are generally
    nonspecific and are dominated by systemic
    effects, particularly fever, weight loss, night
    sweats, anorexia, and weakness
  • Other symptoms depend on the relative severity of
    disease in the organs involved

46
Disseminated TB
47
Laboratory diagnosis
48
Diagnosis
  • Microscopy
  • this is principally applied to sputum but other
    specimens include bronchoalveolar lavage fluid,
    gastric washings, laryngeal swabs, cerebrospinal
    fluid, pleural, pericardial and peritoneal
    effusions, fine needle lymph node aspirates, bone
    marrow aspirates, and tissue biopsies.

49
Diagnosis
  • A wide range of acid-fast smear positivity has
    been reported (31 to 81 percent), but most
    studies find a 50 to 60 percent yield
  • The yield is substantially higher (85 to 100
    percent) on sputum culture

50
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51
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52
Mycobacteria cultures
53
Diagnosis
  • In patients infected with HIV, a positive smear
    for acid-fast bacilli (AFB) is very specific for
    Mycobacterium tuberculosis (MTB), even in a
    setting with a high incidence of Mycobacterium
    avium complex (MAC)

54
Diagnosis
  • At San Francisco General Hospital, for example,
    248 of 271 (92 percent) expectorated sputum
    samples which were positive for AFB grew MTB on
    culture
  • This value is comparable to that found in
    HIV-negative patients.

55
Diagnosis
  • Urine cultures Although genitourinary TB rarely
    occurs in the absence of other sites of
    extrapulmonary disease, it is frequently involved
    in disseminated TB, even in the absence of pyuria
  • In one series, for example, 77 HIV-infected
    patients with extrapulmonary TB whose urine was
    sent for culture grew MTB

56
Diagnosis
  • Invasive testing should be performed when
    noninvasive studies yield no immediate answer and
    the wait for culture results would be detrimental
    to the patient
  • Bronchoscopy is a sensitive technique for
    diagnosing TB
  • An immediate diagnosis can be made from AFB
    smears in about one-half of patients, and the
    sensitivity of cultures approaches 100 percent

57
Diagnosis
  • The central nervous system is frequently involved
    in disseminated TB
  • Given the number of opportunistic infections
    affecting the central nervous system in AIDS,
    there should be a low threshold for collecting
    CSF

58
Diagnosis
  • In a patient with suspected miliary disease and a
    negative sputum examination, bone marrow biopsy
    as well as blood cultures should be performed
  • Blood cultures are positive in 49 percent of
    patients with disseminated disease and CD4 counts
    less than 100/mm3

59
Molecular methods
  • The application of nucleic acid (DNA and RNA)
    amplification techniquesthe polymerase chain
    reaction (PCR) and the ligase chain reaction
    (LCR)is the subject of intense research activity
  • As a result, a number of rapid, sensitive, and
    specific test kits are commercially available

60
Diagnosis of LTBI
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65
TST is considered as positive if gt 5 mm
  • Contacts of an active TB case
  • Subjects with a chest x-ray anomalies (fibrosis)
    suggestive of old (untreated) TB
  • Immunosuppression (including HIV)
  • Drug induced immunosuppression ( gt15 mg/day of
    prednisone)

66
  • Patients with 5 mm or more of induration be
    considered to have a positive test and should
    receive, in addition to chest x-rays, a clinical
    evaluation to rule out TB

Am J Respir Crit Care Med 2005 1721169
67
IFN-? assays
  • Patients T cells release IFN-? when exposed to
    mycobacterial antigens
  • The genes encoding for two antigenic targets,
    ESAT6 and CFP10 are absent in the BCG vaccine
    strain and most environmental mycobacteria

Eur Respir J 2006 281-3
68
IFN-? assays
  • There are two different assay formats
  • ELISA detection after blood is incubated in a
    tube with ESAT6/CPF10 antigens (Quantiferon-Gold)
  • ELISA immunospot technique (T-Spot.TB)
  • Advantage one blood sample no repeated visits
    as in TST
  • Disadvantage cost

