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Tuberculosis in the United States, 2004

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Tuberculosis in the United States, 2004 Thomas R. Navin, MD CDC March 2005 TB Presentation Overview How we count TB cases in the U.S. Descriptive epi Analytic epi New ... – PowerPoint PPT presentation

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Title: Tuberculosis in the United States, 2004


1
Tuberculosis in the United States, 2004
  • Thomas R. Navin, MD
  • CDC
  • March 2005

2
TB Presentation Overview
  • How we count TB cases in the U.S.
  • Descriptive epi
  • Analytic epi
  • New items on the horizon
  • Genotyping
  • New diagnostic tests
  • New drugs

3
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4
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5
TB Case Reports, Missouri, 1994-2004
6
TB Case Rates, Missouri and United States,
1994-2004
Rate per 100,000
7
TB Case Rates, Log Scale
Rate per 100,000
8
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9
Percent Foreign-born TB Cases, United States,
2004
D.C.
57 66
25
26 - 40
67
Percent foreign-born cases over total cases
41 - 56 (foreign-born for U.S. 53.7)
10
TB Case Rates by Race/Ethnicity United States,
1993-2003
Cases per 100,000
Cases per 100,000.All races are non-Hispanic.
In 2003, Asian/Pacific Islander category includes
persons who reported race as Asian only and/or
Native Hawaiian or Other Pacific Islander only.
11
Primary MDR TBUnited States, 1993-2003
12
Primary MDR TB inU.S.-born vs. Foreign-born
Persons, United States, 1993-2003
Resistant
Note Based on initial isolates from persons with
no prior history of TB. MDR TB defined as
resistance to at least isoniazid and rifampin.
13
Estimated HIV Coinfection in Persons Reported
with TB, United States,1993-2002
Coinfection
Note Minimum estimates based on reported
HIV-positive status among all TB cases in the
age group.
14
Characteristics of TB Cases, 2004
Missouri U.S. U.S.
Total cases 131 100.0 100.0
U.S.-born 91 69.5 45.7
Foreign-born 35 26.7 53.1
Marginalized 21 16.0 18.3
Black 48 36.6 27.6
Hispanic 13 9.9 28.7
15
Program Indicators Completion of therapy, 2002
Percentage completing treatment within 1 year
Missouri 84.4
Region 68.8
Rest of U.S. 69.7
16
Program Indicators DOT, 2002
Percentage Receiving DOT
Missouri 87.6
Region 71.0
Rest of U.S. 70.9
DOT or DOTSA
17
Preventable TB Case Analysis
  • Nearly half of Missouris TB cases are
    preventable.
  • The majority of preventable cases (85) involved
    a missed opportunity to screen patients with risk
    factors for TB.

18
Recommendations
  • Physicians in Missouri must remain aware of risk
    factors for TB and test at-risk asymptomatic
    persons
  • - contacts of infectious TB patients
  • - persons with medical risk-factors for TB

19
Universal Genotyping of M. tuberculosis
  • In 2004 CDC established the capacity to conduct
    universal TB genotyping. One isolate from every
    patient with TB can now be genotyped in real
    time.

20
Value of Genotyping
  • Identify and prevent recent transmission
  • Enhance contact investigations
  • Identify nontraditional settings of transmission
  • Facilitate identification of outbreaks
  • Improve clinical management
  • More readily identify false-positive cultures
  • Help distinguish between relapse and reinfection

21
CDC Genotyping Program Laboratory Algorithm
  • Two tiered testing to maximize discriminatory
    power
  • PCR
  • MIRU Variable number tandem
    repeats of

  • mycobacterial interspersed repetitive units
  • Spoligotyping Spacer oligonucleotide
  • IS6110-based RFLP
  • Done only for isolates that match by both PCR
    tests
  • When TB programs request it

22
Spoligotyping
  • PCR probes at 43 different sites

1 2 3 4 5 6 7 8 9 10 . . . . . . . . . . . . .
20 . . . . . . . . . . . . 30 . . . . . . . . . .
. . 40 . . . . 43
23
Spoligotyping
  • Does the probe recombine (hybridize) with
    genetic material at that site?
  • Assign 1 or 0 to each of the 43 probes

No 0
Yes 1
24
Spoligotyping
  • 111-111-111-111-111-111-100-111-111-111-110-000-
    111-111-1

25
Spoligotyping
  • Each triplet gets assigned an octal code
  • Spoligotype then reported as 15 digits
  • 777777477760771

