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Diagnostic & Screening Tests

       Evaluating Clinical Tests
Herald-Leader, 13 October 2011
Science, 14 October 2011
Herald-Leader, 18 October 2011
Herald-Leader, 26 March 2012
NY Times, 30 October 2011
Herald-Leader, 4 April 2012
www.ChoosingWisely.org
Diagnostic & Screening Tests
  Biological               Symptoms
    Onset                   Appear
                                                                             Clinical
                                                 Clinical                   Outcome
               Screening
                                                Diagnosis




                                      Mausner & Kramer, Epidemiology—An Introductory Text, 1985
Diagnostic & Screening Tests


Diagnostic and screening tests attempt to reveal an otherwise
hidden truth about patients (i.e., their health status: diseased
or disease-free).
    •Physical examination
    •Radiographs/Computed Tomography (CT)
    •Blood and urine assays
    •Cytology (Paps smear, Oral brush biopsy)
    •Saliva (HIV testing)
Discrimination & Classification


“The fundamental principle of diagnostic testing [and
screening] rests on the belief that individuals with disease are
different from individuals without disease and that diagnostic
[and screening] tests can distinguish between these two
groups.”
                      Riegelman, Studying a Study and Testing a Test, 2000


   •Valid (i.e., accurate)
      Sensitivity, specificity, ROC
      Predictive values
      Multiple tests
   •Reliable (i.e., precise or repeatable)
      Percent agreement
      Kappa
Discrimination & Classification




 Disease status comes from an external source of “truth”
 regarding the patients in the population:
    •Gold standard or reference standard
        Adequate
        Independent
        Unbiased
        Representative
Interlude: The Gold Standard

Unbiased
  • The procedure used to establish the truth should not bias
    the truth.
  • Surgery or histology  the “truth” will consist of the
    more advanced cases

Representative
   • Cadaver studies of TMJ (older). Patients younger.
   • Caries simulations (drilled holes in teeth) versus natural
     lesions
Interlude: The Gold Standard

Adequate
   •Surgery or autopsy (common in imaging studies)
   •Time between imaging and surgery/biopsy
   •Applies to positive cases
   •Negative cases – clinical follow-up

Independent
   •Histology provides an independent truth.
   •Occasionally all of the available information, including
    the test being tested is used to establish the gold
    standard. Bone lesion for example (BFO). Creates a bias
    in favor of the test
Discrimination & Classification




 “Appearances to the mind are of four kinds. Things either are
 what they appear to be [ ]; or they neither are, nor appear to
 be [ ]; or they are, and do not appear to be [ ]; or they are
 not, and yet appear to be [ ]. Rightly to aim in all these
 cases is the wise man’s task.”
                                                Epictetus (c. 50-120)
                                            Discourses, Bk I, Chp 27
Validity: Sensitivity & Specificity




Sensitivity

 = Ability of the test to correctly identify those with disease
 = Probability of testing positive given the presence of disease
 = TP / (TP + FN)
 = a / (a + c)
Validity: Sensitivity & Specificity




Specificity

 = Ability of the test to correctly identify those without disease
 = Probability of testing negative given the absence of disease
 = TN / (FP + TN)
 = d / (b + d)
Validity: Sensitivity & Specificity

Assume a population of 1000 people of whom 100 have a
disease. Of these 100 people, the test correctly identifies 80.Of
the 900 disease-free people, the test correctly identifies 800.




      Sensitivity     =      a / (a + c) = 80 / 100 = 80%
      Specificity     =      d / (b + d) = 800/ 900 = 89%

                                                        Gordis, 2009, Table 5-1
Validity: Sensitivity & Specificity

Sensitivity and Specificity

  • Inherent characteristics of the test
  • Stable over different populations with different disease
    prevalence
  • Useful for comparing performance of two tests
    (e.g., Digital versus film mammography / Pisano, NEJM 2005)
  • Have a reciprocal relationship with one another
Validity: Sensitivity & Specificity

                         Low cutoff  High sensitivity
                                     Low specificity
                                     False positives



                         Moderate cutoff  balance




                         High cutoff  Low sensitivity
                                      High specificity
                                      False negatives

                                             Courtesy, S. Fleming, 2011
Validity: Receiver Operating Characteristic Curve




                                  X-axis:
                                      False positive ratio
                                      (1-specificity)
                                  Y-axis:
                                      True positive ratio
                                      (sensitivity)
Validity: Receiver Operating Characteristic Curve
Validity: Receiver Operating Characteristic Curve
Validity: Receiver Operating Characteristic Curve