Eur Respir J 2006 281-3
69
IFN-? assays
  • These assays are not as sensitive for diagnosing
    active TB since IFN-? responses decline as TB
    develops

Eur Respir J 2006 281-3
70
75 individuals with active TB and control group
(HS students with ?risk of
infection)
Active TB Immuno? Controls (specificity)
TST 72 37 82
T-Spot.TB 96 100 86
QF-Gold 77 75 92
Eur Respir J 2006 2824-30
71
Guidelines for using the QF-Gold testCDC
2005/54(RR15)49-55
  • FDA approved
  • Diagnosing infection with M. tuberculosis
    including both TB disease and LTBI
  • QF-G can be used in all circumstances in which
    the TST is used

72
Guidelines for using the QF-Gold testCDC
2005/54(RR15)49-55
  • QF-G can be used in place of (and not in addition
    to) TST
  • A positive QF-G result should prompt the same
    public health and medical interventions as a
    positive TST result

73
Treatment
74
Treatment of HIV related tuberculosis
  • The standard WHO recommended antituberculosis
    regimen is a six month course of RIF and INH,
    PZA, together with ETH (or SM) during the first
    two months of treatment
  • Supplementation with daily pyridoxine (vitamin
    B6) to prevent isoniazid induced neuropathy is
    now routine

75
  • There is little or no difference in relapse rate
    between HIV infected and uninfected patients when
    RIF based short course treatment is used
  • Thus, in the absence of drug resistance, the
    standard short course just described is
    recommended

76
Antituberculous drug interactions
  • A number of interactions between antituberculosis
    agents and other drugs have been described
  • Most interactions are associated with RIF due to
    its ability to induce cytochrome CYP450 enzymes
    in the liver which affect the metabolism of many
    other drugs

77
Antituberculous drug interactions
  • The current recommendation is to replace RIF by
    rifabutin, a much less powerful inducer of
    cytochrome enzymes, and to start or continue with
    the antiretroviral drugs

78
Management recommendations for the use of ARV
antituberculosis drugs
  • Frequent communication between TB and HIV care
    providers
  • Adjust dose of rifabutin as needed
  • Use rifampin with efavirenz or ritonavir (gt400 mg
    BID)

Am J Respir Crit Care Med 2001 1647-12
79
Antituberculous drug interactions
  • Even if rifabutin is substituted for RIF, care
    should be exercised in the use of the protease
    inhibitor saquinavir and the non-nucleoside
    reverse transcriptase inhibitors as rifabutin
    decreases their levels, with the risk of
    selection of drug resistant viruses

80
Immune reconstitution syndrome
  • It appears usually after two weeks of ARV
    treatment
  • Most of the patients have far advance AIDS
  • median CD4 35 cells/mm3
  • median viral load 581,694 copies/mL

81
Paradoxical reactions (immune reconstitution
syndrome)
  • These manifest as fever, enlargement of affected
    lymph nodes, and a worsening of the radiological
    appearance

82
Paradoxical reactions (immune reconstitution
syndrome)
  • These reactions are not indicative of treatment
    failure and usually subside spontaneously
  • Treatment should not be modified but short
    courses of steroids may be required for severe
    paradoxical reactions.

83
When should ART be started?
  • ARVs should be given to those with WHO Stage IV
    disease, including individuals with
    extra-pulmonary TB, regardless of CD4
    T-cell count

Int J Tuberc Lung Dis 2005 9946
84
When should ART be started?
  • Those with Stage III conditions, including
    individuals with pulmonary TB (PTB), should have
    CD4 T-cell counts taken into consideration
    treatment is recommended when counts are lt350
    cells/mm3
  • Those with Stage I and II disease should only
    receive ART for CD41 T-cell counts lt200 cells/mm3

