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The Usefulness of HPV Testing ?

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Title: The Usefulness of HPV Testing ?


1
The Usefulness of HPV Testing ?
  • Nick Dudding
  • East Pennine Cytology Training Centre

2
Age-standardised incidence of invasive cervical
cancer (total) and adenocarcinoma of the cervix.
England and Wales 1971-2001
Cancer Trends Office for National Statistics
3
The cervical cancer epidemic that screening has
prevented in the UK
Peto et al. Lancet 2004 364 249
4
Liquid Based Cytology
  • That was all before we started LBC which will
    have improved things even further

5
The Future ?
  • Despite success of LBC still tremendous pressure
    for more change
  • HPV testing
  • Vaccination
  • Automated Screening
  • Molecular markers

6
Why HPV Testing ?
  • HPV is the principal cause of invasive cervical
    cancer and CIN
  • Human papillomavirus is a necessary cause of
    invasive cervical cancer worldwide. JMM
    Walboomers et al. J Pathol 1999 189 12-19
  • The causal relation between human papillomavirus
    and cervical cancer. FX Bosch et al. J Clin Path
    2002 55 244-265

7
Biology of HPV
  • Persistence, type and (? viral load) are the
    important risk factors for CIN
  • High risk HPV types and infection with
  • Multiple HPV types increase risk

8
Biology of HPV
  • High risk types
  • 16, 18, 31, 33, 35, 39, 45, 51, 52, 56, 58, 59,
    6, 73, 82

Munoz et al. NEJM 2003 348 518
9
Biology of HPV
  • HPV infection very common in sexually active
    young women
  • Prevalence drops in women over 30 years
  • Median duration of new infection 8 14 months
  • 40 persistent at 12 24 months

10
ARTISTIC Trial HPV Prevalence by Age at
entryCourtesy of Dr Desai
11
HPV in Cervical Screening
  • What are the potential advantages of HPV testing
    that with regards to cervical screening ?

12
HPV in Cervical Screening
  • Negative predictive value of high risk HPV is
    very high
  • A woman not infected with high risk HPV is at
    almost no risk of developing cervical cancer in
    next ten years
  • It has a high sensitivity
  • Most women with high grade CIN will be identified
    by HPV testing

13
HPV in Cervical Screening
  • Many HPV positive women will NOT have high grade
    disease
  • They have an infection !!!
  • Positive predictive value of high risk HPV is low
  • Lower specificity than cytology
  • More limited utility in under 30,s where
    prevalence is higher

14
HPV in Cervical Screening
  • How might we use it in cervical screening ?

15
HPV in Cervical Screening
  • Triage of low-grade samples
  • Follow-up after treatment
  • Primary screening

16
HPV in Cervical Screening
  • How might we test ?
  • PCR based Tests
  • HCII

17
HC II
  • Easy to do - Simple kit
  • Identifies if any of 13 high risk types are
    present
  • Highly consistent reproducible
  • Cant give info on individual types
  • Important since 16 carries far more risk
  • Needs to be batched to be cost effective

18
Triage of low-grade samples
Borderline or mild dyskaryosis
HPV Test

-
Refer
Repeat / routine
19
Triage of low grade samples
  • Speed up referral
  • Reduce number of re-tests
  • Return women to normal recall earlier
  • Avoid referral for those that don't need it

20
Triage of low-grade samples
  • Positive HPV test more sensitive than repeat
    cytology in triage of women with low grade smear
    abnormality
  • Kaiser-Permanente Study
  • ALTS (ASCUS/LSIL Triage Study)

Manos. JAMA 1999 281 1605 Koutsky et al. JNCI
200092397-402
21
Triage of low-grade samples
  • Abandoned triage of mild dyskaryosis !
  • For ASCUS (BNC) cases
  • One HPV test is as sensitive as serial cytology,
    taken every 6 months over two years

22
Triage of low-grade samples
  • Supported by a Met analysis carried out by Arbyn
  • Triage more sensitive than repeat cytology for
    ASCUS (BNC)
  • Not useful in triage of mild dys

