Section 2. Recommendations for Adults
Cancer
Screening for Bladder Cancer in Adults
Summary of Recommendation
The U.S. Preventive Services Task Force
(USPSTF) recommends against routine screening
for bladder cancer in adults.
Rating: D Recommendation.
|
This USPSTF recommendation was first published by:
Agency for Healthcare Research and Quality, Rockville,
MD. June 2004. http://www.ahrq.gov/clinic/3rduspstf/bladder/blacanrs.htm.
Clinical Considerations
- Bladder cancer is 2 to 3 times more common in men than in women and is unusual before age 50. Bladder cancer is heterogeneous; it is a spectrum of conditions, most of which are not life-threatening.
- Screening tests—such as microscopic urinalysis, urine dipstick, urine
cytology, or such new tests as bladder tumor antigen (BTA) or nuclear matrix
protein (NMP22) immunoassay—can detect bladder cancers that are clinically
unapparent. However, because of the low prevalence of bladder cancer, the
positive predictive value of these tests is low.
- Smoking increases the risk for bladder cancer; about 50% of all cases of
bladder cancer occur in current or former smokers. Smokers should be counseled
on quitting smoking.
- People in occupations that involve exposure to chemicals used in the dye or rubber industries may also have increased risk for bladder cancer. The USPSTF did not review the evidence for targeted screening for those with occupational exposure.
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Genetic Risk Assessment and BRCA Mutation Testing for Breast and Ovarian Cancer Susceptibility
Summary of Recommendations
The U.S. Preventive Services Task Force
(USPSTF) recommends against routine referral for
genetic counseling or routine breast cancer
susceptibility gene (BRCA) testing for women
whose family history is not associated with an
increased risk for deleterious mutations in breast
cancer susceptibility gene 1 (BRCA1) or breast
cancer susceptibility gene 2 (BRCA2).
Rating: D Recommendation.
The USPSTF recommends that women whose
family history is associated with an increased risk
for deleterious mutations in BRCA1 or BRCA2
genes be referred for genetic counseling and
evaluation for BRCA testing.
Rating: B Recommendation.
|
This USPSTF recommendation was first published in Ann Intern Med. 2005;143:355-361. http://www.ahrq.gov/clinic/uspstf05/brcagen/brcagenrs.htm.
Clinical Considerations
- These recommendations apply to women who have not received a diagnosis of breast or ovarian cancer. They do not apply to women with a family history of breast or ovarian cancer that includes a relative with a known deleterious mutation in BRCA1 or BRCA2 genes; these women should be referred for genetic counseling. These recommendations do not apply to men.
- Although there currently are no standardized referral criteria, women with an increased-risk family history should be considered for genetic counseling to further evaluate their potential risks.
- Certain specific family history patterns are associated with an increased risk for deleterious mutations in the BRCA1 or BRCA2 gene. Both maternal and paternal family histories are important. For non-Ashkenazi Jewish women, these patterns include 2 first-degree relatives with breast cancer, 1 of whom received the diagnosis at age 50 years or younger; a combination of 3 or more first- or second-degree relatives with breast cancer regardless of age at diagnosis; a combination of both breast and ovarian cancer among first- and second-degree relatives; a first-degree relative with bilateral breast cancer; a combination of 2 or more first- or second-degree relatives with ovarian cancer regardless of age at diagnosis; a first- or second-degree relative with both breast and ovarian cancer at any age; and a history of breast cancer in a male relative.
- For women of Ashkenazi Jewish heritage, an increased-risk family history includes any first-degree relative (or 2 second-degree relatives on the same side of the family) with breast or ovarian cancer.
- About 2 percent of adult women in the general population have an increased-risk family history as defined here. Women with none of these family history patterns have a low probability of having a deleterious mutation in BRCA1 or BRCA2 genes.
- Computational tools are available to predict the risk for clinically important BRCA mutations (that is, BRCA mutations associated with the presence of breast cancer, ovarian cancer, or both), but these tools have not been verified in the general population. There is no empirical evidence concerning the level of risk for a BRCA mutation that merits referral for genetic counseling.
- Not all women with a potentially deleterious BRCA mutation will develop breast or ovarian cancer. In a woman who has a clinically important BRCA mutation, the probability of developing breast or ovarian cancer by age 70 years is estimated to be 35 percent to 84 percent for breast cancer and 10 percent to 50 percent for ovarian cancer.
- Appropriate genetic counseling helps women make informed decisions, can improve their knowledge and perception of absolute risk for breast and ovarian cancer, and can often reduce anxiety. Genetic counseling includes elements of counseling; risk assessment; pedigree analysis; and, in some cases, recommendations for testing for BRCA mutations in affected family members, the presenting patient, or both. It is best delivered by a suitably trained health care provider.
