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A direct comparison of Kaiser Permanente Care Management Institute (KPCMI), Program in Evidence-based Care (PEBC), University of Michigan Health System (UMHS), and United States Preventive Services Task Force (USPSTF) recommendations for cervical cancer screening is provided in the tables below. The PEBC guideline is broader in scope than the others. In addition to general screening recommendations, PEBC includes recommendations for screening women with special circumstances (immunocompromised or HIV positive women [KPCMI also provides recommendations for this population], pregnant women, and women who have sex with women) and for managing women with abnormal cytology. All of the guidelines consider the role of new screening technologies, such as liquid-based Pap cytology and HPV testing. In formulating their recommendations, KPCMI, PEBC, and UMHS reviewed the conclusions of USPSTF.
Table 1 provides a quick-view glance at the primary interventions considered by each group. Table 2 compares the scope of each of the guidelines. Table 3 compares recommendations concerning whom to screen, screening women with a hysterectomy, and screening tests and testing frequency. Table 4 compares the potential benefits and harms associated with the implementation of each guideline. The level of evidence supporting the major recommendations in the guidelines is also identified, with the definitions of the rating schemes used by KPCMI, PEBC, UMHS, and USPSTF included in Table 5.
Following the content comparison tables, the areas of agreement and differences among the guidelines are identified.
Abbreviations used in the text and tables follow:
TABLE 3: COMPARISON OF RECOMMENDATIONS FOR CERVICAL CANCER SCREENING | |
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Whom To Test (Including when to initiate and discontinue) |
|
KPCMI |
Recommendations: Effectiveness of Cervical Cancer Primary Screening Tests in Asymptomatic, Average-Risk Women Routine cervical cancer screening is recommended for all asymptomatic, average-risk women. (Evidence-based: B) Recommendations: Optimal Age to Begin and End Screening in Asymptomatic, Average-risk Women Initiation of cervical cancer screening is recommended approximately 3 years after first sexual intercourse or by the age of 21, whichever comes first.*‡ (Consensus-based) Routine screening for cervical cancer for women older than age 65 is not recommended if they have had adequate recent screening** with normal results on their last cytology (and HPV test if applicable). (Evidence-based: D)
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PEBC |
Screening Initiation Cervical cytology screening should be initiated within three years of first vaginal sexual activity (i.e., vaginal intercourse, vaginal/oral, and/or vaginal/digital sexual activity) (C-III). Screening Cessation Screening may be discontinued after the age of 70 if there is an adequate negative screening history in the previous 10 years (i.e., 3 to 4 negative tests) (B-II). |
UMHS |
|
USPSTF |
Clinical Considerations
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Screening After Hysterectomy | |
KPCMI |
Recommendations: Optimal Cervical Cancer Screening Strategy for Women Who Have Had a Total Hysterectomy for a Benign Condition. Routine cytology screening is not recommended for women who have had a total hysterectomy for a benign condition unless there was a history of CIN grade 2/3. (Evidence-based: D) Three consecutive negative cytology results with or without HPV testing are recommended prior to discontinuation of screening in women who have a history of CIN grade 2/3 and a subsequent hysterectomy for a benign condition. (Consensus-based) |
PEBC |
|
UMHS |
Clinical Background. Women who have undergone a total hysterectomy (with removal of the cervix) for benign gynecologic disease do not need to undergo screening with vaginal cytology. However, a health care provider should confirm and/or document via physical exam and review of the pathology report (when available) that the cervix was completely removed. Women who have had a subtotal hysterectomy should continue cervical cancer screening as per current guidelines. |
USPSTF |
Clinical Considerations
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Screening Modality and Frequency | |
KPCMI |
Recommendations: Effectiveness of Cervical Cancer Primary Screening Tests in Asymptomatic, Average-Risk Women Either of the following tests are options for cervical cancer screening in asymptomatic, average-risk women under age 30.
All of the following tests are acceptable options for cervical cancer screening in asymptomatic, average-risk women age 30 and older.