          5: Sensitivity = 1 and Specificity = 0
          1: Sensitivity = 0 and Specificity = 1
Validity: Receiver Operating Characteristic Curve




                               ROC can be used for a binary
                               outcome (cancer/no cancer) by
                               creating a multipoint scoring
                               scale.
Validity: Receiver Operating Characteristic Curve
Validity: Performance / Predictive Value

Sensitivity and specificity are useful, but

 • May be numerically different if obtained on a group of
   people with early stages of disease compared with a group
   with more advanced disease.

 • We do not know ahead of time who has the disease and
   who does not. Rather, we get the test results and need to
   interpret the findings.
Validity: Performance / Predictive Value




Positive Predictive Value

 = Ability of the test to correctly identify those who test positive
 = Probability of having the disease given a positive test result
 = TP / (TP + FP)
 = a / (a + b)
Validity: Performance / Predictive Value




Negative Predictive Value

 = Ability of the test to correctly identify those who test negative
 = Probability of not having the disease (i.e., being disease-free)
   given a negative test result
 = TN / (FN + TN)
 = d / (c + d)
Validity: Positive & Negative Predictive Values

Assume a population of 1000 people of whom 100 have a
disease. Of these 100 people, the test correctly identifies 80.Of
the 900 disease-free people, the test correctly identifies 800.




      Positive PV =          a / (a + b) = 80 / 180 = 44%
      Negative PV =          d / (c + d) = 800/ 820 = 98%

                                                        Gordis, 2009, Table 5-7
Validity: Predictive Values & Prevalence
Assume a test with a sensitivity of 80% and specificitity of 90%.
What happens to the predictive values when the prevalence of
the disease varies? To fill in the cells, assume a convenient total
population, in this case 1000.




                                    80                    90

                                    20                   810



  Positive PV = a / (a + b) = 80 / 170 = 0.4706 = 47.1%
  Negative PV = d / (c + d) = 810/ 830 = 0.9759 = 97.6%

                                  After Kramer Clinical Epidemiology and Biostatistics, 1988
Validity: Predictive Values & Prevalence

Assume a test with a sensitivity of 80% and specificitity of 90%.




  Positive PV = a / (a + b) = 400 / 450 = 0.8888 = 88.9%
  Negative PV = d / (c + d) = 100/ 550 = 0.8181 = 81.8%

                                 After Kramer Clinical Epidemiology and Biostatistics, 1988
Validity: Predictive Values & Prevalence

Assume a test with a sensitivity of 80% and specificitity of 90%.




  Positive PV = a / (a + b) = 720 / 730 = 0.9863 = 98.6%
  Negative PV = d / (c + d) = 90/ 270 = 0.3333 = 33.3%

                                 After Kramer Clinical Epidemiology and Biostatistics, 1988
Validity: Predictive Values & Prevalence

Assume a test with a sensitivity of 80% and specificitity of 90%.




  Some additional terms:
   • Pretest probability = prior probability = prevalence
   • Post-test probability = posterior probability =
     positive/negative predictive value
   • Bayes Theorem (Thomas Bayes, 1702-61)
Interlude: Bayes Theorem
Interlude: Bayes Theorem
Interlude: Bayes Theorem
Validity: Predictive Values & Prevalence




                                           Gordis, 2009, Figure 5-12
Validity: Predictive Values & Prevalence




                                    Sackett, Clinical Epidemiology, 1985
Validity: Predictive Values & Prevalence
Multiple Tests: Sequential versus Simultaneous
    Screening test:        Diagnostic test:
       •Less expensive        •More expensive
       •Less invasive         •More invasive
       •Less uncomfortable    •More uncomfortable
                              •More accurate




                          Mausner & Kramer, Epidemiology—An Introductory Text, 1985
Multiple Tests: Sequential
Multiple Tests: Sequential




   Net Sensitivity = 161 / 200 = 80.5%
   Net Specificity = (8740 + 158) / 9,800 = 90.1%
Multiple Tests: Sequential




      Net Sensitivity = 315 / 500 = 63.0%
      Net Specificity = (7600 + 1710) / 9,500 = 98.0%
                                                  Gordis, 2009, Figure 5-8
Multiple Tests: Simultaneous
  Suppose in a population of 1000
  people, 200 have the disease and
  Test A sensitivity = 80%
  Test B sensitivity = 90%
  Net sensitivity = A+, B+ or both

