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Hormones Resource
Center
Increased
Risk of Ovarian Cancer is Linked to Estrogen Replacement
Therapy
article syndicated from NIH
Researchers from the National Cancer Institute
(NCI) have found that women in a large study who
used estrogen replacement therapy after menopause
were at increased risk for ovarian cancer. The
report was published in the July 17, 2002, issue
of JAMA.*
The scientists followed 44,241 women for approximately
20 years. Compared to postmenopausal women not using
hormone replacement therapy, users of estrogen-only
therapy had a 60 percent greater risk of developing
ovarian cancer. The risk increased with length of estrogen
use. The women, who were followed from 1979 to 1998,
were former participants in the Breast Cancer Detection
Demonstration Project, a mammography screening program
conducted between 1973 and 1980.
"The main finding of our study was that postmenopausal
women who used estrogen replacement therapy for 10
or more years were at significantly higher risk of
developing ovarian cancer than women who never used
hormone replacement therapy," said James V. Lacey,
Jr., Ph.D., lead author of the study from NCI's Division
of Cancer Epidemiology and Genetics. The relative risk
for 10 to 19 years of use was 1.8, which translates
to an 80 percent higher risk than non-users, and increased
to 3.2 (a 220 percent higher risk than non-users) for
women who took estrogen for 20 or more years.
Estrogen
is a natural hormone produced primarily by the ovaries.
After
menopause, the ovaries produce
lower levels of the hormones estrogen and progesterone.
By the time natural menopause is complete usually
between ages 45 and 55 hormone output decreases
significantly. As early as the 1940s, women began using
estrogens in high doses to counteract some of the short-term
discomforts of menopause (hot flashes, vaginal drying
and thinning, and urinary tract incontinence and infections).
However, after it became clear in the 1970s that
women who took estrogen alone had a six to eight times
higher risk of developing endometrial cancer (cancer
of the lining of the uterus), doctors began prescribing
progestin along with much lower doses of estrogen.
Progestin is a synthetic form of the natural hormone
progesterone. The addition of progestin to estrogen
therapy reduces the increased risk of endometrial cancer
associated with using estrogen alone. As a result,
it has become increasingly common to prescribe estrogen-progestin
therapy for women who have not had a hysterectomy.
In addition to studying the effect of estrogen use
alone, Lacey and his colleagues looked at whether women
using estrogen-progestin therapy were more likely to
develop ovarian cancer. No increased risk was found.
Lacey
commented, "Even
though our data showed that women who took estrogen
combined with progestin were
not at increased risk for ovarian cancer, only a few
women in our study who developed ovarian cancer had
used estrogen-progestin therapy for more than four
years. So, at this point, there simply aren't enough
data to say whether taking the combined therapy has
any effect on ovarian cancer."
Past studies suggested that postmenopausal hormone
treatments might be effective in preventing or reducing
some of the negative long-term effects of aging, such
as heart disease and osteoporosis. However, the results
from a large multi-center clinical trial, also published
in the July 17 issue of JAMA (JAMA 2002;288:321-333),
showed increases in breast cancer, coronary heart disease,
stroke, and blood clots in the lungs and legs for women
on estrogen-progestin therapy for an average of 5.2
years. The trial, part of the Women's Health Initiative
(WHI), also found fewer cases of hip fractures and
colon cancer among women taking the combined therapy.
However, because overall the harm was greater than
the benefit, the trial was stopped last week, three
years ahead of schedule. The WHI randomized trial for
estrogen alone in women who have had their uterus removed
is continuing.
Lacey
emphasized the complexity of weighing the various
risks and benefits
of hormone use. "Because hormone
therapy may influence so many conditions that affect
women after menopause cardiovascular disease,
osteoporosis, breast cancer, uterine cancer, gallbladder
disease, blood clots, and now potentially ovarian cancer we
should no longer think of a woman basing her decision
to use hormones on the potential risk of just one condition.
Women should continue to talk to their health care
providers about whether hormones might be right for
them."