No recommendation for or against routine use of computer-assisted slide evaluation or automated rescreening of cytology slides. (Evidence-based: I) Recommendations: Cervical Cancer Screening Intervals in Asymptomatic, Average-risk Women The following screening intervals are recommended:
No recommendation for or against routinely providing annual screening tests prior to beginning a triennial screening program. (Evidence-based: I) Recommendations: Triage for ASC-US Results Using HPV Testing in Asymptomatic, Average-risk Women HPV testing is recommended in women of all ages for triage of cytology results indicating ASC-US. (Evidence-based: B) No recommendation for or against the use of HPV testing to triage women with cytologic results higher than ASC-US. (Evidence-based: I) Recommendations: Screening in Women at Increased Risk of Cervical Cancer Cytology and HPV testing are recommended at 6 months following treatment for CIN grade 2/3, and again at 24 months, with colposcopy for any positive result. Routine screening every 3 years can then be resumed indefinitely. (Consensus-based) If HPV testing is not done, two cytology tests at 6 and 12 months after treatment are recommended, with colposcopy for a positive result, then annual cytologic screening indefinitely. (Consensus-based) At least annual cytology with or without HPV testing is recommended for women who are immunosuppressed or HIV-positive. (Consensus-based) Recommendation: Optimal Initial Management of Concurrent HPV-Positive and Cytology-Negative Cervical Screening Results HPV and cytology retesting is recommended in 12 months, rather than immediate colposcopy, for management of women with initial concurrent HPV-positive and cytology-negative screening results. (Consensus-based). |
PEBC |
Optimal Cervical Screening Tool
Screening Interval
Note: These recommendations do not apply to women who have had previous abnormal Pap tests. See management of abnormal cytology section in original guideline document for further information. Screening Women with Special Circumstances
Recommended Management for Women with Abnormal Cytology ASCUS (Atypical squamous cells of uncertain significance)
|
UMHS |
Modality Pap smear of cervical cells or liquid based cervical cytology (ThinPrep®). Frequency
Rationale for Recommendations Screening tests. The ThinPrep® system collects more cells and leads to better quality slides. The ThinPrep system is more sensitive (76% vs. 68%) and specific (86% vs. 79%) than Pap smear. How often should screening be done. Screening intervals will vary depending on the cytologic method used. After women have undergone an initial conventional cervical cancer screening with a Pap smear, the procedure should be performed annually until age 30. If the initial screening test was based on the ThinPrep system, the procedure should be performed at least every two years until age 30. At age 30 or older, a physician and patient may elect to reduce the frequency of screening to every 2 to 3 years if the woman is low-risk (e.g., does not have a history of in utero exposure to DES, is not immunocompromised or HIV+) and has had three consecutive normal or negative cytology results. New screening technology. The United States FDA has approved a computerized device (AutoPap 300) as an adjunct to manual screening. The system is used to rescreen negative smears and approximately 10% to 20% of slides are classified as abnormal using a computerized cellular analysis. These slides are then reviewed by a pathologist. HPV testing. While routine testing on all patients for human HPV has been proposed as an alternative screening test, the high prevalence of HPV in young women and low positive predictive value for higher-grade lesions limits its usefulness. At the University of Michigan, HPV testing for high risk subtypes is currently performed on the ThinPrep samples from patients with an ASC-US pap smear. Patients > age 20 years old and positive for high risk HPV subtypes should be referred for colposcopy. HPV testing is not recommended in women < 20 years old. For patients < 20 years old and ASC-US or low grade abnormalities, repeat pap in 1 year. Adolescent patients are extremely unlikely to develop cervical neoplasia and have a relatively high rate of clearing the virus. If repeat pap in 1 year is still abnormal, then patient should be referred for colposcopy. If negative for high risk HPV subtypes, the women may be followed with a repeat pap smear in one year, based on the negative predictive value, of our current HPV test, being 98%. |
USPSTF |
Clinical Considerations