- A BRCA test is typically ordered by a physician. When done in concert with genetic counseling, the test assures the linkage of testing with appropriate management decisions. Genetic testing may lead to potential adverse ethical, legal, and social consequences, such as insurance and employment discrimination; these issues should be discussed in the context of genetic counseling and evaluation for testing.
- Among women with BRCA1 or BRCA2 mutations, prophylactic mastectomy or oophorectomy decreases the incidence of breast and ovarian cancer; there is inadequate evidence for mortality benefits. Chemoprevention with selective estrogen receptor modulators may decrease incidence of estrogen receptor-positive breast cancer; however, it is also associated with adverse effects, such as pulmonary embolism, deep venous thrombosis, and endometrial cancer. Most breast cancer associated with BRCA1 mutations is estrogen receptornegative and thus is not prevented by tamoxifen. Intensive screening with mammography has poor sensitivity, and there is no evidence of benefit of intensive screening for women with BRCA1 or BRCA2 gene mutations. Magnetic resonance imaging (MRI) may detect more cases of cancer, but the effect on mortality is not clear.
- Women with an increased-risk family history are at risk not only for deleterious BRCA1 or BRCA2 mutations but potentially for other unknown mutations as well. Women with an increased-risk family history who have negative results on tests for BRCA1 and BRCA2 mutations may also benefit from surgical prophylaxis.
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Chemoprevention of Breast Cancer
Summary of Recommendations
The U.S. Preventive Services Task Force
(USPSTF) recommends against routine use of
tamoxifen or raloxifene for the primary prevention
of breast cancer in women at low or average risk
for breast cancer. (See Clinical Considerations for a
discussion of risk.)
Rating: D Recommendation.
The USPSTF recommends that clinicians
discuss chemoprevention with women at high risk
for breast cancer and at low risk for adverse effects
of chemoprevention. (See Clinical Considerations
for a discussion of risk.) Clinicians should inform
patients of the potential benefits and harms of
chemoprevention.
Rating: B Recommendation.
|
This USPSTF recommendation was first published in: Ann Intern Med 2002; 137(1):56-8. http://www.ahrq.gov/clinic/3rduspstf/breastchemo/breastchemorr.htm.
Clinical Considerations
Clinicians should consider both the risk for breast cancer and the risk for adverse effects when identifying women who may be candidates for chemoprevention.
Risk for breast cancer. Older age; a family history of breast cancer in a mother, sister, or daughter; and a history of atypical hyperplasia on a breast biopsy are the strongest risk factors for breast cancer. Table 1 indicates how the estimated benefits of tamoxifen vary depending on age and family history. Other factors that contribute to risk include race, early age at menarche, pregnancy history (nulliparity or older age at first birth), and number of breast biopsies. The risk for developing breast cancer within the next 5 years can be estimated using risk factor information by completing the National Cancer Institute Breast Cancer Risk Tool (the "Gail model," available at http://cancer.gov/bcrisktool/ or 800-4-CANCER). Clinicians can use this information to help individual patients considering tamoxifen therapy estimate the potential benefit. However, the validity, feasibility, and impact of using the Gail model to identify appropriate candidates for chemoprevention have not been tested in a primary care setting. The Gail model does not incorporate estradiol levels or estrogen use, factors that some studies suggest may influence the effectiveness of tamoxifen.
Risk for adverse effects. Women are at lower risk for adverse effects from chemoprevention if they are younger; have no predisposition to thromboembolic events such as stroke, pulmonary embolism, or deep venous thrombosis; or do not have a uterus.
- In general, the balance of benefits and harms of chemoprevention is more favorable for:
- Women in their 40s who are at increased risk for
breast cancer and have no predisposition to
thromboembolic events.
- Women in their 50s who are at increased risk for
breast cancer, have no predisposition to
thromboembolic events, and do not have a
uterus. For example, a woman who is 45 years of age and has a mother, sister, or daughter with
breast cancer would have approximately a 1.6
percent risk for developing breast cancer over the
next 5 years (Table 1). On average, treating such
women with tamoxifen for 5 years would
prevent about three times as many invasive
cancers (8 per 1,000) as the number of serious
thromboembolic complications caused (1 stroke
and 1 to 2 pulmonary emboli per 1,000).
Among women 55 years of age, benefits exceed
harms only for those who are not at risk for
endometrial cancer; and the margin of benefit is
small unless risk for breast cancer is substantially
increased (for example, 4% over 5 years).
- Women younger than 40 years of age have a lower
risk for breast cancer, and thus will not experience
as large an absolute benefit from breast cancer
chemoprevention as older women. Women 60 years
of age and older, who have the highest risk for
breast cancer also have the highest risk for
complications from chemoprevention, with a less
favorable balance of benefits and harms.
- The USPSTF found more evidence for the benefits
of tamoxifen than for the benefits of raloxifene.
Currently, only tamoxifen is approved by the U.S.