  Step 1: 0.8 x 200 = 160 who are A+
  Step *: 0.9 x 200 = 180 who are B+
  Step 2: 0.9 x 160 = 144 who are A+B+
  Step 3: 160 – 144 = 16 who are A+ only
  Step 4: 180 – 144 = 36 who are B+ only
  Step 5: 144 + 16 + 36 = 196 = A+,B+, or
  both
  Step 6: 196/200 = 98%




Courtesy, S. Fleming, 2011
Multiple Tests: Simultaneous
  Suppose in a population of 1000
  people, 800 don’t have the disease
  Test A specificity = 60%
  Test B specificity = 90%
  Net specificity = A- and B-

  Step 1: 0.6 x 800 = 480 who are A-
  Step *: 0.90 x 800 = 720 who are B-
  Step 2: 0.9 x 480 = 432 who are A-
  and B-
  Step 3: 432/800 = 54%




Courtesy, S. Fleming, 2011
Multiple Tests: Simultaneous
Multiple Tests: Simultaneous
Reliability

 Reliability (aka repeatability or precision) is the ability of the
 test to give consistent results when performed more than once
 by on the same individual under the same conditions, even if
 conducted by different examiners.

 Sources of variability (the antithesis of repeatability)
    •Subjects
         BP reading (throughout day, sitting/standing, R/L arm)
         Serum glucose (throughout day, day of the week)
     •Instrumentations
         PSA assay (5% variability even when measuring identical blood
          sample)
     •Observer
         Intra-observer
         Inter-observer
Reliability: Percent Agreement




 Percent agreement
    = number of tests that agree / total number of tests
    = (a + d) / (a + b + c + d)
    = 35 / 40
    = 0.875 = 87.5%
Reliability: Kappa

Measure agreement beyond that expected from chance alone:

Kappa = (percent agreement – chance agreement)
              (1 – chance agreement)

Kappa varies between 0 (no agreement) and 1 (perfect agreement)
   < 0.40      Poor agreement
   0.40 - 0.75 Fair to good agreement
   > 0.75      Excellent

In example, chance agreement = 0.695
Kappa = (0.875 – 0.695)/(1 – 0.695) = 0.180/0.305 = 0.590
Reliability: Kappa




                     Kundel and Polansky, Radiology, 2003
Reliability: Calculating Kappa

Two pathologists independently read and score 75
histopathology slides using their own criteria to subtype the
lesion as Grade II or Grade III




                                                    Gordis, 2009, Figure 5-17
Reliability: Calculating Kappa




          Observed




                                 Gordis, 2009, Figure 5-17
Reliability: Calculating Kappa




             Expected

     Kappa = 90.7% - 51.7% = 39% = 0.81
             100% - 51.7%    48.3%
                                    Gordis, 2009, Figure 5-17
Reliability
Validity and Reliability
Screening


“Screening is defined as the presumptive identification of
unrecognized diseasese or defects by the application of tests,
examinations, or other procedures that can be applied rapidly.”

                                                Friis and Seller, 2009


“For screening to be of benefit, treatment given during the
detectable preclinical phase must result in a better prognosis
than therapy given after symptoms develop.”

                                          Hennekens and Buring, 1987
Screening

Nature of the Disease
   •Important health problem
        Morbidity/Mortality
   •Treatable
         Unethical to screen if untreatable, except to prevent transmission
          (e.g., early cases of AIDS versus protecting blood supply)
   •Relatively high prevalence
         Rare disease  PPV is low & cost per case detected is high
         Exceptions: Phenylketouria (PKU), 1 in 15,000 births, but
          consequences are severe (mental retardation), treatment is
          simple (dietary restriction), screening tests are simple.
   •Detectable preclinical phase (long latency period)
   Biological                 Symptoms
     Onset                     Appear
                                                                    Clinical
                                              Clinical             Outcome
                  Screening
                                             Diagnosis
Screening

Nature of the Test
   •Simple
        Easy to learn and perform
       No complicated patient preparation
   •Rapid
        To administer
        To yield results
   •Safe
        Screened populations are overwhelmingly healthy – keep them
         that way
   •Valid and reliable
        High sensitivity
        Relatively high specificity – accept some FP as there will be
         follow-up confirmatory tests, but what is the cost and morbidity
         of the follow-up, the cost of mislabeling someone, etc.
Screening

Societal Factors
   •Cost
        Relatively inexpensive
       Benefit/cost ratio favorable versus other health care expenditures
   •Acceptable
        Unpalatable or difficult tests  refusal to participate
Resources


Langlotz, Radiology 2003 – supplement to Gordis, especially
for ROC curves.

