How HPV epidemiology drives new cervical cancer screening guidelines L. Stewart Massad, M.D. Dept....
Transcript of How HPV epidemiology drives new cervical cancer screening guidelines L. Stewart Massad, M.D. Dept....
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How HPV epidemiology drivesnew cervical cancerscreening guidelines
L. Stewart Massad, M.D.
Dept. of Obstetrics & Gynecology
Washington University School of Medicine
St. Louis, MO
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Disclosure
• I do not have financial relationships with pharmaceutical or device manufacturers
• This talk does not include unapproved uses of tests
• I have received honoraria and expense reimbursement from ASCCP for guidelines development.
• I have received payment for malpractice consultation (defendants and plaintiffs)
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Learning objectives
• Participants should be able to screen women for cervical cancer, applying the epidemiology and natural history– of human papillomavirus infections
– and of consequent preinvasive/invasive cervical lesions
that underlie new guidelines
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What is the objective of screening?
• To reduce morbidity/mortality from cancer– Not to find abnormal Paps or CIN– Not to find HPV infection
• While minimizing harms from overdiagnosis
Requires balancing sensitivity/specificity
Use a sensitive screen at long intervals to allow regression of self-limited lesions
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Why isn’t finding lesions the objective of screening?
• CIN/SIL/HPV are surrogate markers, not inevitable cancer precursors
• Finding CIN/SIL/HPV not destined to cause morbidity/mortality– Increases anxiety, stigma, treatment pain and
complications, and cost
– Without benefit to patients
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Why isn’t finding lesions the objective of screening?
• We can’t tell which lesions will progress.
• But we know we want to target only:– Persistent HPV infections
– CIN 3 (no margin for error)
– CIN2 in older women (no risk to pregnancies)
– Persistent CIN2 and CIN2,3 in younger women
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Reducing cervical cancer risk to zero is not feasible
• Consensus focuses on level of risk that is acceptable vs harms of screening
• Some cancers are not preventable:– Rapid onset cancers in women 20-30yo– Tight gap junction neoplasms that don’t exfoliate– High grade lesions with low level HPV
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Annual cancer risk, US womenACS: Ca:Cancer J Clin 2014;64:10
Incidence MortalityBreast 235,030 40,000
Lung 108,210 72,330
Colon/rectum 65,000 24,040
Uterine corpus 52,630 8,590
Ovary 21,980 14,270
Cervix 12,360 4,020
Vulva/vagina/other gyn
8,020 1,910
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Current cervical cancer risk is low
SEER 1992-96, all races: Risk in Africa is >30
CaCx rate/100,000 U.S. women
15-19yo 0.2
20-24yo 2.6
25-30yo 7.8
30-34yo 11.4
35-39yo 14.4
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Age-standardized cancer incidence and mortality are low in regions with screening.
Ca Cancer J Clin 2011;61:69-90
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Residual risk
• >40,000,000 Paps annually in US
• >2,000,000 abnormal Paps annually (5%)
• >200,000 CIN2,3 annually (0.5% of all screens)
Many are cancers that screening/Rx will prevent
Cancer risk in unscreened women remains high
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Residual risk
• >50% of cervical cancers occur in un- or underscreened women
• About 1 in 8 cancers follow mismanaged abnormal screening tests
Only ~30% of cancers are screen failures
A perfect screening test will save 1000 lives among 40,000,000 women screened
Spence et al. Prev Med 2007;45:93-106
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HPV and cervical cancer
All cervical cancer is due to HPV infection
but few HPV infections lead to cervical cancer
• >60% of women contract HPV within 2y of first sex– Most contract carcinogenic types, esp. HPV 16
• 90% clear HPV within 2 years of infection• But only persistent high risk infections cause cancer
– HPV- women at low short term risk, even if prior infected.
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Why new guidelines?