Food and Drug Administration (FDA) for the
specific indication of breast cancer
chemoprevention. Although there are biological
reasons to suspect that raloxifene should have
similar benefits, trial data currently are limited to one study in which the primary outcome was
fracture prevention. Additional trials to further
evaluate this drug's efficacy for breast cancer
chemoprevention are underway, including a trial
comparing efficacy and safety of raloxifene and
tamoxifen. Raloxifene is approved by the FDA for
preventing and treating osteoporosis.
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Screening for Breast Cancer
Summary of Recommendations
The U.S. Preventive Services Task Force
(USPSTF) recommends screening mammography,
with or without clinical breast examination (CBE),
every 1-2 years for women aged 40 and older.
Rating: B Recommendation.
The USPSTF concludes that the evidence is
insufficient to recommend for or against routine
CBE alone to screen for breast cancer.
Rating: I Recommendation.
The USPSTF concludes that the evidence is
insufficient to recommend for or against teaching
or performing routine breast self-examination
(BSE). Rating: I Recommendation.
|
This USPSTF recommendation was first published in: Ann Intern Med 2002;137(Part 1):344-6. http://www.ahrq.gov/clinic/3rduspstf/breastcancer/brcanrr.htm.
Clinical Considerations
- The precise age at which the benefits from
screening mammography justify the potential harms
is a subjective judgment and should take into
account patient preferences. Clinicians should
inform women about the potential benefits
(reduced chance of dying from breast cancer),
potential harms (e.g., false-positive results,
unnecessary biopsies), and limitations of the test
that apply to women their age. Clinicians should
tell women that the balance of benefits and
potential harms of mammography improves with
increasing age for women between the ages of 40
and 70.
- Women who are at increased risk for breast cancer
(e.g., those with a family history of breast cancer in a
mother or sister, a previous breast biopsy revealing
atypical hyperplasia, or first childbirth after age 30)
are more likely to benefit from regular
mammography than women at lower risk. The
recommendation for women to begin routine
screening in their 40s is strengthened by a family
history of breast cancer having been diagnosed
before menopause.
- The USPSTF did not examine whether women
should be screened for genetic mutations (e.g.,
BRCA1 and BRCA2) that increase the risk for
developing breast cancer, or whether women with
genetic mutations might benefit from earlier or
more frequent screening for breast cancer.
- In the trials that demonstrated the effectiveness of
mammography in lowering breast cancer mortality,
screening was performed every 12-33 months. For
women aged 50 and older, there is little evidence to
suggest that annual mammography is more effective
than mammography done every other year. For
women aged 40-49, available trials also have not
reported a clear advantage of annual mammography
over biennial mammography. Nevertheless, some
experts recommend annual mammography based
on the lower sensitivity of the test and on evidence
that tumors grow more rapidly in this age group.
- The precise age at which to discontinue screening
mammography is uncertain. Only 2 randomized
controlled trials enrolled women older than 69 and
no trials enrolled women older than 74. Older
women face a higher probability of developing and
dying from breast cancer but also have a greater
chance of dying from other causes. Women with
comorbid conditions that limit their life expectancy
are unlikely to benefit from screening.
- Clinicians should refer patients to mammography
screening centers with proper accreditation and
quality assurance standards to ensure accurate
imaging and radiographic interpretation. Clinicians
should adopt office systems to ensure timely and
adequate followup of abnormal results. A listing of
accredited facilities is available at www.fda.gov/cdrh/mammography/certified.html.
- Clinicians who advise women to perform BSE or
who perform routine CBE to screen for breast
cancer should understand that there is currently
insufficient evidence to determine whether these
practices affect breast cancer mortality, and that
they are likely to increase the incidence of clinical
assessments and biopsies.
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Screening for Cervical Cancer
Summary of Recommendations
The U.S. Preventive Services Task Force
(USPSTF) strongly recommends screening for
cervical cancer in women who have been sexually
active and have a cervix. Rating: A
Recommendation.
The USPSTF recommends against routinely
screening women older than age 65 for cervical
cancer if they have had adequate recent screening
with normal Pap smears and are not otherwise at
high risk for cervical cancer (go to Clinical
Considerations). Rating: D Recommendation.
The USPSTF recommends against routine Pap
smear screening in women who have had a total
hysterectomy for benign disease. Rating: D
Recommendation.
The USPSTF concludes that the evidence is
insufficient to recommend for or against the
routine use of new technologies to screen for
cervical cancer. Rating: I Recommendation.
The USPSTF concludes that the evidence is
insufficient to recommend for or against the
routine use of human papillomavirus (HPV)
testing as a primary screening test for cervical
cancer. Rating: I Recommendation.
|
This USPSTF recommendation was first published by:
Agency for Healthcare Research and Quality, Rockville,
MD. January 2003. http://www.ahrq.gov/clinic/uspstf/
uspscerv.htm.