Pisano et al. NEJM 2005 – example of an application of
concepts.

Linker, AJPH 2012 – and interesting historical perspective of
screening, specifically for scoliosis.

US Preventive Services Task Force (USPSTF) – the source of
many guidelines (and some controversy) regarding screening:
< http://www.uspreventiveservicestaskforce.org/>.

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Diagnotic and screening tests

  • 1. Diagnostic & Screening Tests Evaluating Clinical Tests
  • 6. NY Times, 30 October 2011
  • 9. Diagnostic & Screening Tests Biological Symptoms Onset Appear Clinical Clinical Outcome Screening Diagnosis Mausner & Kramer, Epidemiology—An Introductory Text, 1985
  • 10. Diagnostic & Screening Tests Diagnostic and screening tests attempt to reveal an otherwise hidden truth about patients (i.e., their health status: diseased or disease-free). •Physical examination •Radiographs/Computed Tomography (CT) •Blood and urine assays •Cytology (Paps smear, Oral brush biopsy) •Saliva (HIV testing)
  • 11. Discrimination & Classification “The fundamental principle of diagnostic testing [and screening] rests on the belief that individuals with disease are different from individuals without disease and that diagnostic [and screening] tests can distinguish between these two groups.” Riegelman, Studying a Study and Testing a Test, 2000 •Valid (i.e., accurate) Sensitivity, specificity, ROC Predictive values Multiple tests •Reliable (i.e., precise or repeatable) Percent agreement Kappa
  • 12. Discrimination & Classification Disease status comes from an external source of “truth” regarding the patients in the population: •Gold standard or reference standard Adequate Independent Unbiased Representative
  • 13. Interlude: The Gold Standard Unbiased • The procedure used to establish the truth should not bias the truth. • Surgery or histology  the “truth” will consist of the more advanced cases Representative • Cadaver studies of TMJ (older). Patients younger. • Caries simulations (drilled holes in teeth) versus natural lesions
  • 14. Interlude: The Gold Standard Adequate •Surgery or autopsy (common in imaging studies) •Time between imaging and surgery/biopsy •Applies to positive cases •Negative cases – clinical follow-up Independent •Histology provides an independent truth. •Occasionally all of the available information, including the test being tested is used to establish the gold standard. Bone lesion for example (BFO). Creates a bias in favor of the test
  • 15. Discrimination & Classification “Appearances to the mind are of four kinds. Things either are what they appear to be [ ]; or they neither are, nor appear to be [ ]; or they are, and do not appear to be [ ]; or they are not, and yet appear to be [ ]. Rightly to aim in all these cases is the wise man’s task.” Epictetus (c. 50-120) Discourses, Bk I, Chp 27
  • 16. Validity: Sensitivity & Specificity Sensitivity = Ability of the test to correctly identify those with disease = Probability of testing positive given the presence of disease = TP / (TP + FN) = a / (a + c)
  • 17. Validity: Sensitivity & Specificity Specificity = Ability of the test to correctly identify those without disease = Probability of testing negative given the absence of disease = TN / (FP + TN) = d / (b + d)
  • 18. Validity: Sensitivity & Specificity Assume a population of 1000 people of whom 100 have a disease. Of these 100 people, the test correctly identifies 80.Of the 900 disease-free people, the test correctly identifies 800. Sensitivity = a / (a + c) = 80 / 100 = 80% Specificity = d / (b + d) = 800/ 900 = 89% Gordis, 2009, Table 5-1
  • 19. Validity: Sensitivity & Specificity Sensitivity and Specificity • Inherent characteristics of the test • Stable over different populations with different disease prevalence • Useful for comparing performance of two tests (e.g., Digital versus film mammography / Pisano, NEJM 2005) • Have a reciprocal relationship with one another
  • 20. Validity: Sensitivity & Specificity Low cutoff  High sensitivity  Low specificity  False positives Moderate cutoff  balance High cutoff  Low sensitivity  High specificity  False negatives Courtesy, S. Fleming, 2011
