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HIV point of care testing

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Rationale for POCT HIV test of source in occupational exposure Can avoid empirical PEP Avoid side effects Expense of therapy Reassure employee Reduces duration of ... – PowerPoint PPT presentation

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Title: HIV point of care testing


1
HIV point of care testing
  • Noah Hoffman, June 2006

2
(No Transcript)
3
Time course of typical HIV infection
www.med.sc.edu85/lecture/hiv_time_course.jpg
4
HIV detection how soon after infection?
  • Window period the time between infection and
    seroconversion
  • Symptoms usually appear 2 weeks after infection
  • p24 reduces window period by about 6 days
  • Nucleic Acid detection reduces window period to
    about 11 days after infection
  • Serology
  • IgM detected an average of 5 days after onset of
    symptoms
  • IgG detected an average of 11 days after onset of
    symptoms
  • Almost all patients are seropositive by 3 mos
    after infection
  • Period of highest risk for infection is primary
    infection high viral load without symptoms or
    detectable antibodies

UpToDate Laboratory testing of donated blood,
Primary HIV-1 infection Diagnosis and treatment
AIDS Volume 14(15) 20 October 2000 pp 2333-2339
5
algorithm for laboratory testing of HIV infection
6
Motivation for point of care testing
  • Rapid TAT
  • Permits immediate decision support
  • Ensure follow-up for positive results
  • Provide immediate counseling
  • Available in resource-poor areas

7
Useful settings for rapid HIV testing
  • Labor and delivery
  • Occupational exposure
  • Emergency Department
  • Outreach for high-risk patients

8
Performance of rapid POC HIV tests
http//www.cdc.gov/hiv/rapid_testing/materials/Lab
orDeliveryRapidTesting.pdf
9
PPV of rapid POC HIV tests
http//www.cdc.gov/hiv/rapid_testing/materials/Lab
orDeliveryRapidTesting.pdf
10
Trinity Biotech Uni-Gold Recombigen test principle
  • Recombinant HIV proteins immobilized on a
    nitrocellulose strip and on colloidal gold
    beneath the test region of the strip
  • anti-HIV antibodies binds to antigens on the
    nitrocellulose and colloidal gold particles
  • the antibody-gold complex appears on the strip as
    a pink/red band

11
Uni-Gold Recombigen
  • CLIA-waived for finger stick, whole blood
    moderate complexity with serum, plasma
  • Store at room temperature
  • Screens for HIV-1
  • Results in 10 minutes

http//www.cdc.gov/hiv/rapid_testing/materials/USC
A_Branson.ppt
12
Add 1 drop specimen to well
http//www.cdc.gov/hiv/rapid_testing/materials/USC
A_Branson.ppt
13
Add 4 drops of wash solution
http//www.cdc.gov/hiv/rapid_testing/materials/USC
A_Branson.ppt
14
Positive
Negative
Read results in 10 -12 minutes
http//www.cdc.gov/hiv/rapid_testing/materials/USC
A_Branson.ppt
15
Regulation of POC HIV testing
  • CLIA waived
  • whole blood
  • venipuncture whole blood
  • CLIA moderate
  • serum
  • Requirements for testing under CLIA waiver
  • Sale is restricted to clinical laboratories (Any
    agency that has a CLIA Certificate of Waiver and
    performs the OraQuick test is considered a
    clinical laboratory.)
  • A quality assurance plan is in place
  • Staff have been trained to perform the test using
    manufacturer's instructions
  • Clients receive a Subject Information pamphlet
    before the test is given and receive appropriate
    information when results are provided

http//www.cdc.gov/hiv/rapid_testing/materials/rol
tCLIA.htm
16
Delaney, et al. Ability of Untrained Users to
Perform Rapid HIV Antibody Screening Tests.
Abstract, American Public Health Association
Annual Meeting, October 2002.
  • Study of OraQuick test
  • Health care workers with no lab experience
  • Incorrectly performed tests gave result of
    invald (so no incorrect result given to
    patient)

17
Outcomes of Counseling and One-Time Screening for
HIV Infection after 3 Years in 3 Hypothetical
Cohorts of 10 000 Asymptomatic Adolescents and
Adults
Chou, R. et. al. Ann Intern Med 200514355-73
18
Confirmation of positive rapid tests (OraQuick)
CDC guidelines
  • All preliminary 's must be followed up with
    either a Western blot or immunofluorescent assay
    (IFA) for confirmation.
  • Confirmatory testing can be done on blood
    (plasma, serum or dried blood spots) or oral
    fluid specimens. Urine testing should not be
    performed due to its lower sensitivity
  • With blood specimens, enzyme immunoassay (EIA)
    screening tests prior to the Western blot or IFA
    confirmatory test are optional. If an EIA is
    performed, even if it is non-reactive, the
    specimen must proceed to Western blot or IFA
    testing. For oral fluid testing, both EIA and
    Western blot testing should be performed to
    confirm results.

http//www.cdc.gov/hiv/rapid_testing/materials/qa-
guide.htm
19
Follow up testing for negative confirmatory result
  • Recommended to rule out specimen mixup or
    false-negative confirmatory test
  • For blood specimens, a confirmatory test should
    be repeated with a new specimen
  • For oral fluid specimens, a repeat confirmatory
    test with a blood specimen should be done, since
    the oral fluid test is less sensitive than the
    blood test.