HPV Testing in Women with ASC-US Liquid-based cytology permits testing of specimens for HPV, which may be useful in guiding management of women whose Pap smear reveals atypical squamous cells. |
Patient Education/Counseling | |
KPCMI |
No recommendations offered |
PEBC |
No recommendations offered |
UMHS |
It is important that women who may not need a cervical cytology test obtain appropriate preventive health care, including contraception and prevention counseling, and screening and treatment of sexually transmitted diseases. |
USPSTF |
No recommendations offered |
TABLE 4: BENEFITS AND HARMS | |
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Benefits | |
KPCMI |
|
PEBC |
|
UMHS |
Reductions in Cancer Incidence and Mortality Correlational studies show significant declines in both the incidence of cervical cancer and cervical cancer mortality rates in North American and western Europe following the introduction of screening programs. The reduction in mortality correlated closely with the intensity of the screening. Case control studies support the correlational data and show a decrease in the incidence of invasive cancer by 60 to 90%. Increased frequency of screening is associated with a greater reduction in rate of cervical cancer. |
USPSTF |
Reductions in Cancer Incidence and Mortality Detection of cervical cancer in its earliest stages is lifesaving, as survival of cancer of the cervix uteri depends heavily on stage at diagnosis. Although 92 percent of women will survive 5 years when the cancer is localized, only 13 percent will survive distant disease. Introduction of screening programs to populations naive to screening reduces cervical cancer rates by 60 to 90 percent within 3 years of implementation. This reduction of mortality and morbidity with introduction of the Pap test is consistent and dramatic across populations. Although no prospective trial of Pap screening has ever been conducted, correlational studies of cervical cancer trends in countries in North America and Europe demonstrate dramatic reductions in incidence of invasive cervical cancer and a 20 to 60 percent reduction in cervical cancer mortality. |
Harms | |
KPCMI |
|
PEBC |
None stated |
UMHS |
None stated |
USPSTF |
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TABLE 5: EVIDENCE RATING SCHEMES AND REFERENCES | |||||||||||||||||
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KPCMI |
Recommendations are classified as either "evidence-based (A-D, I)" or "consensus-based."
Label and Language of Recommendations*
[a] All statements specify the population for which the recommendation is intended. *Recommendations should be labeled and given an evidence grade. The evidence grade should appear in the rationale. Evidence is graded with respect to the degree it supports the specific clinical recommendation. For example, there may be good evidence that Drugs 1 and 2 are effective for Condition A, but no evidence that Drug 1 is more effective than Drug 2. If the recommendation is to use either Drug 1 or 2, the evidence is good. If the recommendation is to use Drug 1 in preference to Drug 2, the evidence is insufficient. |
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PEBC |
Quality of Evidence I: Evidence from at least 1 randomized controlled trial II: Evidence from at least 1 clinical trial without randomization, from cohort or case-controlled analytic studies, or from multiple time series studies or dramatic results from uncontrolled experiments III: Evidence from opinions of respected authorities based on clinical experience, descriptive studies, or reports of expert committees Strength of Recommendation A: Good evidence for efficacy and substantial clinical benefit support recommendation for use. B: Moderate evidence for efficacy or only limited clinical benefit support recommendation for use. C: Evidence for efficacy is insufficient to support a recommendation for or against use, but recommendations may be made on other grounds. D: Moderate evidence for lack of efficacy or for adverse outcome supports a recommendation against use. E: Good evidence for lack of efficacy or for adverse outcome supports a recommendation against use. |
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UMHS |
Levels of evidence reflect the best available literature in support of an intervention or test: A = Randomized controlled trials B = Controlled trials, no randomization C = Observational trials D = Opinion of expert panel |
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USPSTF |