Clinical Considerations
- The goal of cytologic screening is to sample the
transformation zone, the area where physiologic
transformation from columnar endocervical
epithelium to squamous (ectocervical) epithelium
takes place and where dysplasia and cancer arise. A
meta-analysis of randomized trials supports the
combined use of an extended tip spatula to sample
the ectocervix and a cytobrush to sample the
endocervix.2
- The optimal age to begin screening is unknown.
Data on natural history of HPV infection and the
incidence of high-grade lesions and cervical cancer
suggest that screening can safely be delayed until 3
years after onset of sexual activity or until age 21,
whichever comes first.3 Although there is little value
in screening women who have never been sexually
active, many U.S. organizations recommend routine
screening by age 18 or 21 for all women, based on
the generally high prevalence of sexual activity by
that age in the U.S. and concerns that clinicians
may not always obtain accurate sexual histories.
- Discontinuation of cervical cancer screening in older
women is appropriate, provided women have had
adequate recent screening with normal Pap results.
The optimal age to discontinue screening is not clear,
but risk of cervical cancer and yield of screening
decline steadily through middle age. The USPSTF
found evidence that yield of screening was low in
previously screened women after age 65. New
American Cancer Society (ACS) recommendations
suggest stopping cervical cancer screening at age 70.
Screening is recommended in older women who
have not been previously screened, when
information about previous screening is unavailable,
or when screening is unlikely to have occurred in
the past (e.g., among women from countries without
screening programs). Evidence is limited to define
"adequate recent screening." The ACS guidelines
recommend that older women who have had three
or more documented, consecutive, technically
satisfactory normal/negative cervical cytology tests,
and who have had no abnormal/positive cytology
tests within the last 10 years, can safely stop
screening.3
- The USPSTF found no direct evidence that annual
screening achieves better outcomes than screening
every 3 years. Modeling studies suggest little added
benefit of more frequent screening for most women.
The majority of cervical cancers in the United
States occur in women who have never been
screened or who have not been screened within the
past 5 years; additional cases occur in women who
do not receive appropriate followup after an
abnormal Pap smear.4,5 Because sensitivity of a
single Pap test for high-grade lesions may only be
60-80 percent, however, most organizations in the United
States recommend that annual Pap smears be
performed until a specified number (usually two or
three) are cytologically normal before lengthening
the screening interval.6 The ACS guidelines suggest
waiting until age 30 before lengthening the
screening interval3; the American College of
Obstetricians and Gynecologists (ACOG) identifies
additional risk factors that might justify annual
screening, including a history of cervical neoplasia,
infection with HPV or other sexually transmitted
diseases (STDs), or high-risk sexual behavior,7 but
data are limited to determine the benefits of these
strategies.7
- Discontinuation of cytological screening after total
hysterectomy for benign disease (e.g., no evidence of
cervical neoplasia or cancer) is appropriate given the
low yield of screening and the potential harms from
false-positive results in this population.8,9 Clinicians
should confirm that a total hysterectomy was
performed (through surgical records or inspecting
for absence of a cervix); screening may be
appropriate when the indications for hysterectomy
are uncertain. ACS and ACOG recommend
continuing cytologic screening after hysterectomy
for women with a history of invasive cervical cancer
or DES exposure due to increased risk for vaginal
neoplasms, but data on the yield of such screening
are sparse.
- A majority of cases of invasive cervical cancer occur
in women who are not adequately screened.4,5
Clinicians, hospitals, and health plans should
develop systems to identify and screen the subgroup
of women who have had no screening or who have
had inadequate past screening.
- Newer Food and Drug Administration (FDA)-approved technologies, such as the liquid-based cytology (e.g., ThinPrep®), may have improved
sensitivity over conventional Pap smear screening,
but at a considerably higher cost and possibly with
lower specificity. Even if sensitivity is improved,
modeling studies suggest these methods are not
likely to be cost-effective unless used with screening
intervals of 3 years or longer. 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. HPV
DNA testing for primary cervical cancer screening
has not been approved by the FDA and its role in
screening remains uncertain.
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Screening for Colorectal Cancer
Summary of Recommendation
The U.S. Preventive Services Task Force
(USPSTF) strongly recommends that clinicians
screen men and women 50 years of age or older for
colorectal cancer. Rating: A Recommendation.
|
This USPSTF recommendation was first published in: Ann Intern Med 2002;137:129-31. http://www.ahrq.gov/clinic/3rduspstf/colorectal/colorr.htm.
Clinical Considerations
- Potential screening options for colorectal cancer
include home fecal occult blood testing (FOBT),
flexible sigmoidoscopy, the combination of home
FOBT and flexible sigmoidoscopy, colonoscopy,
and double-contrast barium enema. Each option
has advantages and disadvantages that may vary for
individual patients and practice settings. The choice
of specific screening strategy should be based on
patient preferences, medical contraindications,
patient adherence, and available resources for testing
and followup. Clinicians should talk to patients
about the benefits and potential harms associated
with each option before selecting a screening
strategy.