  • 21. Validity: Receiver Operating Characteristic Curve X-axis: False positive ratio (1-specificity) Y-axis: True positive ratio (sensitivity)
  • 22. Validity: Receiver Operating Characteristic Curve
  • 23. Validity: Receiver Operating Characteristic Curve
  • 24. Validity: Receiver Operating Characteristic Curve 5: Sensitivity = 1 and Specificity = 0 1: Sensitivity = 0 and Specificity = 1
  • 25. Validity: Receiver Operating Characteristic Curve ROC can be used for a binary outcome (cancer/no cancer) by creating a multipoint scoring scale.
  • 26. Validity: Receiver Operating Characteristic Curve
  • 27. Validity: Performance / Predictive Value Sensitivity and specificity are useful, but • May be numerically different if obtained on a group of people with early stages of disease compared with a group with more advanced disease. • We do not know ahead of time who has the disease and who does not. Rather, we get the test results and need to interpret the findings.
  • 28. Validity: Performance / Predictive Value Positive Predictive Value = Ability of the test to correctly identify those who test positive = Probability of having the disease given a positive test result = TP / (TP + FP) = a / (a + b)
  • 29. Validity: Performance / Predictive Value Negative Predictive Value = Ability of the test to correctly identify those who test negative = Probability of not having the disease (i.e., being disease-free) given a negative test result = TN / (FN + TN) = d / (c + d)
  • 30. Validity: Positive & Negative Predictive Values Assume a population of 1000 people of whom 100 have a disease. Of these 100 people, the test correctly identifies 80.Of the 900 disease-free people, the test correctly identifies 800. Positive PV = a / (a + b) = 80 / 180 = 44% Negative PV = d / (c + d) = 800/ 820 = 98% Gordis, 2009, Table 5-7
  • 31. Validity: Predictive Values & Prevalence Assume a test with a sensitivity of 80% and specificitity of 90%. What happens to the predictive values when the prevalence of the disease varies? To fill in the cells, assume a convenient total population, in this case 1000. 80 90 20 810 Positive PV = a / (a + b) = 80 / 170 = 0.4706 = 47.1% Negative PV = d / (c + d) = 810/ 830 = 0.9759 = 97.6% After Kramer Clinical Epidemiology and Biostatistics, 1988
  • 32. Validity: Predictive Values & Prevalence Assume a test with a sensitivity of 80% and specificitity of 90%. Positive PV = a / (a + b) = 400 / 450 = 0.8888 = 88.9% Negative PV = d / (c + d) = 100/ 550 = 0.8181 = 81.8% After Kramer Clinical Epidemiology and Biostatistics, 1988
  • 33. Validity: Predictive Values & Prevalence Assume a test with a sensitivity of 80% and specificitity of 90%. Positive PV = a / (a + b) = 720 / 730 = 0.9863 = 98.6% Negative PV = d / (c + d) = 90/ 270 = 0.3333 = 33.3% After Kramer Clinical Epidemiology and Biostatistics, 1988
  • 34. Validity: Predictive Values & Prevalence Assume a test with a sensitivity of 80% and specificitity of 90%. Some additional terms: • Pretest probability = prior probability = prevalence • Post-test probability = posterior probability = positive/negative predictive value • Bayes Theorem (Thomas Bayes, 1702-61)
  • 38. Validity: Predictive Values & Prevalence Gordis, 2009, Figure 5-12
  • 39. Validity: Predictive Values & Prevalence Sackett, Clinical Epidemiology, 1985
  • 41. Multiple Tests: Sequential versus Simultaneous Screening test: Diagnostic test: •Less expensive •More expensive •Less invasive •More invasive •Less uncomfortable •More uncomfortable •More accurate Mausner & Kramer, Epidemiology—An Introductory Text, 1985
  • 43. Multiple Tests: Sequential Net Sensitivity = 161 / 200 = 80.5% Net Specificity = (8740 + 158) / 9,800 = 90.1%
  • 44. Multiple Tests: Sequential Net Sensitivity = 315 / 500 = 63.0% Net Specificity = (7600 + 1710) / 9,500 = 98.0% Gordis, 2009, Figure 5-8
  • 45. Multiple Tests: Simultaneous Suppose in a population of 1000 people, 200 have the disease and Test A sensitivity = 80% Test B sensitivity = 90% Net sensitivity = A+, B+ or both Step 1: 0.8 x 200 = 160 who are A+ Step *: 0.9 x 200 = 180 who are B+ Step 2: 0.9 x 160 = 144 who are A+B+ Step 3: 160 – 144 = 16 who are A+ only Step 4: 180 – 144 = 36 who are B+ only Step 5: 144 + 16 + 36 = 196 = A+,B+, or both Step 6: 196/200 = 98% Courtesy, S. Fleming, 2011
