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Pap Smear Test Frequently Asked Questions:
What is a Pap test and who gets tested?
The pap test is a screening test for malignant and
premalignant changes of the cervix. A positive result indicates
that there may be a problem and that further diagnostic
procedures must be done. The Pap test is not a diagnostic test.
It cannot be used to exclude a cancer of the cervix for a person
who has symptoms that could be due to a cervical cancer. Pap
tests are done on women who have no symptoms of cancer and have
no findings suggesting a cancer. Thus, Pap tests are done only
on women who are normal. If the woman has symptoms or findings
suggestive of cancer of the cervix then a diagnostic test must
be done to exclude a cancer or to diagnose a cancer. Diagnostic
tests are usually biopsies. This is the single most important
lesson to learn: if you have a symptom or a finding that could
be due to a cancer of the cervix, a normal Pap test never
excludes the possibility of cancer.
In the vast majority of instances, an abnormal Pap test
results in the diagnosis of a minor change on the cervix. Some
of these changes will be premalignant, but most will be of minor
significance. They will all have to be evaluated, diagnosed and
treated, but most will be easily and effectively treated.
Occasionally, a real cancer will be present which is why this is
such an important test. Most cancers are visible on examination
and can be biopsied as soon as they are seen. Sometimes the
cancers are inside the cervix beyond view and the only
indication that it is there is the abnormal Pap test.
Pap test screening is recommended for all women beginning at
age 18 years or at the onset of sexual activity, if earlier. The
screening interval is usually every year, although, if there
have been no previous abnormal tests, the interval may be
extended. The Pap test is performed by gently scraping cells
from the cervix, smearing them onto a microscope slide and
sending it to a pathology laboratory for evaluation. There are
two reporting systems in current use. The older system which
reported the result in one of five classes is being replaced by
the newer Bethesda System.
Classification of Pap Test results
Class I - Normal
Class II - Atypical, inflammation or uterine cells seen
Class III - Dysplastic, mild, moderate or severe
Class IV - Carcinoma-in-situ
Class V - Carcinoma-in-situ
Bethesda System
Adequacy Satisfactory Limited Unsatisfactory Descriptive
Normal Benign Epithelial cell abnormality Atypical squamous
cells of unknown significance Low grade squamous intraepithelial
lesion High grade squamous intraepithelial lesion Glandular cell
abnormality Atypical glandular cells Adenocarcinoma
What it means:
The cells obtained during the Pap test are removed from the
outermost layer of cells from the surface of the cervix. The
cervix is covered by an epithelial layer of cells that is 12-24
cells thick. This surface covering, called the epithelium, rests
on a basement membrane beneath which are the deeper tissues that
make up the substance of the cervix. The cells of this surface
epithelium progress from large round cells at the basement
membrane to flat cells at the surface.
Squamous (squay-mus) means flat and refers to the flat cells
at the surface. This covering is called a squamous epithelium.
In addition to the progression of the shape of the cells from
the lowermost large round cells to the outermost flat cells, the
nuclei of the cells also change. Those cells lowermost along the
basement membrane have a large nucleus that becomes
progressively more compact and smaller as the cells approach the
surface. On exposed squamous epithelium such as skin the
outermost cells have lost their nuclei completely and the cells
are filled with keratin to produce a protective keratin layer.
On the cervix there is normally no keratin layer and the
outermost cells have a very small dense nucleus.
When there is a disorder of the normal progression of cells
from the lower to outermost layer then that is called a
dysplasia. If this disorder of maturation is limited to the
inner third of the epithelium then that is a mild dysplasia; if
two-thirds of the thickness then a moderate dysplasia; if almost
the full thickness then a severe dysplasia. If the outermost
cells look the same as those along the basement membrane then
that is a full thickness disorder and is called a
carcinoma-in-situ.
A carcinoma-in-situ is a premalignant change and can become a
cancer if not treated. It is thought that there is a progression
from mild to moderate to severe dysplasia before developing
carcinoma-in-situ. It may take years for this progression to
develop into a cancer. Often the early changes will resolve
spontaneously. If these dysplastic cells penetrate the basement
membrane and invade into the deeper tissues then that is a
cancer.
There are other terms for these dysplastic changes. The more
modern term is intraepithelial neoplasia, grade I, II and III.