Arbyn 2005 Gynae Oncol 99S7 S11
23
HPV triage in UK ?
  • NHS LBC pilots
  • 45 BNC 82 Mild were HPV positive
  • Reduced rate of repeat smears
  • 52 86
  • Increase in rates of referral to colposcopy
  • 64 138

Legood. BMJ 2006 332 79-83 Moss. BMJ 2006 332
83-85
24
HPV triage in UK ?
  • Cost effective under current UK screening
    protocols
  • Appropriate management strategies would need to
    be developed

Legood. BMJ 2006 332 79-83 Moss. BMJ 2006 332
83-85
25
TOMBOLA
  • Trial Of Management of Borderline and Other Low
    grade Abnormal smears
  • Based on conventional samples
  • Expected to report anytime now
  • First indications NOT as positive as one might
    have expected

26
TOMBOLA
  • BSCC 2007
  • 34 of women with BNC HPV positive
  • 61 of women with mild dys HPV positive
  • A single HPV test insufficient to warrant
    colposcopy
  • No compelling economic reason to adopt Triage

27
Sentinel sites
  • NHSCSP has started rolling out HPV triage via
    sentinel sites
  • Just started
  • 6 centres
  • Sheffield, Norfolk Norwich, Bristol,
    Manchester, Liverpool and Northwick park
  • Using HC II
  • HPV testing carried out in Manchester

28
Sentinel protocol
  • BNC / Mild dys HPV positive
  • refer
  • At Colp
  • High grade CIN treat
  • CIN I / neg colp / mild dys gt
  • cytology again at 6 months

29
Summary - Triage
  • We await results with interest
  • Efficacy of triage for BNC is almost certain
  • Less certain for mild
  • ? Refer HPV positive women straight away or
    repeat again in 6 or 12 months
  • To look closely at cost effectiveness
  • Particularly the link with 14 day turnaround
  • Will LBC increase performance of cytology ?

30
Follow up after Treatment
  • Currently women with excised / treated CIN II /
    III are followed by annual smears for 10 years

31
Follow up after Treatment
  • Also being investigated by the Sentinel sites
  • HPV and cytology at 6 months
  • If negative routine recall
  • If HPV cytology positive gt colposcopy
  • If only one positive, another cytology test in 6
    months.

32
Summary - Follow up after Treatment
  • Within UK programme seems to carry enormous
    benefits

33
Primary Screening by HPV Testing
  • Sensitivity of HPV testing is higher than
    cytology,
  • Direct referral for colposcopy of all women aged
    gt 30 who are HPV positive in one screening round
    would detect almost all high-grade CIN and
    invasive cancer
  • (Meijer 2000)

34
Primary Screening by HPV Testing
  • Remember however that many of these women do not
    have HG disease at that time
  • Just a viral infection that might regress
  • 10 year risk of CIN III with HPV ve test
  • 13.6 in younger women
  • 21 in older women (Kjear et al. Cancer
    Res200666(21)10630-6)
  • Increase referrals to colposcopy
  • Sacrifice specificity for sensitivity ?

35
HART study (HPV in Addition to Routine Testing)
  • HPV testing could be used for primary
    screening in women older than 30 years, with
    cytology used to triage HPV-positive women.
  • HPV-positive women with normal or borderline
    cytology could be managed by repeat testing after
    12 months.

Cuzick et al. Lancet 2003 362 1871-1876
36
Primary Screening by HPV Testing
  • POBOSCAM Oct 2007 Lancet
  • Naucler Sweden NEJM Oct 2007
  • Both compared conventional Pap smears to HPV
    testing by PCR
  • Both suggested that you detect CIN III earlier
  • Can safely extend screening interval to six
    years!

37
Primary Screening by HPV Testing
  • Both detect high grade CIN earlier
  • Could be detecting some CIN II / III that might
    have regressed (esp CIN II)
  • Might need a better test that can separate
    regressive from progressive HPV infections might
    be needed

Khan et al. J Natl Cancer Inst 2005 97 1072-0
38
Primary Screening by HPV Testing
  • Both do not take into account the vast difference
    between conventional LBC samples
  • Do not take into account women aged lt 30
  • Everyone retrained
  • Artistic gives a glimpse of this!

