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HPV test
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HPV Testing Uses and Abuses
Barbara S. Apgar, MD, MS
Professor of Family Medicine
University of Michigan Medical Center
Ann Arbor, Michigan
Objectives
• Understand the current uses of HPV testing.
• Discuss when HPV testing is or is not indicated.
• Compare the sensitivity of HPV testing and cervical cytology for cervical cancer screening.
Progression to Invasion
Persistent positivity with oncogenic HPV types is uncommon but required for progression
Cervical cancer
Apgar, Brotzman, Spitzer
Sigurdsson K et al. Int J Cancer 2007;2682-2687.
HPV Types in CIN 2, CIN 3 and Cervical Cancer,
Iceland, 1990-1994 and 1999-2003
#2
#
1
Hybrid Capture 2: FDA approved
• Low risk HPV types
• 6, 11, 42, 43, 44
• High risk HPV types
• 16, 18, 31, 33, 35, 39, 45, 51, 52, 56, 58, 59, 68
Triage, management and co-testing should be
by HR HPV types only
Methods to detect HPV DNA
• Pooled mixture of probes for high-risk HPV types:
• 16, 18, 31, 33, 35, 39, 45, 51, 52, 56, 58, 59, 68 + 66.
• Does not distinguish individual types.
• Polymerase chain reaction.
• Molecular amplification method identifying a small amount of a target DNA.
• Identification of specific type of HPV.
FDA-approved HPV DNA tests
• Hybrid Capture 2 HPV DNA Assay (13 pooled)-Quigen
• HPV types: 16, 18, 31, 33, 35, 39, 45, 51, 52,
• 56, 58, 59, 68.
• HPV detected by chemiluminescence
• Cervista HPV HR (14 pooled).
• Same HPV types as HC 2 + HPV type 66.
• Cervista HPV 16/18.
• HPV type-specific test (genotyping).
FDA-approved HPV tests
• cobas 4800 HPV test. (approved 2011)-Roche
• PCR-based.
• 14 HR HPV types.
• Genotyping for HPV 16 and 18 integrated into the assay.
• Concurrently detects remaining 12 types as a group.
Aptima HPV test (GenProbe)-FDA 2013
Detects E6/E7 mRNA expression of 14 HR HPV types
Approved for testing on Hologic system.
HPV E6/E7 overexpression: necessary condition for the start and progression of cervical neoplasia.
E6 and E7 inactivates p53 and pRb suppressor proteins.
Is correlation between HPV mRNA and CIN 3 a true biomarker of risk?
94% and 100% of women with CIN 3 and cancer were + for E6/E7 mRNa activity. (Castle et al. Clin CA 2007;13)
HPV mRNA detection
• HPV mRNA detection may improve specificity.
• It is unknown which lesions will regress or progress.
• Increased monitoring needed.
• Detection of mRNA transcripts may allow clinicians to know whether or not HPV is actively replicating E6 and E7 oncogenes.
• Bottom line: May be able to stratify risk of progression to CIN 3 in women with abnormal cytology.
Brown AJ et al. Best Prac Res Clin OG 2012;26:233
HPV tests for detection of CIN 2 and 3 Cuzick J et al. Br J Cancer 2013;108(4):908-913
• HPV tests should be FDA approved or supported by peer-reviewed published data on sensitivity and specificity.
• Performance should be similar to assays used in clinical trials.
• Tests should have documented clinical performance characteristics (92% +/- 3% sensitivity for CIN 3+)
• > 85% specificity in screening setting.
Saslow D et al. ACA Cancer J Clin. 2012;62(3):147-72.
Stoler MH et al. Am J Clin Pathol. 2007;127(3):335-7.
Home brewed HPV assays
• Some molecular labs have developed their own HPV assays.
• Usually PCR-based.
• Problem: cut-offs are not clinically validated.
• Not FDA-approved.
• What does a positive or negative result actually mean? Exercise caution!
HPV DNA Testing
Areas of clinical utility
Co-testing with cervical cytology in women > 30.
• Assess the risk of recurrence/persistence after treatment of CIN 2,3 (cotesting).
• “Preferred” option for ASC-US triage because of cost and predictive value.
• “Acceptable” option for LSIL triage in postmenopausal women.
HPV testing not recommended
• Routine screening in women < age 30 (except ASCUS triage).
