Human Papillomavirus (HPV) Testing to Improve Cervical Cancer Screening in the Mississippi Delta
| Status: | Completed |
|---|---|
| Conditions: | Women's Studies |
| Therapuetic Areas: | Reproductive |
| Healthy: | No |
| Age Range: | 26 - 65 |
| Updated: | 4/17/2018 |
| Start Date: | January 24, 2007 |
| End Date: | June 25, 2015 |
HPV Testing to Improve Cervical Cancer Screening in the Mississippi Delta (Mississippi Delta Project)
Background:
- Cancer of the cervix (bottom third of the uterus, or womb) can be prevented by regular
Pap tests (also called Pap smears), which check for changes in the cells of the cervix.
Because many women in the United States have regular Pap smears, cervical cancer is not
common in this country. However, the disease is common among women in the Mississippi
Delta because of poor participation in screening programs.
- The major causes of cervical cancer are persistent human papillomaviruses (HPV)
infection by cancer-associated HPV types and lack of screening. These viruses cause an
infection that often goes away by itself, but if it does not go away, over a long time
lead to cervical cancer. HPV causes cervical abnormalities, which are detected by Pap
smears and then treated.
Objectives:
-To determine whether an at-home self-collection method for obtaining cells from the cervix
can be a simple, safe and inexpensive way to screen for cervical cancer for women who don t
go to the health clinic regularly.
Eligibility:
- Women who reside in the counties of Leflore, Sunflower, Washington or Tallahatchie,
Mississippi.
- Women between 26 and 65 years of age who are not pregnant and who have not had a
hysterectomy.
Design:
Screening study participants undergo the following:
- The doctor takes a cervical sample using the same self-collection device that women will
use at home to self-collect.
- Pelvic examination and Pap test. For this test, the woman lies on an exam table and the
doctor inserts an instrument called a speculum into the vagina, opening it to see the
cervix. A special brush is used to take a few cells from the cervix. The cells are
placed on a glass slide and sent to a lab for examination.
- Cervical cell specimen collection using an at-home self-collection kit that participants
will use at home after 2 weeks
- At-home self-collection by participant after 2 weeks.
- Referral to a doctor for follow-up care, if needed.
- Colposcopy (see below) in all women with a Pap test that is abnormal or positive for HPV
and for some women with a normal smear.
Colposcopy study participants undergo the following:
- The doctor takes a cervical sample using the same self-collection device that women will
use at home to self-collect.
- Colposcopy, an exam in which the doctor examines the cervix using a light and looks
through a magnifying device to see if there is any abnormal tissue on the cervix. During
this exam, the doctor may remove a small sample of tissue to diagnose any abnormality.
Participants also have a sample collected using the self-collection kit.
- At-home cervical sample collection by participant after 2 weeks.
- Notification if further medical care is required and treatment if the biopsy looks
abnormal.
- Cancer of the cervix (bottom third of the uterus, or womb) can be prevented by regular
Pap tests (also called Pap smears), which check for changes in the cells of the cervix.
Because many women in the United States have regular Pap smears, cervical cancer is not
common in this country. However, the disease is common among women in the Mississippi
Delta because of poor participation in screening programs.
- The major causes of cervical cancer are persistent human papillomaviruses (HPV)
infection by cancer-associated HPV types and lack of screening. These viruses cause an
infection that often goes away by itself, but if it does not go away, over a long time
lead to cervical cancer. HPV causes cervical abnormalities, which are detected by Pap
smears and then treated.
Objectives:
-To determine whether an at-home self-collection method for obtaining cells from the cervix
can be a simple, safe and inexpensive way to screen for cervical cancer for women who don t
go to the health clinic regularly.
Eligibility:
- Women who reside in the counties of Leflore, Sunflower, Washington or Tallahatchie,
Mississippi.
- Women between 26 and 65 years of age who are not pregnant and who have not had a
hysterectomy.
Design:
Screening study participants undergo the following:
- The doctor takes a cervical sample using the same self-collection device that women will
use at home to self-collect.
- Pelvic examination and Pap test. For this test, the woman lies on an exam table and the
doctor inserts an instrument called a speculum into the vagina, opening it to see the
cervix. A special brush is used to take a few cells from the cervix. The cells are
placed on a glass slide and sent to a lab for examination.