- The optimal interval for screening depends on the
test. Annual FOBT offers greater reductions in
mortality rates than biennial screening but produces
more false-positive results. A 10-year interval has
been recommended for colonoscopy on the basis of
evidence regarding the natural history of
adenomatous polyps. Shorter intervals (5 years)
have been recommended for flexible sigmoidoscopy
and double-contrast barium enema because of their
lower sensitivity, but there is no direct evidence
with which to determine the optimal interval for
tests other than FOBT. Case-control studies have
suggested that sigmoidoscopy every 10 years may be
as effective as sigmoidoscopy performed at shorter
intervals.
- The USPSTF recommends initiating screening at
50 years of age for men and women at average risk
for colorectal cancer, based on the incidence of
cancer above this age in the general population. In
persons at higher risk (for example, those with a
first-degree relative who receives a diagnosis with
colorectal cancer before 60 years of age), initiating
screening at an earlier age is reasonable.
- Expert guidelines exist for screening very high-risk
patients, including those with a history suggestive of
familial polyposis or hereditary nonpolyposis colorectal cancer, or those with a personal history of ulcerative colitis.10 Early screening with colonoscopy
may be appropriate, and genetic counseling or
testing may be indicated for patients with genetic
syndromes.
- The appropriate age at which colorectal cancer
screening should be discontinued is not known.
Screening studies have generally been restricted to
patients younger than 80 years of age, with
colorectal cancer mortality rates beginning to
decrease within 5 years of initiating screening. Yield
of screening should increase in older persons
(because of higher incidence of colorectal cancer),
but benefits may be limited as a result of competing
causes of death. Discontinuing screening is therefore
reasonable in patients whose age or comorbid
conditions limit life expectancy.
- Proven methods of FOBT screening use guaiac-based
test cards prepared at home by patients from
three consecutive stool samples and forwarded to
the clinician. Whether patients need to restrict their
diet and avoid certain medications is not
established. Rehydration of the specimens before
testing increases the sensitivity of FOBT but
substantially increases the number of false-positive
test results. Neither digital rectal examination
(DRE) nor the testing of a single stool specimen
obtained during DRE is recommended as an
adequate screening strategy for colorectal cancer.
- The combination of FOBT and sigmoidoscopy may
detect more cancers and more large polyps than
either test alone, but the additional benefits and
potential harms of combining the 2 tests are
uncertain. In general, FOBT should precede
sigmoidoscopy because a positive test result is an
indication for colonoscopy, obviating the need for
sigmoidoscopy.
- Colonoscopy is the most sensitive and specific test
for detecting cancer and large polyps but is
associated with higher risks than other screening
tests for colorectal cancer. These include a small risk
for bleeding and risk for perforation, primarily
associated with removal of polyps or biopsies
performed during screening. Colonoscopy also
usually requires more highly trained personnel,
overnight bowel preparation, sedation, and longer
recovery time, which may necessitate transportation
for the patient. It is not certain whether the
potential added benefits of colonoscopy relative to
screening alternatives are large enough to justify the
added risks and inconvenience for all patients.
- Initial costs of colonoscopy are higher than the costs
of other tests. Estimates of cost-effectiveness,
however, suggest that, from a societal perspective,
compared with no screening, all methods of
colorectal cancer screening are likely to be as cost-effective
as many other clinical preventive services-less
than $30,000 per additional year of life gained.
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Lung Cancer Screening
Summary of Recommendation
The U.S. Preventive Services Task Force
(USPSTF) concludes that the evidence is
insufficient to recommend for or against screening
asymptomatic persons for lung cancer with either
low dose computerized tomography (LDCT),
chest x-ray (CXR), sputum cytology, or a
combination of these tests. Rating: I
Recommendation.
|
This USPSTF recommendation was first published in: Ann Intern Med 2004;140:738-9. http://www.ahrq.gov/clinic/3rduspstf/lungcancer/lungcanrs.htm.
Clinical Considerations
- The benefit of screening for lung cancer has not
been established in any group, including
asymptomatic high-risk populations such as older
smokers. The balance of harms and benefits
becomes increasingly unfavorable for persons at
lower risk, such as nonsmokers.
- The sensitivity of LDCT for detecting lung cancer
is four times greater than the sensitivity of CXR.
However, LDCT is also associated with a greater
number of false-positive results, more radiation
exposure, and increased costs compared with CXR.
- Because of the high rate of false-positive results,
many patients will undergo invasive diagnostic
procedures as a result of lung cancer screening.
Although the morbidity and mortality rates from
these procedures in asymptomatic individuals are
not available, mortality rates due to complications
from surgical interventions in symptomatic patients
reportedly range from 1.3 percent to 11.6 percent; morbidity
rates range from 8.8 percent to 44 percent, with higher rates
associated with larger resections.
- Other potential harms of screening are potential
anxiety and concern as a result of false-positive tests,
as well as possible false reassurance because of false-negative
results. However, these harms have not
been adequately studied.