• Women > 24 years with ASC-H, LSIL, HSIL, AGC (except postmenopausal LSIL reflex HPV testing).
• Women considering HPV vaccination.
• Routine STI screening.
• As part of sexual assault workup.
HPV Genotyping
Both DNA and mRNA tests available
Prognostic information seems similar.
5 year risk of CIN2+ if HPV 16 = ~10%
Risk of CIN2+ is lower if HPV 18 , but there is association for adenocarcinoma.
Bottom line: ASCCP guidelines show genotyping acceptable without recommending for or against use
Allows for clinician discretion and patient choice
2013 ASCCP management guidelines
Wright TC, et al. J Lower Genital Tract Disease, 2007; 11: 201-222 and 223-239
Comments on HPV genotyping
• Not recommended yet: Women with ASC-US.
• Cotesting.
• Genotyping triages cytology negative, HPV 16/18+ to colposcopy.
• Colposcopy is indicated for all women with HPV+ ASCUS regardless of genotyping result.
• Threshold for colposcopy exceeded by both groups.
Are guidelines being followed?
• Estimated that > 50% of the 75 million US Pap tests performed in 2010 in the US were:
• Outside guideline compliance.
• Therefore, unnecessary.
• More anxiety in woman with negative Pap and HPV + results than in woman with normal Pap and unknown HPV status.
Solomon D et al. CA Cancer J Clin 2007;105.
Kitchener HC et al. Int J Gynecol Ca 2008;18
Berkowitz Z et al. Obstet Gynecol 2010;116.
2010 CDC survey of IM, FP, ObGyn 950 Pap test providers
• Primary outcomes were responses to clinical case vignette of a 35 year old woman who had cervical cancer screening.
• Negative Pap and + HPV test (co-testing).
• Questions: when to do the next Pap and HPV test? Adherent with guidelines or not?
Berkowitz Z et al. Obstet Gynecol 2010;116.
Results of 2010 CDC survey
• > 80% of all physicians reported that HPV DNA testing with Pap has higher sensitivity than Pap alone.
• 35 year old: negative Pap and + HPV test.
• 54% recommended HPV test at the same time as the Pap (adherent with guidelines).
Conclusions of 2010 CDC Survey
• About 50% of women > 30 years did not receive recommended management of Pap negative, HPV+ cotesting.
Knowledge of HPV tests - CDC
• 12% of clinicians did not know there was a high
risk and low risk HPV test.
• 56% of clinics use high risk tests only.
• 25% use both high and low risk HPV tests.
• Bottom line: low risk HPV testing adds cost without
additional value to health care.
High and low-risk HPV testing reported by clinical specialties
0
10
20
30
40
50
60
70
Family Practice Int Med ObGyn Mid-level
High risk HPV
High and low risk HPV
Lee, Berkowitz, Zahava, Saralya. OG 2011;118:4-13
Low risk HPV testing
• Screens for non-oncogenic HPV types.
• Serves no purpose in the context of cervical cancer
screening.
• Low risk testing should not be performed for genital
warts. Does not change management.
• Bottom line: + low risk HPV test is clinically
insignificant but …..unnecessary follow-up is not.
Why order low risk HPV tests?
• Clinician confusion.
• It is on the lab req as a check-box option.
• Financial gain to clinician or clinic or institution.
• Low and high risk HPV billed the same (doubles the cost.
• Test marketing by industry.
• 2007: 45% of labs offered low risk HPV testing. (Arch Pathol Lab Med 2008;132)
• Need attributed to reimbursement and demand.
Requests to check HPV status
• Direct to consumer advertising associated with significant increases in HPV test use by clinicians. (Price et al. Med Care 2011;49.)
• Screening for HPV status outside cervical cancer screening should be avoided.
Value of co-testing women < 30 yrs
• 50 % of clinicians and clinics do HPV co-testing in women < 30 years (not adherent).
• % of clinicians doing co-testing for this age group doubled since 2004.
• Despite significant rate of transient HPV infections in this age group.
• Problem: Women < age 30 referred to colposcopy after co-testing.
Other issues with co-testing
• About 6% prevalence of women with discordant results will require additional follow-up.
•
• Problems:
• Repetition of co-testing annually or biannually rather than triannually.
• Repeating co-testing < 3 years if new sexual partner.
Berkowitz Z et al. Obstet Gynecol 2010;116.