CIN2+ in <30% of women with HPV+ ASC-US and LSIL
• True despite HPV being found in 100% of HPV+ ASC-US, 85% of LSIL
Thus, most abnormal Paps represent benign HPV infections that will clear, not precancer
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Winer R L et al. Am. J. Epidemiol. 2003;157:218-226
HPV cumulative incidence among women sexually active but HPV- at enrollment
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Hariri S et al. J Infect Dis. 2011;204:566-573
Weighted prevalence of low-risk and high-risk HPV among US women 14–59yo, CDC
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30-month rates of clearance/persistence/progression of oncogenic HPV among women <30yo, US NCI, GuanacasteRodriguez AC et al. JNCI 2008;100:513-7
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61%
8%
Rodriguez AC et al. J Natl Cancer Inst. 2008;100:513-17.
Rapid clearance of HPV in Women >30
* Histological progression
*
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CIN behavior mirrors HPV
• >75% of CIN1 regress without treatment
• Only 10% develop CIN3 within 2y (no cancers)
• Most rapid-onset CIN are HPV infections with little neoplastic potential
• >65% of adolescents clear CIN2 within 3y
• >50% of adults clear CIN2 without treatment
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What is the natural history of LSIL/CIN1 in adolescents?
Moscicki AB et al. Lancet 2004;364:1678-83
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Similar high likelihood of clearance of newly acquired HPV in young women
Franco E L et al. J Infect Dis. 1999;180:1415-1423
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Early screening may be futile
• Better grasp of the futility of early screening– “Cervical cancer screening has little or no impact
on rates of invasive cervical cancer up to age 30.”
Many European health programs delay screening till 25-30 years of age
» Sasieni et al BMJ 2009;339:328
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Short Pap intervals = more colposcopy, little added benefit
• Screening harms: lifetime risk of colposcopy– Screening q3y: 760 colpos/1000 women
– Screening q2y: 1080 colpos/1000 women
– Screening annually: 2000 colpos/1000 women
Stout NK et al. Arch Intern Med 2008;168:181.
Kulasingam S et al. 2011. AHRQ Publication No.11-05157-EF-1.
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Dillner J et al. BMJ 2008;337:a1754
5y CIN3+ risk after neg cotest similar to 1y risk after neg Pap
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Treatment saves but also costs lives
Women with LEEP more likely to have Preterm birth (O.R. 1.7)
LBW (O.R. 1.8)
PPROM (O.R. 2.7)
Single studies show association with perinatal death, incompetent cervix
Risk rises with depth, # LEEPs
Similar findings after CKC or laser cone
Absolute risk increase is small
Kyrgiou M et al. Lancet 2006;367:489-98 and Bruinsma et al BJOG 2007;114:70-80
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Consensus Conference Sponsored by
• American Society of Colposcopy and Cervical Pathology (ASCCP)
• American Cancer Society (ACS)
• American Society of Clinical Pathology (ASCP)
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ACS/ASCCP/ASCP guidelines development process
• 2009-2011: 3 organizations created 6 working groups as well as a data group to aid in literature review and evidence evaluation
• Participating organizations:
AHRQ, AAFP, ABOG,ACHA, ACOG, ASHA, AmSoc Cytopath, AmSoc Cytotech, CDC, Ctrs for Medicare/Medicaid, CAP, FDA, NCI, NCCN, NPWH, PPFA, SCC, SGO, SGOC, USPSTF, Veterans Health Admin
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ACS/ASCCP/ASCP guidelines development process
After formal evidence review• Recommendations posted to ASCCP website for
public comment 10/19-11/9/11– Revisions made based on comments as needed
• Consensus conference 11/17-18/11
• After discussion, recommendations approved by at least 2/3 majority
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ACS/ASCCP/ASCP guidelines development process
Assumptions
• Benefits of screening– Cancer is the ideal endpoint but unrealistic
– CIN3 is a reliable surrogate marker for sensitivity
– CIN2 is hard to diagnose, often regresses: not a target for screening, though still a target for treatment
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ACS/ASCCP/ASCP guidelines development process
Assumptions
• Screening interval– Development of invasive cancer should be
unlikely before next screen
– Earlier detection of CIN3+ is a benefit• Even if studies of less sensitive tests show similar
CIN3 detection, no increased cancer risk during later screening rounds
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ACS/ASCCP/ASCP guidelines development process
Assumptions
• Harms of screening– Anxiety over a positive test
– Stigmatization
– Pain/bleeding from procedures
– Treatment-related pregnancy loss
– Number of colposcopies is a marker for these
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ACS/ASCCP/ASCP guidelines development process
Assumptions• Preventing all cervical cancer is unrealistic
– No test has 100% sensitivity
• Reasonable risk is determined by the strategy of cytology alone at 2-3y intervals– Screening strategies with similar results acceptable
• Women at similar risk for cancer should be managed similarly
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ACS/ASCCP/ASCP guidelines development process
Assumptions• Conventional/liquid-based Paps perform similarly
• HPV tests should have ≥90% sensitivity for CIN3+ and CIN2+– Comparability of FDA-approved HPV tests can’t be
assumed– Utility of unapproved/exempt tests is unknown
• These should not be used in screening
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Changes from 2002 guidelines
• Retains 21yo start to screening– No longer 3y after sex or 21yo, as before 2002
• Longer Pap screening intervals– Screen q3y ages 21-29—was annually– Screen q3y 30-65
• New technology allows long interval:– Cotesting preferred q5y over Paps
• Stop at age 65, not 70– Retains guideline to stop after hyst for benign disease
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When to start screening
• “Begin at age 21 years”
• Younger women “should not be screened regardless of the age of sexual initiation or other risk factors.”