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Screening for Oral Cancer
Summary of Recommendation
The U.S. Preventive Services Task Force
(USPSTF) concludes that the evidence is insufficient
to recommend for or against routinely screening
adults for oral cancer. Rating: I Recommendation.
|
This USPSTF recommendation was first published by:
Agency for Healthcare Research and Quality, Rockville,
MD. February 2004. http://www.ahrq.gov/clinic/3rduspstf/oralcan/oralcanrs.htm.
Clinical Considerations
- Direct inspection and palpation of the oral cavity is
the most commonly recommended method of
screening for oral cancer, although there are little
data on the sensitivity and specificity of this
method. Screening techniques other than inspection
and palpation are being evaluated but are still
experimental.
- Tobacco use in all forms is the biggest risk factor for
oral cancer. Alcohol abuse combined with tobacco
use increases risk.
- Clinicians should be alert to the possibility of oral
cancer when treating patients who use tobacco or
alcohol.
- Patients should be encouraged to not use tobacco
and to limit alcohol use in order to decrease their
risk for oral cancer as well as heart disease, stroke,
lung cancer, and cirrhosis.
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Screening for Ovarian Cancer
Summary of Recommendation
The U.S. Preventive Services Task Force
(USPSTF) recommends against routine screening
for ovarian cancer. Rating: D Recommendation.
|
This USPSTF recommendation was first published in:
Ann Fam Med 2004;2:260-2. http://www.ahrq.gov/clinic/3rduspstf/ovariancan/ovcanrs.htm.
Clinical Considerations
- There is no existing evidence that any screening
test, including CA-125, ultrasound, or pelvic
examination, reduces mortality from ovarian cancer.
Furthermore, existing evidence that screening can
detect early-stage ovarian cancer is insufficient to
indicate that this earlier diagnosis will reduce
mortality.
- Because there is a low incidence of ovarian cancer in
the general population (age-adjusted incidence of
17 per 100,000 women), screening for ovarian
cancer is likely to have a relatively low yield. The
great majority of women with a positive screening
test will not have ovarian cancer (i.e., they will have a
false-positive result). In women at average risk, the
positive predictive value of an abnormal screening
test is, at best, approximately 2 percent (i.e., 98 percent of
women with positive test results will not have
ovarian cancer).
- The positive predictive value of an initially positive
screening test would be more favorable for women
at higher risk. For example, the lifetime probability
of ovarian cancer increases from about 1.6 percent in a
35-year-old woman without a family history of
ovarian cancer to about 5 percent if she has 1 relative and
7 percent if she has 2 relatives with ovarian cancer. If
ongoing clinical trials show that screening has a
beneficial effect on mortality rates, then women at
higher risk are likely to experience the greatest
benefit.
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Screening for Pancreatic Cancer
Summary of Recommendation
The U.S. Preventive Services Task Force
(USPSTF) recommends against routine screening
for pancreatic cancer in asymptomatic adults
using abdominal palpation, ultrasonography, or
serologic markers. Rating: D Recommendation.
|
This USPSTF recommendation was first published by:
Agency for Healthcare Research and Quality, Rockville,
MD. February 2004. http://www.ahrq.gov/clinic/3rduspstf/pancreatic/pancrers.htm.
Clinical Considerations
- Due to the poor prognosis of those diagnosed with
pancreatic cancer, there is an interest in primary
prevention. The evidence for diet-based prevention
of pancreatic cancer is limited and conflicting.
Some experts recommend lifestyle changes that may
help to prevent pancreatic cancer, such as stopping
the use of tobacco products, moderating alcohol
intake, and eating a balanced diet with sufficient
fruit and vegetables.
- Persons with hereditary pancreatitis may have a
higher lifetime risk for developing pancreatic cancer.11 However, the USPSTF did not review the
effectiveness of screening these patients.
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Screening for Prostate Cancer
Summary of Recommendation
The U.S. Preventive Services Task Force
(USPSTF) concludes that the evidence is
insufficient to recommend for or against routine
screening for prostate cancer using prostate specific
antigen (PSA) testing or digital rectal examination
(DRE). Rating: I recommendation.
|
This USPSTF recommendation was first published in:
Ann Intern Med 2002;137:915-6. http://www.ahrq.gov/clinic/3rduspstf/prostatescr/prostaterr.htm.
Clinical Considerations
- Prostate specific antigen (PSA) testing and digital
rectal examination (DRE) can effectively detect
prostate cancer in its early pathologic stages. Recent
evidence suggests that radical prostatectomy can
reduce prostate cancer mortality in men whose
cancer is detected clinically. The balance of
potential benefits (the reduction of morbidity and
mortality from prostate cancer) and harms (false-positive
results, unnecessary biopsies, and possible
complications) of early treatment of the types of
cancers found by screening, however, remains
uncertain. Therefore, the benefits of screening for
early prostate cancer remain unknown. Ongoing
screening trials, and trials of treatment versus
"watchful waiting" for cancers detected by
screening, may help clarify the benefits of early
detection of prostate cancer.
