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Initial Results of the Study of Tamoxifen and
Raloxifene (STAR) Released: Osteoporosis Drug Raloxifene Shown to be as
Effective as Tamoxifen in Preventing Invasive Breast Cancer
Cancer Research of the Ozarks Participated in Clinical Trial
April 17, 2006
Initial results of the Study of Tamoxifen and Raloxifene, or STAR, show that
the drug raloxifene, currently used to prevent and treat osteoporosis in
postmenopausal women, works as well as tamoxifen in reducing breast cancer
risk for postmenopausal women at increased risk of the disease. Cancer
Research of the Ozarks participated in this clinical trial, one of the
largest breast cancer prevention trials ever conducted.
In STAR, both drugs reduced the risk of developing invasive breast cancer by
about 50 percent. In addition, within the study, women who were
prospectively and randomly assigned to take raloxifene daily, and who were
followed for an average of about four years, had 36 percent fewer uterine
cancers and 29 percent fewer blood clots than the women who were assigned to
take tamoxifen. Uterine cancers, especially endometrial cancers, are a rare
but serious side effect of tamoxifen. Both tamoxifen and raloxifene are
known to increase a woman's risk of blood clots.
STAR enrolled 19,747 postmenopausal women who were at increased risk of the
disease. Participants were randomly assigned to receive either 60 mg of
raloxifene (Evista®) or 20 mg of tamoxifen (Nolvadex®) daily for five years.
The trial is coordinated by the National Surgical Adjuvant Breast and Bowel
Project (NSABP), a network of cancer research professionals, and is
sponsored by the National Cancer Institute (NCI), part of the National
Institutes of Health.
"In 1998, the landmark Breast Cancer Prevention Trial showed that tamoxifen
could reduce the risk of invasive breast cancer in premenopausal and
postmenopausal women by nearly 50 percent," said Norman Wolmark, M.D., NSABP
chairman. "Today, we can tell you that for postmenopausal women at increased
risk of breast cancer, raloxifene is just as effective, without some of the
serious side effects known to occur with tamoxifen."
Women taking either drug had equivalent numbers of strokes, heart attacks,
and bone fractures. Both raloxifene and tamoxifen are known to protect bone
health; it is estimated that half a million postmenopausal women are
currently taking raloxifene by prescription to prevent or treat
osteoporosis. Additionally, the initial results from STAR suggest that
raloxifene does not increase the risk of developing a cataract, as tamoxifen
does.
"Although no drugs are without side effects, tamoxifen and raloxifene are
vital options for women who are at increased risk of breast cancer and want
to take action," said Leslie Ford, M.D., associate director for clinical
research in NCI's Division of Cancer Prevention. "For many women,
raloxifene's benefits will outweigh its risks in a way that tamoxifen's
benefits do not."
The STAR researchers also tracked known menopausal side effects that occur
with both drugs and monitored the participants' quality of life. The data
show that side effects of both drugs were mild to moderate in severity, and
quality of life was the same for both drugs.
Participants in STAR are now receiving information about which drug they
were taking. Women assigned to raloxifene will continue to be provided with
the drug until they have completed five years of treatment. Those women
assigned to tamoxifen can choose to continue taking tamoxifen or to receive
raloxifene to complete their five years of treatment.
Study details include:
STAR enrolled 19,747 women. This data analysis is based on the 19,471 women
for whom complete study information was available.
The numbers of invasive breast cancers in both groups of women were
statistically equivalent. Among the 9,745 women in the raloxifene group, 167
developed invasive breast cancer, compared to 163 of 9,726 women in the
tamoxifen group.
More than half of the women who joined STAR had had a hysterectomy and,
therefore, were not at risk of uterine cancer. For those women with a
uterus, 36 of 4,732 who were assigned to take tamoxifen developed uterine
cancers (mainly endometrial cancer) compared to 23 of 4,712 women who were
assigned to take raloxifene.
In STAR, women in the raloxifene group had 29 percent fewer deep vein
thromboses (blood clots in a major vein) and pulmonary embolisms (blood
clots in the lung) than women in the tamoxifen group. Specifically, 87 of
9,726 women in the tamoxifen group had a deep vein thrombosis compared to 65
of 9,745 women taking raloxifene. In addition, 54 of 9,726 women taking
tamoxifen developed pulmonary embolisms compared to 35 of 9,745 women taking
raloxifene.
The number of strokes occurring in both groups of women was statistically
equivalent: 53 of 9,726 women in the tamoxifen group and 51 of 9,745 women
in the raloxifene group had a stroke during the trial. There was no
difference in deaths from strokes: 6 of 9,726 women in the tamoxifen group
and 4 of 9,745 women in the raloxifene group died from this event. Women at
increased risk of stroke (those with uncontrolled hypertension or
uncontrolled diabetes, or a history of stroke, transient ischemic attack, or
atrial fibrillation) were not eligible to participate in STAR.
While tamoxifen has been shown to reduce, by half, the incidence of lobular
carcinoma in situ (LCIS) and ductal carcinoma in situ (DCIS), raloxifene did
not have an effect on these diagnoses. (LCIS and DCIS are sometimes called
noninvasive breast cancers.) Of the 9,726 women taking tamoxifen, 57
developed LCIS or DCIS, compared to 81 of 9,745 taking raloxifene. This
result confirms data reported in a large study of raloxifene in the
treatment of osteoporosis (the Continued Outcomes Relevant to Evista or CORE
Trial) in 2004.
Women who participated in STAR were postmenopausal, at least 35 years old,
and had an increased risk of breast cancer as determined by their age,
family history of breast cancer, personal medical history, age at first
menstrual period, and age at first live birth. Before participating in the
study, the women were instructed about the potential risks and benefits of
tamoxifen and raloxifene and then were asked to sign an informed consent
document.
The maker of tamoxifen, AstraZeneca Pharmaceuticals, Wilmington, Del., and
the maker of raloxifene, Eli Lilly and Company, Indianapolis, Ind., provided
their drugs and matching placebos for the trial without charge to
participants. Eli Lilly and Company also gave NSABP support to defray
recruitment costs at the participating centers and to help local
investigators conduct the study.
For more information about STAR, including links to media materials and a
fact sheet, visit NCI's STAR home page at http://www.cancer.gov/star or one
of NSABP's Web sites at http://www.nsabp.pitt.edu and
http://foundation.nsabp.org.
For a Q&A related to the STAR results, go to: http://www.cancer.gov/newscenter/pressreleases/STARresultsQandA.
For B-roll related to the STAR results, go to www.thenewsmarket.com for
digitized, downloadable B-roll, or call the NCI Media Relations Branch at
(301) 496-6641 for a Beta-tape copy.
For tools used to calculate a woman's risk of breast cancer, visit http://cancer.gov/bcrisktool
or http://breastcancerprevention.com.
Cancer Research of the Ozarks is a joint venture of St. John's Health System
and CoxHealth. For information on the local trial at Cancer Research of the
Ozarks contact St. John's Media Relations at 417-820-2426 or CoxHealth at
269-4113. At least one participant is willing to talk to local news media.
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