- Cervical cell specimen collection using an at-home self-collection kit that participants
will use at home after 2 weeks
- At-home self-collection by participant after 2 weeks.
- Referral to a doctor for follow-up care, if needed.
- Colposcopy (see below) in all women with a Pap test that is abnormal or positive for HPV
and for some women with a normal smear.
Colposcopy study participants undergo the following:
- The doctor takes a cervical sample using the same self-collection device that women will
use at home to self-collect.
- Colposcopy, an exam in which the doctor examines the cervix using a light and looks
through a magnifying device to see if there is any abnormal tissue on the cervix. During
this exam, the doctor may remove a small sample of tissue to diagnose any abnormality.
Participants also have a sample collected using the self-collection kit.
- At-home cervical sample collection by participant after 2 weeks.
- Notification if further medical care is required and treatment if the biopsy looks
abnormal.
Background: Cytology screening programs have effectively reduced cervical cancer incidence
and mortality in the U.S. by greater than 75%. However, these programs requiring repeated
clinician-administered Pap smears do not adequately cover medically-underserved populations.
Based partly on HREB/DCEG etiologic research, we now know that carcinogenic types of human
papillomavirus (HPV) cause virtually all cases of cervical cancer. Supported by our
translational work with DCP, HPV DNA testing is already approved by the FDA as an adjunctive
screening modality to cytology in this country and as a primary screening modality to
cytology in this country and as a primary screening modality internationally. A validated
screening program of HPV DNA testing of self-collected cervicovaginal specimens would permit
wider coverage screening than cytology in the populations underserved by cytology-based
testing like the Mississippi Delta region.
Objective: To assess the technical feasibility (i.e. non-inferiority or equivalence to
cytology for detection of cervical precancer and cancer) of cervical cancer screening based
on self-collection and HPV DNA testing of cervicovaginal specimens from women aged greater
than or equal to 30 years old who live in the Mississippi Delta.
Methods: One thousand women will be enrolled during 18 months, including 500 attending
colposcopy due to cytologic abnormality, 250 women who regularly attend a screening clinic,
and 250 unscreened women who have not had a Pap smear within the last 3 years (according to
current screening guidelines) but recruited to attend a screening. Three clinical specimens
will be collected from each woman. A cervicovaginal specimen (for HPV testing) and a cervical
specimen (for cytology and HPV testing) will be collected from each woman by the physician.
At the time of the clinic visit women will be give a kit for self-collection of a second
cervicovaginal specimen (for HPV testing) to be returned by mail within two weeks. All three
specimens from each woman will be tested by two clinical DNA tests that use pooled-probes for
detection of carcinogenic HPV: an FDA-approved signal amplification test (Hybrid Capture 2
from Digene) and a new DNA amplification test (AMPLICOR from Roche) currently in clinical
trials. Specimens will also be tested retrospectively by a research PCR asay that detects 37
HPV types, which will help us evaluate the performance of the two clinical HPV tests. Women
attending their screening visit who test positive by cytology (atypical squamous cells of
undetermined significance or worse) or for carcinogenic HPV will be referred to colposcopy
along with a random sample of HPV negative, cytologic negative women (n equals 100).
Analysis: We will compare the clinical performance of HPV DNA testing of self-collected
specimens to that of cytology (at a threshold of atypical squamous cells of unknown
significance (ASCUS) or more severe) for detection of histologically confirmed cervical
intraepithelial neoplasia grade 2 (CIN2) or more severe (greater than or equal to CIN2).
Cytology results will be based on standard-of-care cytology screening for women attending the
screening visit and repeat cytology for women attending colposcopy. An estimated 150 cases of
greater than or equal to CIN2 will be identified. This is an equivalence study, where we wish
to reject the null hypothesis that HPV self-testing is greater than 10% less sensitive than
cytology. Assuming cytology has a 75% sensitivity for greater than or equal to CIN2, a sample
size of 150 subjects has 84% power (alpha=0.05) (one-sided non-inferiority or equivalence
test of correlated proportions) to rule out a 10% decrement in sensitivity for
self-collection with HPV DNA testing compared with cytology will guide whether the new
technique could be broadly introduced for cervical cancer screening.
and mortality in the U.S. by greater than 75%. However, these programs requiring repeated
clinician-administered Pap smears do not adequately cover medically-underserved populations.