- Despite the absence of firm evidence of
effectiveness, some clinicians may opt to perform
prostate cancer screening for other reasons. Given
the uncertainties and controversy surrounding
prostate cancer screening, clinicians should not
order the PSA test without first discussing with the
patient the potential but uncertain benefits and the
possible harms of prostate cancer screening. Men
should be informed of the gaps in the evidence, and
they should be assisted in considering their personal
preferences and risk profile before deciding whether
to be tested.
- If early detection improves health outcomes, the
population most likely to benefit from screening
will be men aged 50 to 70 who are at average risk,
and men older than 45 who are at increased risk
(African American men and men with a family
history of a first-degree relative with prostate
cancer).12 Benefits may be smaller in Asian
Americans, Hispanics, and other racial and ethnic
groups that have a lower risk of prostate cancer.
Older men and men with other significant medical
problems who have a life expectancy of fewer than
10 years are unlikely to benefit from screening.12
- PSA testing is more sensitive than DRE for the
detection of prostate cancer. PSA screening with the
conventional cut-point of 4.0 ng/ml detects a large
majority of prostate cancers; however, a significant
percentage of early prostate cancers (10 percent to 20 percent)
will be missed by PSA testing alone.13 Using a lower
threshold to define an abnormal PSA detects more
cancers at the cost of more false positives and more
biopsies. The yield of screening in terms of cancer
detected declines rapidly with repeated annual
testing.12 If screening were to reduce mortality,
biennial PSA screening could yield as much benefit
as annual screening.
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Counseling to Prevent Skin Cancer
Summary of Recommendation
The U.S. Preventive Services Task Force
(USPSTF) concludes that the evidence is
insufficient to recommend for or against routine
counseling by primary care clinicians to prevent
skin cancer. Rating: I Recommendation.
|
This USPSTF recommendation was first published by:
Agency for Healthcare Research and Quality, Rockville, MD.
October 2003. http://www.ahrq.gov/clinic/3rduspstf/skcacoun/skcarr.htm.
Clinical Considerations
- Using sunscreen has been shown to prevent
squamous cell skin cancer. The evidence for the
effect of sunscreen use in preventing melanoma,
however, is mixed. Sunscreens that block both
ultraviolet A (UV-A) and ultraviolet B (UV-B) light
may be more effective in preventing squamous cell
cancer and its precursors than those that block only
UV-B light. However, people who use sunscreen
alone could increase their risk for melanoma if they
increase the time they spend in the sun.
- UV exposure increases the risk for skin cancer
among people with all skin types, but especially
fair-skinned people. Those who sunburn readily
and tan poorly, namely those with red or blond hair
and fair skin that freckles or burns easily, are at
highest risk for developing skin cancer and would
benefit most from sun protection behaviors. The
incidence of melanoma among whites is 20 times
higher than it is among blacks; the incidence of
melanoma among whites is about 4 times higher
than it is among Hispanics.
- Observational studies indicate that intermittent or
intense sun exposure is a greater risk factor for
melanoma than chronic exposure. These studies
support the hypothesis that preventing sunburn,
especially in childhood, may reduce the lifetime risk
for melanoma.
- Other measures for preventing skin cancer include
avoiding direct exposure to midday sun (between the
hours of 10:00 AM and 4:00 PM) to reduce
exposure to ultraviolet (UV) rays and covering skin
exposed to the sun (by wearing protective clothing
such as broad-brimmed hats, long-sleeved shirts, long
pants, and sunglasses).
- The effects of sunlamps and tanning beds on the risk
for melanoma are unclear due to limited study design
and conflicting results from retrospective studies.
- Only a single case-control study of skin self-examination
has reported a lower risk for melanoma
among patients who reported ever examining their
skin over 5 years. Although results from this study
suggest that skin self-examination may be effective in
preventing skin cancer, these results are not
definitive.
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Screening for Skin Cancer
Summary of Recommendation
The U.S. Preventive Services Task Force
(USPSTF) concludes that the evidence is
insufficient to recommend for or against routine
screening for skin cancer using a total-body skin
examination for the early detection of cutaneous
melanoma, basal cell cancer, or squamous cell skin
cancer. Rating: I Recommendation.
|
This USPSTF recommendation was first published in:
Am J Prev Med 2001;20(3S):44-6. http://www.ahrq.gov/clinic/ajpmsuppl/skcarr.htm.
Clinical Considerations
- Benefits from screening are unproven, even in high-risk
patients. Clinicians should be aware that fair-skinned
men and women aged > 65, patients with
atypical moles, and those with > 50 moles constitute
known groups at substantially increased risk for
melanoma.
- Clinicians should remain alert for skin lesions with
malignant features noted in the context of physical
examinations performed for other purposes.