1 2 3 4 5 6 7 8 9 10 . . . . . . . . . . . . .
20 . . . . . . . . . . . . 30 . . . . . . . . . .
. . 40 . . . . 43
111 7
000 0
100 4
110 6
7 7 7 7 7 7 7 7
7 7
Always 1 or 0 for last probe
26
MIRU Mycobacterial
Interspersed Repetitive Units
  • Also uses PCR technologybut on a different part
    of the DNA
  • Looks at 12 different loci and counts Variable
    Number Tandem Repeats (VNTR)

27
MIRU
Sample Printout
Locus 6 3 repeats
Locus 4 3 repeats
CEQ 8000 Automated Sequencer
Locus 7 1 repeat
28
MIRU
  • Looks at 12 different loci and counts VNTR
  • MIRU-VNTR pattern is then reported as a 12-digit
    number
  • Example 123323153323
  • means there are
  • 3 repeats at Locus 6

29
Reading Lab Report
  • Look at spoligotype and MIRU pattern (i.e., the
    PCR tests) is the first step
  • If dont match any other isolate, then not part
    of a cluster, no further testing needed
  • If match another isolates PCR results, may
    indicate recent transmission

30
When To Ask For RFLP?
  • To decide if isolates with matching spoligo and
    MIRU are truly clusteredwhen you need additional
    evidence for or against match
  • Not necessarily needed
  • An unusual PCR cluster is likely a true
    cluster
  • If it is obvious that the persons with matching
    isolates transmitted TB among each other

31
RFLP
  • Third method
  • Less automated, requires more lab resources
  • Experienced laboratorian must eyeball
  • Each genotyping lab will assign unique number to
    each distinct RFLP in its database
  • The PCR tests use standardized coding
  • But the RFLP label in itself has no meaning
    outside the lab which assigned it

32
RFLP
  • Lab assigns unique number or label to each RFLP
    in its database
  • RFLP designation arbitrary and does not
    correspond to genetic make-up

Ex 051 052 051
33
Presence of Any Epidemiologic Links Discovered
during Contact/Cluster Investigations of 555
Cases in Intrasite Genotyping Clusters (NTGSN)
34
Interferon-gamma Assays
  • QuantiFERON Gold
  • T Spot TB assay

35
Interferon-gamma Assays
  • QuantiFERON Gold now FDA approved
  • Measures IFN release from T cells
  • Based on M. tuberculosis specific antigens
  • ESAT6 and CFP10
  • Should not give false-positive result due to
  • BCG vaccination
  • Nontuberculous mycobacteria
  • CDC working on publishing guidelines for use

36
Interferon-gamma Assays
  • T Spot TB assay
  • Enzyme-linked immunospot assay
  • Counts number of T cells producing IFN
  • Based on ESAT6 and CFP10
  • Not yet FDA approved (available in Europe)

37
Treatment regimens for tuberculosisNew drug
candidates
  • Andrew Vernon, MD, MHS
  • Chief, Clinical and Health Systems Research
    Branch
  • Division of TB Elimination
  • March 2005

with thanks to Rick OBrien
38
2004 Distribution of TB Trials Consortium
Clinical Sites
Barcelona
Kampala
28 clinical sites worldwide CDC
Administrative, Statistical, and Data Management
Center
Rio de Janeiro
Durban
39
New drugs
  • Moxifloxacin
  • Ethambutol congeners (SQ-109)
  • Diarylquinolines
  • Nitroimidazole (PA-824)

40
Fluoroquinolones
  • No cross-resistance with other TB drugs
  • Commonly used for MDR TB
  • Role in therapy of drug susceptible TB uncertain

41
Relative TB activity of Fluoroquinolones
HIGHEST Gatifloxacin, Moxifloxacin,
Sparfloxacin NEXT Levofloxacin LOWER
Ciprofloxacin , Ofloxacin
42
Features of Quinolones and TB Therapy
Drug Serum Peak Half life TB
MIC Ciprofloxacin 750 2.3 4 2.0 Ofloxacin
400 4.6 7 2.0 Levofloxacin 500 6.0
7 1.0 Sparfloxacin 400 1.3
20 0.5 Gatifloxacin 400 4.4
7 0.5 Moxifloxacin 400 4.5 12 0.5
43
Activity of Moxi in Combination Therapy
2/5 mice had 1 cfu each
2.5 logs
6/6 mice culture pos.
3/6 mice culture pos.
44
Clinical Trails of Moxifloxacin
  • Multiple studies substituting moxi for ethambutol
  • CDC plans phase II trial substituted moxi for INH
    (MRZE) vs. the standard control regimen (HRZE)
  • Will measure sputum-culture conversion
  • If successful, future plan to move clinical
    trials of Moxi in very short regimens (lt6 months)