Castle PE et al. Obstet Gynecol 2009;113. Katki HA et al. Lancet Oncol 2012; 12: 663
Katki HA, et al. Lancet Oncol 2012; 12: 663
Proportion of Co-Test Results in
331,061 Kaiser women > 30 years
92.5%
2.4%
3.7% 1.4%
Discordant
Kaiser Study
N=331,818 women > 30
years in prospective co-
testing study
Katki HA, et al. Lancet Oncol 2011;
12: 663
Cumulative Risk Of Invasive Disease
Based on Initial Co-Test
Conclusions of CDC Report 2011
• Many clinicians report guideline-adherent HPV testing.
• Some also report inappropriate HPV testing (no clinical indication).
• Low risk HPV testing (33%).
• HPV co-testing in women < age 30 (60%).
• Consequences: increased medical costs, unnecessary follow-up tests, patient anxiety and alarm about HPV status.
Why use HPV testing for detection of CIN 2,3 and cancer?
Increased sensitivity of carcinogenic HPV testing for detection
of CIN 2,3 and cancer.
Increases the efficiency of cervical cancer screening by better
risk stratification than cytology alone.
Necessary role of persistent carcinogenic
HPV infections in the development
of serious lesions
Finding carcinogenic HPV types
does not
provide a diagnosis of CIN 3 or
cancer
It identifies a group of women in
whom CIN 3+ is more likely
Compensation for the limitations of
cytology, colposcopy, histology
Relied on repeated annual
or
biennial Pap screening
Used CIN 2 as a threshold for
treatment to provide an
additional margin of safety
even though CIN 2 can regress
Adopted an expanded role for the
detection of carcinogenic HPV DNA
in the clinical management of
cervical abnormalities
Triage of Postmenopausal Women
with LSIL
62 year old postmenopausal woman
with atrophy.
LSIL cytology. No HPV testing.
Always normal Pap tests.
HPV testing in postmenopausal women with LSIL and no HPV test?
• Prevalence of CIN 2,3 drops with increasing age.
• Accuracy of LSIL as a marker for HPV drops in older women.
• Postmenopausal women can be managed less aggressively than premenopausal women.
• ASCCP: No HPV test: Acceptable options include reflex HPV DNA testing, repeat cytology at 6 and 12 mos. and colposcopy.
Postmenopausal women with LSIL
• If the HPV is negative or no CIN identified at
colposcopy, repeat cytology in 12 months.
• If either the HPV test is + or repeat cytology is >
ASCUS, colposcopy.
• If 2 consecutive repeat cytology tests are
negative, routine screening.
There is something new on the horizon
Photo courtesy of Alan Waxman, MD
What happens to HPV after tx for CIN 2,3 ?
• Most women become HPV negative after treatment of CIN 2,3 provided recurrent/persistent disease not present.
• Women who fail treatment have high rates of HPV positivity.
• HPV testing has high negative predictive value.
• Useful in post-treatment surveillance.
HPV follow-up after treatment CIN 2.3
Systematic review Paraskevaidis et al. Ca Treatment Rev 2004;30:205-11
Treatment Outcome
HPV status Success Failure
n=672 n=204
Negative 84% 17%
Positive 16% 83%
Clearance of HPV after treatment for CIN 2,3 or persistent CIN 1
Moore et al. Obstet Gynecol 2011;117:101-108
1207 treated women prospectively studied.
Treated LEEP, cone, or laser ablation.
Followed with colpo, cytology 2-6, 12
months after tx, then annually until HPV
cleared.
Genotyping done.
45% had laser ablation
55% had excision.
Time to clearance of HPV
HPV types No. with HPV type at baseline
No. (% cleared) Median time to clearance (months)
HPV 16 418 387(93) 5.9
HPV 18 99 96(97) 5.9
HPV 31 149 142(95) 5.4
HPV 39 89 79(89) 6.3
Almost all women with HPV types 16, 18 had clearance and 50%
cleared within 6 months.
Moore et al. Obstet Gynecol 2011;117:101-108
HPV testing post-tx predicting residual disease in subsequent TAH specimens n=115
Sensitivity Specificity Accuracy*
Resection
Margin 75% 53% 61%
HPV Testing 85% 67% 73%
Predictive value of resection margin was much improved when used
in combination with HPV DNA testing
Park JY et al. Obstet Gynecol 2009;114:87-92
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