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Rationale for later screening start
• Cervical cancer rare in teens (<1:1,000,000)• Early onset CaCx may not be preventable• HPV—including HRHPV—occurs in over
80% of sexually active adolescents• HPV infections usually transient
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Others start screening later
• Europeans begin screening at 25-30 years of age– Screen only every 3-5 years– But they have central screening systems with
organized recall
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When to start screening
• Avoid screening adolescents– Cancer risk low– Abnormalities may prompt treatment for lesions
likely to resolve
• Sexually active adolescents need care for contraception and STD screening/treatment– These don’t require Pap testing– No speculum needed for asymptomatic women– STD testing can be done using urine
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Screening intervals
• Ages 21-29– Cytology alone q3y
– HPV testing “should not be used to screen”• Not as a component of cotesting• Not as a primary stand-alone screen
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Rationale for longer intervals
• Sensitivity of single Pap smear only 50-70%
– Cancer risk 18mo after 3 neg Paps = 1.5/100,000
– Cancer risk 36mo after 3 neg Paps = 4.7/100,000
99,997 women screened uselessly to help 3
• Risk of HSIL/cancer <3y after negative Pap not significantly higher than risk after 1y
• Longer Pap screening intervals (e.g., 5y) inappropriate for mobile US population
Sawaya GF et al. Acta Cytol 2005;49:391-7
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Rationale for avoiding HPV tests
• Prevalence of carcinogenic HPV approaches 20% in teens-early 20s
• Most carcinogenic HPV infections resolve
• Identifying carcinogenic HPV that will resolve leads to repeated call-back, anxiety, interventions without benefit
• May be useful in follow-up, esp after treatment
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Screening intervals
• Ages 30-65– Cotesting (cytology + HPV test) q5y (preferred)
– Cytology alone q3y (acceptable)
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Why prefer cotesting?
• Adding HPV tests to cytology– Increases detection of prevalent CIN3
– Decreases CIN3 in subsequent screening rounds
– Therefore lower risk after neg screen
– So a 5y interval between screens achieves risk of CIN3 equal to that after cytology alone done at 1-3y intervals
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Why prefer cotesting?
• Adding HPV tests to cytology– Enhances detection of adenocarcinoma/AIS
• Increasingly prevalent yet often missed by Pap alone
– Q3y vs q5y cotests: 10y cancer risk for 40yo woman was about 0.6%
– Extending screening to q5y minimizes colposcopies, so reduces harms of a more sensitive test.
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Why not require cotesting?
• Some sites may lack access to HPV testing• Financial, logistical
• Cytology remains effective– It just requires more frequent visits with more risk of
loss to follow-up, more colposcopy for equivocal results
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Why not annual cotesting?
• High NPV of one cotest means most abnormal screens at 1-3y intervals represent transient HPV infection, not precancer
• Harms are amplified for minimal benefit
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When to stop screening
• Stop at age 65 for women with adequate negative prior screening, no CIN2+ within the last 20y.