Asymmetry, border irregularity, color variability,
diameter > 6 mm ("A," "B," "C," "D"), or rapidly
changing lesions are features associated with an
increased risk of malignancy. Suspicious lesions
should be biopsied.
- The USPSTF did not examine the outcomes related
to surveillance of patients with familial syndromes,
such as familial atypical mole and melanoma
(FAM-M) syndrome.
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Screening for Testicular Cancer
Summary of Recommendation
The U.S. Preventive Services Task Force
(USPSTF) recommends against routine screening
for testicular cancer in asymptomatic adolescent
and adult males. Rating: D Recommendation.
|
This USPSTF recommendation was first published by:
Agency for Healthcare Research and Quality, Rockville,
MD. February 2004. http://www.ahrq.gov/clinic/3rduspstf/skcacoun/skcarr.htm.
Clinical Considerations
- The low incidence of testicular cancer and favorable
outcomes in the absence of screening make it
unlikely that clinical testicular examinations would
provide important health benefits. Clinical
examination by a physician and self-examination are
the potential screening options for testicular cancer.
However, little evidence is available to assess the
accuracy, yield, or benefits of screening for testicular
cancer.
- Although currently most testicular cancers are
discovered by patients themselves or their partners,
either unintentionally or by self-examination, there
is no evidence that teaching young men how to
examine themselves for testicular cancer would
improve health outcomes, even among men at high
risk, including men with a history of undescended
testes or testicular atrophy.
- Clinicians should be aware of testicular cancer as a
possible diagnosis when young men present to them
with suggestive signs and symptoms. There is some
evidence that patients who present initially with
symptoms of testicular cancer are frequently
diagnosed as having epididymitis, testicular trauma,
hydrocele, or other benign disorders. Efforts to
promote prompt assessment and better evaluation
of testicular problems may be more effective than
widespread screening as a means of promoting early
detection.
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Routine Vitamin Supplementation to Prevent Cancer and Cardiovascular Disease
Summary of Recommendations
The U.S. Preventive Services Task Force
(USPSTF) concludes that the evidence is
insufficient to recommend for or against the use of
supplements of vitamins A, C, or E; multivitamins
with folic acid; or antioxidant combinations for the
prevention of cancer or cardiovascular disease.
Rating: I Recommendation.
The USPSTF recommends against the use of
beta-carotene supplements, either alone or in
combination, for the prevention of cancer or
cardiovascular disease. Rating: D Recommendation.
This USPSTF recommendation was first published in:
Ann Intern Med 2003;139:51-5. http://www.ahrq.gov/clinic/3rduspstf/vitamins/vitaminsrr.htm. |
Clinical Considerations
- The USPSTF did not review evidence regarding
vitamin supplementation for patients with known
or potential nutritional deficiencies, including
pregnant and lactating women, children, the elderly,
and people with chronic illnesses. Dietary
supplements may be appropriate for people whose
diet does not provide the recommended dietary
intake of specific vitamins. Individuals may wish to
consult a health care provider to discuss whether
dietary supplements are appropriate.
- With the exception of vitamins for which there is
compelling evidence of net harm (e.g., beta-carotene
supplementation in smokers), there is little reason
to discourage people from taking vitamin
supplements. Patients should be reminded that
taking vitamins does not replace the need to eat a
healthy diet. All patients should receive information
about the benefits of a diet high in fruit and
vegetables, as well as information on other foods
and nutrients that should be emphasized or avoided
in their diet (2002 USPSTF recommendation
on counseling to promote a healthy diet).
- Patients who choose to take vitamins should be
encouraged to adhere to the dosages recommended
in the Dietary Reference Intakes (DRI) of the
Institute of Medicine. Some vitamins, such as A and
D, may be harmful in higher doses; therefore, doses
greatly exceeding the Recommended Dietary
Allowance (RDA) or Adequate Intake (AI) should
be taken with care while considering whether
potential harms outweigh potential benefits.
Vitamins and minerals sold in the United States are
classified as "dietary supplements," and there is a
degree of quality control over content if they have a
U.S. Pharmacopeia (USP) seal.14 Nevertheless,
imprecision in the content and concentration of
ingredients could pose a theoretical risk not
reflected in clinical trials using calibrated
compounds.
- The adverse effects of beta-carotene on smokers
have been observed primarily in those taking large
supplemental doses. There is no evidence to suggest
that beta-carotene is harmful to smokers at levels
occurring naturally in foods.
- The USPSTF did not review evidence supporting
folic acid supplementation among pregnant women
to reduce neural tube defects. In 1996, the USPSTF
recommended folic acid for all women who are
planning, or capable of, pregnancy (see 1996
USPSTF chapter on screening for neural tube
defects).15
- Clinicians and patients should discuss the possible
need for vitamin supplementation when taking
certain medications (e.g., folic acid supplementation
for those patients taking methotrexate).
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