Quality of Evidence The USPSTF grades the quality of the overall evidence for a service on a 3-point scale (good, fair, poor): Good: Evidence includes consistent results from well-designed, well-conducted studies in representative populations that directly assess effects on health outcomes. Fair: Evidence is sufficient to determine effects on health outcomes, but the strength of the evidence is limited by the number, quality, or consistency of the individual studies, generalizability to routine practice, or indirect nature of the evidence on health outcomes. Poor: Evidence is insufficient to assess the effects on health outcomes because of limited number or power of studies, important flaws in their design or conduct, gaps in the chain of evidence, or lack of information on important health outcomes. Strength of Recommendations The U.S. Preventive Services Task Force (USPSTF) grades its recommendations according to one of five classifications (A, B, C, D, I) reflecting the strength of evidence and magnitude of net benefit (benefits minus harms). A. The USPSTF strongly recommends that clinicians provide [the service] to eligible patients. The USPSTF found good evidence that [the service] improves important health outcomes and concludes that benefits substantially outweigh harms. B. The USPSTF recommends that clinicians provide [this service] to eligible patients. The USPSTF found at least fair evidence that [the service] improves important health outcomes and concludes that benefits outweigh harms. C. The USPSTF makes no recommendation for or against routine provision of [the service]. The USPSTF found at least fair evidence that [the service] can improve health outcomes but concludes that the balance of benefits and harms is too close to justify a general recommendation. D. The USPSTF recommends against routinely providing [the service] to asymptomatic patients. The USPSTF found at least fair evidence that [the service] is ineffective or that harms outweigh benefits. I. The USPSTF concludes that the evidence is insufficient to recommend for or against routinely providing [the service]. Evidence that the [service] is effective is lacking, of poor quality, or conflicting and the balance of benefits and harms cannot be determined. |
The Kaiser Permanente Care Management Institute (KPCMI), the Program in Evidence-based Care (PEBC), the University of Michigan Health System (UMHS), and the United States Preventive Services Task Force (USPSTF) present recommendations for cervical cancer screening. All four groups rank the level of evidence for each major recommendation. All four also provide, in narrative form, the explicit reasoning behind their judgments for all major recommendations.
The guidelines differ in scope. UMHS, for instance, in addition to its cervical cancer screening recommendations, presents recommendations for breast cancer, colorectal cancer, and prostate cancer screening (USPSTF provides recommendations for these other topics in separate guidelines). PEBC provides recommendations concerning management of women with abnormal cytology. Excepting the topic of HPV testing in screened women with abnormal cytology results, these additional topics are not included in this synthesis, which focuses on primary screening for cervical cancer.
KPCMI, UMHS, and USPSTF are in agreement concerning when to initiate cervical screening, with all three groups recommending that screening be started within 3 years after the onset of vaginal intercourse, or by age 21. PEBC agrees that screening should be started within 3 years of onset of first vaginal sexual activity, but does not include an age criterion (see Areas of Differences below).
General agreement also exists among the four guidelines concerning when to stop screening. All four groups recommend that screening be discontinued in older women who have had adequate recent screening (i.e., at least three normal Pap smears within the prior 10 years) and who have no risk factors for cervical cancer. The guidelines differ, however, concerning the precise age at which screening should be discontinued in older women; these differences are discussed below.
KPCMI, PEBC, UMHS, and USPSTF agree that screening is not necessary in women who have had a total hysterectomy for benign gynecologic disease. However, these guidelines are in general agreement regarding the need to continue screening when there is inadequate documentation of the reason for the hysterectomy and/or when risk factors for cervical cancer (such as cervical dysplasia or HPV) are present. KPCMI specifies that screening is not recommended in this population unless there was a history of CIN 2/3. They also note that three consecutive cytology results with or without HPV testing are recommended prior to discontinuation of screening in women who have a history of CIN 2/3 and a subsequent hysterectomy for a benign condition.