  • 46. Multiple Tests: Simultaneous Suppose in a population of 1000 people, 800 don’t have the disease Test A specificity = 60% Test B specificity = 90% Net specificity = A- and B- Step 1: 0.6 x 800 = 480 who are A- Step *: 0.90 x 800 = 720 who are B- Step 2: 0.9 x 480 = 432 who are A- and B- Step 3: 432/800 = 54% Courtesy, S. Fleming, 2011
  • 49. Reliability Reliability (aka repeatability or precision) is the ability of the test to give consistent results when performed more than once by on the same individual under the same conditions, even if conducted by different examiners. Sources of variability (the antithesis of repeatability) •Subjects BP reading (throughout day, sitting/standing, R/L arm) Serum glucose (throughout day, day of the week) •Instrumentations PSA assay (5% variability even when measuring identical blood sample) •Observer Intra-observer Inter-observer
  • 50. Reliability: Percent Agreement Percent agreement = number of tests that agree / total number of tests = (a + d) / (a + b + c + d) = 35 / 40 = 0.875 = 87.5%
  • 51. Reliability: Kappa Measure agreement beyond that expected from chance alone: Kappa = (percent agreement – chance agreement) (1 – chance agreement) Kappa varies between 0 (no agreement) and 1 (perfect agreement) < 0.40 Poor agreement 0.40 - 0.75 Fair to good agreement > 0.75 Excellent In example, chance agreement = 0.695 Kappa = (0.875 – 0.695)/(1 – 0.695) = 0.180/0.305 = 0.590
  • 52. Reliability: Kappa Kundel and Polansky, Radiology, 2003
  • 53. Reliability: Calculating Kappa Two pathologists independently read and score 75 histopathology slides using their own criteria to subtype the lesion as Grade II or Grade III Gordis, 2009, Figure 5-17
  • 54. Reliability: Calculating Kappa Observed Gordis, 2009, Figure 5-17
  • 55. Reliability: Calculating Kappa Expected Kappa = 90.7% - 51.7% = 39% = 0.81 100% - 51.7% 48.3% Gordis, 2009, Figure 5-17
  • 58. Screening “Screening is defined as the presumptive identification of unrecognized diseasese or defects by the application of tests, examinations, or other procedures that can be applied rapidly.” Friis and Seller, 2009 “For screening to be of benefit, treatment given during the detectable preclinical phase must result in a better prognosis than therapy given after symptoms develop.” Hennekens and Buring, 1987
  • 59. Screening Nature of the Disease •Important health problem Morbidity/Mortality •Treatable  Unethical to screen if untreatable, except to prevent transmission (e.g., early cases of AIDS versus protecting blood supply) •Relatively high prevalence  Rare disease  PPV is low & cost per case detected is high  Exceptions: Phenylketouria (PKU), 1 in 15,000 births, but consequences are severe (mental retardation), treatment is simple (dietary restriction), screening tests are simple. •Detectable preclinical phase (long latency period) Biological Symptoms Onset Appear Clinical Clinical Outcome Screening Diagnosis
  • 60. Screening Nature of the Test •Simple  Easy to learn and perform No complicated patient preparation •Rapid  To administer  To yield results •Safe  Screened populations are overwhelmingly healthy – keep them that way •Valid and reliable  High sensitivity  Relatively high specificity – accept some FP as there will be follow-up confirmatory tests, but what is the cost and morbidity of the follow-up, the cost of mislabeling someone, etc.
  • 61. Screening Societal Factors •Cost  Relatively inexpensive Benefit/cost ratio favorable versus other health care expenditures •Acceptable  Unpalatable or difficult tests  refusal to participate
  • 62.
  • 63. Resources Langlotz, Radiology 2003 – supplement to Gordis, especially for ROC curves. Pisano et al. NEJM 2005 – example of an application of concepts. Linker, AJPH 2012 – and interesting historical perspective of screening, specifically for scoliosis. US Preventive Services Task Force (USPSTF) – the source of many guidelines (and some controversy) regarding screening: < http://www.uspreventiveservicestaskforce.org/>.