The term carcinoma-in-situ, CIS, has been dropped since the word
carcinoma means cancer and this is not a cancer. CIN III,
cervical intraepithelial neoplasia grade III, means a full
thickness dysplasia and has replaced CIS.
These premalignant changes can only be diagnosed by a biopsy
of the cervix. The pathologist has to have a piece of tissue to
evaluate not just a collection of scraped off cells. The Pap
test is just a collection of scraped off cells. If these are
abnormal, i.e. large round cells with a large nucleus that
should not be on the surface, the pathologist can recognize them
and report the test as abnormal. But, he cannot diagnose the
true condition without an adequate biopsy specimen. Obtaining an
adequate tissue biopsy specimen is the result of a comprehensive
evaluation of the cervix following the report of an abnormal Pap
test.
Evaluation of an abnormal pap test:
If a Pap test report indicates a malignant or premalignant
condition the patient is reexamined and the Pap test repeated.
The cervix is viewed with a magnifying instrument called a
colposcope. Acetic acid, ordinary table vinegar, is applied to
the cervix. This causes the nucleus of the outermost cells to
swell with water and not transmit light. The cervix is
illuminated with light from the colposcope. The areas that do
not transmit light reflect it back to the colposcopist.
Reflected light is white, so white areas are sought. The
outermost cells of the normal cervix have a very small nucleus
and will transmit light. If they have a large round nucleus then
they are dysplastic and will not transmit light. White areas are
the dysplastic areas. The whiter the area the worse the
dysplasia.
Abnormal blood vessels can also be seen. Neoplasia means new
growth. New growth means new blood vessels. Often these new
blood vessels are abnormal. These abnormal vessels can be seen
through the colposcope. The worse the vessels appear, the worse
is the dysplasia. Cancers have the worst vascular appearance of
all the changes that can occur on the cervix.
During a colposcopic examination the first determination is
if there are abnormal areas. If so, can the entire abnormal area
be seen? If so, then the most abnormal areas are biopsied. If
the entire abnormal area cannot be seen then that cervix cannot
be evaluated colposcopically. Usually the abnormal area extends
up into the endocervical canal beyond view. In this case the
canal must be removed to evaluate the cervix adequately. There
are several techniques for removing the canal. Sometimes a cone
biopsy is done. This removes a circular portion of the cervix
extending up the canal to an apex. The specimen is shaped like a
cone. A more modern technique that can be done in the office is
called a LEEP. This means Loop Electrosurgical Excision
Procedure, and removes portions of the cervix with an
electrified thin wire loop.
If the colposcopic evaluation is satisfactory, meaning all
the abnormal areas can be seen, then the most abnormal areas are
biopsied and sent to the pathologist. The pathology report will
indicate the diagnosis. It will be either something minimal,
some degree of dysplasia, or CIN, possibly even a cancer. But
whatever it is, it is the diagnosis, and the abnormal Pap test
has been evaluated. If the colposcopy is unsatisfactory, then
either a cone biopsy or a LEEP needs to be done and the
pathological report of that material will be the diagnosis. If a
specimen is scraped from the endocervix ( endocervical
curettage, ECC) and shows dysplasia then a cone or LEEP also is
indicated. Only after a diagnosis has been established can
treatment be recommended.
Treatment of pre-malignant conditions:
Once a diagnosis has been established treatment can be
performed. Treatment of dysplasia is usually simple and almost
100 percent effective. It is not even mandatory that it be
treated. It is not treated during pregnancy. It need not even be
specifically diagnosed during pregnancy. During pregnancy all
that need be done is to be assured that there is no invasive
cancer present. This can often be accomplished by careful repeat
colposcopic examinations, without a biopsy. Mild dysplasia may
go away by itself without treatment.
If a cone biopsy or LEEP were done that had removed the
abnormal areas it would be therapeutic as well as diagnostic.
Otherwise, the abnormal area can be destroyed by freezing (cryocautery),
vaporization (laser), removal by biopsy, cone, LEEP, or even
hysterectomy if necessary. Hysterectomy may be best in certain
circumstances, but is seldom a medical necessity for dysplasia.
If the biopsy shows an invasive cancer then staging procedures
need to be done and appropriate treatment given. This is an
entirely different problem and will usually require referral to
an oncologic specialist.