45
Congeners of Ethambutol
  • Targeting the enzymes involved in long chain
    fatty acid metabolism unique to mycobacteria
  • Based on computerized screening of possible
    compounds for predicted activity based on organic
    structure (Dr. Cliff Barry and colleagues
    NIAID)
  • Current lead compound SQ-109 moving into animal
    and human trials soon (Sequella Inc.)

46
Diarylquinolines (DARQ)(lead compound R207910)
47
Nitroimidazoles
  • Potent bactericidal antitubercular compound
    series
  • Narrow spectrum of activity (TB specific)
  • Promising efficacy comparable to INH in animal
    models
  • Active on non-replicating (latent?) TB
  • Leading candidate PA-824

48
PA-824 development
  • Acquired by Global Alliance for TB Drug
    Development
  • Currently being developed in partnership with
    Chiron
  • Animal efficacy studies promising
  • Animal and human toxicology studies to begin soon

49
What are the prospects for more new drugs soon?
  • Moxifloxacin in multiple clinical trials
  • Ethambutol congeners (SQ-109) moving to
    clinical phase
  • Diarylquinolines (DARQ) moving to clinical
    phase
  • Nitroimidazole (PA-824) in pre-clinical phase

50
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51
Case of the Week An 18-year-old man with no
clinically significant medical history presented
with a 6-month history of an increasing mass on
the left side of his back
52
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53
Overview of National TB Surveillance System
  • Data reported from 59 reporting areas
  • 50 states
  • D.C. and New York City
  • Puerto Rico
  • 6 jurisdictions in Pacific and Caribbean

54
U.S. TB Case Definition
  • Incident cases, active disease
  • Three alternatives
  • 1. Bacteriological confirmation (81)
  • 80 culture confirmed
  • 2. Clinical evidence (12)
  • 3. provider diagnosis ( 7)

55
TB MorbidityUnited States, 1999-2003
Year Cases Rate
2000 16,377 5.8 2001 15,989
5.6 2002 15,075 5.2 2003 14,874
5.1 2004 14,511 4.9
Cases per 100,000
56
TB Case Rates by Age Group and Sex, United
States, 2003
Cases per 100,000

Cases per 100,000.
57
Cohort Effect and TB Mortality Rates,
Massachusetts
1880 data
Cohort of 1880
Frost, Amer J Hyg, 1939
58
TBI Risk Factors - US-born population
Factor Adjusted Odds Ratio 95 CI
Race-Ethnicity    
White Non-Hispanic 1.0  
Black Non-Hispanic 7.5 3.6- 15.3
Mexican-American 5.2 2.5- 10.5
Other 2.6 0.2- 30.3
Socio-Economic Status    
Poverty Income Ratio gt 1 1.0  
Poverty Income ratio lt 1 1.9 1.0-  3.8
Sex    
Female 1.0  
Male 1.9 1.1- 3.1
Age Group    
1-14 years 1.0  
15-24 years 2.2 0.2- 30.9
25-44 years 6.0 1.2- 29.2
45-64 years 21.4 4.7- 97.0
65 years 34.3 6.0- 196.2
59
TBI Risk Factors Foreign-born population
Factor Adjusted Odds Ratio 95 CI
Race-Ethnicity    
White Non-Hispanic 1.0  
Black Non-Hispanic 1.0 0.4- 2.3
Mexican-American 0.9 0.4- 2.1
Other 1.0 0.4-2.5
Socio-Economic Status    
Poverty Income Ratio gt 1 1.0  
Poverty Income ratio lt 1 1.7 0.7-4.0
Sex    
Female 1.0  
Male 2.0 1.3-3.0
Age Group    
1-14 years 1.0  
15-24 years 1.0 0.3- 4.9
25-44 years 2.0 0.9- 4.7
45-64 years 3.0 1.2- 7.6
65 years 1.0 0.3-3.0
60
Relative Risk of TB Each Year After Initial
Infection1
1. Sutherland I. KNCV 1968
61
TB Outbreaks Grow Slowly
62
Case-Patients by Date of Diagnosis Oklahoma,
2001-2002 (N35)
Culture confirmed
Clinical Case
Index
2001
2002
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