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Diagnostic Tests for Influenza: the Tortoise and the Hare

Diagnostic Tests for Influenza: the Tortoise and the Hare. Arthur E. Crist, Jr., Ph.D. Director, Clinical Microbiology Ph. (717) 851-2393 E-mail: acrist@wellspan.org. Influenza Virus - Schematic. Conventional Cell Culture.

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Diagnostic Tests for Influenza: the Tortoise and the Hare

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  1. Diagnostic Tests for Influenza: the Tortoise and the Hare Arthur E. Crist, Jr., Ph.D. Director, Clinical Microbiology Ph. (717) 851-2393 E-mail: acrist@wellspan.org

  2. Influenza Virus - Schematic

  3. Conventional Cell Culture • Inoculation of specimens into cell culture: Madin-Darby canine kidney cell line (MDCK), primary rhesus monkey kidney cells (RMK), Vero cells, MRC-5 human diploid embryonic lung fibroblasts • If CPE, hemadsorption (HAD) with 0.5% suspension guinea pig red blood cells followed by DFA if positive • In the absence of CPE, “blind” (HAD) at days 2 and 7 followed by FA if positive

  4. Cell Culture

  5. Will cell culture replace fertilized eggs?

  6. Cell Culture - CPE Uninfected Infected

  7. Hemadsorption

  8. Hemadsorption +DFA

  9. Shell Vial Cell Culture • The use of shell vials for more rapid isolation and identification of Influenza • MDCK, RMK, mink lung cells (Mv1Lu) • R-Mix: Mv1Lu and A549 cells • Centrifugation • shell vials inoculated, incubated, and “blind” stained at day 1 and 5 for Influenza A and B

  10. Fong, C.K.Y., et. al. 2000. J. Clin. Microbiolo. 38: 4660-4662

  11. Huang, V.T., et al. 2000. J. Clin. Microbiol. 38: 422-423

  12. Performance of RT-PCR, Shell Vial, and Tube Culture for Influenza Zitterkopf, N.L., et. al. 2006. J. Clin. Microbiol. 44: 3366-3367

  13. Comparison of Culture, Serology and PCR Diagnostic Tests Concordance of positive results with three test methods Serology (61%) 41 11 116 418 (43%) 8 42 97 Culture (55%) RT-PCR (70%)

  14. Direct and Indirect FA Tests:Direct Specimen Testing or Culture Confirmation

  15. Bartels/Intracel • Monoclonal Antibodies • Indirect Procedure • 1o Antibody - 30 min • Conjugate - 30 min • Approved for culture confirmation and direct specimen detection

  16. Chemicon • Light Diagnostics • Monoclonal Antibodies • Direct - 30 min • Approved for culture confirmation and direct specimen detection

  17. Chemicon • SimulFluorTM • Dual color fluorescence: Flu A and Flu B detection in one well • Direct - 30 min • Approved for culture confirmation and direct specimen detection

  18. DAKO • ImagenTM • Monoclonal Antibodies • Direct Procedure • Conjugated Ab - 15 min • Approved for culture confirmation and direct specimen detection Flu A Flu B

  19. Diagnostic Products • Monoclonal Antibodies • Direct Procedure • 15 min - Package insert • 30 min works better • Approved for direct specimen and culture confirmation testing

  20. FA - Advantages • Relatively inexpensive • Amenable to batch testing • Rapid (1-2 hrs) • Able to assess specimen quality

  21. FA - Disadvantages • Subjective read • High complexity test • Fluorescent microscope • Highly trained personnel • Longer turnaround times

  22. Rapid Influenza Assays • Enzyme Immunoassay (EIA) Directigen Flu A and Directigen Flu A+B (Becton Dickinson) • Endogenous Viral-Encoded Assay (EVEA) ZstatFlu (ZymeTx) • Optical Immunoassay (OIA) Flu OIA (Biostar) • Lateral-Flow Immunoassay (LFIA) QuickVue Influenza (Quidel)

  23. CLIA Status Moderate Complexity Directigen Flu A Directigen Flu A+B Flu OIA Waived Status QuickVue Influenza ZstatFlu

  24. Comparison of Rapid Tests

  25. Comparison of Rapid Tests

  26. Directigen Flu A Test Directigen Flu A+B Assay

  27. ZstatFlu

  28. ZstatFlu

  29. Biostar Flu OIA

  30. Biostar OIA

  31. QuickVue Influenza

  32. Comparison of Rapid Tests Prevalence rates were all >18%

  33. Performance Characteristics

  34. Performance Characteristics

  35. Rapid (POC)Tests: Advantages • Rapid turn around time • Rapid outbreak identification • Cost-effective (?) • Widespread testing available • Less expertise required • Optimize antibiotic and antiviral usage

  36. Rapid Tests: Concerns • Specimen adequacy • No viral isolates available for further characterization • Loss of surveillance data • Live, attenuated intranasal vaccine can produce positive results (culture positive too!) • Variable performance characteristics • Result interpretation- poor positive predictive values during low prevalence • Improper treatment choices

  37. Percent Positive By Specimen Type Covalciuc, K.A., et al. 1999. J. Clin.Microbiol. 37: 3971-3974

  38. Patient Age and Onset of Testing Steininger, C., et al. 2002. J. Clin. Microbiol. 40: 2051-2056

  39. Correlation between number of DFA-positive cells and EIA result a No samples were in the category of 25 to 50 positive cells.

  40. Predictive Value • The probability of the presence or absence of disease given the test result • PPV is the probability of disease in a patient with a positive test result • NPV is the probability of not having disease when the test result is negative. • Determined by • sensitivity and specificity of the test • prevalence of disease in the population being tested

  41. Hypothetical Influenza Test Performance • Prevalence = 1 in 5 • Sensitivity = 95% • Specificity = 96% • PPV = 85.6% • NPV = 96% • Prevalence = 1 in 100 • Sensitivity = 95% • Specificity = 96% • PPV = 19.2% • NPV = 99.9% Which test is best? Know the test performance characteristics and the epidemiology of the disease

  42. False Positive EIA’s • Tampa, FL - 16 Flu A positives by EIA in the period from August to the end of October – none confirmed • NY State Dept. of Health (December 2006) 60 specimens that were flu EIA positive sent for confirmatory testing. Only one of them positive by RT-PCR

  43. Rapid Tests: Optimizing Use • Educate clinicians on predictive values & limitations of test results • Confirm early, late and out-of-season positives • Confirm peak-season negatives, if applicable • Use prevalence indicators to decide: • When to test • When to qualify result • When to confirm results

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