Previous studies looking at the effect of postmenopausal
hormones on ovarian cancer risk have been inconsistent.
Some reported increased risk with estrogen use while
others reported either no effect or a protective one.
Most of these earlier studies were relatively small
and limited by incomplete information about ovarian
cancer risk factors.
Two recent large studies found a link between hormone
use and ovarian cancer. A large prospective study published
last year (JAMA 2001;285:1460-1465) showed that
postmenopausal estrogen use for 10 or more years was
associated with increased risk of ovarian cancer mortality,
and a recent Swedish study (J. Natl. Cancer Inst. 2002;94:497-504)
reported that estrogen use alone and estrogen-progestin
used sequentially (progestin used on average 10 days/month)
may be associated with an increased risk for ovarian
cancer. In contrast, estrogen-progestin used continuously
(progestin used on average 28 days/month) seemed to
confer no increased ovarian cancer risk.
Lacey said that some of the unknowns concerning hormone
use and ovarian cancer include the following:
-
Duration vs. dose of estrogen therapy
It is not clear from this study whether the increased risk with estrogen
use is due to higher doses of estrogen, longer duration of estrogen
use, or both dose and duration. It is also not clear whether
long-term use of
lower-dose estrogen is associated with ovarian cancer.
-
Duration of estrogen-progestin therapy
Most women in this study were on the combined therapy for less than
four years, so more data will be needed to determine whether
estrogen-progestin
use increases risk. The effect of long-term use of estrogen-progestin
therapy is not known.
-
The type of estrogen-progestin regimen
The continuous regimen involves taking both hormones simultaneously
throughout the month. The sequential regimen, on the other hand,
involves taking estrogen
every day, and progestin for 10 to 14 days each month.
-
Use of more than one type of hormone replacement
therapy
For instance, after taking estrogen alone, some women changed to a
combined regimen after reports of increased endometrial cancer risk
with estrogen
alone. More data are needed to analyze the effect of switching from
one regimen to another.
-
The
form of estrogen administratio
Most studies have analyzed the use of estrogens in pill form, but
it can also be administered by patches, shots, and creams.
Every
year, about 23,000 U.S. women are diagnosed with
ovarian cancer and 14,000 women die from the disease.
A woman's lifetime risk of developing ovarian cancer
is 1.7 percent. This means that in a group of 100 women
followed from birth to age 85, fewer than two would
get ovarian cancer. In comparison, about 13 women would
get breast cancer (lifetime risk is 13.3 percent),
fewer than three women would develop uterine cancer
(lifetime risk is 2.7 percent), and between 16 and
32 women would develop osteoporosis.
An estimated 40 million U.S. women will experience
menopause during the next 20 years, and women today
are living approximately one-third of their life after
menopause.
Anywhere from 20 percent to 45 percent of U.S. women
take some form of hormone therapy between the ages
of 50 and 75. According to industry estimates, about
8 million U.S. women use estrogen alone and about 6
million U.S. women use estrogen-progestin therapy.
About 20 percent of hormone users continue for more
than five years.
For
background information on hormone replacement therapy: http://newscenter.cancer.gov/pressreleases/estrogenplus.html.
For
more information on recent studies on hormone therapy: http://cancer.gov/clinicaltrials/digest-page-menopausal-hormone-use.
Call
the NCI's Cancer Information Service for information
about hormone replacement therapy and cancer risk.
The number is 1-800-422-6237 (1-800-4-CANCER). For
hearing impaired callers, TTY: 1-800-332-8615.
*The
study is titled "Menopausal hormone
replacement therapy and risk of ovarian cancer." The
authors are James V. Lacey, Jr., Pamela J. Mink,
Jay H. Lubin, Mark E. Sherman, Rebecca Troisi, Patricia
Hartge, Arthur Schatzkin, and Catherine Schairer. JAMA 2002;288:334-341.
article
syndicated from National
Institutes of Health:
http://www.nih.gov/news/pr/jul2002/nci-16.htm
EMBARGOED FOR RELEASE - Tuesday,
July 16, 2002 - 4:00 p.m. EDT

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