All of the guidelines address use of HPV DNA testing as a primary screening tool for cervical cancer (i.e., performed on all women screened), and there is overall agreement that it is not currently appropriate as a primary screening tool. USPSTF found insufficient evidence to recommend for or against the routine use of HPV testing as a primary screening test for cervical cancer. UMHS notes that while routine testing on all patients for HPV has been proposed as an alternative screening test, the high prevalence of HPV in young women and low positive predictive value for higher-grade lesions limits its usefulness. Similar to the other groups, PEBC notes that the two technology assessments (reviewed by the guideline developers) that examined HPV testing indicated that it should not be routinely recommended as a primary screening test. KPCMI notes that HPV testing has not been FDA approved as a standalone test for primary screening.
Regarding the use of HPV DNA testing combined with conventional and/or liquid-based cytology, KPCMI, PEBC, and UMHS all recommend HPV testing on liquid from the Pap test for the subset of women with an ASC-US Pap smear result (PEBC specifically notes that this applies to women aged 30 or older). (NGC note: discussion of recommendations related to follow-up for abnormal Pap smear results are beyond the scope of this synthesis. See the original guideline documents for more information on this topic).
UMHS recommends that women, particularly teens and young women, receive education about appropriate preventive health care, contraception, and prevention of sexually transmitted diseases. The other three guidelines do not address this topic.
PEBC differs from the other three guidelines in that it does not specify an age by which screening should be initiated; the other guidelines indicate screening should start within three years of onset of sexual activity or by age 21. The PEBC guideline developers chose not to include a specific age to initiate screening, citing lack of evidence to support a particular age over another. The guideline states that linking Pap testing to the initiation of vaginal sexual activity is also more practical than choosing a specific age. PEBC points out that Pap smear screening has evolved since the 1950's into a highly effective cancer prevention tool; this has occurred without randomized controlled trials, and the benefit of this test is so evident that trials involving withholding the test are unethical. Therefore, there is little evidence in the literature to indicate the optimal timing for the initiation and cessation of cervical screening. PEBC notes that previous cervical screening guidelines have made recommendations for the initiation and cessation of screening based on limited evidence, previous practice, and expert consensus.
The guidelines all recommend screening be initiated within 3 years of onset of sexual activity, but they differ in how sexual activity is defined. USPSTF uses the most general term, recommending screening begin within three years of onset of "sexual activity." UMHS, however, uses the more limited term "vaginal intercourse." KPCMI uses the term "sexual intercourse." PEBC recommends that screening begin within three years of "first vaginal sexual activity," which is defined as "vaginal intercourse, vaginal/oral and/or vaginal/digital sexual activity." PEBC justifies this recommendation by pointing out that it is recognized that vaginal transmission of HPV can occur with sexual activities other than intercourse, including vaginal/oral and/or vaginal/digital activity.
Although all four groups agree that screening can be discontinued in low-risk older women, the groups recommend different age cut-offs. PEBC recommends discontinuing screening at age 70, whereas KPCMI and USPSTF recommend stopping at age 65. USPSTF notes that it found limited evidence to determine the benefits of screening in women older than age 65, that screening women older than this is associated with an increased risk for potential harms (including false-positive results and invasive procedures), and that the potential harms are likely to exceed benefits. UMHS recommends that, for women who have previously undergone routine screening, screening be discontinued at either age 65 (citing USPSTF) or age 70 (citing ACS/NCCN). UMHS further adds that many women older than age 65 have never been screened or have been screened fewer than two times for cervical cancer and that these women would most likely benefit from continued screening efforts. Concerning this difference in opinions as to whether screening should be discontinued at age 65 or at age 70, PEBC states that the literature regarding the cessation of cervical screening is sparse and problematic. Studies have often included women who had never been screened with those who have had adequate screening histories, making an evaluation of the evidence difficult.
The organizations also differ in their recommendations concerning the screening interval for asymptomatic, low or average risk women. PEBC recommends screening be done annually until there are three consecutive negative Pap tests, and thereafter every 2 to 3 years (every 3 years if screening is supported by an adequate recall mechanism). For low-risk women, UMHS recommends that screening be done annually with conventional cytology or every 2 years with LBP technology until age 30. At that age, the screening interval can be lengthened to every 2 to 3 years (in women who have had three consecutive normal tests and are at low risk for cervical cancer).