• Screening “should not resume for any reason, even if a woman reports having a new sexual partner.”
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When to stop screening
• Adequate negative prior screening is defined as– 3 consecutive negative cytology results or– 2 consecutive negative cotests– within the 10 years before ceasing screening– with the most recent test within 5 years.
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Rationale for stopping at 65yo
• CIN2+ is rare after age 65– Most abnormal screens, even HPV+, are false
positive, i.e., don’t reflect precancer
• HPV risk remains 5-10%
• Colpo/biopsy/treatment more difficult– Harms are magnified
• Incident HPV infection unlikely to lead to cancer within remaining lifetime
Chen HC et al. JNCI 2011;103:1387-96. Rodrigues AC et al. JNCI 2009;101:721-8
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Rationale for stopping after hyst
• Vag cancer rate is 7/million/yr
• 663 vag cuff Paps needed to find one VAIN
• 2066 women followed after hyst for avg 89mo– 3% had VAIN, 0 had cancer
• Risk of Pap abnormality after hyst = 1%– Most abnormal screens, even HPV+, are false
positive, i.e., don’t reflect precancer– Equal risk of breast cancer in men--mammography?
Pearce KF et al. NEJM 1996;335:1559-62. Piscitelli JT et al. AJOG 1995;173:424-30
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When to stop screening
• Stop at hysterectomy with removal of cervix and no history of CIN2+
• “Evidence of adequate negative prior screening is not required”
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When NOT to stop at 65yo
• History of– Prior Cervical or endometrial cancer– In utero DES exposure– HIV infection or other immunocompromise
• If Hx CIN2, CIN3, or AIS– Continue “routine screening” for at least 20
years, “even if this extends screening past age 65.”
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Screening after treatment of CIN2+
• 2012 Management algorithm recommends “Routine screening” after 3 negative cotests– How to manage after prior Paps/no cotests?– Stop at age 65?– Stop after hysterectomy for CIN2+?
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Management of Women with Biopsy-confirmed Cervical Intraepithelial Neoplasia - Grade 2 and 3 (CIN2,3) *
Either Excision† or Ablation of T-zone *
Cotesting at 12 and 24 months
2x NegativeResults
Any test abnormal
Diagnostic Excisional Procedure †
Adequate Colposcopy Inadequate Colposcopy orRecurrent CIN2,3 orEndocervical sampling is CIN2,3
ColposcopyWith endocervical sampling
*Management options will vary in special circumstances or if the woman is pregnant or ages 21-24†If CIN2,3 is identified at the margins of
an excisional procedure or post-procedure ECC, cytology and ECC at 4-6mo is preferred, but repeat excision is acceptable and hysterectomy is acceptable if re-excision is not feasible.
Repeat cotestingin 3 years
© Copyright , 2012, American Society for Colposcopy and Cervical Pathology. All rights reserved.
Routine screening
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Screening after treatment of CIN2+
• Evidence is unclear• How to manage after prior Paps/no cotests?
– Consider 2-3 Paps = 1 cotest (so annual Paps x 10y should convey similar risk)
• Stop at age 65? ACOG: continue at least 20y– Judgment: Stop only if multiple prior neg screens
• Stop after hysterectomy for CIN2+?– Judgment: Only if multiple prior neg Paps– Avoid cotesting: meaning of Pap-/HPV+?
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Primary HPV screening
• Expert panel voted 3/12/14 to recommend– Requires cobas HPV test in ThinPrep media– Start age 25– Interval uncertain (SGO/ASCCP writing guidance)– Sensitivity is high, specificity good if:
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Summary: the 2011 standards
USPSTF ACS/ASCCP/ASCP
When to start? 21yo 21yo
How often? Q3y PapsQ5y cotests ages 30-64
Q3y Paps ages 21-29Q5y cotest ages 30-64 preferred Q3y Paps remain an option
When to stop? 65yo if adequate prior screens
65yo if 3 neg Paps or 2 neg cotestsAfter hyst for benign disease
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Conclusion
• “Perhaps the largest immediate gain in reducing burden of cervical cancer incidence and mortality could be attained by increasing access to screening (regardless of the test used) among women who are currently unscreened or screened infrequently.”
ACS, 20012