39
ARTISTIC TRIAL
  • A Randomised Trial In Screening To Improve
    Cytology
  • 25,000 women (20 65) in Manchester
  • Investigating potential of primary screening
  • Doing a cost benefit analysis
  • Expecting full results anytime now
  • First results NOT as good as expected

40
ARTISTIC TRIAL
  • Preliminary data suggests that liquid based
    cytology plus HPV is NOT more sensitive over 2
    screening rounds than cytology alone

41
ARTISTIC TRIAL
  • High grade dyskaryosis rates over study period
  • Revealed arm (effect of HPV Cyto)
  • 1.9 - 0.37
  • Concealed arm (effect of LBC only)
  • 1.6 - 0.33

42
ARTISTIC TRIAL
  • ARTISTIC has been extended to 6 years

43
Summary - HPV Testing
  • Offers potential
  • Might add cost so will have to do the cost
    benefit analyses
  • Appropriate management strategies
  • Will have to decide which way to test
  • PCR v Hybrid capture
  • Improve specificty of HPV testing by using
    techniques that home in on individual types
  • Work out how to deal with those aged lt 30

44
Summary - HPV Testing
  • Pity we couldnt let LBC bed in
  • None of big studies compare with LBC and ARTISTIC
    gives a glimpse of what might have been achieved
  • Need to look at impact on laboratories 14 day
    turnaround
  • Automation could make HPV testing less
    competitive

45
Summary - HPV Testing
  • CONCERNS
  • A lack of knowledge in the general public
  • Could money be better spent on coverage ?

46
HPV Testing
  • Excessive or misguided use of HPV testing will
    increase costs without adding benefit
  • Like most revolutionary technologies, HPV
    testing must be managed wisely to do good rather
    than harm

Mark Schiffman. BMJ 200633261-62
47
Vaccination
  • Currently two on the market
  • Gardasil (Merck) protects against
  • HPV 16, 18 6, 11
  • Cervarix (GSK) protects against
  • HPV 16,18

48
Vaccination
  • In UK should start this September
  • Start at 12, 2 year opt in up to 18
  • In UK expect decision on which soon
  • As of October 2007
  • Gardisal licensed in 80 countries
  • Cervarix in 30

49
Vaccination
  • It will cost around 250 for the three doses
    needed.
  • Gardisal also protects against 6 11 and will
    thus reduce the problems caused by genital warts
  • GSK has a stronger adjuvant and possibly better
    cross protection
  • ? HPV types 45, 31 52

50
Vaccination
  • Politically driven decision
  • Add massive cost
  • Screening will have to continue

51
Prophylactic Vaccines
  • Can you think of any potential problems?

52
Prophylactic Vaccines
  • Problems?
  • Everyone has to the vaccine
  • Doesnt protect against all cancers so screening
    will have to continue

53
HPV types in Cervical Cancer
57.6
16
vaccine types
71.7
18
77.4
45
81.3
31
85.0
X
87.9
33
90.1
52
91.8
58
93.3
35
94.6
59
95.7
56
0
20
40
60
80
100
Proportion of cancers associated with HPV types
HPV 16/18 vaccine could prevent gt 70 of cervical
cancers
Munoz N, Bosch FX, et al. IARC Multicenter
Cervical Cancer Study Group. N Engl J Med 2003
348 51827.
54
Prophylactic Vaccines
  • Problems?
  • What might happen to coverage
  • Will have marked effect on the method of
    screening
  • Some suggesting we will need HPV or automation

55
Summary
  • Screening as we know it is under considerable
    threat
  • None of the modalities discussed however will
    remove need for screening
  • Screening will continue but how and where?
  • Money better spent on improving coverage?

56
The Future ?
  • Must make sure that new tests are brought into
    the cytology laboratory
  • Often assumed that new tests such as hybrid
    capture and the molecular tests will be done in
    specialist or virology labs
  • These labs are optimally staffed

57
The Future ?
  • Since Cytology laboratories would have the staff
    and space we should take on these roles
  • UK BMS staff with their strong generic training
    are well placed to adapt to such tests
  • Ensure managers are aware of this

58
Contact details
  • Nick.dudding_at_sth.nhs.uk
  • 0114 271 2538
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