Int J Tuberc Lung Dis 2005 9946
85
Treatment of LTBI
86
Incidence of active TB in PPD positive subjects
according to risk factor
Risk factor TB cases /1000 patient-years
TB infectionlt1 year 12.9
TB infection 1-7 years 1.6
HIV infection 35-162
IV drug use (HIV negative) 10
x-ray abnormality (old TB) 2-13.6
Weight loss gt15 2.6
Weight loss 10-14 2.0
87
Treatment of LTBI
  • It has been used for more than 30 years
  • Evidence is classified as
  • A preferred treatment
  • B acceptable alternative
  • C offer if A and B are not an option
  • I randomized clinical trial
  • II clinical trail not randomized
  • III experts opinion

88
  • Targeted testing and treatment for LTBI are
    strongly recommended at the time the diagnosis of
    HIV infection is established (AII)

Am J Respir Crit Care Med 2005 1721169
89
  • Persons with known or suspected HIV infection who
    have contact with a patient with infectious
    pulmonary TB should be offered a full course of
    treatment for LTBI regardless of the initial
    result of tuberculin skin testing once active TB
    has been ruled out (AII)

Am J Respir Crit Care Med 2005 1721169
90
Prophylaxis against TB in co-infected persons
  • In view of the very high risk of a co-infected
    person developing active TB, and the adverse
    effect of this disease on the immune status and
    survival of the patient, there is a very good
    theoretical case for provision of prophylactic
    treatment for those at risk

91
Treatment of LTBI
  • In the initial studies, a 12 month course of
    isoniazid was found to lower the incidence of
    tuberculosis in co-infected persons
  • Subsequently, shorter combination regimens have
    also been shown to be effective

92
Drugs Duration (months) Interval HIV- HIV
INH 9 Daily Bi-weekly A(II) B(II) A(II) B(II)
INH 6 Daily Bi-weekly B(I) B(II) C(I) C(I)
RIF-PZA 2 2-3 Daily Bi-weekly B(II) C(II) A(I) C(I)
RIF 4 Daily B(II) B(II)
93
  • An HIV-infected patient who is severely
    immunocompromised and whose initial tuberculin
    skin test result is negative should be retested
    after the initiation of antiretroviral therapy
    and immune reconstitution, when CD4 cell counts
    are greater than 200 cells/?l (AII)

Am J Respir Crit Care Med 2005 1721169
94
  • BCG VACCINATION

95
Is BCG effective?
  • Results of randomized controlled trials (RCT) and
    case control studies (CCS) showed the protective
    efficacy against tuberculosis as uncertain and
    unpredictable, as protective efficacy varied from
    0 to 80

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97
BCG a meta-analysis
  • Meta-analysis of over 1,200 articles from
    international publications
  • Only 14 prospective trials and 12 case-control
    studies met the selection criteria

JAMA 1994 271698-702
98
BCG a meta-analysis
  • Combining data from the trials the RR for TB
    among those vaccinated with BCG was 0.49 (95CI,
    0.34 to 0.70) protective effect 51
  • Combining data from the case-control studies, the
    OR for BCG vaccination against TB was 0.50
    (95CI 0.39 to 0.64)

JAMA 1994 271698-702
99
Immunization of children at risk of infection
with HIV
  • The available data is not adequate to permit
    definitive conclusions about the effectiveness of
    BCG vaccine to protect HIV-infected children or
    adults against tuberculosis

Bull World Health Org 20038161
100
BCG vaccination
  • There is a risk that vaccination with Bacille
    Calmette-Guérin (BCG), a living attenuated
    vaccine, will cause infectious complications in
    HIV positive persons
  • There is a small increase in the incidence of
    adverse effects of BCG in the children of HIV
    infected women, but most such effects are mild

101
  • A consensus view currently exists, however, that
    BCG should not be given to infants with active
    HIV disease and that the vaccine is
    contraindicated in older asymptomatic children
    who are found to be HIV positive

102
Adverse events associated with BCG vaccination in
children infected with HIV
Dissemination 0-31
Lymphadenitis 0-24
Bull World Health Org 20038161
103
Adverse events associated with BCG vaccination in
children infected with HIV
  • More than 28 cases of disseminated BCG infection
    have been reported in HIV-infected children and
    adults
  • Progressive immune suppression can lead to the
    reactivation of latent BCG organisms, causing
    regional or disseminated disease

Bull World Health Org 20038161
104
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