Once a premalignant condition has been treated then the woman
should be reexamined every three months for at least a year and
have a Pap test done. If all goes well then she should be
reexamined annually. If the woman was pregnant when the abnormal
Pap test was found and examination at that time was not
suggestive of cancer then her definitive examination and biopsy
can be deferred until six weeks postpartum.
The cause of Dysplasia:
The cause of cervical dysplasia and cervical cancer is
unknown. Current studies strongly implicate the Human Papilloma
Virus (HPV), as at least a cofactor in its development. This is
the same virus that causes genital warts. There are over sixty
sub-types of HPV that have been isolated, only a few of which
are associated with cervical cancer. HPV can be transmitted by
direct physical contact. Once there is an infection with HPV it
will probably always be in the tissue. Complete obliteration of
the virus from the body is not currently feasible and probably
not necessary. All of us probably have a multitude of viruses of
which we are unaware and which cause us no discernible problem.
If you have been told that your Pap test indicates the
presence of HPV, do not be alarmed. If a definite viral change
can be seen with the colposcope then it can be obliterated with
cryocautery, laser or left alone. Only dysplasias need to be
treated. You are not at great risk for developing cervical
cancer. Continue to have annual Pap tests and treat any
dysplasia if it is diagnosed.
Where did the HPV come from? Who knows, it may have been
there for years. The point is that it is unknowable; there is no
way to find out. Since it is of no demonstrable detriment to
your health it is not worth the time worrying about where it
came from. Some studies have demonstrated that about one third
of college students have evidence of past or present infection
with HPV. It is not unusual to find it reported on Pap tests in
women in their seventh decade.
Pap test mistakes:
The major error with the Pap test is not so much with
misinterpretation of the slide by the pathology laboratory, but
by the misapplication of a screening test for a diagnostic test.
It is well known that at least 10 percent of women with an
obvious visible palpable cervical cancer have a non-suspicious
Pap test. This is because there is such a large amount of
inflammation and necrosis associated with the cancer that all
that is on the slide is this debris. The pathologist cannot see
the cancer cells in the midst of all the debris.
When a woman has a symptom such as bleeding after
intercourse, bleeding between periods, a watery or foul watery
discharge, then a cancer of the cervix must be excluded. Only a
thorough examination and biopsies can rule out a cervical
cancer. A Pap test cannot rule out a cancer. A cervical cancer
is usually visible on examination. If the cervix looks abnormal
it must be biopsied. A Pap test cannot rule out a cancer. If a
woman has symptoms that could be caused by a cervical cancer and
the cervix looks normal then a biopsy from inside the
endocervical canal must be done. A biopsy from inside the uterus
may also be necessary. A Pap test never rules out a cancer.
IF YOU HAVE ABNORMAL BLEEDING, A WATERY DISCHARGE, OR FOUL
WATERY DISCHARGE, YOU MUST HAVE A DIAGNOSTIC TEST TO RULE OUT
CANCER. NEVER, NEVER, NEVER, EVER ACCEPT A NORMAL PAP TEST AS
PROOF OF THERE BEING NO CANCER.
Another error is to treat on the basis of the Pap test rather
than on the basis of the diagnosis. An abnormal Pap test never
leads to treatment. An abnormal Pap test is not a diagnosis.
Treatment cannot be performed until a diagnosis is obtained. An
abnormal Pap test leads to diagnosis by colposcopy and biopsy,
then to treatment. If a simple hysterectomy is done because of
an abnormal Pap test, most women will have had an unneeded
hysterectomy. If a cancer is present, a simple hysterectomy may
be fatal. Cancers cannot be treated by simple means.
Many women do not obtain annual Pap tests. Many who do think
that a normal Pap test means that they are cancer free. The Pap
test evaluates only the squamous epithelium covering the visible
part of the cervix. The endocervical canal has a glandular
epithelium that is not easily evaluated by Pap tests. This
glandular epithelium can also become malignant and not be
detected. Cancers of the uterus, ovaries and fallopian tubes are
not usually detected by the Pap test.
The Pap test is an excellent screening test. It is easy to
do, easy to interpret, easy to evaluate when abnormal and most
importantly can find changes before they become malignant. These
premalignant changes are easy to treat. Cancers are hard to
treat.
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