20
Rapid HIV-1 Antibody Testing during Labor and
Delivery for Women of Unknown HIV Status
  • The CDC provides recommendations for rapid
    testing of mothers in labor with unknown HIV
    status
  • 40 of the mothers of the 280370 HIV-infected
    infants born in 2000 were not known to have HIV
    infection before delivery
  • When ARV prophylaxis is administered during
    labor or within the first 12 hours after birth,
    the risk of perinatal HIV transmission is reduced
    from 25 to 913
  • Diagnosis offers opportunity for close follow up
    and referral after delivery

http//www.cdc.gov/hiv/rapid_testing/rt-labordeli
very.htm
21
Key elements of CDC recommendations for rapid
perinatal HIV testing
  • Consider establishing standing orders (e.g.,
    provide routine rapid HIV testing if there is no
    documentation of prenatal HIV test results unless
    the woman declines
  • CDC recommends an opt-out approach, in which
    women are informed that HIV testing will be
    routinely done if her HIV status is unknown
    during labor and delivery but that she may
    decline testing
  • Ensure confidentiality
  • A positive (or reactive) result from a rapid HIV
    test is considered a preliminary positive and
    must be followed up with a confirmatory test

22
Approach to a positive rapid HIV test in labor
and delivery setting
  • Confirm result
  • Begin antiretroviral prophylaxis for mother and
    neonate
  • all ARV prophylaxis will be stopped if the
    confirmatory test result is negative
  • Management of labor
  • artificial rupture of membranes and invasive
    monitoring should be avoided
  • Episiotomy should be avoided if clinically
    appropriate.
  • There is no evidence that C-section reduces risk
    of MTCT in an uncomplicated pregnancy once
    membranes have ruptured C-section may be
    indicated before membrane rupture
  • postpone breastfeeding until the confirmatory
    results are available
  • Ensure follow up for mother and baby!

23
Experience with LD rapid HIV testing MIRIAD
study
  • Multicenter study of acceptance of HIV testing
    sensitivity, specificity, PPV TAT.
  • Ora-Quick test was evaluated
  • 7381 of 91707 women eligible
  • 84 consent rate
  • 34 positives (7/1000)
  • sens 100, spec 99.9, PPV 90 (76 for EIA)
  • TAT for blood collection to result 66 minutes
    (28 hours for EIA)

24
Occupational HIV exposure 1995-2004 (CDC data)
  • 28,010 occupational exposures to blood and body
    fluids
  • 1,350 (5.3) to HIV-positive sources
  • 15,301 (60.0) to HIV-negative sources
  • 8,859 (34.7) to sources of unknown HIV status
  • 58.4 of people exposed to known HIV source took
    PEP
  • Median time to initiation of therapy was 2 hours

MMWR 2005 54(RR09)1-17
25
Risk of HIV transmission by exposure type
Antiretroviral postexposure prophylaxis after
sexual, injection-drug use, or other
nonoccupational exposure to HIV in the United
States. MMWR. 2005, 541-20. PMID 15660015
26
Risk factors following occupational exposure to
HIV
  • Route of exposure
  • Percutaneous exposure to HIV-infected blood
    0.3 average risk
  • Mucous membrane exposure 0.09
  • Nonintact skin ? (probably lt MM)
  • Type/mechanism/circumstance of injury
  • Higher risk deep injury, visible blood on/in
    needle, hollow needle, intravenous/intraarterial
    procedure
  • Source of material
  • Patients with terminal disease (higher viral
    load, presence of more virulent stains?)

MMWR. 2005. Vol 54, No RR91
27
Treatment following occupational exposure to HIV
  • Less severe, eg solid needle or superficial
    injury.
  • More severe, eg large-bore hollow needle, deep
    puncture, visible blood on device, or needle used
    in patients artery or vein.

28
Rationale for POCT HIV test of source in
occupational exposure
  • Can avoid empirical PEP
  • Avoid side effects
  • Expense of therapy
  • Reassure employee
  • Reduces duration of uncertainty

29
References
  • Rapid HIV-1 Antibody Testing during Labor and
    Delivery for Women of Unknown HIV Status A
    Practical Guide and Model Protocol (CDC)
    http//www.cdc.gov/hiv/rapid_testing/rt-labordeli
    very.htm
  • Bulterys M, et al. Rapid HIV-1 testing during
    labor a multicenter study. JAMA. 2004,
    292219-23. PMID 15249571
  • Updated U.S. Public Health Service Guidelines for
    the Management of Occupational Exposures to HIV
    and Recommendations for Postexposure Prophylaxis
    MMWR. 2005. Vol 54, No RR91
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