In contrast, USPSTF found no direct evidence that annual screening achieves better outcomes than screening every 3 years; it recommends screening be done (with conventional smears) at least every 3 years for all women. KPCMI similarly recommends that asymptomatic, average-risk women should have cytology (either conventional or LBP cytology is appropriate) every 3 years. They also recommend an interval of 3 years for cytology and HPV testing (recommended for women aged 30 and older). In contrast to UMHS and PEBC, KPCMI makes no recommendation for or against routinely providing annual screening tests prior to beginning a triennial screening program. USPSTF similarly acknowledges that most organizations in the U.S. recommend that annual Pap smears be performed until a specified number (usually 2 or 3) are cytologically normal before lengthening the screening interval, but states that data are limited to determine the benefits of this strategy.
KPCMI, PEBC, and UMHS agree that annual cytology is recommended for high-risk women (such as women with previous abnormal Pap tests, women that are immunocompromised, HIV positive women). USPSTF does not provide formal recommendations regarding the high-risk population, but notes that liquid-based cytology permits testing of specimens for HPV, which may be useful in guiding management of women whose Pap smear reveals atypical squamous cells.
KPCMI, PEBC and UMHS recommend both conventional and LBP technology. UMHS finds that the ThinPrep® LBP system collects more cells, leads to better quality slides, and is both more sensitive and specific than the Pap smear. PEBC recommends LBP cytology as the preferred tool, although conventional smear technology is an acceptable alternative. KPCMI notes that both conventional and liquid-based cytology testing are options. In contrast to the other three guidelines, USPSTF found insufficient evidence to make a recommendation either for or against LBP technology, noting that evidence to determine the sensitivity and specificity of LBP cytology is limited, that no studies of LBP cytology have assessed cervical cancer outcomes, and that LBP cytology (ThinPrep®, AutoCyte PREP®) is cost-effective only if used at screening intervals of 3 years or longer.
The choice of screening technology impacts on the recommended screening interval. UMHS recommends that a longer screening interval be used with LBP cytology (i.e., at least every 2 years until age 30) than with conventional cytology (i.e., annually until age 30). PEBC also points out that the introduction of LBP technology will lead to increased costs that will have to be balanced with other screening efficiencies.
In contrast to the other three groups, which all provide specific recommendations regarding the use of HPV testing, USPSTF notes that they found poor evidence to determine the benefits and potential harms of HPV screening as an adjunct or alternative to regular Pap smear screening. Unlike the other three guidelines, the USPSTF guideline was released prior to FDA approval of a combined HPV/cytology screening procedure. They note, however, that liquid-based cytology permits testing of specimens for HPV, which may be useful in guiding management of women whose Pap smear reveals ASC.
In contrast to PEBC and UMHS, both of which recommend HPV testing only in the event of ASC-US, KPCMI is the only group to recommend combined use of cytology and HPV for asymptomatic, low or average risk women. KPCMI notes that cytology (conventional or liquid-based) and HPV testing is an acceptable option for screening in asymptomatic, average-risk women age 30 and older.
This Synthesis was prepared by ECRI on September 1, 2005. The information was verified by UMHS on October 5, 2005, and by USPSTF on October 14, 2005. This synthesis was revised March 3, 2006 to include new recommendations from the Cancer Care Ontario Program in Evidence-based Care (PEBC). The updated information was verified by PEBC on April 5, 2006. The information was updated on October 26, 2007 to remove BWH recommendations and again on November 27, 2007 to remove recommendations from ACS. This synthesis was revised on January 27, 2008 to add KPCMI recommendations. The information was verified by KPCMI on February 22, 2008.
Internet citation: National Guideline Clearinghouse (NGC). Guideline synthesis: Screening for cervical cancer. In: National Guideline Clearinghouse (NGC) [website]. Rockville (MD): 2005 Oct (revised 2008 Mar). [cited YYYY Mon DD]. Available: http://www.guideline.gov.