Based partly on HREB/DCEG etiologic research, we now know that carcinogenic types of human
papillomavirus (HPV) cause virtually all cases of cervical cancer. Supported by our
translational work with DCP, HPV DNA testing is already approved by the FDA as an adjunctive
screening modality to cytology in this country and as a primary screening modality to
cytology in this country and as a primary screening modality internationally. A validated
screening program of HPV DNA testing of self-collected cervicovaginal specimens would permit
wider coverage screening than cytology in the populations underserved by cytology-based
testing like the Mississippi Delta region.
Objective: To assess the technical feasibility (i.e. non-inferiority or equivalence to
cytology for detection of cervical precancer and cancer) of cervical cancer screening based
on self-collection and HPV DNA testing of cervicovaginal specimens from women aged greater
than or equal to 30 years old who live in the Mississippi Delta.
Methods: One thousand women will be enrolled during 18 months, including 500 attending
colposcopy due to cytologic abnormality, 250 women who regularly attend a screening clinic,
and 250 unscreened women who have not had a Pap smear within the last 3 years (according to
current screening guidelines) but recruited to attend a screening. Three clinical specimens
will be collected from each woman. A cervicovaginal specimen (for HPV testing) and a cervical
specimen (for cytology and HPV testing) will be collected from each woman by the physician.
At the time of the clinic visit women will be give a kit for self-collection of a second
cervicovaginal specimen (for HPV testing) to be returned by mail within two weeks. All three
specimens from each woman will be tested by two clinical DNA tests that use pooled-probes for
detection of carcinogenic HPV: an FDA-approved signal amplification test (Hybrid Capture 2
from Digene) and a new DNA amplification test (AMPLICOR from Roche) currently in clinical
trials. Specimens will also be tested retrospectively by a research PCR asay that detects 37
HPV types, which will help us evaluate the performance of the two clinical HPV tests. Women
attending their screening visit who test positive by cytology (atypical squamous cells of
undetermined significance or worse) or for carcinogenic HPV will be referred to colposcopy
along with a random sample of HPV negative, cytologic negative women (n equals 100).
Analysis: We will compare the clinical performance of HPV DNA testing of self-collected
specimens to that of cytology (at a threshold of atypical squamous cells of unknown
significance (ASCUS) or more severe) for detection of histologically confirmed cervical
intraepithelial neoplasia grade 2 (CIN2) or more severe (greater than or equal to CIN2).
Cytology results will be based on standard-of-care cytology screening for women attending the
screening visit and repeat cytology for women attending colposcopy. An estimated 150 cases of
greater than or equal to CIN2 will be identified. This is an equivalence study, where we wish
to reject the null hypothesis that HPV self-testing is greater than 10% less sensitive than
cytology. Assuming cytology has a 75% sensitivity for greater than or equal to CIN2, a sample
size of 150 subjects has 84% power (alpha=0.05) (one-sided non-inferiority or equivalence
test of correlated proportions) to rule out a 10% decrement in sensitivity for
self-collection with HPV DNA testing compared with cytology will guide whether the new
technique could be broadly introduced for cervical cancer screening.
- INCLUSION CRITERIA:
Five-hundred women attending colposcopy and 500 women receiving cytology screening,
including 250 unscreened women, will be recruited for the study. Non-pregnant,
non-hysterectomized women aged 26-65 will be recruited.
EXCLUSION CRITERIA:
Women under 26 or over 65 years of age.
Pregnant women or women having given birth to a child in the past 8 weeks. To insure women
included in the study are not pregnant, we will ask women during the consenting process if
they are pregnant. Women who answer yes for either query will be excluded. Participants
will also receive a reminder call for their 2-week self-collection. At that time, women
again will be asked if they are pregnant. If any woman answers yes, she will be instructed
to not self-collect.
Women who have had a total hysterectomy.
Women who have an overt cancerous lesion visible upon exam by the clinician.
Other reasons to exclude women include the inability to speak English, the appearance of
mental incompetence, or refusal to participate or sign the informed consent form.
We found this trial at
1
site
9609 Medical Center Drive
Bethesda, Maryland 20892
Bethesda, Maryland 20892
1-800-422-6237
National Cancer Institute , 9000 Rockville Pike The National Cancer Institute (NCI) is part of...
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